CPG Management of Ischaemic Stroke (2nd Edition)
CPG Management of Ischaemic Stroke (2nd Edition)
CPG Management of Ischaemic Stroke (2nd Edition)
CLINICAL PRACTICE GUIDELINES DEVELOPMENT GROUP AUTHORS (in alphabetical order) PROF DR HAMIDON BASRI Chairperson A/PROF DR CHIN SZE PIAW DR LOOI IRENE DR MAK CHOON SOON A/PROF DR MOHAMED SOBRI MUDA DATO DR MD. HANIP RAFIA PROF DR TAN KAY SIN DR ZARIAH ABDUL AZIZ Consultant Neurologist University Putra Malaysia, Selangor Consultant Cardiologist International Medical University, KL Consultant Neurologist Hospital Seberang Jaya, Penang Consultant Neurologist Gleneagles Hospital, KL Consultant Neuroradiologist University Kebangsaan Malaysia Medical Centre, KL Consultant Neurologist Hospital Kuala Lumpur, KL Consultant Neurologist University Malaya Medical Centre, KL Consultant Neurologist Hospital Sultanah Nur Zahirah, Terengganu
EXTERNAL REVIEWERS (in alphabetical order) DR HJ BAHANORDIN BIN JAAFAR PROF DR GOH KHEAN JIN DATO DR LOH THIAM GHEE DATO DR MOHD RANI JUSOH DATO DR MUHAMMAD RADZI BIN ABU HASSAN ASSOC PROF DR NOOR AZAH ABD AZIZ PROF DATO DR RAYMOND AZMAN ALI PROF DR TAN CHONG TIN Physician of Rehabilitation Medicine Hospital Serdang, Selangor Consultant Neurologist University Malaya Medical Centre, KL Consultant Neurologist Sime Darby Medical Centre, Selangor Consultant Neurologist Ampang Puteri Hospital, KL Consultant Physician Hospital Sultanah Bahiyah, Kedah Family Medicine Specialist University Kebangsaan Malaysia Medical Center, KL Consultant Neurologist University Kebangsaan Malaysia Medical Centre, KL Consultant Neurologist University Malaya Medical Centre, KL
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RATIONALE AND PROCESS OF GUIDELINE DEVELOPMENT Rationale Stroke is a leading cause of death and disability in Malaysia. Thus, guidelines on the management are imperative to ensure best available therapy is instituted. The clinical practice guidelines (CPG) on ischaemic stroke was developed to provide clear and concise approach to all clinicians on the current concepts in the management of ischaemic stroke patients.
In Malaysia, a significant number of stroke patients are managed by non-neurologists. Therefore, it is important to summarise and adapt relevant clinical trial data and current treatment strategies to our local practice. The first CPG on ischaemic stroke was published in 2006. Since then, there have been many new developments in the management of ischaemic stroke. As a result, an update of the latest and current guidelines would be most appropriate
Process This current CPG is the initiative of the Stroke Council of the Malaysian Society of Neurosciences. A panel of committee members was appointed comprising of neurologists, a cardiologist and a radiologist from the ministry of health, universities and the private sectors. Authors from the first CPG were invited to contribute on new updates before being discussed by panel members. The discussion started from early 2010 before being finalised and sent for the appointed reviewers.
The group members met several times throughout the development of the guideline. All retrieved literature were appraised by individual members and subsequently presented for discussion during group meetings. All statements and recommendations formulated were agreed collectively by members of the Expert Panel. Where the evidence was insufficient the recommendations were derived by consensus of the Panel. The draft was then sent to local external reviewers for comments. The level of recommendation and the grading of evidence used in this guideline was adapted from the U.S/ Canadian Preventive Services Task Force, an the Guidelines for Clinical Practice Guideline, Ministry Of Health Malaysia 2003. The principles and layout follows the methodology stated in the Guidelines for Clinical Practice Guidelines booklet published by the Medical Development division of the Ministry of Health Malaysia. A standard methodology based on a systematic review of current evidence was used to look at the literature. These guidelines have been presented to the Chairman of the Health Technology Assessment and Clinical Practice Guidelines Council of the Ministry of Health Malaysia for review and approval.
Objectives
These guidelines are intended to provide awareness and education in identifying symptoms and signs of stroke scope of various types and causes of ischaemic stroke These guidelines are intended to provide evidence in management of acute ischaemic stroke primary and secondary prevention of ischaemic stroke These guidelines however do not cover management of cerebral haemorrhage stroke rehabilitation (already outlined in Stroke Rehabilitation Guidelines 2000)
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Clinical Questions
The clinical questions to be addressed by these guidelines include: i) What is the current best practice for the management of acute ischaemic stroke? ii) What are the strategies in stroke prevention? iii) What are the effective non pharmacological modification in managing patient with stroke?
These guidelines are to be applied to adults with ischaemic stroke as well as those at risk of developing stroke.
Target Population
Target Group
These guidelines are developed for all healthcare providers involved in the management and prevention of ischaemic stroke in adults. KEY TO EVIDENCE STATEMENTS AND GRADES OF RECOMMENDATIONS LEVELS OF EVIDENCE SCALE I II 1 II 2 Evidence obtained from at least one properly randomized controlled trial Evidence obtained from well-designed controlled trials without randomization Evidence obtained from well-designed cohort or case-control analytic studies, preferably from more than one centre or research group Evidence obtained from multiple time series with or without the intervention. Dramatic results in uncontrolled experiments (such as the results of the introduction of penicillin treatment in the 1940s) could also be regarded as this type of evidence Opinions of respected authorities, based on clinical experience, descriptive studies and case reports; or reports of expert committees
II 3
III
Source : U.S./ CANADIAN PREVENTIVE SERVICES TASK FORCE GRADES OF RECOMMENDATIONS A B C At least one meta analysis, systematic review, or randomized controlled trial (RCT), or evidence rated as good and directly applicable to the target population Evidence from well conducted clinical trials, directly applicable to the target population, and demonstrating overall consistency of results; or evidence extrapolated from meta analysis, systematic review or RCT Evidence from expert committee reports, or opinions and/or clinical experiences of respected authorities; indicates absence of directly applicable clinical studies of good quality
Source : Guidelines for CLINICAL PRACTICE GUIDELINES, Ministry of Health Malaysia 2003
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SUMMARY OF RECOMMENDATIONS The following are management steps in which levels of evidence have been established. Primary Prevention Factors Hypertension Recommendation Treat medically if BP>140mmHg systolic and/or >90mmHg diastolic. Lifestyle changes if BP between 130-139mmHg systolic and/or 80-89mmHg diastolic. Target BP for diabetics is <130mmHg systolic and <80mmHg diastolic. Hypertension should be treated in the very elderly (age > 70 yrs) to reduce risk of stroke. Diabetes mellitus Strict blood pressure control is important in diabetics. Maintain tight glycaemic control. Hyperlipidaemia High risk group: keep LDL < 2.6mmol/l. 1 or more risk factors: keep LDL < 3.4mmol/l. No risk factor: keep LDL < 4.2mmol/l. Smoking Aspirin therapy Cessation of smoking. 100mg aspirin every other day may be useful in women above the age of 65. III II-1 I C B A I B Level of evidence I I I I I Grade A A A A A
Post menopausal Oestrogen based HRT is not recommended for Hormone primary stroke prevention. Replacement therapy Alcohol Avoid heavy alcohol consumption.
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General Management of Acute Ischaemic Stroke Factors Airway & Breathing Recommendation Ensure clear airway and adequate oxygenation. Elective intubation may help some patients with severely increased ICP. Mobilization Blood Pressure Mobilize early to prevent complications Do not treat hypertension if < 220mmHg systolic or < 120mmHg diastolic. Mild hypertension is desirable at 160-180/90-100mmHg . Blood pressure reduction should not be drastic. Proposed substances: Labetolol 10-20mg boluses at 10 minute intervals up to 150-300mg or 1 mg/ml infusion, rate of infusion for labetolol as 1-3mg/min or Captopril 6.25-12.5mg orally.
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Blood Glucose
Treat hyperglycaemia (Random blood glucose >11 mmol/l) with insulin. Treat hypoglycaemia (Random blood glucose <3 mmol/l) with glucose infusion.
C C C C B C B B B
Nutrition
Perform a water swallow test. (Refer appendix F) Insert a nasogastric tube if the patient fails the swallow test. PEG is superior to nasogastric feeding only if prolonged enteral feeding is required.
Search for infection if fever appears and treat with appropriate antibiotics early. Use anti-pyretics to control elevated temperatures. Hyperventilate to lower intracranial pressure. Mannitol (0.25 to 0.5 g/kg) intravenously administered over 20 minutes lowers intracranial pressure and can be given every 6 hours. If hydrocephalus is present, drainage of cerebrospinal fluid via an intraventricular catheter can rapidly lower intracranial pressure. Hemicraniectomy and temporal lobe resection have been used to control intracranial pressure and prevent herniation among those patients with very large infarctions of the cerebral hemisphere. Ventriculostomy and suboccipital craniectomy is effective in relieving hydrocephalus and brain stem compression caused by large cerebellar infarctions.
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II-3
II-3
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Acute Stroke therapy Treatment rt-Pa Recommendations Intravenous rt-PA (0.9mg/kg, maximum 90mg), with 10% of the dose given as a bolus followed by a 60-minute infusion, is recommended within 4.5 hours of onset of ischaemic stroke. (new recommendation) Reasonable to consider intra-arterial thrombolysis in selected patients with major stroke syndrome of <6 hours duration and ineligible for intravenous thrombolysis. (new recommendation) Endovascular mechanical thrombectomy May be reasonable to perform mechanical disruption to restore cerebral blood ow in selected patients with major stroke syndrome of <8 hours duration and ineligible for or failing intravenous thrombolysis. (new recommendation) Concentric Merci or other endovascular device can be useful for extraction of intra-arterial thrombi in appropriately selected patients, but the utility of the device in improving outcomes is still unclear. (new recommendation) Aspirin Start aspirin within 48 hours of stroke onset. Use of aspirin within 24 hours of rt-PA is not recommended. Anticoagulants The use of heparins (unfractionated heparin, low molecular weight heparin or heparinoids) is not routinely recommended as it does not reduce the mortality in patients with acute ischaemic stroke. Level of evidence I Grade A
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I II-1 I
A A A
Neuroprotective A large number of clinical trials testing a variety of Agents neuroprotective agents have been completed. These trials have thus far produced negative results. To date, no agent with neuroprotective effects can be recommended for the treatment of patient with acute ischaemic stroke at this time.
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AntiCoagulation following Acute Cardioembolic Stroke Treatment Aspirin Warfarin Recommendations All patients should be commenced on aspirin within 48 hours of ischaemic stroke. Adjusted-dose warfarin may be commenced within 2-4 days after the patient is both neurologically and medically stable. Level of Grade Evidence I II-2 A C
Heparin Adjusted-dose unfractionated heparin may be started (unfractionated) concurrently for patients at very high risk of embolism. Anticoagulation Anticoagulation may be delayed for 1-2 weeks if there has been substantial haemorrhage. Urgent routine anticoagulation with the goal of improving neurological outcomes or preventing early recurrent stroke is not recommended. Urgent anticoagulation is not recommended for treatment of patients with moderate-to-large cerebral infarcts because of a high risk of intracranial bleeding complications. Stroke Unit Treatment Stroke unit Recommendations Every hospital should be encouraged to set up a stroke unit. Stroke units significantly reduce death, dependency, institutionalisation and length of hospital stay. A stroke unit should be managed by a multidisplinary stroke team. An efficient referral and rehabilitation network should be established to ensure the success of stroke units.
III III I
C C A
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Cardiac conditions predisposing to Ischaemic stroke Major Risk Conditions Atrial Fibrillation Additional risk factors Risk factors to be access by CHA2DS2-VASc Score. (Refer Appendix E) (new recommendation) Recommendation
CHA2DS2-VASc Recommended score antithrombotic therapy 2 1 OACa Either OACa or aspirin 75-325mg daily. Preferred: OAC rather than aspirin. Either aspirin 75-325mg daily or no antithrobotic therapy. Preferred: no antithrombotic therapy rather than aspirin.
Oral Anticoagulant
Aspirin 75-325mg daily is sufficient for patients < 65 years old with lone AF and no additional risk factors. (new recommendation) Dabigatran etexilate is superior (150mg bid) and as effective (110mg bid) compared to warfarin, in preventing stroke and systemic embolism in non-valvular atrial fibrillation. (new recommendation) Bleeding rates are similar with warfarin for 150mg bid but lower bleeding rates for 110mg bid. * Dabigatran etexilate does not require routine INR monitoring. (new recommendation)
Oral factor Xa inhibitors have also been shown to be at least as effective as VKA in their latest trials. However, at the time of writing, these agents are not yet licensed for stroke prevention in atrial fibrillation in Malaysia. (new recommendation)
Prosthetic Moderate risk: Heart Valves Bileaflet or tilting disk Life-long warfarin (Mechanical) aortic valves in NSR High risk: Bileaflet or tilting disk Life-long warfarin (target INR aortic valves in AF; 3.0; range 2.5-3.5) Bileaflet or tilting disk mitral valve in AF or NSR. Very high risk: Caged-ball and Life-long warfarin caged-disk designs; (target INR 3.0; range 2.5-3.5) documented plus aspirin 75-150mg daily stroke/TIA despite adequate therapy with warfarin.
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II-2
II-3
II-1
Bioprosthetic High risk: heart valves AF; left atrial thrombus at surgery; previous CVA/TIA or systemic embolism.
If high risk factors present, consider warfarin for 3-12 months or longer. For all other patients, give warfarin for 3 months post-op, then aspirin 75-150mg daily. If high risk factors present, consider long-term warfarin. For all other patients start aspirin 75-150mg daily.
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Mitral Stenosis
High risk: AF; previous stroke/TIA; left atrial thrombus; left atrial diameter > 55mm on echo. High risk: Acute/recent MI (<6 mos); extensive infarct with anterior wall involvement; previous stroke/TIA. Very high risk: If risk factors present without LV thrombus: consider warfarin for 3-6 months followed by aspirin 75-150mg daily. III C II-3 II-2 B B
MI and LV dysfunction
If LV thrombus is present, consider warfarin for 6-12 Severe LV dysfunction months. For dilated cardiomyopathies (EF < 28%); LV including peripartum, consider aneurysm; spontaneous echo long-term warfarin. contrast; LV thrombus; dilated non-ischaemic cardiomyopathies.
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Recommended warfarin dose INR target 2.5 [range 2.0 to 3.0] unless stated otherwise Secondary Prevention Factors Treatment Antiplatelets Single agent Aspirin Alternatives: Clopidogrel Ticlopidine Trifusal Cilostazol Recommendations Level of Grade evidence
The recommended dose of aspirin is 75mg to 325mg daily. The recommended dose is 75mg daily. or The recommended dose is 250mg twice a day. The recommended dose is 600mg daily. (new recommendation) The recommended dose is 100mg twice a day. (new recommendation)
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I I I I
A A A A
Double Therapy
Combination therapy of clopidogrel and aspirin is not superior to clopidogrel or aspirin alone; but with higher bleeding complication. (new recommendation) ACE-inhibitor based therapy should be used to reduce recurrent stroke in normotensive and hypertensive patients. ARB-based therapy may benefit selected high risk populations.
Anti-hypertensive treatment
B A C C
Lipid reduction should be considered in all subjects with previous ischaemic strokes. All diabetic patients with a previous stroke should have good glycaemic control. All smokers should stop smoking
Endarterectomy, Angioplasty & Stenting Treatment Carotid Endarterectomy (CEA) Recommendations Indicated for most patients with stenosis of 70-99% after a recent ischaemic event in centres with complication rates of less than 6%. Earlier intervention (within 2 weeks) is more beneficial. May be indicated for patients with stenosis of 50-69% after a recent ischaemic event in centres with complication rates of less than 6%. CEA is not recommended for patients with stenosis of less than 50%. Patients should remain on antithrombotic therapy before and after surgery. Carotid angioplasty & stenting (CAS) CAS represents a feasible alternative to carotid endarterectomy for secondary stroke prevention when surgery is undesirable, technically difficult or inaccessible. Distal protection devices should be used during the procedure and anti-platelet agents such as clopidogrel be initiated. The long-term safety and efficacy of CAS is not known. Intracranial angioplasty & stenting (IAS) Role of IAS in intra-cranial stenoses, asymptomatic stenoses and acute stroke is unclear and not recommended. Level of Grade evidence A I
II-1 III
B C
II-2 II-2
B B
I III II-2
A C C
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Stroke in Special Circumstances Treatment Aspirin Recommendations Young Ischaemic stroke If the cause is not identified, aspirin is usually given. There are currently no guidelines on the appropriate duration of treatment. Cerebral Venous thrombosis Heparin Anticoagulation appears to be safe, and cerebral haemorrhage is not a contra-indication for anticoagulation. Simultaneous oral warfarin should be commenced. The appropriate length of treatment is unknown. II-I B III C Level of Grade evidence
Warfarin
III III
C C
Endovascular It is currently considered for patients with extensive thrombolysis disease and clinical deterioration. ABBREVIATIONS AF: ASA: CAS: CEA: CVA: EF: IAS: ICP: LV: NSR: MI: PEG: PFO: TIA: atrial fibrillation atrial septal aneurysm carotid angioplasty and stenting carotid endarterectomy cerebrovascular accident ejection fraction intracranial angioplasty and stenting intracranial pressure left ventricle normal sinus rhythm myocardial infarction percutaneous endoscopic gastrostomy patent foramen ovale transient ischaemic attack
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TABLE OF CONTENTS STATEMENT OF INTENT & REVIEW OF GUIDELINES CLINICAL PRACTICE GUIDELINES DEVELOPMENT GROUP RATIONALE AND PROCESS OF GUIDELINE DEVELOPMENT OBJECTIVES, QUESTIONS ANDTARGETS KEY TO EVIDENCE STATEMENTS AND GRADES OF RECOMMENDATIONS SUMMARY OF RECOMMENDATIONS ABBREVIATIONS TABLE OF CONTENTS 1. 2. 3. 4. 5. 6. 7. INTRODUCTION & EPIDEMIOLOGY DEFINITION & CLASSIFICATION DIAGNOSIS PROGNOSIS CAUSE AND PATHOPHYSIOLOGY INVESTIGATIONS ACUTE TREATMENT General Management Reperfusion of Ischaemic Brain Stroke Unit PREVENTION Primary Secondary CARDIOEMBOLISM REVASCULARISATION PROCEDURES Primary Prevention Secondary Prevention Angioplasty or Stenting STROKE IN SPECIAL CIRCUMSTANCES Young Stroke Stroke in Pregnancy IMPLEMENTING THE GUIDELINES CONCLUSION REFERENCES APPENDIX A. OCSP Classication B. Stroke Pathophysiology Algorithm C. Management of Suspected Stroke/TIA Algorithm D. Therapeutic Agents Available in Malaysia E. CHA2DS2-VAS Score F. Swallowing Test G. Resources - Societies & Associations H. 9 KPI Recommended by Stroke Council Malaysian Society I. National Institutes of Health Stroke Scale (NIHSS) J. Modified Rankin Scale Acknowledgements
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8. 9. 10.
1 INTRODUCTION & EPIDEMIOLOGY Stroke is a global health problem and is the second commonest cause of death and a leading cause of adult disability worldwide.1 Annually 15 million people worldwide suffer a stroke. Of these, 5 million die and another 5 million are left permanently disabled.2 It is presently among the top four leading causes of death in ASEAN countries, with the crude death rate ranging from 10.9/100 000 (Thailand) to 54.2 per 100 000 (Singapore).3 Ministry of Health statistics show stroke consistently as one of the top five leading cause of death since 2000s. Data in 2009 show cerebrovascular disease causing a mortality of 8.43 per 100 000 population (see table 1).4 There is no incidence or prevalence data available for the country. Table 1: Top 5 Mortality rate in MOH hospitals 20094 Mortality (rate per 100 000 population) 1. Heart Diseases and Diseases of Pulmonary Circulation 2. Septicaemia 3. Malignant neoplasm 4. Pneumonia 5. Cerebrovascular Diseases
Stroke mortality rates vary across the globe, with a ten-fold difference in age-adjusted mortality rates and Disability Adjusted Living Years (DALYs) lost between the highest and lowest ranked countries. National income was a particular strong predictor of stroke burden and mortality. Mortality rates were 3.5 fold higher in low-income countries than in middle-income countries.5 Atherothromboembolism is the major cause of ischaemic stroke worldwide but there are interethnic differences in stroke mortality and subtype. Small vessel infarction (lacunar infarcts) were more commonly seen among Asians when compared to Caucasians in one study.6 There is also possible variation in stroke types among Chinese with a higher proportion of haemorrhagic strokes and studies also highlight the importance of intracranial arterial stenosis as a cause of stroke among Chinese.7 There is a greater predominance of intracranial atherosclerotic vascular disease compared to extracranial or carotid artery disease in Asians.8 2 DEFINITION & CLASSIFICATION OF STROKE Definition of Stroke Stroke is a clinical syndrome characterized by rapidly developing clinical symptoms and/or signs of focal, and at times global, loss of cerebral function, with symptoms lasting more than 24 hours or leading to death, with no apparent cause other than that of vascular origin. Definition of Transient Ischaemic Attack (TIA) A Clinical syndrome characterized by an acute loss of focal cerebral or monocular function with symptoms lasting less than 24 hours and which is thought to be due to inadequate cerebral or ocular blood supply as a result of arterial thrombosis or embolism. Why classify stroke? Classification of stroke has numerous implications during immediate stroke supportive care and rehabilitation, for prognostic purposes, guides cost effective investigations for underlying cause
as well as aids decisions for therapy and secondary stroke prevention strategies. Furthermore, classifications are useful in setting up stroke registries and data banks as well as for epidemiological studies. Oxfordshire Community Stroke Project (OCSP) is a handy clinical classification to use (refer to appendix A). 3 DIAGNOSIS In general, the diagnosis of stroke is made by evaluating and analysing information derived from a good history, physical examination and supplemented with selected diagnostic tests. Because of the nature of the illness and the dramatic manner of the neurological deficits, history is of utmost importance. Every effort must be made to obtain information from the patient, family members, friends, or witnesses. The diagnosis should provide answers to the following questions: 1. What is the neurological deficit? 2. Where is the lesion? 3. What is the lesion? 4. Why has the lesion occurred? 5. What are the potential complications and prognosis? The signs and symptoms of a stroke depend on the type, location and the extent of the affected brain tissue. Stroke patients usually have a sudden or rapid onset of focal neurological symptoms, within minutes to an hour. Some patients may, however, have a stepwise or gradual worsening or waxing and waning symptoms. A third of all strokes occur during night sleep, therefore, the weakness is first noted on waking up in the morning. A full neurological examination, including the patients conscious level and tests of higher mental function (such as the mini-mental state examination) is mandatory. Every positive and negative finding should point to the site of the lesion. These can be divided into 2 broad groups: a) clinical features that are caused by anterior circulation stroke (carotid artery), and b) those caused by posterior circulation stroke (vertebrobasilar system) (see table 1). Table 1. Clinical Features of Stroke Anterior (carotid) artery circulation Middle cerebral artery Aphasia (dominant hemisphere) Hemiparesis / plegia Hemisensory loss/disturbance Homonymous hemianopia Parietal lobe dysfunction, e.g. astereognosis, agraphaesthesia, impaired two-point discrimination, sensory and visual inattention, left-right dissociation and acalculia Anterior cerebral artery Weakness of lower limb more than upper limb
Posterior (vertebrobasilar) artery circulation Homonymous hemianopia Cortical blindness Ataxia Dizziness or vertigo Dysarthria Diplopia Dysphagia Horners syndrome Hemiparesis or hemisensory loss contralateral to the cranial nerves palsy Cerebellar signs Table 2. Differential diagnosis of stroke Differential diagnosis of stroke1 Metabolic/toxic encephalopathy (hypoglycaemia, non-ketotic hyperglycaemia, Wernicke-Korsakoff syndrome, drug intoxication) Epileptic seizures (postictal Todds paresis) Hemiplegic migraine Structural intracranial lesions ( e.g. subdural haematoma, brain tumour, arteriovenous malformation) Encephalitis (e.g. herpes simplex virus), brain abscess, tuberculoma Head injury Hypertensive encephalopathy Relapsing Multiple Sclerosis Conversion disorders Hyperviscosity syndrome Peripheral nerve lesions (e.g. Guillain-Barre Syndrome) 4 PROGNOSIS Prognosis of stroke depends on the stroke type, size and location. Haemorrhagic stroke has a higher mortality than ischaemic stroke.1-4 However patients with haemorrhagic stroke show a better neurological and functional recovery.5 Brainstem infarct, large hemispheric infarct and cardio embolic stroke also carry a poor prognosis.6 Lacunar infarct has the lowest mortality rate.7 Survival after stroke There is a decline in stroke mortality in both men and women suffering from ischaemic or haemorrhagic stroke at all ages in many countries over the past few decades.8.9 This can be attributed to the introduction of stroke units which provide organized stroke care and a better control of stroke risk factors resulting in milder stroke.10-15 A patient who survives the first 30 days after a first-ever stroke has an annual death risk of 9-10%.16,17 Studies in recent years showed that case fatality rates after a first-ever stroke (all types combined) were 10% at one week, 20% at one month, 30% at one year, 60% at 5 years16,17 and 76% at 10 years.18
In a local study published in 2003, the in-hospital mortality in ischaemic stroke was 11% while for haemorrhagic stroke is much higher, at 27.3%.19 Death occurring within the first 30 days after stroke is commonly due to the direct effect of brain damage.4 Thereafter, mortality is usually caused by complications of immobilisation (bronchopneumonia, deep vein thrombosis), recurrent stroke and coronary heart disease.16 Risk factors for stroke mortality Previous use of antiplatelet drugs nearly halves the risk of early death in patient with ischaemic stroke while old age, atrial fibrillation, ischaemic heart disease and diabetes mellitus increase the risk of early death6 Diabetes mellitus, both diastolic and systolic hypertension, smoking, increased cardiothoracic ratio, pre-existing coronary heart disease are risk factors for long term stroke mortality.20 Recurrent stroke The recurrent rates are 4% in the first month and 12% in the first year. Thereafter the risk falls to about 4-5% per year, so that by 5 years, 30% will have suffered a recurrent stroke.21, 22 Disability After a first-ever stroke, about 60% of the patients are alive at 5 years.18 One-third of stroke survivors exhibit some from of persistent disability after initial stroke episode. Up to 58% patients with stroke who survive the first stroke regains independence in activities in daily living, with most functional recovery occurs within the first 2 months of stroke. Less functional recovery is observed during the next 4 to 5 months after stroke. Improvement in functional recovery is less than certain after 6 months, however known predictors of disability are older age, a very low premorbid level of activities before the stroke and subsequent recurrent stroke.24
5 CAUSE & PATHOPHYSIOLOGY Three main causes of ischaemic stroke are: 1. Atherothromboembolism (50%) 2. Intracranial small vessel disease (penetrating artery disease) (25%) 3. Cardiogenic embolism (20%) Other causes include arterial dissection, trauma, vasculitis (primary/secondary), metabolic disorders, congenital disorders and other less common causes such as migraine, pregnancy, oral contraceptives, etc. Atheroma affects mainly the large and medium sized arteries at places of confluence, branching or tortuosity of vessels. The process begins in childhood as fatty streaks and progresses over years with gradual buildup of fibrolipid plaque and infiltration of inflammatory cells, eventually narrowing the vessel lumen. The final step occurs with ulceration and platelet-fibrin thrombus formation on the plaque surface. The atherothrombotic plaque can grow to obstruct a vessel, with intraluminal propagation of the thrombus proximally or distally to cause occlusion, or embolism occurs from the plaque surface to occlude smaller distant vessel(s). Intracranial small vessel disease is thought to be due to lipohyalinosis but other causes may include microatheroma and angionecrosis, or thromboembolism from a larger artery. The clinical syndrome caused by this is lacunar infarction due to occlusion of small perforating arteries.
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Vascular risk factors associated with increased risk of stroke: NON-MODIFIABLE Age Sex Ethnicity / Race Family history of stroke MODIFIABLE High Blood Pressure (systolic and diastolic) Cigarette smoking Diabetes mellitus Atrial Fibrillation Coronary heart disease Hyperlipidaemia Obesity & physical inactivity Raised Homocysteine levels High dietary salt intake Heavy alcohol consumption Previous stroke
Embolism from the heart causes approximately 20% of all ischaemic strokes. The most common causes are atrial fibrillation and valvular heart disease. Not all cardiac sources pose similar threat in causing stroke. The algorithm in appendix b outlines the steps to a diagnosis of ischaemic stroke and the various causes which need investigation to identify the underlying cause for the stroke. Despite thorough investigations, in up to 40% of strokes no definite cause can be found, especially in young stroke patients. 6 - INVESTIGATIONS The following investigations for patients with ischaemic stroke are recommended in order to achieve the following objectives:1. Confirm the diagnosis 2. Determine the stroke mechanism 3. Risk stratification and prognostication 4. Identify potentially treatable large obstructive lesions of the cerebrovascular circulation
Random blood glucose Urea & electrolytes Clotting profile* NEXT DAY Lipid profile (fasting) Glucose (fasting) OPTIONAL TESTS (in selected patients) VDRL autoimmune screen ESR, antinuclear Factor, Rheumatoid Factor, anti double stranded DNA antibodies, C3 C4 levels, etc Thrombophilia screen & Serum fibrinogen, Anti-thrombin III, Protein C, Protein S, Factor lupus anticoagulant V-Leiden, anti-phospholipid antibodies Homocysteine (fasting) C reactive protein *if thrombolysis is considered Other investigations 12 lead ECG Ambulatory ECG Imaging For all suspected stroke Chest x-ray CT brain In selected patients ECHO cardiography MRI (magnetic resonance imaging) Carotid duplex Ultrasound Transcranial Doppler Ultrasound MR angiography (MRA) CT angiography (multislice CT scan) MR venography Contrast angiogram Mandatory For suspected arrhythmias or sinoatrial node disease
Exclude anaemia, polycythaemia, thrombocytosis, thrombocytopenia, etc Exclude hypoglycemia, new diagnosis of diabetes mellitus Hydration status, excludes electrolyte imbalances Baseline
Mandatory The emergency neuroimaging scan of choice for all patients Differentiates haemorrhage from infarction Confirms site of lesion, cause of lesion, extent of brain affected For suspected cardioembolism, assess cardiac function Sensitive Not available in emergency setting, limited by expense Useful tool to select patients for thrombolysis where available Allows identification of extracranial vessel disease Identifies intracranial vessel disease with prognostic and therapeutic implications Non invasive tool to assess intra- and extra-cerebral circulation Objective assessment of vessel stenosis Non invasive tool to assess intra- and extra-cerebral circulation. Involves intravenous contrast injection In suspected cerebral venous thrombosis Gold standard assessment of cerebral vasculature Reserved for patients planned for intervention
7 ACUTE TREATMENT GENERAL MANAGEMENT The general management of acute stroke includes supportive care and treatment of acute complications. This is important to improve mortality and functional disability. Oxygen and Airway Support Adequate tissue oxygenation is imperative to prevent hypoxia and potential worsening of the (Level II-3 to III) neurological injury.1-5 Observation Regular observation is mandatory to recognise impaired pulmonary function (pulse oxymeter), circulatory function (pulse rate, blood pressure), NIHSS, Head Chart, GCS and to recognise (Level III) complications from mass effect.1 (new recommendation) Mobilisation Most patients are first treated with bed rest, but mobilisation should begin as soon as the patients condition is judged to be stable.6-9 Mobilisation of acute stroke patients, in bed and out of bed as early as possible is currently recommended to prevent general and neurological complications.Helping patients to get out of bed very early is recommended, with other mobilization exercise including passive and full-range of motion exercise, transfer from bed to chair, balance and trunk support are done in stages. It is however unclear whether very early mobilization (within 48hours) independently improves outcome although no significant harms were identified.8,9 (new recommendation) (Level II-3) Blood Pressure Hypertension following stroke is quite common. However, its optimal management has not been established.1,10-12 (Level II-3 to III) Very high blood pressure should be reduced gradually. Proposed drugs: Labetolol 10-20mg boluses at 10 minute intervals up to 150-300mg or 1mg/ml infusion, at the rate of influsion for labetolol as 1-3mg/min or Captopril. Sublingual use of a calcium antagonist, such as nifedipine, should be avoided because of rapid decline in blood pressure.12 (Level II-3) Blood Glucose Hyperglycaemia following acute stroke is strongly associated with subsequent mortality and (Level II-3) impaired neurological recovery. This applies to diabetics and non-diabetics.13, 14 Nutrition Sustaining nutrition is important as malnutrition after a stroke might interfere with recovery.15 Persons with infarctions of the brain stem, multiple strokes, large hemispheric lesions, or depressed consciousness are at the greatest risk for aspiration. Swallowing impairments are associated with an increased mortality. Early initiation of percutaneous placement of an endogastric (PEG) tube feeding has not been shown to improve long-term outcome.16 A water swallow test (refer to Appendix F) should be performed before the patient is allowed to eat or drink.A wet voice after swallowing, incomplete oral-labial closure,or coughing reflex on swallowing indicates high risk of developing aspiration. A videofluoroscopic modified barium (Level III) swallow examination can be performed later if indicated.1,17 If the patient fails the swallowing test, a nasogastric tube should be inserted to prevent aspiration. (PEG) tube is superior to nasogastric tube feeding if a prolonged need for devices is anticipated.18 (level II-1)
7
Infection Infection is the commonest complication after an acute stroke especially pneumonia and urinary tract infection.19 The appearance of fever should prompt a search for infection and appropriate antibiotic therapy (Level III) should be administered early.19 Bladder catheters should be avoided if possible 1 Fever A meta-analysis suggested that fever after stroke onset is associated with marked increase in mortality and morbidity.20 Anti-pyretics should be used to control elevated temperatures in acute stroke patients.20, 21 (Level II-1) Raised Intracranial Pressure Cerebral oedema and increased intracranial pressure largely occur with large cerebral infarctions. The head of the bed can be elevated by 20 to 30 degrees in an attempt to help venous drainage. Hyperventilation is an emergency measure that acts almost immediately; a reduction of the PCO2 by 5 to 10mmHg can lower intracranial pressure by 25% to 30%.1,22 (LeveL II-2) Mannitol (0.25 to 0.5g/kg) intravenously administered over 20 minutes lowers intracranial pressure and can be given every 6 hours.23 The usual maximum daily dose is 2 g/kg. (Level II-2) If hydrocephalus is present, drainage of cerebrospinal fluid via an intraventricular catheter can rapidly lower intracranial pressure.1 (Level III) Hemicraniectomy and surgical decompressive therapy with 48 hours after symtoms onset is recommended to control intracranial pressure and prevent herniation among those patients with (Level I-1) very large infarctions of the cerebral hemisphere.24-26 Ventriculostomy and suboccipital craniectomy is effective in relieving hydrocephalus and brain stem compression caused by large cerebellar infarctions.27,28 (Level II-2) Recommendation: Factors Airway & Breathing Recommendation Ensure clear airway and adequate oxygenation. Elective intubation may help some patients with severely increased ICP. Mobilization Blood Pressure Mobilize early to prevent complications. Do not treat hypertension if < 220mmHg systolic or < 120mmHg diastolic. Mild hypertension is desirable at 160-180/90-100 mmHg. Blood pressure reduction should not be drastic. Proposed substances: Labetolol 10-20mg boluses at 10 minute intervals up to 150-300mg or 1mg/ml infusion, rate of infusion for labetolol as 1-3mg/min or Captopril 6.25-12.5mg orally. III II-3 III III C C C C Level of Grade evidence
Blood Glucose
Treat hyperglycaemia (Random blood glucose >11mmol/l) with insulin. Treat hypoglycaemia (Random blood glucose< 3 mmol/l) with glucose infusion.
C C C C B C B B B
Nutrition
Perform a water swallow test. Insert a nasogastric tube if the patient fails the swallow test. PEG is superior to nasogastric feeding only if prolonged enteral feeding is required.
Search for infection if fever appears and treat with appropriate antibiotics early. Use anti-pyretics to control elevated temperatures. Hyperventilate to lower intracranial pressure. Mannitol (0.25 to 0.5g/kg) intravenously administered over 20 minutes lowers intracranial pressure and can be given every 6 hours. If hydrocephalus is present, drainage of cerebrospinal fluid via an intraventricular catheter can rapidly lower intracranial pressure. Hemicraniectomy and surgical decompressive therapy with 48 hours after symtoms onset is recommended to control intracranial pressure and prevent herniation among those patients with very large infarctions of the cerebralhemisphere. Ventriculostomy and suboccipital craniectomy is effectivein relieving hydrocephalus and brain stem compression causedby large cerebellar infarctions.
III
II-3
II-3
REPERFUSION OF ISCHAEMIC BRAIN In cerebral infarcts, restoration of perfusion to the ischaemic brain tissue is a key therapeutic strategy. The concept of the existence of an ischaemic penumbra is fundamental to the current approach to treatment of ischaemic stroke: although a core of infarct tissue might not be salvageable, adjacent dysfunctional tissue might be saved if the circulation is restored and metabolism is normalized. Intravenous Thrombolysis With rt-PA Intravenous rt-PA (0.9mg/kg, maximum 90mg), with 10% of the dose given as a bolus followed by a 60-minute infusion, is recommended within 4.5 hours of onset of ischaemic stroke.5,7 (new recommendation) (Level 1, Grade A) The use of streptokinase is contraindicated in acute ischaemic stroke due to poor clinical outcome.6 (Level 1, Grade A) Intravenous rt-PA can be given only if the following is available: 1. A physician with expertise in the diagnosis and management of stroke. 2. Appropriate neuroimaging tests are available 24 hours a day 3. Capability to manage the complications of thrombolysis, particularly intracranial haemorrhage. Characteristics of Patients With Ischaemic Stroke Who Could Be Treated With rt-PA
1. 2. 3. 4. 5. 6. 7. 8. 9. Diagnosis of ischaemic stroke causing measurable neurological deficit. The neurological signs should not be clearing spontaneously. The neurological signs should not be minor and isolated. Caution should be exercised in treating a patient with major deficits. Onset of symptoms <4.5 hours before beginning treatment. No contraindication for thrombolytic therapy. Blood pressure less than 185mm Hg systolic and/or less than 110mm Hg diastolic. Brain CT is normal or minimal change. The patient or family understand the potential risks and benefits from treatment.
10
Old age is not a contraindication but it is not wise to use it in patients above 75 years old. Caution is advised before giving intravenous rt-PA to persons with severe stroke.
Regimen for Treatment of Acute Ischaemic Stroke with Intravenous rtPA 1. Infuse 0.9mg/kg maximum of 90 mg over 60 minutes with 10% of the dose given as a bolus dose over 1 minute. 2. Admit the patient to an intensive care unit or a stroke unit for monitoring. 3. Perform neurological assessments every 15 minutes during the infusion of rt-PA and every 30 minutes for the next 6 hours and then every hour until 24 hours from treatment. 4. If the patient develops severe headache, acute hypertension, nausea or vomiting discontinue the infusion if agent is still being administered and obtain a CT scan of brain. 5. Measure blood pressure every 15 minutes for the first 2 hours, every 30 minutes for the next 6 hours and then every hour until 24 hours from treatment. 6. Increase blood pressure measurements if a systolic blood pressure >180mmHg or diastolic blood pressure >105mmHg is recorded. Administer anti-hypertensive medications to maintain blood pressure at or below these levels. 7. Delay placement of nasogastric tubes, indwelling bladder catheters or intra-arterial pressure catheters. 8. Avoid antiplatelet drugs for the first 24 hours after administration of rt-PA.
Management of Bleeding Complications Haemorrhagic transformation should be considered as a cause of neurological deterioration following the use of a thrombolytic agent. If an urgent brain CT confirms a haemorrhage, stop the rt-Pa infusion. Obtain blood samples for coagulation tests, infuse fresh frozen plasma and cryoprecipitate, and seek immediate neurosurgical opinion. Intra-arterial thrombolysis (new recommendation) Intra-arterial thrombolysis is an option for the treatment of selected patients who have major stroke of <6 hours duration due to occlusions of the middle cerebral artery, internal carotid and carotid terminus who are not otherwise candidates for intravenous rtPA.1-3 Level II-2, Grade C Intra-arterial thrombolysis should be considered only if the following is available: 1. A physician with expertise in the diagnosis and management of stroke. 2. A physician with expertise and experience managing Intravenous rt-PA cases. 3. Appropriate neuroimaging tests including perfusion and angiography are available 24 hours a day. 4. Interventional Neuroradiologist or qualified physician with experience of endovascular intracranial work. 5. Capability to manage the complications of thrombolysis, particularly intracranial haemorrhage as in intravenous thrombolytic therapy. Endovascular mechanical thrombectomy (new recommendation) Endovascular mechanical thrombectomy uses MERCI device or other mechanical devices, endovascularly, to disrupt the clot and restore cerebral blood ow. It may be performed up to <8 hours duration in selected patients with major stroke syndrome and ineligible for or failing intravenous thrombolysis (4-7). However, the utility of the device in improving outcomes after stroke is unclear. Level III, Grade C
11
Endovascular mechanical thrombectomy should be considered only if the following is available: 1. A physician with expertise in the diagnosis and management of stroke. 2. A physician with expertise and experience managing Intravenous rt-PA cases. 3. Appropriate neuroimaging tests including perfusion and angiography are available 24 hours a day. 4. Interventional Neuroradiologist or qualified physician with experience of endovascular intracranial work. 5. Interventional Neuroradiologist or qualified physician familiar to handle endovascular mechanical thrombectomy devices. 6. Capability to manage the complications of thrombolysis, particularly intracranial haemorrhage as in intravenous thrombolytic therapy. Recommendations Treatment rt-Pa Recommendations Level of Grade evidence I A
Intravenous rt-PA (0.9mg/kg, maximum 90mg), with 10% of the dose given as a bolus followed by a 60-minute infusion, is recommended within 4.5 hours of onset of ischaemic stroke.5,7
Start aspirin within 48 hours of stroke onset. Use of aspirin within 24 hours of rt-PA is not recommended. The use of heparins (unfractionated heparin, low molecular weight heparin or heparinoids) is not routinely recommended as it does not reduce the mortality in patients with acute ischaemic stroke.
Aspirin Anticoagulants
I II-1 I
A A A
Neuroprotective A large number of clinical trials testing a variety of Agents neuroprotective agents have been completed. These trials have thus far produced negative results. To date, no agent with neuroprotective effects can be recommended for the treatment of patient with acute ischaemic stroke at this time. STROKE UNIT
All patients with acute stroke should ideally have access to stroke units. There is clear evidence that treatment of patients with stroke in stroke units significantly reduces death, dependency, institutionalisation and length of hospital stay compared to treatment in a general medical ward.1-7 (Level I) This benefit is independent of patients age, sex, co morbidity and stroke severity.1,8 (Level I)
A stroke unit is a dedicated unit in the hospital exclusively managing stroke patients. A team of specially trained staff provides coordinated multidisciplinary care throughout 24 hours to patients on a stroke unit. The core disciplines of the stroke team are: medical (neurologist, geriatrician or general physicians with interest in stroke), medical rehabilitation physician, pharmacist, nursing, physiotherapy, occupational therapy and speech therapy. In bigger centres, it may include neurosurgeon, social worker and dietitian. Effectiveness of a stroke unit is not necessarily related to a certain medical specialty. A stroke unit runs by general physician, geriatrician, neurologist or specialist in rehabilitation medicine may be equally effective.1 (new recommendation) (Level I)
12
Stroke units are available in several categories: (1) The acute stroke unit which accepts patients acutely but discharged patients early, usually within 1 week. (2) The combined acute and rehabilitation stroke unit admitting patients acutely but also provide rehabilitation for several weeks. (3) The rehabilitation stroke unit which accepts patients after a delay of 1 or 2 weeks and focuses on rehabilitation for several weeks or months if necessary. Of these, only the combined acute and rehabilitation stroke unit, and the rehabilitation stroke unit have proven effectiveness in terms of reduced mortality and handicap.1 (Level I) Possible reasons for stroke unit benefits include early acute treatment, reduced incidence of infection and systemic complications as well as early and more intense rehabilitation.9 (Level I) Stroke unit can only work optimally if a well-established referral and rehabilitation network is available. This also includes co-operation with primary care physician in primary and secondary stroke prevention. 9 KPI is the measurement index for effectiveness of a stroke unit. (Refer to Appendix H and I) (new recommendation) Recommendation: Treatment Stroke unit Recommendations Every hospital should set up a stroke unit. Stroke units significantly reduces death, dependency, institutionalisation and length of hospital stay. A stroke unit should be managed by a multidisciplinary stroke team. An efficient referral and rehabilitation network should be established to ensure the success of stroke units. Level of Grade evidence I I I III A A A C
8 PREVENTION PRIMARY PREVENTION Primary prevention is the key factor in any plan to reduce the incidence of stroke. This should be targeted to the whole population as well as high-risk groups by increasing awareness and promoting healthy lifestyles to reduce risk factors for stroke. The strategies should be integrated in the overall programme of health promotion for vascular diseases. Although the following factors are non-modifiable, they identify individuals at highest risk of stroke and those who may benefit from rigorous prevention or treatment of modifiable risk factors. Age: The cumulative effects of aging on the cardiovascular system and the progressive nature of stroke risk factors over a prolonged period of time age substantially increase stroke risk. The risk of stroke doubles in each successive decade after 55 years of.1,2
13
Sex: Stroke is more prevalent in men than women.1 Overall, men also have higher age-specific stroke incidence rates than women.3 Exceptions are in 35 to 44 year-olds and in those over 85 years of age in whom women have slightly greater age-specific incidence than men.3 Circumstances such as oral contraceptive use and pregnancy uniquely contribute to the risk of stroke in women.4-6 Family History: Both paternal and maternal history of stroke may be associated with increased risk. This may be mediated through genetic and shared environmental factors.7,8 Medical Therapy Aspirin Aspirin may benefit women above the age of 65 in the primary prevention of stroke.9 (Level II-I) Recommendation: 100mg aspirin every other day may be useful in women above the age of 65. Hypertension Hypertension is a major risk factor for both cerebral infarction and intracerebral haemorrhage.10 The incidence of stroke increases in proportion to both systolic and diastolic blood pressures. Isolated systolic hypertension is an important risk factor for stroke in the elderly (systolic blood pressure >140mmHg and diastolic blood pressure <90mmHg).34 Large randomized controlled trials and meta-analyses have confirmed that reduction in blood 12-15 pressure reduces stroke incidence. (Level I) Lowering the systolic blood pressure by 10mmHg is associated with a reduction in risk of stroke by about a third, irrespective of baseline blood pressure levels.29 (Level I) Combination therapy is more likely to achieve target blood pressures. Recent published studies suggest that certain classes of anti-hypertensives may have additional benefits above and beyond lowering of blood pressure30,31 but no definite recommendations can be made. (Level I) Hypertension in the very elderly should be treated to reduce the risk of stroke, with reduction of stroke risk in elderly with hypertension, isolated hypertension and previous stroke.32 (Level I) Smoking All forms of smoking, both active and passive is a major risk factor for stroke.18 Smokers who (Level III) stopped for more than 5 years have the same risk as non-smokers.19 Alcohol Heavy alcohol drinking, more than 3 units/day (1unit = 1glass wine = 1 pack of hard liquor), increases the risk of stroke while light or moderate alcohol intake is protective against all strokes.20 (Level II-2) Post menopausal Hormone Replacement therapy Stroke rates rapidly rise in women once they become menopausal. The Nurses Health Study (6-year follow-up of 59,337 postmenopausal women) showed only a weak association between stroke and oestrogen replacement. However, the Womens Health Initiative Estrogen Plus.
14
Progestin Study ( E+P Study) showed a 31% increase in the risk of stroke due to E + P.21 (Level I) Diabetes Case-control studies of stroke patients and prospective epidemiological studies have confirmed an independent effect of diabetes on ischaemic stroke, with an increased relative risk in diabetics (Level II-2) ranging from 1.8- to nearly 6-fold.22 Tight control of hypertension in diabetics significantly reduced stroke incidence.23 (Level I)
Tight glycemic control (Hb A1c < 6%) is important and supported by epidemiology and a meta-analysis.24 (Level II-2) Asymptomatic Carotid Stenosis Atrial fibrillation See Revascularization Procedures See CardioEmbolism & Stroke
Hyperlipidaemia Recent epidemiological studies have shown an association between raised serum lipids and risk of ischaemic stroke.25-26 In the high risk group, (those with cardiovascular disease, occlusive arterial disease or diabetes) statin therapy reduces the incidence of coronary events and ischaemic strokes even amongst individuals with normal cholesterol concentrations.27, 28 (Level I) Well-Documented Modifiable Risk Factors. Factors Hypertension Recommendation Treat medically if BP>140mmHg systolic and/or >90mmHg diastolic.18 Lifestyle changes if BP between 130-139mmHg systolic and/or 80-89mmHg diastolic. Target BP for diabetics is <130mmHg systolic and <80mmHg diastolic.18 Hypertension should be treated in the very elderly (age > 70 yrs) to reduce risk of stroke.34 Diabetes mellitus Strict blood pressure control is important in diabetics.23 Maintain tight glycaemic control.24 Hyperlipidaemia High risk group: keep LDL < 2.6mmol/l 1 or more risk factors: keep LDL < 3.4mmol/l Smoking Aspirin therapy No risk factor: keep LDL < 4.2mmol/l Cessation of smoking. 100mg aspirin every other day may be useful in women above the age of 65. III II-1 I C B A I B Level of evidence I I I I I Grade A A A A A
Post menopausal Oestrogen based HRT is not recommended for Hormone primary stroke prevention. Replacement therapy Alcohol Avoid heavy alcohol consumption.
15
II-2
SECONDARY PREVENTION Secondary Prevention of Stroke Secondary prevention are strategies used after a stroke to prevent recurrence. This should be tailored according to individual stroke pathogenesis based on neuroimaging and investigations. (see Investigations) The risk for recurrent vascular events after a stroke or transient ischaemic attack is approximately 5% per year for stroke, 3% per year for myocardial infarction and 7% per year for any one of stroke, myocardial infarction or vascular death.1 This figure is even higher is certain populations especially those with high cerebrovascular atherosclerotic burden and for patients with ipsilateral high grade (70%) extracranial carotid stenosis.2 Anti-platelet therapy There is substantial evidence to support the value of aspirin. A 25% risk reduction of stroke was seen in all patients with strokes who have received aspirin.3 Aspirin given within 48 hours has also been shown to be beneficial in reducing recurrent stroke and death.3-5 Studies comparing the effects of different dosages of aspirin failed to show differences in stroke recurrences.6-9 Aspirin: The recommended dose of aspirin post- stroke is 75mg to 325mg orally daily (Level I) Alternative antiplatelet medications can be considered for patients with aspirin allergy, aspirin failure, aspirin intolerance or aspirin contraindications based on the evidence presented below. Ticlopidine: Previous clinical trials have demonstrated that ticlopidine is slightly superior to aspirin.10-11 Blood monitoring is essential as neutropenia is the most significant side-effect.10 Severe neutropenia usually occurs within 3 months. Thus, baseline full blood count should be performed every 2-3 weeks within this time frame. Ticlopidine can be used if the patient has recurrent symptoms despite aspirin. The recommended dose of ticlopidine is 250mg orally twice a day. (Level I)
Clopidogrel: Clopidogrel is a newer thienopyridine derivative. It is slightly superior to 325 mg of aspirin.12 It may be more beneficial than aspirin in several settings including patients with contraindications or adverse effects to aspirin and in high risk subjects with multiple risk factors (i.e. with a previous stroke, peripheral artery disease, symptomatic coronary disease and diabetes.)13 The recommended dose is 75mg daily. (Level I)
Triflusal: Triflusal is a viable alternative to aspirin in secondary prevention of ischaemic stroke at a dosage of 600mg daily. There is less haemorhagic complications compared to aspirin. Triflusal is licensed in Malaysia for the secondary prevention of ischaemic stroke.14 (Level I) (new recommendation) Cilostazol: Cilostazol is also another alternative in the secondary prevention of acute ischaemic stroke at the dosage of 100mg b.d. However, at the time of writing, cilostazol is under regulatory review for secondary ischaemic stroke prevention in Malaysia.15 (new recommendation) (Level I)
16
Aspirin plus dipyridamole slow release: This combination is superior to aspirin or dipyridamole alone.16 The combination of aspirin (50mg) plus dipyridamole (400mg) doubles the effect of (Level I) aspirin or dipyridamole alone. Recommendation: The recommended dose of aspirin is 50 to 325mg daily & slow release (Level I) dipyridamole 400mg orally daily* *Slow release dipyridamole is not available in Malaysia. Regular dipyridamole can be used with gradual titrations up to the required dosage, but may be limited by side-effects. Aspirin and clopidogrel combination: Recent evidence from a large trial in post-stroke patients which compared clopidogrel 75mg alone against clopidogrel 75mg and 100mg of aspirin over an 18 month period17 have shown an excess of gastrointestinal and major intracranial bleeding in the combination arm. The trial results do not support the addition of aspirin to clopidogrel in stroke patients for the purpose of long term secondary prevention. The use of this combination of antiplatelet drugs can only be used in selected high risk patients, who experience stroke recurrence despite monotherapy, when the benefit outweighs the risk. Anticoagulation with warfarin Long-term anticoagulation with warfarin after a stroke may reduce recurrent events in patients with atrial fibrillation. For patients without atrial fibrillation, modern clinical trials such as the WARSS study suggest that warfarin was not more effective compared to aspirin alone.18 In the latest study (WASID) comparing warfarin with high-dose aspirin (1300mg daily) in patients with intra-cranial stenosis, patients on warfarin had an excess of major haemorrhage and deaths.19 Recommendations: Warfarin is indicated for secondary stroke prevention for patients with atrial fibrillation. (Level I) Warfarin is not indicated for secondary stroke prevention for patients in sinus rhythm in absence of other conditions predisposing to cardio-embolic risk. (Level I) Anti-hypertensive treatment Reduction of blood pressure after the acute phase of the cerebrovascular event results in a further reduction of vascular events. This benefit has been noted in both ischaemic and haemorrhagic stroke with hypertensive and normotensive subjects.20 Meta-analyses of randomized controlled trials confirm approximately 30 40% reduction in stroke risk with blood pressure lowering.21 In one study, the combination of an ACE-inhibitor and thiazide diuretic has been beneficial in both hypertensive and normotensive stroke patients when started two weeks after the event.22 Another study has proven the superiority of an angiotensin receptor blocker, losartan (ARBs) over a beta-blocker (atenolol) in a specific group of high risk patients with left ventricular hypertrophy including subjects with previous stroke.23
17
In the post-stroke situation (2 weeks or more after a stroke), ACE-inhibitor based therapy has been shown to reduce recurrent stroke in normotensive and hypertensive patients.24 (Level I) Other classes of anti-hypertensives (ARB-based) therapy appear to be effective in selected high risk populations.25,26 (Level I) Target blood pressure of absolute levels are not certain but targets based on hypertension guidelines (local or international) can be followed but should be individualized.27 (Level II-1) The choice of antihypertensive drug therapy (single or combination) should also be individualized (Level II-1) based on current evidence and specific patient characteristics.27 Carotid Endarterectomy (CEA) See Revascularization Procedures
Lipid lowering Statins have been proven to reduce vascular events among high risk patients including subjects (Level I) with previous strokes.28,29 Other risk factors The control of risk factors such as better glycaemic control in diabetes and smoking cessation have not been the subject of major randomized secondary prevention clinical trials. Although diabetes is recognized as an independent risk factor for ischaemic stroke, better diabetes control results only in a reduction of microvascular but not macrovascular complications.30 Inferences can also be drawn from the positive results of primary prevention trials. (see primary prevention section). Nevertheless, better control of these risk factors should be advocated for better overall health after an ischaemic stroke. (Level III)
Recommendation:
Factors Treatment Antiplatelets Single agent Aspirin Alternatives: Clopidogrel Ticlopidine Trifusal Cilostazol
Recommendations
The recommended dose is 75mg daily.12 The recommended dose is 250mg twice a day.10,11 The recommended dose is 600mg daily.14 (new recommendation) The recommended dose is 100mg twice a day.15 (new recommendation)
I I I I
A A A A
18
Double Therapy
Combination therapy of clopidogrel and aspirin is not superior to clopidogrel or aspirin alone; but with higher bleeding complication. (new recommendation) ACE-inhibitor based therapy should be used to reduce recurrent stroke in normotensive and hypertensive patients.24 ARB-based therapy may benefit selected high risk populations.25,26
Anti-hypertensive treatment
B A C C
Lipid reduction should be considered in all subjects with previous ischaemic strokes.28,29 All diabetic patients with a previous stroke should have good glycaemic control. All smokers should stop smoking
9 CARDIOEMBOLISM Cardioembolic stroke accounts for about 20% of all ischaemic strokes.1-3 They are in general severe, prone to early recurrence, more likely when there is documented source of embolism, and involvement of different cerebrovascular territories or multiple infarctions.The predominant pathogenic process for stroke associated with cardiac disease is embolism due to formation of intra-atrial and intra-ventricular thrombus. Atrial fibrillation (AF) whether chronic or paroxysmal, is the most common cause of cardioembolism and accounts for 50% of all cardiogenic emboli. Other high risk conditions are prosthetic heart valves, rheumatic mitral valvular disease, acute myocardial infarction and severe left ventricular dysfunction. Non-thrombotic embolism may result from atrial myxoma and endocarditis. Investigations are directed at demonstrating cardiac sources of embolism in the absence of significant atherosclerosis or other vascular disease. All patients with CVA/TIA require a 12-lead electrocardiograph. A 24-hour or 48-hour Holter monitor may be required for diagnosis of paroxsysmal AF. In addition, all patients under 45 years of age and those in whom baseline investigations did not reveal an apparent cause for CVA will require a transthoracic echocardiogram (TTE). Patients in whom there is high suspicion of cardioembolism not found on TTE may undergo a trans-esophageal echocardiogram (TEE). Conditions in which this method is superior to TTE include identifying thrombi in left atrium and left atrial appendage, patent foramen ovale, atrial septal aneurysm and aortic arch atheroma.3,4 Oral anticoagulation may reduce the risk of first and subsequent strokes for selected high-risk cardiac conditions but must be weighed against the risk of haemorrhagic complications.1,2,5,6 (see table b) Patients with minor risk cardiac conditions (such as mitral valve prolapse, mitral regurgitation, atrial septal aneurysm and patent foramen ovale) without additional risk factors may be offered (Level III) aspirin 75-325mg/day for primary prevention of stroke.
19
If patients were aspirin intolerant then consider: clopidogrel 75mg daily, ticlopidine 250mg bd or dipyridamole 400mg daily.1 (Level III) Anticoagulation is not indicated for non-thrombotic causes of cardiac emboli and may cause substantial intracranial haemorrhage in infective endocarditis of native valves.1 Anticoagulation is not proven to reduce recurrent stroke in the first 14 days following an acute cardioembolic event [I, A] with the possible exception of prosthetic heart valves, recent MI, presence of intra-cardiac thrombus, AF with additional risk factors and previous CVA.3 (see table a) (Level III)
Table a. Anticoagulation for the patient with acute cardioembolic stroke Treatment Warfarin Recommendations Adjusted-dose warfarin may be commenced within 2-4 days after the patient is both neurologically and medically stable. Level of Grade Evidence
II-2
Heparin Adjusted-dose unfractionated heparin may be started (unfractionated) concurrently for patients at very high risk of embolism. Anticoagulation Anticoagulation may be delayed for 1-2 weeks if there has been substantial haemorrhage. Urgent routine anticoagulation with the goal of improving neurological outcomes or preventing early recurrent stroke is not recommended. Urgent anticoagulation is not recommended for treatment of patients with moderate-to-large cerebral infarcts because of a high risk of intracranial bleeding complications.
III III I I
C C A A
20
Additional risk factors Risk factors to be access by CHA2DS2-VASc Score. (Refer Appendix E) (new recommendation)
Recommendation
CHA2DS2-VASc Recommended score antithrombotic therapy 2 1 OACa Either OACa or aspirin 75-325mg daily. Preferred: OAC rather than aspirin. Either aspirin 75-325mg daily or no antithrobotic therapy. Preferred: no antithrombotic therapy rather than aspirin.
Oral Anticoagulant
Aspirin 75-325mg daily is sufficient for patients < 65 years old with lone AF and no additional risk factors. (new recommendation) Dabigatran etexilate is superior (150mg bid) and as effective (110mg bid) compared to warfarin, in preventing stroke and systemic embolism in non-valvular atrial fibrillation. (new recommendation) Bleeding rates are similar with warfarin for 150mg bid but lower bleeding rates for 110mg bid. * Dabigatran etexilate does not require routine INR monitoring. (new recommendation)
Oral factor Xa inhibitors have also been shown to be at least as effective as VKA in their latest trials. However, at the time of writing, these agents are not yet licensed for stroke prevention in atrial fibrillation in Malaysia. (new recommendation)
Prosthetic Moderate risk: Heart Valves Bileaflet or tilting disk Life-long warfarin (Mechanical) aortic valves in NSR High risk: Bileaflet or tilting disk Life-long warfarin (target INR aortic valves in AF; 3.0; range 2.5-3.5) Bileaflet or tilting disk mitral valve in AF or NSR. Caged-ball and Life-long warfarin caged-disk designs; (target INR 3.0; range 2.5-3.5) documented plus aspirin 75-150mg daily stroke/TIA despite adequate therapy with warfarin.
21
II-2
II-3
II-1
Bioprosthetic High risk: heart valves AF; left atrial thrombus at surgery; previous CVA/TIA or systemic embolism
If high risk factors present, consider warfarin for 3-12 months or longer For all other patients, give warfarin for 3 months post-op, then aspirin 75-150mg daily If high risk factors present, consider long-term warfarin For all other patients start aspirin 75-150mg daily
III
III
Mitral Stenosis
High risk: AF; previous stroke/TIA; left atrial thrombus; left atrial diameter > 55mm on echo. High risk: Acute/recent MI (<6 mos); extensive infarct with anterior wall involvement; previous stroke/TIA. Very high risk: If risk factors present without LV thrombus: consider warfarin for 3-6 months followed by aspirin 75-150mg daily III C II-3 II-2 B B
MI and LV dysfunction
If LV thrombus is present, consider warfarin for 6-12 Severe LV dysfunction months For dilated cardiomyopathies (EF < 28%); LV aneurysm; including peripartum, consider long-term warfarin spontaneous echo contrast; LV thrombus; dilated non-ischaemic cardiomyopathies.
III
III
Recommended warfarin dose INR target 2.5 [range 2.0 to 3.0] unless stated otherwise
HAS-BLED7,8 stands for hypertension, abnormal renal/liver function, stroke, bleeding history or predisposition, labile INR, elderly (age over 65), and drugs/alcohol concomitantly; the maximum possible score is 9with 1 point for each of the components (with abnormal renal/liver function, for example, possibly scoring two if both are present and similarly drugs/alcohol possibly contributing 2 points). "Drugs" refers to any medications that increase bleeding risk during anticoagulation, such as aspirin, nonsteroidal anti-inflammatory drugs (NSAIDs), or even steroids on top of warfarin, and "alcohol" refers to alcohol abuse. (new recommendation) Risk of bleeding as follow: see chart HAS-BLED score 0 1 2 3 n 798 1286 744 187 Bleeds, n 9 13 14 7
22
10 REVASCULARISATION PROCEDURES Surgical procedures in stroke management may be classified to procedures performed to prevent first stroke occurrence (primary prevention in asymptomatic patients) or following a stroke event (secondary prevention). PRIMARY PREVENTION Carotid endarterectomy (CEA) has been compared to conservative medical therapy for asymptomatic patients without prior history of TIA or stroke but for whom imaging of the carotid arteries has revealed a definite stenosis. There have been 5 published randomized studies but only 2 are sufficiently powered to detect outcomes between surgery and conservative approach. The absolute 5-year risk reduction for patients with 70-99% carotid artery stenosis (by ultrasound) was 5.4% in the recent follow-up of the ACST trial,1 which was consistent with the ACAS study2 from North America (5.9% absolute 5-year risk reduction). This translates into 1% annual stroke rate reduction. Patients who are asymptomatic and receiving appropriate medical therapy face only a 2% annual stroke rate without CEA. Surgical morbidity and mortality often exceed this beneficial risk reduction. In the ACST and ACAS trials, surgery-related events was 3.1% and 2.3% respectively.1-2 In an unselected patient group undergoing CEA in a centre without proper auditing of the surgeons or centres operative records, the complications are likely to outweigh the benefits of CEA. Furthermore asymptomatic patients should not be offered CEA if their 5-year probability of dying from unrelated causes are high. Finally, in the NASCET study, nearly 45% of all strokes occurring in patients with asymptomatic stenosis may be attributable to lacunar infarcts or cardioembolism.5 Recommendation: Endarterectomy may be considered in patients with high-grade asymptomatic carotid stenosis (70-99%) when performed by a surgeon with less than 3% morbidity / mortality rate. (Level I) Careful patient selection, guided by comorbid conditions, life expectancy, and patient preference, followed by a thorough discussion of the risks and benefits of the procedure is required. It is important that asymptomatic patients receive appropriate medical treatment and be fully evaluated for other treatable causes of stroke.
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SECONDARY PREVENTION 2 large randomized trials (NASCET and ECST) have compared the outcomes of patients with recent cerebrovascular symptoms treated conservatively or with carotid endarterectomy.10-11 Long term follow-up and a meta-analysis is available for these trials.12 Standardizing for the same measurements and definitions yielded highly consistent results among all 3 trials. In general, CEA is highly beneficial for patients with carotid stenosis 70-99% producing a 16% absolute 5-year risk reduction (ARR). For patients with 50-69% stenosis, the 5-year ARR was 4.6%. No benefit was observed for patients with milder degrees of stenosis. Subgroup analyses revealed that benefit in surgery was greatest in men, aged 75 years or older, and those randomized within 2 weeks of their stroke event. The studies excluded patients with medical co-morbidities, previous neck irradiation, recurrent stenosis following previous endarterectomy. Extracranial-intracranial anastomosis between the superficial temporal and middle cerebral arteries (EC-IC Bypass) has not been shown to be beneficial for secondary stroke prevention by the EC/IC Bypass Study Group. Recommendations: CEA is indicated for patients with carotid stenosis of 70-99% without a severe neurological deficit with recent ischaemic events (less than 180 days) in centres with a perioperative complications (Level I) rate for all strokes and deaths of less than 6%. Early CEA is indicated for patients with carotid stenosis of 70-99% without a severe neurological deficit within 2 weeks of recent ischaemic events in centres with a perioperative complications rate for all strokes and deaths of less than 6%. (Level II-1) CEA may be indicated for patients with carotid stenosis of 50-69% without a severe neurological deficit with recent ischaemic events (less than 180 days) in centres with a perioperative complications rate for all strokes and deaths of less than 6%. (Level III) CEA is not recommended for patients with carotid stenosis less than 50%. (Level I)
CEA should not be performed in centres not exhibiting low complications rates similar to those seen with NASCET or ECST. (Level I) Patients should remain on antithrombotic therapy before and after surgery. EC/IC Bypass is not recommended for secondary stroke prevention. (Level II-2) (Level I)
ANGIOPLASTY OR STENTING This is a rapidly evolving field in stroke treatment and prevention. Several randomized trials have compared extra-cranial carotid angioplasty and stenting (CAS) to carotid endarterectomy (CEA).1-5 CAS represents a feasible alternative to carotid endarterectomy for secondary stroke (Level II-2) prevention when surgery is undesirable, technically difficult or inaccessible.6-8
24
In recent studies, the 4 years outcome in death, stroke and myocardial infarction were similar in CAS and CEA. However, the periprocedural rate of stroke was higher in the CAS group while the periprocedural rate of myocardial infarction was higher in the CEA group. Selection of patients for either CAS or CEA may require attention to age, with younger patients having a slightly better outcome with CAS and older patients having a better outcome with CEA.15,16,17 (new recommendation) The criteria needed for a centre to do CAS must be: (new recommendation) 1) highly qualified surgeons and interventionists 2) surgeons and interventionists that are credentialed 3) must use distal embolic protection device 4) use of dual antiplatelet therapy after CAS for at least 4 weeks Intracranial artery stenting (IAS) is also technically feasible but has also not been proven as an established treatment modality. Re-stenosis rate up to 30% have been reported.16 The clinical data has much less evidence with more controversy compared to carotid angioplasty.17-18 The role of CAS in intra-cranial stenoses, asymptomatic stenoses and acute stroke is unclear and not recommended.9-11 (Level II-2) Recommendations: Careful selection of patients by centers experienced in cerebrovascular disease is recommended. As angioplasty with or without stenting is still an investigational procedure, it should be carried out under appropriate clinical trial protocols. Treatment Carotid Endarterectomy (CEA) Recommendations Indicated for most patients with stenosis of 70-99% after a recent ischaemic event in centres with complication rates of less than 6%.1,2 Earlier intervention (within 2 weeks) is more beneficial. May be indicated for patients with stenosis of 50-69% after a recent ischaemic event in centres with complication rates of less than 6%. CEA is not recommended for patients with stenosis of less than 50%. Patients should remain on antiplatelet therapy before and after surgery. Carotid CAS represents a feasible alternative to carotid angioplasty and endarterectomy for secondary stroke prevention when stenting (CAS) surgery is undesirable, technically difficult or inaccessible. Distal protection devices should be used during the procedure. Use of dual antiplatelet for at least 4 weeks after CAS. (new recommendation) The long term safety (for 4 years) for CAS is as good as CEA. (new recommendation) Intracranial angioplasty & stenting (IAS) Role of IAS in intra-cranial stenoses, asymptomatic stenoses and acute stroke is unclear and not recommended.
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II-1 III
B C
I II-2 II-2
A B B
I I I II-2
A A A C
11 STROKE IN SPECIAL CIRCUMSTANCES STROKE IN THE YOUNG Stroke is a rare occurrence before the age of 45. Young stroke is usually caused by a variety of conditions which are distinct from degenerative arterial disease. Across a broad range of causes, stroke in the young is associated with better prognosis than in the elderly. Nevertheless, the socioeconomic impact is often substantial. This discussion will cover ischaemic infarction; stroke in childhood will be excluded. Young stroke may be broadly classified into two groups: (i) atherothrombotic disease caused by accelerated atherosclerosis and (ii) non-atherothrombotic stroke. The cause can be identified in approximately half the cases. The list below is not exhaustive. Atherothrombotic Pro-thrombotic states Atherothrombotic Uncommon before age 45, incidence increases with age Classic vascular risk factors present Non atherothrombotic Abnormal blood rheology dehydration, polycythaemia, thrombocythaemia, paraproteinaemia, etc Hypercoaguable states malignancy, pregnancy, oestrogens, hyperhomocysteinaemia, anti-phospholipid antibodies, deficiency protein c, protein s, carrier state of Factor V-Leyden, etc Abnormal cellular components sickle cell disease, leukaemia, etc Atrial fibrillation Valvular lesions PFO (patent foramen ovale), ASA (atrial septal aneurysm), etc see Cardioembolism Trauma, vascular dissection, cystic medial necrosis, fibromuscular dysplasia, hereditary haemorrhagic telangiectasia Vasculitis primary / secondary to infection / drug-related - Primary SLE, PAN, Takayasus (primary) arteritis, granulomatous angiitis - Complication of infection meningitis, syphilis, chicken pox, HIV/AIDS - Drug-related heroin, LSD, cocaine, amphetamines, ephedrine, phenylpropanolamine Migraine Moya-moyas disease Metabolic disorders mitochondrial cytopathies, leukodystrophy (CADASIL), etc
Miscellaneous
26
This condition is associated with a significant mortality ranging from 5 to 30 percent from retrospective studies. Notable for its occurrence in young children and the peri-partum state. Headache, seizures and imaging appearance should alert to this possibility. An increased thrombotic tendency occurs in low-flow states (including dehydration), hypercoagulable states (primary and secondary) as well as abnormalities of the vessel wall caused by infection, inflammation, trauma or cancer. Often, more than one risk factor is necessary for the development of CVT. Hence, even in the presence of a known risk factor such as pregnancy and dehydration, an underlying cause should be excluded.
Investigation of the Young Stroke I. Identify the cause / predisposing factor A) Search for classical vascular risk factors B) Special diagnostic tests (see section on Investigations) i. Fasting homocysteine ii. Auto-antibody screen, including antiphospholipid antibodies iii. Coagulation screen if indicated: - Serum fibrinogen - Anti-thrombin III - Protein C and Protein S - Factor V-Leyden C) Radiological investigations (see chapter Investigations) Recommendations: Treatment Aspirin Recommendations Young Ischaemic stroke If the cause is not identified, aspirin is usually given. There are currently no guidelines on the appropriate duration of treatment. Cerebral Venous thrombosis Heparin Anticoagulation appears to be safe, and cerebral haemorrhage is not a contra-indication for anticoagulation. Simultaneous oral warfarin should be commenced. The appropriate length of treatment is unknown. Mannitol (0.25 to 0.5 g/kg) intravenously administered over 20 minutes lowers intracranial pressure and can be given every 6 hours. (new recommendation) II-I B III C Level of evidence Grade
Warfarin Mannitol
III III
C C
Endovascular It is currently considered for patients with extensive thrombolysis disease and clinical deterioration.
III
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STROKE AND PREGNANCY Introduction The reported incidence of pregnancy-related stroke varies widely, but probably lies between 11 and 26 deliveries per 100,000.3,4,5,6,7 Although uncommon, stroke is a leading cause of maternal death. The naturally increased risk is compounded by any hypercoagulable state (inherited or acquired), intracranial vascular lesion or arterial hypertension. Pregnancy also imposes additional haemodynamic demands, more so when there is a concomitant cardiac disorder. (new recommendation) Caesarean delivery has been shown to be associated with a 3-12 times increased risk of peripartum and postpartum stroke. 8,9 (new recommendation) I. Ischaemic stroke in pregnancy and the puerperium Any of the causes of ischaemic stroke in the young, including cerebral venous thrombosis (see previous section) may present during pregnancy and the puerperium. In addition, the following causes of ischaemic stroke are peculiar to the pregnant state: a) b) c) d) II. a) b) c) d) peripartum cardiomyopathy amniotic fluid embolism disseminated intravascular coagulation hypotensive emergency borderzone infarction,Sheehans syndrome Haemorrhagic stroke in pregnancy eclampsia hypertension in pregnancy choriocarcinoma rupture of berry aneurysm, arteriovenous or other vascular malformation
Treatment of ischaemic stroke in pregnancy Issues to be considered Risks to both the mother and foetus have to be considered. When there is conflict, the welfare of the mother must take precedence. a) Teratogenicity Aspirin may be used throughout pregnancy. Safety of the other anti-platelet agents has not been established. Warfarin is contraindicated in the first trimester and needs to be substituted with heparin (either unfractionated or low molecular weight heparin, depending on the condition under treatment). Level III, Grade C Risk of bleeding Use of anti-thrombotic treatment needs to be closely coordinated with the obstetrician. Foetal loss Drugs associated with risk of spontaneous abortion and premature labour are to be avoided. Haemorrhagic risk to the newborn Any potential impact on the newborn must be assessed. This is most crucial for anticoagulants. Excretion in breast milk The following drugs may not be used when breast-feeding: - Warfarin, Ticlopidine, Clopidogrel, Dipyridamole
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b) c)
d) e)
12 IMPLEMENTING THE GUIDELINES: (new recommendation) At present there are existing barriers which can create difficulties in applying the recommendations in the CPG including: 1. Poor understanding/limited knowledge of stroke 2. Delay in patient arriving the Emergency Department 3. Inadequate training of the healthcare providers 4. Insufficient resources in the management of Ischemic stroke 5. Poor coordination between primary and secondary/tertiary health care 6. No National database of Stroke for planning of services Therefore in the steps towards implementation of the CPG, there must be strong commitment to: 1. Ensure widespread distribution of the CPG to health care personnel via printed copies, electronic websites, etc. 2. Re-enforce training of health care personnel by regular seminars or workshops to ensure information is made available 3. Develop multidisciplinary teams at hospital and community level to include involvement of rehabilitation clinicians (physiotherapists, occupational therapists, speech & language pathologist), medical social worker, counselor and support from community level (NGOs). Expertise and personnel involved however, depend on the expertise, locality and resources available in the area. 4. Creating a clinical provision pathway linking services of acute management, transfer of care and post-discharged management between hospital and primary care services for better coordination in overall stroke management. 5. Ensure screening and monitoring facilities are available at all sites 6. Ensure availability of the drugs mentioned in the CPG 7. Develop coordinated linkage between specialists and primary health care teams so that referral for further management is readily available 8. Collect a database of stroke for the country 9. Ensure awareness of stroke among public in aspects of primary prevention, early symptoms and services available for stroke survivors in the community. A national surveillance data should be in the future planning. In the meantime clinical audit indicators for quality management were proposed for this CPG are: 1-To initiate deep vein thrombosis (DVT) prophylaxis. 2-To discharge the patients with antithrombotic therapy. 3-To initiate anticoagulation therapy for patients with atrial fibrillation. 4-To administer thrombolytic therapy to eligible patients. 5-To initiate antithrombotic therapy by end of day two upon hospitalization. 6-To discharge the patients with cholesterol reducing medication. 7-To conduct Dysphagia Screening 8-To educate patients on Stroke as a disease. 9-To assessed patients suitability for rehabilitation The above clinical audit indicators for quality management were consolidated into the 9 KPI recommended by Stroke Council, Malaysian Society of Neurosciences which is also being used in Malaysia National Stroke Registry. (Refer Appendix H)
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13 CONCLUSION Over the last decade, major advances have been made in acute management of ischaemic stroke. These advances have occurred along with advances in imaging methods as well as treatments for primary and secondary prevention. Some of the recommendations may be adopted for general use while there are others that may only be used in controlled settings with highly experienced and dedicated teams. Further ongoing studies and clinical trials will better define the usage of agents in terms of identifying particular subgroups of patients who are best suited for certain kinds of therapy based on underlying pathophysiology and cause of stroke. The general care of stroke patients in the ward still plays a vital role in the quest to achieve better outcomes. Many complications can be anticipated and avoided in the acute stroke setting as well as in the rehabilitation period. Basic infrastructure for acute stroke care is already available but reorganization and strengthening of various components such as manpower, training and networking are necessary to enable multidisciplinary inputs to avail early for the patients benefit. Ideally this would be done in the setting of stroke units. There is also urgent need to strengthen all the components of in-hospital and after-discharge care. Research, audit and epidemiological studies are needed to be carried out to know the pattern of illness in our own community, what happens to patients and what kind of support systems are available to them outside the hospital. There are reports of ethnic differences in stroke prevalence as well as risk factor prevalence although the reasons are not fully understood. Clearly there must be impetus to gain information on ethnic and racial differences in stroke incidence, prevalence and vascular risk factors in Malaysia which can have major impact on clinical and public health services on a population level. Finally, of importance is the management of stroke to be recognized as an acute medical emergency and for therapeutic nihilism to be abolished as standard practice. Although not available everywhere, therapeutic options are available in the first few hours after stroke onset. Education of the general population on symptoms of stroke and the urgency to arrive at a hospital for treatment will fundamentally change the outlook for many stroke survivors.
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14 REFERENCES
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7- Acute Treatment
1. 2. 3. 4. 5. 6. 7. Hacke Wet al. Intravenous thrombolysis with recombinant tissue plasminogen activator for acute hemispheric stroke: the European Cooperative Acute Stroke Study (ECASS).JAMA, 1995;274:1017-1025. The National Institute of Neurological Disorders and Stroke rt-PA Stroke Study Group. Tissue plasminogen activator for acute ischemic stroke, England J Med.1995;333:1581-1587 Hacke et al. Randomised double blind placebo controlled trial of thrombolytic therapy with alteplase in acute ischemic stroke ( ECASS II ): European Australasian Acute Stroke Study Investigators. Lancet 1998;352:1245-1251 Clark WM et al. Recombinant tissue type plasminogen activator (alteplase) for ischemic stroke 3 to 5 hours after symptom onse :the ATLANTIS study: a randomized controlled trial. JAMA. 1999;282:2019-2026 Warlow C, Warlaw J. Therapeutic thrombolysis for acute ischaemic stroke.BMJ 2003;326:233-234 Hommel et al. Termination of trial of Streptokinase for acute ischemic stroke: MAST Study Group. Lancet, 1995;345-57 Hacke W, Kaste M, Bluhmki E, Brozman M, Davalos A, Guidetti D, Larrue V, Lees KR, Medeghri Z, Machnig T, Schneider D, von Kummer R, Wahlgren N, Toni D; ECASS Investigators. Thrombolysis with alteplase 3 to 4.5 hours after acute ischemic stroke. N Engl J Med 2008;359:1317-29. Diserens K, Michel P, Bogousslavsky J. Early Mobilization after stroke. A review of literature. Cerebrovasc Dis. 2006; 22 (2-3): 183-90 Bernhardt J, Thury MNT, Collier JM, Legg LA. Very early versus delayed mobilization after stroke.2009. Cochrane Review. Issue 1 Adams HP Jr, del Zoppo G, Alberts MJ, et al. Guidelines for the early management of adults with ischemic stroke: a guideline from the American Heart Association/ American Stroke Association Stroke Council, Clinical Cardiology Council, Cardiovascular Radiology and Intervention Council, and the Atherosclerotic Peripheral Vascular Disease and Quality of Care Outcomes in Research Interdisciplinary Working Groups: the American Academy of Neurology afrms the value of this guideline as an educational tool for neurologists [published corrections appear in. Stroke 2007;38:1655e711. e38 and 2007;38:e96. Gobin YP, Starkman S, Duckwiler GR, et al. MERCI 1: a phase 1 study of Mechanical Embolus Removal in Cerebral Ischemia. Stroke 2004;35:2848e54. Smith WS, Sung G, Saver J, et al. Multi MERCI Investigators. Mechanical thrombectomy for acute ischemic stroke: nal results of the Multi MERCI trial. Stroke 2008;39:1205e12. Phatouros CC, Higashida RT, Malek AM, et al. Endovascular stenting of an acutely thrombosed basilar artery: technical case report and review of the literature. Neurosurgery 1999;44:667e73. The Penumbra Pivotal Stroke Trial Investigators. The Penumbra Pivotal Stroke Trial: Safety and Effectiveness of a New Generation of Mechanical Devices for Clot Removal in Intracranial Large Vessel Occlusive Disease. Stroke. 2009;40:2761-2768.
8. 9. 10.
Stroke unit 1. Stroke Unit Trialists Collaboration. A collaborative systemic review of the randomized trials of organized inpatient (stroke unit) care after first stroke. BMJ 1997;314: 1151-59 2. Indredavik B et al. Benefit of a Stroke Unit; A Randomised Controlled Trial. Stroke 1997;22(8):1026-1031 3. Langhorne P et al. Do stroke units save lives? Lancet 1993;342:395-398 4. Jgrensen HS et al. The effects of a stroke unit: Reductions in mortality, discharge rate to nursing home, length of hospital stay, and cost. Stroke 1995;26(7):1178-1182 5. Indredavik B et al. Longterm effect of treatment in a stroke unit. Stroke 1997;28:1861-1866 6. Indredavik B et al. 10 years follow up after stroke unit treatment. Stroke 1999;30:1524-1527 7. Karla L et al. Alternative strategies for stroke care: a prospective randomized controlled trial. Lancet 2000;356:894-899 8. Jgensen HS et al. Who benefit from treatment and rehabilitation in a stroke unit? A community based study. Stroke 2000; 31:434-439 9. Evan A et al. Can difference in management process explain different outcomes between stroke unit and stroke team care? Lancet 2001;358:1586-1592 General Management 1. Adams HP, Adams RJ, Brott T, Zoppo GJ, Furlan A, Goldstein LB et al. Guidelines for the early management of patients with ischaemic stroke: a scientific statement from thr stroke council of the American Stroke Association. Stroke 2003; 34:1056-1082. 2. Krieger D, Hacke W. The intensive care of the stroke patient. In: Barnett HJM, et al, eds. Stroke: Pathophysiology, Diagnosis and Management. 3rd ed. New York: Churchill Livingstone; 1998. 3. Grotta J, Pasteur W, Khwaja G, Hamel T, Fisher M, Ramirez A. Elective intubation for neurologic deterioration after stroke. Neurology. 1995; 45: 640644. 4. Adams HP Jr. Management of patients with acute ischaemic stroke. Drugs. 1997; 54 (suppl 3): 6069. 5. Treib J, Grauer MT, Woessner R, Morgenthaler M. Treatment of stroke on an intensive stroke unit: a novel concept. Intensive Care Med. 2000; 26: 15981611. 6. Langhorne P. Measures to improve recovery in the acute phase of stroke. Cerebrovasc Dis. 1999; 9 (suppl 5): 25. 7. BB Hamidon, AA Raymond. Risk Factors and Complications of acute ischaemic stroke patients at HUKM. Malaysian Med J Malaysia 2003 ; 58:307-313 8. Linn SL, Granat MH, Lees KR. Prevention of shoulder subluxation after stroke with electrical stimulation. Stroke. 1999; 30: 963968. 9. Tutuarima JA, van der Meulen JH, de Haan RJ, van Straten A, Limburg M. Risk factors for falls of hospitalized stroke patients. Stroke. 1997; 28: 297301. 10. Brott T, Lu M, Kothari R, et al. Hypertension and its treatment in the NINDS rt-PA Stroke Trial. Stroke. 1998; 29: 15041509. 11. Powers WJ, Acute hypertension after stroke:the scientific basis for treatment decisions. Neurology 1993; 43:461-467. 12. Grossman E, Messerli FH, Grodzicki T, Kowey P. Should a moratorium be placed on sublingual nifedipine capsules given for hypertensive emergencies and pseudoemergencies? JAMA. 1996; 276: 13281331. 13. BB Hamidon, AA Raymond. The impact of diabetes mellitus on in-hospital stroke mortality. J Postgrad Med 2003; 49:306-308 14. Scott JF, Robinson GM, French JM, OConnel JE, Alberti KG, Gray CS. Glucose Potassium Insulin Infusions in the treatment of acute stroke patients with mild to moderate hyperglycaemia. Stroke 1999; 30:793-799 15. Robbins J. The evolution of swallowing neuroanatomy and physiology in humans: a practical perspective. Ann Neurol. 1999; 46: 279280. 16. The FOOD Trial Collaboration. Lancet 2005: 365: 764-72 17. Addington WR, Stephens RE, Gilliland K, Rodriguez M. Assessing the laryngeal cough reflex and the risk of developing pneumonia after stroke. Arch Phys Med Rehabil. 1999; 80: 150154. 18. Wijdicks EF, McMahon MM. Percutaneous endoscopic gastronomy after acute stroke: complications and outcome. Cerebrovasc Dis. 1999; 9: 109111. 19. BB Hamidon, AA Raymond, MI Norlinah, SB Jefferelli.The predictors of early infection after an acute ischaemic stroke. Singapore Med J 2003; 44(2):73-76 20. Hajat C, Hajat S, Sharma P. Effects of post-stroke pyrexia on stroke outcome: a meta-analysis of studies in stroke patients. Stroke. 2000; 31: 410414.
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Wang Y, Lim LL, Levi C, Heller RF, Fisher J. Influence of admission body temperature on stroke mortality. Stroke. 2000; 31: 404409. Gujjar AR, Deibert E, Manno EM, Duff S, Diringer MN. Mechanical ventilation for ischemic stroke and intracerebral hemorrhage: indications, timing, and outcome. Neurology. 1998; 51: 447451. Manno EM, Adams RE, Derdeyn CP, Powers WJ, Diringer MN. The effects of mannitol on cerebral oedema after large hemispheric cerebral infarct. Neurology. 1999; 52: 583587. Schwab S, Steiner T, Aschoff A, et al. Early hemicraniectomy in patients with complete middle cerebral artery infarction. Stroke. 1998; 29: 18881893. Sakai K, Iwahashi K, Terada K, Gohda Y, Sakurai M, Matsumoto Y. Outcome after external decompression for massive cerebral infarction. Neurol Med Chir. 1998; 38: 131135. Mori K, Ishimaru S, Maeda M. Unco-parahippocampectomy for direct surgical treatment of downward transtentorial herniation. Acta Neurochir. 1998; 140: 12391244. Hornig CR, Rust DS, Busse O, Jauss M, Laun A. Space-occupying cerebellar infarction: clinical course and prognosis. Stroke. 1994; 25: 372374. Cho DY, Chen TC, Lee HC. Ultra-early decompressive craniectomy for malignant middle cerebral artery infarction : Surgical Neurology 2003; 60: 227 232
8- Prevention
Primary prevention 1. Brown RD, Whisnant JP, Sicks JD, et al. Stroke incidence, prevalence, and survival: secular trends in Rochester, Minnesota, through 1989. Stroke. 1996;27:373380. 2. Wolf PA, DAgostino RB, ONeal MA, et al. Secular trends in stroke incidence and mortality: the Framingham Study. Stroke. 1992;23: 3. 15511555. 4. Sacco RL, Boden-Albala B, Gan R, et al. Stroke incidence among white, black, and Hispanic residents of an urban community: the northern Manhattan Stroke Study. Am J Epidemiol. 1998;147:259 268. 5. Kittner SJ, Stern BJ, Feeser BR, et al. Pregnancy and the risk of stroke. N Engl J Med. 1996;335:768 774. 6. Qureshi AI, Giles WH, Croft JB, et al. Number of pregnancies and risk for stroke and stroke subtypes. Arch Neurol. 1997;54:203206. 7. Mosca L, Manson JE, Sutherland SE, et al. Cardiovascular disease in women: a statement for healthcare professionals from the American Heart Association Writing Group. Circulation. 1997;96:2468 2482. 8. Welin L, Svardsudd K, Wilhelmsen L, et al. Analysis of risk factors for stroke in a cohort of men born in 1913. N Engl J Med. 1987;317: 9. 521526. 10. Kiely DK, Wolf PA, Cupples LA, et al. Familial aggregation of stroke: the Framingham Study. Stroke. 1993;24:1366 1371. 11. Ridker PM, Cook NR, Lee IM, et al. A randomized trial of low dose aspirin in the primary prevention of cardiovascular disease in women. N Engl J Med. 2005 ;352: 1293304. 12. Wolf PA. Cerebrovascular risk. In: Izzo JL Jr, Black HR, Goodfriend TL, et al. Hypertension Primer: The Essentials of High Blood Pressure. Baltimore, Md: Lippincott Williams & Wilkins; 1999. 13. Joint National Committee. The sixth report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Arch Intern Med. 1997;157:24132446. 14. Staessen JA, Fagard R, Thijs L et al. Randomised double-blind comparison of placebo and active treatment for older patients with isolated systolic hypertension .The Lancet; 1997;350: 757-764 15. The ALLHAT group. JAMA. 2002; 283(15): 1967-75 16. SHEP Reseach Group. JAMA. 1991; 265(24): 3255-64 17. Dahlof B, Devereux RB, Kjeldsen SB et. al. Cardiovascular morbidity and mortality in the Losartan intervention for endpoint reduction in hypertension study (LIFE): A rendomised trial against atenolol. Lancet. 2002 359: 1004-10 18. The Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure JNC 7). 19. American Diabetes Association Clinical Practice Recommendations 2006. Diabetes Care. Vol21 Suppl 1. 20. Wolf PA, DAgostino RB, ONeal MA, et al. Secular trends in stroke incidence and mortality: the Framingham Study. Stroke. 1992;23: 21. elkind et. al. stroke vol37 jan2006, 22. kammersgaard et.al. cerebro vasc disease: vol 21: 2005 23. Risks and benefits of Estrogen plus Progestin in healthy Postmenopausal Women. JAMA. 2002; 266: 321-333 24. Brown SA et. al. Arterioscler Thromb 1993; 13: 1558-66 25. Tuomilehto J, Rastenyte D. Diabetes and glucose intolerance as risk factors for stroke. J Cardiovasc Risk. 1999;6:241249. 26. Stamler J, Vaccaro O, Neaton J et. al. Multiple Risk Factor Intervention Trial Research Group. (1993) Diabetes, other risk factors and cardiovascular mortality for men screened in the Multiple Risk Factor Intervention Trial. Diabetes Care (16): 434-444 27. Scandinavian Simvastatin Survival Study Group. Randomised trial of cholesterol lowering in 4444 patients with coronary heart disease: the Scandinavian Simvastatin Survival Study (4S). Lancet. 1994;344: 13831389. 28. Heart Protection Study Collaborative Group. Lancet 2004. 363: 757-67 29. Lawes CMM, Bennett DA, Feigin VL, Rodgers A. Blood pressure and stroke. An overview of published reviews. Stroke 2004; 35: 776 785 30. Staessen JA. Brikenhager WH. Evidence that the new antihypertensives are superior to older drugs. Lancet 2005; 366; 869-71 31. Verdecchia P, Reboldi G, Angeli F, Gattobigio R, Bentivoglio M, thijs L, Staessen JA, Porcellati C. angiotensin-converting-enzyme (ACE) inhibitors and calcium channel blockers (CCBs) for coronary heart disease and stroke prevention. Hypertension 2005: 46: 386-392 32. Trenkwalder P, Elmfeldt D, Hofman A, Lithell H, Olofsson B, Padametriou V, Skoog I, Zanchetti A. The study on cognition and prognosis in the elderly (SCOPE) major cardiovascular events and stroke in subgroups of patients. Blood Pressure 2005: 14; 31-37 33. Randomized Evaluation of Long-term anticoagulant therapy, Connolly SJ., et al. N Engl J Med 2009;361:1139-1151. 34. The Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure: The JNC 7 Report. JAMA. 2003;289(19):2560-2571
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Secondary Prevention Warlow CP, Dennis MS, Van Gijn et. al. Preventing recurrent stroke and other serious vascular events. In: Stroke: a practical guide to 1. management. Oxford: Blackwell Science, 2001:653-672. Huan Li, Wong KS Long term mortality and recurrent stroke risk among Chinese stroke patients with predominantly intracranial atheroscle2. rosis Stroke 2003;34:2361-2366. Antithrombotic Trialists Collaboration. Collaborative meta-analysis of randomized clinical trials of anti-platelet therapy for prevention of 3. death, myocardial infarction and stroke in high risk patients. BMJ 2002; 324:71-86. The International Stroke Trial (IST): a randomised trial of aspirin, subcutaneous heparin, both, or neither among 19435 patients with acute 4. ischaemic stroke. International Stroke Trial Collaborative Group. Lancet 1997;349: 1569-81. CAST: randomised placebo-controlled trial of early aspirin use in 20,000 patients with acute ischaemic stroke. CAST (Chinese Acute 5. Stroke Trial) Collaborative Group. Lancet 1997;349:1641-9. Chen ZM, Sandercock P, Pan HC, et al. Indications for early aspirin use in acute ischemic stroke: A combined analysis of 40000 6. randomized patients from the Chinese acute stroke trial and the international stroke trial. On behalf of the CAST and IST collaborative groups. Stroke 2000;31:1240-9. 7. Dutch TIA Trial Study Group: A comparison of two doses of aspirin (30 mg vs 283 mg a day) in patients after a transient ischemic attack or a minor ischemic stroke N Engl J Med 1991; 325: 1261-1266. 8. Algra A, van Gijn: Aspirin at any dose above 30 mg offers only modest protection after cerebral ischaemia J Neurol Neurosurg Psychiatry 1996;60:197-199. 9. Farrell B, Goodwin J, Richards S, Warlow C. The United Kingdom transient ischaemic attack (UK-TIA) aspirin trial:Final results. J Neurol Neurosurg Psychiatry 1991;54:1044-1054. 10. Gent M, Blakely JA, Easton JD, Ellis DJ, Hachinski VC, Harbison JW, Panak E, Roberts RS, Sicurella J, Turpie AG The Canadian American Ticlopidine Study(CATS) in thromboembolic stroke. Lancet. 1989 June 3:1215-20. 11. Goyan JE. The trials of a long term clinical trial: The ticlopidine aspirin stroke study and the Canadian American Ticlopidine Study. Control Clin Trials.1989 Dec; 10( Suppl 4):S236-S244. 12. CAPRIE steering committee. A randomized, blinded trial of clopidogrel versus aspirin in patients at risk of ischaemic events (CAPRIE). Lancet 1996;348:1329-1339. 13. Ringleb PA, Bhatt DL, Hirsch AT, Topol EJ, Hacke W. Benefit of clopidogrel over aspirin is amplified in patients with a history of ischemic events. Stroke.2004 Feb;35(2):528-32. 14. Guidelines for Management of Ischaemic Stroke and Transient Ischaemic Attack 2009. Website accessed; http://www.eso-stroke.org. 18th January 2011. 15. Shinohara Y, Katayama Y, Uchiyama S, et al, for the CSPS 2 group. Cilostazol for prevention of secondary stroke (CSPS 2): an aspirin controlled, double blind, randomized non inferiority trial. Lancet Neurology 2010;9:959-68. 16. Diener H, Cunha L, Forbes C, Silvenius J, Smets P, Lowenthal A European stroke prevention study 2, dipyridamole and acetylsalicylic acid in the secondary prevention of stroke J Neurol Sci 1996; 143: 1-13. 17. HC Diener, Bogousslavsky J, Brass LM, Cimminiello C, Csiba L, Kaste M, Leys D, Matias-Guiu J, Rupprecht H on behalf of the MATCH investigators. Aspirin and clopidogrel compared with clopidogrel alone after recent ischaemic stroke or transient ischaemic attack in high risk patients (MATCH): randomized, double blind, placebo-controlled trial Lancet 2004;364:331-37. 18. Mohr JP, Thompson JLP, Lazar RM, et al for the WARSS Study Group. New Eng J Med 2001;345:1444-1445. 19. Chimowitz MI, Lynn MJ, Howlett-Smith H, et al. for the WASID Trial Investigators. New Eng J Med 2005;352:1305-1316. 20. Gueyffier F, Boissel JP, Boutitie F, et.al. Effect of antihypertensive treatment in patients having already suffered from stroke. Gathering the evidence. The INDANA Project Collaborators. Stroke 1997;28:2557-62. 21. Lawes CCM, Bennett Da, Feigin VL, Rodgers A. blood pressure and stroke: an overview of published reviews. Stroke 2004; 35: 776 785. 22. PROGRESS Collaborative Group:Randomized trial of a perindropril-based blood pressure lowering regiment among 6105 individuals with previous stroke or transient ischaemic attack Lancet 2001;358:1033-1041. 23. Lindholm LH, Ibsen H, Dahlof B, Devereux RB, Beevers RB, de Faire U, Fyhrquist F et. al. Cardiovascular morbidity and mortality in patients with diabetes in the Losartan Intervention for endpoint reduction in hypertension study(LIFE): a randomized trial against atenolol. Lancet 2002;359:1004-1010. 24. Heart Outcomes Prevention Evaluation study investigators. Effects of an angiotensin-convertingenzyme inhibitor, ramipril, on cardiovascular events in high-risk patients. N Engl J Med 2000;342:145-53. 25. Jikei Heart Study Group. Valsartan in a Japanese population with hypertension and other cardiovascular disease: a randomised, open -label, blinded endpoint morbidity-mortality study. Lancet 2007;369:1431-1439. 26. The ONTARGET Investigators. Telmisartan, Ramipril, or Both in Patients at High Risk for Vascular Events. N Engl J Med 2008;358:1547-59. 27. American Heart Association Guidelines on Prevention of Stroke in patients with Ischaemic stroke or TIA. Stroke 2006; 37: 577-617. 28. Prospective Studies Collaboration Cholesterol, diastolic blood pressure and stroke 13,000 strokes in 450,000 people in 45 prospective cohorts Lancet 1995; 346: 1647-1653. 29. Heart Protection Study Collaborative Group. MRC/BHF Heart Protection Study of cholesterol lowering with simvastatin in 20536 high-risk individuals: a randomized placebo-controlled trial. Lancet 2002;360:7-22. 30. UK Prospective Diabetes Study (UKPDS) Group Intensive blood-glucose control with sulphonylureas or insulin compared with conventional treatment and risk complications in patients with type 2 diabetes (UKPDS 33) Lancet 1998;352:837-853. 31. Connolly SJ, Ezekowitz MD, Yusuf S, et al. Dabigatran versus warfarin in patients with atrial fibrillation. N Eng J Med 2009;361:1139-51. 32. Patel MR, Mahaffey KW, Grag J, et al. Rivaroxaban versus warfarin in nonvalvular atrial fibrillation. N Eng J Med 2011;365:883-91. 33. Granger CB, Alexander JH, McMurray JJV, et al. Apixaban versus warfarin in patients with atrial fibrillation. N Eng J Med 2011. DOI: 10.1056/NEJMoa1107039.
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9- Cardioembolism
1. 2. 3. 4. 5. 6. 7. 8. 9. 10. 11. 6 ACCP Consensus Conference on Antithrombotic Therapy (co-chairs: J Dalen, J Hirsch, G Guyatt) CHEST 119/1 (Suppl.) Jan 2001 ABC of antithrombotic therapy (eds GY Lip, A Blann) BMJ Publishing (London) 2003 Guidelines for the early management of patients with ischemic stroke. A scientific statement from the stroke council of the American Stroke Association. (Adams HP, chair). Stroke 2003;34:1056-1083. McNamara RL, Lima AC, Whelton PK, Pore NR. Ecocardiographic identification of cardiovascular sources of emboli to guide clinical management of stroke: A cost-effectiveness analysis. Ann Intern Med 1997;127:775-787. Lip GYH. Thromboprophylaxis for atrial fibrillation. Lancet 1999;353:4-6. Bonow RO, Carobello D, de Leon AC, et al. ACC/AHA guidelines for the management of patients with valvular heart disease. J Am Coll Cardiol 1998;32:1486-8. Lip GYH, Frison L, Halperin JL, et al. Comparative validation of a novel risk score for predicting bleeding risk in anticoagulated patients with atrial fibrillation. J Am Coll Cardiol 2011; 57:173-80. Pisters R, Lane DA, Nieuwelaat R, et al. A novel, user-friendly score (HAS-BLED) to assess one-year risk of major bleeding in atrial fibrillation patients: The Euro Heart Survey. Chest 2010; 138:1093-100. Connolly SJ, Ezekowitz MD, Yusof S, et al. Dabigatran versus warfarin in patients with atrial fibrillation. N Eng J Med 2009; 361:1139-51. Patel MR. Mahaffey KW, Grag J et al. Rivaroxaban versus warfarin in nonvalvular atrial fibrillation. N Eng J Med 2011; 365:883-91. Granger CB, Alexander JH, McMurray JJV, et al. Apixaban versus warfarin in patients with atrial fibrillation. N Eng J Med 2011. DOI: 10.1056/NEJMoa1107039.
th
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APPENDIX A Oxfordshire Community Stroke Project Classification (OCSP) Total Anterior Circulation Stroke (TAC) All of Hemiplegia contralateral to the cerebral lesion, usually with ipsilateral hemisensory loss Hemianopia contralateral to cerebral lesion New disturbance of higher cerebral function (dysphasia, visuospatial) Pathological definition Occlusion of a single deep (LS) perforating artery 5% can be due to haemorrhage Occurs at strategic sites More likely seen on MRI than CT scan Classical lacunar syndromes correlated with relevant lacunes at autopsy Motor / sensory deficit + hemianopia Motor/sensory deficit + new higher cerebral dysfunction New higher cerebral dysfunction + hemianopia New higher cerebral dysfunction alone A pure motor/sensory deficit less extensive than for LAC (eg. confined to one limb, or to face and hand but not to whole arm) Ipsilateral cranial nerve palsy (single / multiple) with contralateral motor and/or sensory deficit Bilateral motor and/or sensory deficit Disorder of conjugate eye movement (horizontal/vertical) Cerebellar dysfunction without ipsilateral long tract sign Isolated hemianopia or cortical blindness
Any of
Any of
Other signs include Horners sign, nystagmus, dysarthria, hearing loss, etc Code last letter as follows: (S) (I) (H) Syndrome: Indeterminate pathogenesis, prior to imaging (e.g. TACS) Infarct (e.g., TACI) Haemorrhage (e.g., TACH)
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ISCHAEMIC STROKE
EMBOLISM
OTHER CAUSES
HYPOPERFUSION
CARDIOGENIC Atrial fibrillation Valve disease Ventricular thrombi PFO and ASA Intracardiac tumour
INTRACRANIAL
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Ischaemic Stroke
infarction
Airway, Breathing, Circulation Hydration Blood Pressure monitoring Neurological Status monitoring Anticipate & treat complications Begin Rehabilitation
Multidisciplinary Team Approach Proper Positioning Early mobilization Physiotherapy Occupational therapy Speech therapy Treat spasticity Treat depression
Neurorehabilitation
Education
Patient & Caregiver
Antiplatelet therapy Treat risk factors Treat specific underlying cause Therapeutic lifestyle modification (new recommendation)
Secondary Prevention
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APPENDIX D Therapeutic Agents Available in Malaysia Anti-platelets Cyclo-oxygenase inhibitors Acetylsalicylic acid (Aspirin) Triflusal (new) Adenosine Diphosphate Receptor Antagonists Ticlopidine Clopidogrel Other Antiplatelet Agents - Dipyridamole - Cilostazol (new)
Anticoagulants IV
Unfractionated Heparin (UFH) Heparin Low Molecular Weight Heparin (LMWH) Nadroparin Enoxaparin Fondaparinux
Oral Thrombolytics
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CHA2DS2VASc score and stroke rate (a) Risk factor for stroke and thrombo-embolism in non-valvular AF
Major risk factors Previous stroke, TIA, or systemic embolism Age 75 years Clinically relevant non-major risk factors Heart failure of moderate to severe LV systolic dysfunction (e.g. LV EF 40%) Hypertension - Diabetes mellitus Female sex - Age 65-74 years Vascular diseasea
(b) Risk factor-based approach expressed as a point based scoring system, with the acronym CHA2DS2VASc
(Note: maximum score is 9 since age may contribute 0, 1, or 2 ponits) Score 1 1 2 1 2 1 1 1 9 Patients (n=7329) 1 422 1230 1730 1718 1159 679 294 82 14 Adjusted stroke rate (%/yearb) 0% 1.3% 2.2% 3.2% 4.0% 6.7% 9.8% 9.6% 6.7% 15.2% Risk factors Congestive heart failure/LV dysfunction Hypertension Age 75 Diabetes mellitus Stroke/TIA/thrombo-embolism Vascular diseasea Age 65-74 Sex category (i.e. female sex) Maximum score
See text for definitions. Prior myocardial infarction, peripheral artery disease, aortic plaque. Actual rates of stroke in contemporary cohorts may vary from these estimates. Based on Lip et al.53 AF = atrial brillation; EF = ejection fraction (as documented by echocardiography, radionuclide ventriculography, cardiac catheterization, cardiac magnetic resonance imaging, etc.); LV = left ventricular; TIA = transient ischaemic attack.
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APPENDIX F (new recommendation) Swallowing Test Various water swallowing tests are available; recommended as follow. 1. Kidd Water Test Description: Clinical examination includes pharyngeal sensation assessed by orange stick, tongue and facial movement, speech, sensory and perceptual function and muscle strength also assessed. Ability to swallow also assessed by patient swallowing 50 ml of water in 5 ml allotments. Source: Kidd D, Lawson J, Nesbitt R, MacMahon J. Aspiration in acute stroke: a clinical study with videofluroscopy. Quarterly Journal of Medicine. 1993 86:825-829. 2. Nishiwaki et al. Description: Scores 6 items including lip closure, tongue movement, palatal elevation, gag reflex, voice quality and motor speech function. Also includes a saliva swallowing test. After patient swallows 1 teaspoon of water twice, asked to drink the rest of the water from a cup for a total of 30 ml. Source: Nishiwaki K, Tsuji T, Liu M, Hase K, Tanaka N, Fujiwara T. Identification of a simple screening tool for dysphagia in patients with stroke using factor analysis of multiple dysphagia variables. J Rehabil Med. 2005 Jul;37(4):247-51. 3. CODA Standardized Swallowing Assessment (SSA) Description: Pre-swallowing check list if passed is followed by teaspoon sips of water 3 times, followed by half glassful of water. (Grade A, strong evidence Westergren, 2006). Source: Perry, L. Screening swallowing function of patients with acute stroke. Part one: identification, implementation and initial evaluation of a screening tool for use by nurses. Journal of Clinical Nursing 2001; 10: 463-473.
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APPENDIX G Resources Societies & Associations Malaysian Society of Neurosciences Mailing Address: Level 15, CREST, 3 Two Square, No 2, Jalan 19/1, 46300 Petaling Jaya, Selangor. Website: www.neuro.org.my
NASAM (National Stroke Association of Malaysia) 1. NASAM Headquarters No 12, Jalan 7/2 46050 Petaling Jaya Selangor Darul Ehsan Tel: 03-7956 4840 / 7956 1876 Fax: 03-7956 2275 Email : [email protected] Open : Mon-Fri: 9am - 5pm NASAM Penang No 9, Jesselton Crescent 10350 Pulau Pinang Tel: 04-229 8050 Tel: 04-226 0563 Email : [email protected] Open : Mon-Fri: 10am - 12noon 5. NASAM Ampang No 9, Lorong Awan 1 68000 Ampang Selangor Darul Ehsan Tel: 03-4256 1234 Fax: 03-4256 5360 Email : [email protected] Open : Mon-Fri: 9am - 4pm NASAM Perak No. 9, Lorong Pinji Off Jalan Pasir Puteh 31560 Ipoh, Perak Tel: 05-321 1089 Fax: 05-322 4759 Email : [email protected] Open : Mon-Fri: 9am - 5pm NASAM Kuantan A2134 Lorong Kubang Buaya 2 25250 Kuantan, Pahang Tel/Fax: 09-566 8195 Email : [email protected]
2.
6.
3.
NASAM Johor No 59, Jalan Cendera Serene Park 80300 Johor Bahru, Johor Tel: 07-223 0075 Fax: 07-223 0076 Email : [email protected] NASAM Sabah Kompleks Badan-Badan Sukarela Wisma Pandu Puteri KM4 Jalan Tuaran 88801 Kota Kinabalu Tel: 08-826 1568 Fax: 08-826 8568 Email : [email protected] Open : Mon-Fri: 9am - 5pm
7.
4.
8.
NASAM Malacca 5132-C, Jalan Datuk Palembang Bukit Baru 75150, Melaka Tel/Fax: 06-231 0177 Email : [email protected] Open : Mon-Fri: 10am - 12noon 2pm - 4pm
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9 KPI Recommended by Stroke Council Malaysian Society of Neurosciences (MSN) 2011 (Used in Malaysian National Stroke Registry)
43
7. Limb Ataxia Check finger-nosefinger; heel-shin; and score only if out of proportion to paralysis 8. Sensory Use safety pin. Check grimace or withdrawal if stuporous. Score only stroke-related losses. 9. Best Language Describe cookie jar picture, name objects, read sentences. May use repeating, writing, stereognosis 10. Dysarthria Read list of words 11.Extinction/Neglect Simultaneously touch patient on both hands, show fingers in both visual fields, ask about deficit, left hand.
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0 = No symtoms at all. 1 = No significant disability despite symtoms; Able to carry out all usual duties and activities. 2 = Slight disability; Unable to carry out all previous activities, but able to look after own affairs without assistance. 3 = Moderate disability requiring some help, but able to walk without assistance. 4 = Moderate severe disability; Unable to walk without assistance and unable to attend to own bolidy needs without assistance. 5 = Severe disability; Bedridden, incontinent, and requiring constant nursing care and attention. 6 = Dead.
45
Stroke Resources on World-wide Web 1. 2. National Stroke Foundation www.strokefoundation.com.au Stroke Centre at Washington University www.strokecenter.org American Heart Association www.americanheart.org American Academy of Neurology www.aan.com 5. 6. 7. American Stroke Association www.strokeassociation.org. European Stroke Initiative (EUSI) www.eusi-stroke.com Royal College of Physician www.rcplondon.cu.uk/pubs/books/str oke Stroke Association www.stroke.org.uk
3. 4.
8.
SOURCES OF FUNDING The development of the CPG on Management of Ischaemic Stroke was supported financially by Boehringer Ingelheim (M) Sd. Bhd. DISCLOSURE STATEMENT The panel members had completed disclosure forms. None held shares in pharmaceutical firms or acted as consultants to such firms. (Details are available upon request from the CPG Secretariat)
ACKNOWLEDGEMENTS The chairperson of this guideline would like to express his gratitude and appreciation to the following for their contribution: All members of the work group and the reviewers for their dedication and commitment. Boehringer Ingelheim for providing secretarial support. Health Technology Assessment division of Ministry of Health. Dato Dr Rosli Mohd Ali, Consultant Cardiologist, IJN. Dato Dr Omar Ismail, Consultant Cardiologist, Penang General Hospital. Prof Dr Sim Kui Hian, Consultant Cardiologist, Sarawak General Hospital. Dr Lam Khai Huat, Consultant Cardiologist, Assunta Hospital.
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CLINICAL PRACTICE
GUIDELINES
MANAGEMENT OF ISCHAEMIC STROKE
2nd EDITION AUGUST 2011
MH/P/PAK/235.12(GU)