Aha Guidelines For Stemi
Aha Guidelines For Stemi
Aha Guidelines For Stemi
10-year risk of developing symptomatic CHD should be calculated for all patients with 2 major risk factors to assess the need for primary prevention strategies.
Onset of STEMI
ACC/AHA Guidelines for the Management of Patients with ST-Elevation Myocardial Infarction
Prehospital EMS providers should administer 162 to 325 mg of aspirin (chewed) to chest pain patients suspected of having STEMI unless contraindicated or already taken by the patient. Although some trials have used enteric-coated aspirin for initial dosing, more
Options for Transport of Patients With STEMI and Initial Reperfusion Treatment
Hospital fibrinolysis: Door-to-Needle within 30 min.
EMS on-scene
Encourage 12-lead ECGs. Consider prehospital fibrinolytic if capable and EMS-to-needle within 30 min.
InterHospital Transfer
PCI capable
GOALS
5 min. Patient
8 min.
EMS
EMS Transport
Prehospital fibrinolysis EMS transport EMS-to-needle EMS-to-balloon within 90 min. within 30 min. Patient self-transport Hospital door-to-balloon within 90 min.
Dispatch 1 min.
Options for Transport of Patients With STEMI and Initial Reperfusion Treatment
Patients receiving fibrinolysis should be risk-stratified to identify need for further revascularization with percutaneous coronary intervention (PCI) or coronary artery bypass graft surgery (CABG). All patients should receive late hospital care and secondary prevention of STEMI.
Fibrinolysis Not PCI Capable PCI Capable Noninvasive Risk Stratification Rescue Ischemia driven Late Hospital Care and Secondary Prevention
PCI or CABG
Primary PCI
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Myocarditis
Hyperkalemia Bundle-branch blocks Vasospastic angina Hypertrophic cardiomyopathy
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Chest-wall pain
Pleurisy Peptic ulcer disease Panic attack
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Electrocardiogram
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Electrocardiogram
Show 12-lead ECG results to emergency physician within 10 minutes of ED arrival in all patients with chest discomfort (or anginal equivalent) or other symptoms of STEMI. In patients with inferior STEMI, ECG leads should
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Laboratory Examinations
Laboratory examinations should be performed as part of the management of STEMI patients, but should not delay the implementation of reperfusion therapy. Serum biomarkers for cardiac damage Complete blood count (CBC) with platelets International normalized ratio (INR) Activated partial thromboplastin time (aPTT) Electrolytes and magnesium Blood urea nitrogen (BUN) Creatinine Glucose Complete lipid profile
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Imaging
Patients with STEMI should have a portable chest X-ray, but this should not delay implementation of reperfusion therapy (unless a potential contraindication is suspected, such as aortic dissection). Imaging studies such as a high quality portable chest X-ray, transthoracic and/or transesophageal echocardiography, and a contrast chest CT scan or an MRI scan should be used for differentiating STEMI from aortic dissection in patients for whom this distinction is initially unclear.
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Oxygen
Supplemental oxygen should be administered to patients with arterial oxygen desaturation (SaO2 < 90%).
It is reasonable to administer supplemental oxygen to all patients with uncomplicated STEMI during the first 6 hours.
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Nitroglycerin
Patients with ongoing ischemic discomfort should receive sublingual NTG (0.4 mg) every 5 minutes for a total of 3 doses, after which an assessment should be made about the need for intravenous NTG.
Intravenous NTG is indicated for relief of ongoing ischemic discomfort that responds to nitrate therapy, control of hypertension, or management of pulmonary congestion.
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Nitroglycerin
Nitrates should not be administered to patients with:
systolic pressure < 90 mm Hg or to 30 mm Hg below baseline severe bradycardia (< 50 bpm) tachycardia (> 100 bpm) or suspected RV infarction.
Nitrates should not be administered to patients who have received a phosphodiesterase inhibitor for erectile dysfunction within the last 24 hours (48 hours for tadalafil).
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Analgesia
5 to 15 minute intervals) is the analgesic of choice for management of pain associated with STEMI.
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Aspirin
Aspirin should be chewed by patients who have
not taken aspirin before presentation with STEMI. The initial dose should be 162 mg (Level of Evidence: A) to 325 mg (Level of Evidence: C)
Although some trials have used enteric-coated aspirin for initial dosing, more rapid buccal absorption occurs with nonenteric-coated formulations.
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Beta-Blockers
Oral beta-blocker therapy should be administered promptly to those patients without a contraindication, irrespective of concomitant fibrinolytic therapy or performance of primary PCI.
It is reasonable to administer intravenous betablockers promptly to STEMI patients without contraindications, especially if a tachyarrhythmia or hypertension is present.
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Reperfusion
Given the current literature, it is not possible to say
definitively that a particular reperfusion approach is superior for all pts, in all clinical settings, at all times of day The main point is that some type of reperfusion therapy should be selected for all appropriate pts with suspected STEMI The appropriate & timely use of some reperfusion therapy is likely more important than the choice of therapy
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Reperfusion
The medical system goal is to facilitate rapid recognition and treatment of patients with STEMI such that door-toneedle (or medical contactto-needle) time for initiation of fibrinolytic therapy can be achieved within 30 minutes or that door-to-balloon (or medical contacttoballoon) time for PCI can be kept within 90 minutes.
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Reperfusion
Patient Transport Inhospital Reperfusion
Goals
D-N 30 min 5 min < 30 min D-B 90 min
Prehospital ECG MI protocol Critical pathway Bolus lytics Quality Greater use of improvement Dedicated 9-1-1 PCI team program Prehospital Rx
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Symptom Recognition
PreHospital
ED
Cath Lab
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Reperfusion Options for STEMI Patients Step One: Assess Time and Risk.
Risk of STEMI
Risk of Fibrinolysis
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Fibrinolysis
In the absence of contraindications, fibrinolytic therapy should be administered to STEMI patients with symptom onset within the prior 12 hours. In the absence of contraindications, fibrinolytic therapy should be administered to STEMI patients with symptom onset within the prior 12 hours and new or presumably new left bundle branch block (LBBB).
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Fibrinolysis
In the absence of contraindications, it is reasonable to administer fibrinolytic therapy to STEMI patients with symptom onset within the prior 12 hours and 12-lead ECG findings consistent with a true posterior MI. In the absence of contraindications, it is reasonable to administer fibrinolytic therapy to patients with symptoms of STEMI beginning in the prior 12 to 24 hours who have continuing ischemic symptoms and ST elevation > 0.1 mV in 2 contiguous precordial leads or 2 adjacent limb leads.
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Fibrinolysis
Fibrinolytic therapy should not be administered to asymptomatic patients whose initial symptoms of STEMI began more than 24 hours earlier. Fibrinolytic therapy should not be administered to patients whose 12-lead ECG shows only ST-
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Primary PCI should be performed in patients with severe congestive heart failure (CHF) and/or pulmonary edema (Killip class 3) and onset of symptoms within 12 hours.
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Rescue PCI
Rescue PCI should be performed in patients less than 75 years old with ST elevation or LBBB who develop shock within 36 hours of MI and are suitable for revascularization that can be performed within 18 hours of shock.
Rescue PCI should be performed in patients with severe CHF and/or pulmonary edema (Killip class 3) and onset of symptoms within 12 hours.
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Rescue PCI
Rescue PCI is reasonable for selected patients 75 years or older with ST elevation or LBBB or who develop shock within 36 hours of MI and are suitable for revascularization that can be performed within 18 hours of shock. It is reasonable to perform rescue PCI for patients with one or more of the following:
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IABP
PCI IRA
PCI IRA
Staged CABG
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Assessment of Reperfusion
It is reasonable to monitor the pattern of ST elevation, cardiac rhythm and clinical symptoms over the 60 to 180 minutes after initiation of fibrinolytic therapy. Noninvasive findings suggestive of reperfusion include: Relief of symptoms Maintenance and restoration of hemodynamic and/or electrical instability Reduction of 50% of the initial ST-segment elevation pattern on follow-up ECG 60 to 90 minutes after initiation of therapy.
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Aspirin
A daily dose of aspirin (initial dose of 162 to 325 mg orally; maintenance dose of 75 to 162
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Thienopyridines
In patients for whom PCI is planned, clopidogrel should be started and continued: 1 month after bare-metal stent 3 months after sirolimus-eluting stent
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Thienopyridines
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Thienopyridines
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An intravenous ACE inhibitor should not be given to patients within the first 24 hours of STEMI because of the risk of hypotension (possible exception: refractory hypotension).
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Hospital Management
ACC/AHA Guidelines for the Management of Patients with ST-Elevation Myocardial Infarction
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Arrhythmia
Administer Furosemide IV 0.5 to 1.0 mg/kg Morphine IV 2 to 4 mg Oxygen/intubation as needed Nitroglycerin SL, then 10 to 20 mcg/min IV if SBP greater than 100 mm Hg Dopamine 5 to 15 mcg/kg per minute IV if SBP 70 to 100 mm Hg and signs/symptoms of shock present Dobutamine 2 to 20 mcg/kg per minute IV if SBP 70 to 100 mm Hg and no signs/symptoms of shock
Bradycardia
Tachycardia
Check Blood Pressure See Section 7.7 in the ACC/AHA Guidelines for Patients With ST-Elevation Myocardial Infarction
Check Blood Pressure Systolic BP Greater than 100 mm Hg and not less than 30 mm Hg below baseline
Nitroglycerin 10 to 20 mcg/min IV
ACE Inhibitors Short-acting agent such as captopril (1 to 6.25 mg) Further diagnostic/therapeutic considerations (should be considered in nonhypovolemic shock) Diagnostic Therapeutic Pulmonary artery catheter Intra-aortic balloon pump Echocardiography Reperfusion/revascularization Angiography for MI/ischemia Additional diagnostic studies
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NPJT
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Arrhythmias During Acute Phase of STEMI: Pump Failure / Excess Sympathetic Tone
Arrhythmia Sinus Tach Afib / Flutter PSVT Treatment Treat cause; beta blocker Treat cause; slow ventricular rate; DC shock Vagal maneuvers; beta blocker, verapamil / diltiazem; DC shock
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Junctional
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Escape Rhythm
Duration of AVB
Mortality Rx
2 - 3 days
Low Observe
Transient
High (CHF, VT) PM (ICD)
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Recommendations for Treatment of Atrioventricular and Intraventricular Conduction Disturbances During STEMI
Atrioventricular Conduction INTRAVENTRICULAR First degree AV block Mobitz I second degree AV block CONDUCTION Normal ANTERIOR MI NON-ANTERIOR ANTERIOR MI NON-ANTERIOR ACTION CLASS ACTION CLASS ACTION CLASS ACTION CLASS ACTION CLASS Normal Observe I Observe I Observe I Observe IIb Observe IIa A III A III A III A* III A III TC III TC IIb TC IIb TC I TC I TV III TV III TV III TV III TV III Observe I Observe IIb Observe IIb Observe IIb Observe IIb Old or New III A III A III A* III A III Fascicular block A IIb TC I TC IIa TC I TC I (LAFB or LPFB) TC TV III TV III TV III TV III TV III Observe I Observe III Observe III Observe III Observe III Old bundle A III A III A III A* III A III branch block TC IIb TC I TC I TC I TC I TV III TV IIb TV IIb TV IIb TV IIb Observe III Observe III Observe III Observe III Observe III New bundle A III A III A III A* III A III branch block TC I TC I TC I TC I TC I TV IIb TV IIa TV IIa TV IIa TV IIa Observe III Observe III Observe III Observe III Observe III Fascicular A III A III A III A* III A III block + RBBB TC I TC I TC I TC I TC I TV IIb TV IIa TV IIa TV IIa TV IIa Observe III Observe III Observe III Observe III Observe III Alternating A III A III A III A* III A III left and right TC IIb TC IIb TC IIb TC IIb TC IIb bundle branch TV I TV I TV I TV I TV I block Mobitz II second degree AV block ANTERIOR MI NON-ANTERIOR ACTION CLASS ACTION CLASS Observe III Observe III A III A III TC I TC I TV IIa TV IIa Observe III Observe III A III A III TC I TC I TV IIa TV IIb Observe III Observe III A III A III TC I TC I TV IIa TV IIa Observe III Observe III A III A III TC IIb TC IIb TV I TV I Observe III Observe III A III A III TC IIb TC IIb TV I TV I Observe III Observe III A III A III TC IIb TC IIb TV I TV I
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EF < 0.30
EF 0.31 - 0.40
EF > 0.40
Yes
+
NEJM 349: 1836,2003
EPS
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YES
ST-segment elevation?
NO
Is Is ischemia ischemia controlled controlled by by escalation escalation of of medical medical therapy? therapy? NO NO
Refer Refer for for urgent urgent catheterization catheterization (consider (consider IABP) IABP)
YES YES
NO NO
Modified from Braunwald. Heart Disease: A Textbook of Cardiovascular Medicine. 6th ed. Philadelphia, PA: WB Saunders Co. Ltd. 2001:1195.
Revascularization Revascularization with with PCI PCI and/or and/or CABG CABG as as dictated dictated by by anatomy anatomy
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Revascularization as Indicated
Pharmacological Stress
Submaximal Symptom Symptom-Limited Adenosine Exercise Test Exercise Test or Dipyridamole Before Discharge Before or After Discharge Nuclear Scan
Dobutamine Echo
Exercise Echo
Exercise Nuclear
Medical Therapy
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No Stent Implanted
No ASA allergy
No Indications for Anticoagulation Preferred: ASA 75 to 162 mg Class I; LOE: A Alternative: ASA 75 to 162 mg Warfarin (INR 2.0 to 3.0) Class: IIa; LOE: B OR Warfarin (INR 2.5 to 3.5) Class IIa; LOE: B Indications for Anticoagulation ASA 75 to 162 mg Warfarin (INR 2.0 to 3.0) Class I; LOE B OR Warfarin (INR 2.5 to 3.5) Class I; LOE: B No Indications for Anticoagulation Preferred: Clopidogrel 75 mg Class I; LOE: C Alternative: Warfarin INR (2.5 to 3.5) Class I; LOE: B
ASA Allergy
Indications for Anticoagulation
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No ASA Allergy
ASA Allergy
ASA 75 to 162 mg Clopidogrel 75 mg Warfarin (INR 2.0 to 3.0) Class: IIb; LOE: C
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Long-Term Management
ACC/AHA Guidelines for the Management of Patients with ST-Elevation Myocardial Infarction
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Recommendations
If blood pressure is 120/80 mm Hg or greater: Initiate lifestyle modification (weight control, physical activity, alcohol moderation, moderate sodium restriction, and emphasis on fruits, vegetables, and low-fat dairy products) in all patients. If blood pressure is 140/90 mm Hg or greater or 130/80 mm Hg or greater for individuals with chronic kidney disease or diabetes: Add blood pressure-reducing medications, emphasizing the use of beta-blockers and inhibitors of the renin-angiotensinaldosterone system.
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Recommendations
Assess risk, preferably with exercise test, to guide prescription.
Encourage minimum of 30 to 60 minutes of activity,
preferably daily but at least 3 or 4 times weekly (walking, jogging, cycling, or other aerobic activity) supplemented by an increase in daily lifestyle activities (e.g., walking breaks at work, gardening, household work).
Cardiac rehabilitation programs are recommended for patients with STEMI.
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Recommendations
Start dietary therapy in all patients (< 7% of total calories as saturated fat and < 200 mg/d cholesterol). Promote physical activity and weight management. Encourage increased consumption of omega-3 fatty acids. Assess fasting lipid profile in all patients, preferably within 24 hours of STEMI. Add drug therapy according to the following guide: LDL-C < 100 mg/dL (baseline or on treatment): Statins should be used to lower LDL-C. LDL-C 100 mg/dL (baseline or on treatment): Intensify LDL-Clowering therapy with drug treatment, giving preference to statins.
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Recommendations
If TGs are 150 mg/dL or HDL-C is < 40 mg/dL: Emphasize weight management and physical activity. Advise smoking cessation. If TG is 200 to 499 mg/dL: After LDL-Clowering therapy, consider adding fibrate or niacin. If TG is 500 mg/dL: Consider fibrate or niacin before LDL-Clowering therapy. Consider omega-3 fatty acids as adjunct for high TG.
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Recommendations
Appropriate hypoglycemic therapy to achieve near-normal fasting plasma glucose, as indicated by HbA1c. Treatment of other risk factors (e.g., physical activity, weight management, blood pressure, and cholesterol management).
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Antiplatelet In the absence of contraindications, start aspirin agents/ 75 to 162 mg/d and continue indefinitely. anticoagulants
75 mg/day or warfarin.
Manage warfarin to INR 2.5 to 3.5 in postSTEMI patients when clinically indicated or for
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Recommendations
ACE inhibitors in all patients indefinitely; start early in stable, high-risk patients (ant. MI, previous MI, Killip class 2 [S3 gallop, rales, radiographic CHF], LVEF < 0.40). Angiotensin receptor blockers in patients who are intolerant of ACE inhibitors and with either clinical or radiological signs of heart failure or LVEF < 0.40.
Aldosterone blockade in patients without significant renal dysfunction or hyperkalemia who are already receiving therapeutic doses of an ACE inhibitor, have LVEF 0.40, and have either diabetes or heart failure.
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Aspirin
Fibrinolytic
162-325 mg chewed
tPA,TNK, rPA, SK 60U/kg (4000) 12 U/kg/h (1000) aPTT 1.5 - 2 x C Oral daily
UFH Beta-blocker
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ACEI
ARB
Aldo Blocker
Oral Daily
Statin
No renal dysf, Same as K+ < 5.0 mEq/L during On ACEI, Hosp. HF or DM Start w/o lipid Indefinitely, profile LDL << 100
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Hormone Therapy
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Hormone Therapy
Postmenopausal women who are already taking estrogen plus progestin at the time of STEMI should not continue hormone therapy.
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Antioxidants
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The psychosocial status of the patient should be evaluated, including inquiries regarding symptoms of depression, anxiety, or sleep disorders and the social support environment.
Treatment with cognitive-behavioral therapy and selective serotonin reuptake inhibitors can be useful for STEMI patients with depression that occurs in the year after hospital discharge.
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Cardiac Rehabilitation
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