How Stable Are Medicines Moved From Original Packs Into Compliance Aids
How Stable Are Medicines Moved From Original Packs Into Compliance Aids
How Stable Are Medicines Moved From Original Packs Into Compliance Aids
uk)
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How stable are medicines moved from original packs into compliance aids?
In this article, Claire Church and Jane Smith have compiled a table based on information received from manufacturers about the possible stability of their medicines after removal from their packaging and placement in compliance aids
he use of compliance aids has increased in both primary and secondary care over recent years. Compliance aids aim to act as a reminder for patients to take their medicines, enabling them to manage their own often complex and confusing drug regimens. They also act as a visual prompt for carers, indicating that patients have taken their medicines, or at least removed them from the device. The use of these aids involves the transfer of medicines from the manufacturers original packaging to the compliance aid. The original packaging is designed to protect the contents to appropriate pharmacopoeial and quality standards for a variety of criteria, eg, water vapour transmission, as required in the product licence. However, the compliance aid cannot guarantee the same level of protection. Many systems are not disposable and are frequently reused without cleaning.The hazards associated with physical, chemical and microbiological cross-contamination could be a major risk factor. All other dispensing containers are designed for single use. Compliance aids have limited available space for each dose, are not airtight and offer less moisture and light protection than original packs. Doubts are raised as to the stability of medicines that have been transferred to compliance aids: is there a deterioration in quality and can this result in a reduction of efficacy to an unacceptable level? Despite the increased dispensing of medicines in this way, guidance on their stability in these systems is limited and little new information has been published in recent years. Certain products are particularly unsuitable for transferring into compliance aids, but even this information is often not readily available. The Royal Pharmaceutical Society, in it Medicines, ethics and practice guide (section 3.4.7) says that medicines should not be left in sealed monitored dosage systems for
longer than eight weeks and that certain medications should not be placed in monitored dosage systems. These include effervescent tablets, dispersible tablets, buccal tablets, sublingual tablets, significantly hygroscopic preparations and solid dose cytotoxic preparations. A general article by Roger Walker in The Pharmaceutical Journal in 19922 contained information on around 70 products from 53 pharmaceutical manufacturers. The leading article in the same journal discussed the lack of data and concluded: Manufacturers and regulatory authorities urgently need to catch up with current practice.3 In response to these articles a series of letters appeared a few weeks later.4 A medicines and prescribing bulletin for health care professionals in East Lancashire published data on approximately 30 products in November 2000.5 The medicines information department at Pinderfields General Hospital has collated data that are largely derived from pharmaceutical manufacturers and not in-house stability data. This was last updated in January 2004 and contains information on 176 products. This currently unpublished document is available to other medicines information departments and may be available in the future on the UK Medicines Information website: www. ukmi.nhs.uk. In an attempt to provide clearer updated guidance on potential stability problems, we approached pharmaceutical manufacturers for their opinion on the stability of their products in compliance aids.
original packs to compliance aids as it may be outside the terms of their product licence. For the majority of manufacturers any information they provide is based on anecdotal evidence or in-house studies as no formal studies would have been carried out. Wyeth Laboratories requested its own disclaimer to be used as well, since it believed this would be a more accurate reflection of its products and is as follows: The product information provided in this article has been provided by the marketing authorisation holders for these products.The marketing authorisation holders only recommend that their products are stored in accordance with the summary of product characteristics for each product and that storage of products in any other way is entirely at the pharmacists own risk. These products are highlighted in the Table by an asterix (*) in the additional information column.
Data presentation
The Table now contains a list of 392 products in alphabetical order by generic name. Defined against each name is the brand name (if applicable), company, stability code and any other additional information relating to stability.The stability data have been classified into six groups according to the data received. Each group was allocated a code for ease of numbering in the Table linked to the extent of suitability for use in a compliance aid. Stability codes were allocated as follows: 1. Do not put into a compliance aid. 2. No stability data available, therefore company does not recommend putting in a compliance aid. (Refer to SPC for additional stability information.) 3. No stability data available, therefore company does not recommend putting in a compliance aid. Reason for concern is stated, eg, light-sensitive. Individual pharmacists must accept responsibility for putting in a compliance aid. Risks can be minimised by additional safeguards, eg, use of a black bag. 4. No stability data available, but it is probably suitable to put in a compliance aid. 5. Stability data available in an alternative container, but not necessarily in a compliance aid. 6. Stability data available which state that it is suitable to put in a compliance aid. The additional information that relates to stability is based on that received from the
21 January 2006 The Pharmaceutical Journal (Vol 276) 75
Data collection
Fifty medical information departments of pharmaceutical companies in the UK were contacted by telephone during November and December 2002 and asked whether their solid oral dosage forms could be transferred to a compliance aid. No specific brand of aid was specified. Information in writing was received from all the pharmaceutical companies contacted and these data covered 243 products. A further exercise to confirm data was carried out in September 2004 and we now have information on 392 products (see Table). All but one company agreed to their data to be used in this article provided the following disclaimer is included and strongly emphasised: It is important to note that the individual manufacturers do not endorse this practice of transferring medicines from the
Claire Church, BPharm, MRPharmS, is community liaison pharmacist at Southmead Hospital, Bristol. Jane Smith, MSc,MRPharmS, is acting principal pharmacist, service development, at North Bristol NHS Trust (formerly senior pharmacist, patient services at Southmead Hospital). Correspondence to: Mrs Church (e-mail [email protected]).
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manufacturers and is the best available from the resources at the time of compilation. The Table does not represent an exhaustive list and many companies were keen to remind professionals that the most suitable and current source of information regarding the stability of a medicinal product can be obtained direct from the medicine information department of the respective pharmaceutical companies. SPCs may be a reference source for determining the stability of a product within the original packaging.These can be accessed online on the Electronic Medicines Compendium website at www.medicines.org.uk. Omission of a medicine from the Table does not mean that the medicine is suitable for putting in a compliance aid.
General exclusions
Using the information obtained, more general guidelines for the transfer of solid oral dosage forms from original packs to compliance aids have been written. They assume that all compliance aids will be stored at ambient temperature, in a dry environment and away from direct sunlight. However, we would suggest some general exclusions, based on the published and unpublished data reviewed: Medicinal products which are likely to be susceptible to the effects of moisture, including Effervescent, dispersible, and soluble products, which are unsuitable for packing in compliance aids owing to their hygroscopic nature. Ingress of moisture into the compliance aid may impair dispersal or dissolution properties of the product, or chemical drug degradation of the product may occur. Buccal and mucosal products, which may be unsuitable since they are formulated to dissolve and so are sensitive to moisture. Significantly hygroscopic products, which are generally unstable, as either the formulation or the active component is sensitive to moisture. Medicinal products that are susceptible to the effects of prolonged exposure to light Medicinal products that are required to be kept refrigerated Medicinal products the handling of which is likely to be harmful to individuals compliance aid. However, this practice is avoided in our dispensary since the publication of a warning in The Pharmaceutical Journal which concerned two incidents, one fatal, when the patients concerned swallowed a whole blister resulting in intestinal perforation.6 It is also more difficult to remove the dose from a small area of packaging. It was interesting that different companies sometimes offered conflicting advice for the same product, eg, omeprazole. This may be due to different production processes, different stability testing or one manufacturer being more cautious than another. The survey carried out suggests that most solid oral dosage forms can be safely transferred to a compliance aid for a short period. There are, however, both general and specific exceptions to this and it is important that pharmacists, patients and carers are aware of these (see Panel above). As the practice of using compliance aids continues to grow, with an ageing population and greater care in patients homes, there is a necessity for short-term stability data for all medicines. We would encourage manufacturers, when applying for a new product licence, to provide data on the stability of the product when redispensed into a compliance aid.This would be particularly useful for products that
are unstable.This information could be made available in the SPC. It is essential that action is taken now to fill this information gap and so benefit patients and practice in the future.
Conclusion
This survey has revealed that although some information can be obtained from the pharmaceutical companies there is still a shortage of short-term stability data for the transfer of medication to compliance aids. Since the publication of the leading article in The Pharmaceutical Journal in 19923 little appears to have changed in the availability of this stability information. It is impracticable to prevent the use of compliance aids until such data becomes available. It is hoped that this collection of data in a compact format will provide some assistance in the interim. ACKNOWLEDGEMENTS We thank the medicines information departments of the various pharmaceutical companies and also the following pharmacists for their help in compiling this article: Hazel Arnold, senior pharmacist, quality assurance; Alison Yeo, formerly senior pharmacist, medicines information; Eve Wood, formerly patient services pharmacist; Katy Seager, formerly locum pharmacist (all at Southmead Hospital, Bristol); and Richard Cattell, director, South West Medicines Information and Training. References
1. Royal Pharmaceutical Society of Great Britain. Medicines, ethics and practice: a guide for pharmacists (number 27). London; The Society; 2003. 2. Walker R. Stability of medicinal products in compliance devices. Pharmaceutical Journal 1992;248:1246. 3. Dealing with dosage aids (leading article). Pharmaceutical Journal 1992;248:99. 4. Stability of medicines dispensed in compliance devices (letters). Pharmaceutical Journal 1992;248:1745. 5. Stability of medicines in compliance aids and monitored dose systems. Interface 2000; no 45. 6. Blister-strip warning. Pharmaceutical Journal 1996;256:85.
Discussion
Out of 392 products investigated, none had had stability tests carried out on them within a compliance aid. The Medicines and Healthcare products Regulatory Agency (MHRA), which issues product licences, requires companies to provide evidence of stability of the medicine in its original pack until its stated expiry date, if stored as recommended. The licence only covers storage in the original packaging and transfer to any other container cannot be advocated without extensive stability testing being carried out. Most companies will not recommend transferring medicines from original packs to compliance aids due to the absence of stability studies. They cannot guarantee the bioavailability, efficacy or palatability of any formulation that is stored outside its original container. Many companies indicated that they do not have any stability data to support the storage in compliance aids, and therefore cannot recommend the practice. Some stated that storage in such devices would be an unlicensed use of their product and as such would remain the responsibility of the pharmacist or physician. Most companies were sympathetic to pharmacists position and appreciate the fact that the use of compliance aids is becoming increasingly popular or indeed necessary and that it is obviously impractical to prevent the use of them. Some companies replied with more useful comments that included:We do not have any relevant stability studies, but these tablets are generally stable and we are not aware of any specific reason why they should not be stored in a compliance aid for x number of days. Even more useful replies were from the companies that provided information on the chemical and physical properties of their drug, eg, hygroscopicity, light sensitivity. This at least enables a pharmacist to make a judgement on whether to include or exclude a drug from a compliance aid in the absence of hard evidence. Several companies offered a solution to avoid removal from their packaging by suggesting cutting around the blister and putting the dosage form (still in the blister) into the
76 The Pharmaceutical Journal (Vol 276) 21 January 2006
Future research
We have initiated joint research with our regional quality assurance officer to carry out in-house stability testing of specific drugs in compliance aids that we routinely use. At the time of writing, the stability of dispersible and enteric coated aspirin has been investigated. This was carried out in various compliance aids at normal (3550%) and high (up to 85%) humidity. We hope to extend this to other products and publish the data. We have liaised with the other two Bristol hospitals and the local primary care trusts with the aim of developing a common policy. This will reduce the problems that arise when patients using compliance aids are transferred between primary and secondary care. We plan to work with medicines information pharmacists to ensure that the resources we and Pinderfields have developed are presented in a suitable format for web presentation.
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The stability of drugs in compliance aids, based on information provided by manufacturers (acarbose to co-careldopa)
Brand name Buspar Cabaser Dostinex Cacit Didronel PMO Probably stable for 7 days Should be stored with desiccant Effervescent tablet is moisture sensitive Cacit is moisture sensitive Company BSM Pfizer Pfizer P&G P&G Code 2 4 1 1 1 Additional information
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Amias Acepril Capoten Acezide Capozide BMS 2 Susceptible to moisture Protect from light Probably stable for up to 4 weeks Sensitive to moisture AstraZeneca BMS BMS BMS 2 2 2 2 Generic name Buspirone Cabergoline Cabergoline Calcium carbonate Calcium carbonate and etidronate Candesartan Captopril Captopril Captopril/ hydrochlorothiazide Captopril/ hydrochlorothiazide Carbamazepine Carbenoxolone sodium Carvedilol Cefaclor Cefaclor MR Cefadroxil Cefprozil Cefradine Celecoxib Chlordiazepoxide Chloroquine phosphate/ proguanil HCl Chlorpromazine Tegretol / Retard Pyrogastrone Eucardic Distaclor Distaclor MR Baxan Cefzil Velosef Celebrex Librium Avloclor/Paludrine Largactil Neoral Stugeron/Forte Modalim Ciproxin Hawgreen Novartis Janssen-Cilag SS Bayer 3 1 2 2 1 Cephalon UK SS Roche Lilly Lilly BMS BMS BMS Pfizer Valeant AstraZeneca 1 2 3 4 1 2 2 1 2 2 2 Powder is hygroscopic Ciclosporin Cinnarizine Ciprofibrate Ciprofloxacin Can cause contact dermatitis when handled (wear gloves); must be protected from light Ethanol vaporises out of the capsule when out of the original packaging Not known to be hygroscopic May absorb a small amount of water over time; light sensitive over time Probably stable for 6 months Protect from light Probably stable for 4 weeks Should only be dispensed in glass bottles Protect from moisture Store in dark Probably stable for 7 days Protect from light Citalopram Clarithromycin Clarithromycin XL Clobazam Clomethiazole Clomipramine Clonazepam Clopidogrel Cloral Betaine Clozapine Co-amilofruse 5/40 Co-amilofruse Co-amilofruse Co-amilozide Co-beneldopa Co-beneldopa dispersible Co-careldopa Cipramil Klaricid Klaricid Frisium Heminevrin Anafranil Rivotril Plavix Welldorm Clozaril Lasoride Madopar Madopar dispersible Sinemet Lundbeck Abbott Abbott Sanofi Aventis AstraZeneca Cephalon UK Roche SS Alphashow Novartis Generics (UK) Borg CP APS Roche Roche BMS 4 3 2 4 1 2 3 2 4 2 4 3 2 2 4 5 1 Probably stable for 14 days Stable for at least 14 days Powder is hygroscopic
Generic name Acarbose Acetazolamide Aciclovir Aciclovir Aciclovir dispersible Alendronate 5mg
Code 4 2 2 2 1 5
Dispersible tablet Stable for 3 months at 40C and 75% relative humidity
MSD Leo
2 1
Moisture sensitive; can become sticky out of original packaging and congeal with other tablets in the compliance aid
SS GSK BMS
2 2 2
Hygroscopic Hygroscopic Not suitable as sensitive to atmospheric moisture Probably not suitable as sensitive to moisture Potential to be hygroscopic
Articles
Soluble tablet
Alfuzosin Allopurinol Amiloride/ hydrochlorothiazide Amiodarone Amiodarone Amisulpride Amlodipine Amphotericin Anastrazole Apomorphine Aripiprazole Aspirin Aspirin Aspirin Aspirin EC Atenolol Atenolol Atenolol/chlortalidone Atenolol/co-amilozide Atenolol/nifedipine Atazanavir sulphate Atorvastatin Auranofin Baclofen Baclofen Bambuterol HCl Benperidol Beta-cardone Betahistine Betamethasone Betamethasone Bexarotene Bicalutamide Bisoprolol Bisoprolol Bisoprolol Bumetanide Buprenorphine HCl Buprenorphine HCl
Cordarone SS Alpharma Solian SS Istin Pfizer Fungilin BSM Arimidex AstraZeneca Uprima Abbott Abilify BSM Angettes BSM Alpharma Nu-Seals Lilly Caprin Pinewood Tenormin AstraZeneca CP Tenoretic/Tenoret 50 AstraZeneca Kalten AstraZeneca Tenif AstraZeneca Reyataz BSM Lipitor Pfizer Ridaura Yamanouchi Lioresal Cephalon UK APS Bambec AstraZeneca Benquil Hansam Sotalol Celltech Serc Solvay Betnelan Celltech Betnesol Celltech Targretin Zeneus Pharma Casodex AstraZeneca Cardicor Merck APS IVAX Burinex Leo Temgesic RB Subutex RB
2 2 1 1 2 4 2 1 1 1 2 1 2 2 2 2 2 2 3 2 1 2 2 2 2 2 2 1 4 2 2 2 4 4 2 2
78 Brand name Erymax Erythromid Erythroped A Company Celltech Zeneus Pharma Abbott Abbott Code Additional information 2 4 3 Protect from light 2 Probably stable for 6 months Stable for 6 months at 25C and relative humidity of 60% Generic name Ergometrine Erythromycin Erythromycin BP Erythromycin ethylsuccinate Erythromycin stearate Escitalopram Esomeprazole Etidronate disodium Ethamsylate Ethinylestradiol Etoposide Felodipine Ferrous fumarate/ folic acid Ferrous sulphate Erythocin Cipralex Nexium Didronel Dicynene Vepesid Plendil Pregaday Cytotoxic Ferrograd Ferrograd C Ferrograd folic Proscar MSD Abbott 2 1 Women should not handle crushed or broken tablets when they are or potentially may be pregnant (if the dispenser and/or carer is male or not pregnant the stability code can be changed to 2) GSK Pfizer BMS SS 2 4 2 2 Abbott Abbott 2 2 Alpharma 4 Abbott Lundbeck AstraZeneca P&G SS Celltech BMS AstraZeneca Celltech 2 4 5 2 2 2 1 2 2 Probably stable for maximum of 14 days (could taint other tablets) Ferrous sulphate Ferrous sulphate/ sodium ascorbate Ferrous sulphate/ folic acid Finasteride Floxapen Diflucan Florinef Moditen Probably stable for up to 4 weeks Probably stable for 4 weeks Probably stable for 4 weeks Probably stable for 4 weeks Protect from light Probably stable for 8 days Flucloxacillin Fluconazole Fludrocortisone Fluphenazine HCl Fluphenazine/ nortriptyline Fluoxetine Flupentixol Flupentixol Flurazepam Flurbiprofen Flutamide Fosinopril Furosemide Furosemide Furosemide/potassium Gabapentin Gemfibrozil Gliclazide Glipizide Gliquidone Haloperidol Hydroxycarbamide Hydroxychloroquine Hydroxyzine Motival Prozac Depixol Fluanxol Dalmane Froben/SR Drogenil Staril Lasikal Neurontin Lopid Diamicron/MR Glibenese Glurenorm Hydrea Plaquenil Atarax SS Lilly Lundbeck Lundbeck Valeant Abbott Schering Plough BMS Alpharma CP Borg Pfizer Pfizer Servier Pfizer SS IVAX BMS SS Pfizer 2 4 4 4 2 2 2 2 4 2 3 2 2 4 2 2 4 1 2 4 Probably stable for 7 days Cytotoxic Probably stable for 7 days
The stability of drugs in compliance aids, based on information provided by manufacturers (co-careldopa to hydroxyzine)
Articles
Normax Septrin Valoid Danol Dantrium Ledermycin Neoclarityn Dexedrine Eudemine Voltarol Arthrotec
Code Additional information 1 Powder is hygroscopic 1 Blue dye can fade on light exposure; also moisture will cause levodopa to turn black on prolonged exposure Celltech 2 GSK 2 CP 2 Celltech 2 Amdipharm 3 Light sensitive SS 2 P&G 2 Goldshield 2 Schering Plough 4 Unlikely to be hygroscopic Organon 4 Unlikely to be any issues Celltech 2 Celltech 2 Novartis 2 Pfizer 1 Misoprostol is extremely moisture sensitive and may degrade
Hygroscopic
Co-danthrusate Co-trimoxazole Codeine phosphate Colchicine Cyclizine Danazol Dantrolene sodium Demeclocycline Desloratidine Dexamethasone Dexamfetamine sulphate Diazoxide Diclofenac EC/SR/Retard Diclofenac and misoprostol Didanosine chewable Didanosine EC Didronel PMO Digitoxin Digoxin Diltiazem hydrochloride Diltiazem Diltiazem Diltiazem Diltiazem Dipyridamole MR
Videx Videx EC Lanoxin Dilzem Slozem Adizem SR/XL Angitil SR/XL Tildiem/LA/Retard Persantin Retard
BMS BMS P&G Celltech GSK Zeneus Pharma Merck Napp Trinity SS BI
1 2 1 2 4 4 2 2 4 2 5
Asasantin Retard
BI
3 2 4 2 4
Moisture sensitive; stable for 30 days out of the original container, eg, plastic dispensing bottle Stable for 30 days out of the original container, eg, plastic dispensing bottle Protect from light
Dipyridamole MR/ aspirin Dipyridamole Disopyramide Docusate sodium Domperidone Domperidone/ paracetamol Donepezil Dosulepin tablets and capsules Dosulepin Doxazosin Doxazosin
Aricept -
4 4
2 2 1
Not recommended for inclusion in compliance aid; SPC states must be stored in the original package
2 2 1
May hydrolyse at high temperature and in the presence of moisture; 10% loss of potency occurred when exposed to 40C and 75% humidity for 13 weeks
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Ergocalciferol
Celltech
The stability of drugs in compliance aids, based on information provided by manufacturers (ibuprofen to paracetamol/codeine)
Brand name Flagyl Minocin MR Loniten Zispin Hygroscopic; as an alternative, can write days of the week on lidding paper of each tablet pouch Moisture sensitive and may degrade Company Hawgreen Wyeth Pfizer Organon Code 3 4 2 1 Additional information Must be protected from light Probably stable for 7 days*
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Generic name Metronidazole Minocycline Minoxidil Mirtazapine orodispersible Misoprostol Modafinil Morphine sulphate Moxifloxacin Nadolol Naftidofuryl Nalidixic acid Naltrexone Naproxen and misoprostol Nevirapine Nicardipine Nicardipine Nicorandil Nifedipine Cytotec Provigil MST Continus Avelox Corgard Praxilene Negram Nalonex Napratec Should be stable for 7 days BI Yamanouchi Yamanouchi Sanofi Aventis Bayer Bayer 1 4 2 3 5 1 Pfizer Cephalon UK Napp Bayer SS Merck SS BMS Pfizer 1 2 2 4 2 2 2 2 2 Protect from light. Stable for at least 7 days in a dry environment Very light sensitive Very light sensitive and will significantly degrade very quickly; moisture can affect release mechanism Should be stable for 7 days Probably stable for up to 4 weeks 2 4 2 4 2 1 4 Nifedipine Nifedipine Nimodipine Nitrazepam Nizatidine Norethisterone Nystatin Olanzapine Coracten SR/XL Nimotop Mogadon Axid Utovlan Nystan Zyprexa Celltech Bayer Valeant Lilly Pfizer BMS Lilly Viramune Cardene Cardene SR Ikorel Adalat Retard and capsules Adalat LA Olanzapine Velotabs Zyprexa Velotabs Lilly Celltech Generics (UK) AstraZeneca 1 2 1 5 Hygroscopic Stable for 14 days at room temperature (2530C) and relative humidity up to 75% Stable for 3 months at 25C and relative humidity of 60% Powder is hygroscopic Probably stable for up to 4 weeks; sensitive to light; wear gloves if breaking or dividing the tablets due to potential contact dermatitis Particularly fragile/brittle may disintegrate due to moisture in the air Olsalazine sodium Dipentum tablets and capsules Omeprazole capsules Omeprazole capsules Losec Omeprazole MUPS Orphenadrine Oxybutynin Oxybutynin Oxybutynin XL Losec MUPS Disipal Cystrin Ditropan Lyrinel XL AstraZeneca Yamanouchi SS SS Janssen-Cilag 5 2 2 2 1 Hygroscopic; packaged in high density polyethylene bottles with a dessicant Creon Solpadol Solvay Alpharma SS SS 2 4 2 1 Probably stable for up to 28 days Pancreatin Paracetamol Paracetamol/codeine caplet/capsules Paracetamol/codeine effervescent tablets
Generic name Ibuprofen Indapamide Inositol nicotinate Irbesartan Irbesartan /hydrochlorothiazide Isoniazid Isosorbide mononitrate Isosorbide mononitrate Isosorbide mononitrate Isosorbide mononitrate Isosorbide mononitrate Isosorbide mononitrate Ketoprofen Ketoprofen Ketoprofen MR Labetolol hydrochloride Lamivudine Lamotrigine Lansoprazole
CoAprovel Cedocard Retard Elantan LA Imdur Monomax SR/XL Ketocid Orudis Oruvail Trandate Epivir Lamictal Zoton
BMS Celltech Alpharma IVAX Pfizer Schwartz AstraZeneca Trinity Trinity Hawgreen Hawgreen Celltech GSK GSK Wyeth
2 2 4 4 2 2 5 4 4 3 3 2 2 2 4
Stable for one month Probably stable for 4 weeks Probably stable for 4 weeks Must be protected from light Must be protected from light
Zoton FasTab
Wyeth
Probably stable for up to 4 weeks in a compliance aid which offers a barrier against moisture* Highly moisture sensitive*
2 2 2 2 2
Zestoretic
AstraZeneca
4 1 2 2 2
Probably stable for 7 days Moisture sensitive and could change colour
Articles
Cytotoxic
Lansoprazole orodispersible Levothyroxine Levothyroxine Lisinopril Lisinopril Lisinopril/ hydrochlorothiazide Lisinopril/ hydrochlorothiazide Lithium Loperamide Lopinavir/ritonavir Losartan Medroxyprogesterone acetate Medroxyprogesterone acetate Megestrol Memantine HCl Meloxicam Mesalazine Methionine Metformin Methotrexate Methylphenidate HCl Methylphenidate HCl Methylphenidate HCl Metolazone Metoprolol tartrate
Provera Megace Ebixa Mobic Asacol Glucophage Maxtrex Ritalin Concerta XL Equasym Metenix 5 Betaloc SA
Pfizer BMS Lundbeck BI P&G Celltech Merck Pfizer Cephalon UK Janssen-Cilag Celltech Borg AstraZeneca
2 2 2 4 1 2 2 1 2 1 2 3 2
80 Brand name Reductil Zocor Beta-cardone Sotacor Lasilactone Company Abbott MSD Celltech BMS IVAX Alpharma Borg Code Additional information 2 2 2 2 3 Protect from light 2 3 Protect from light Stable for 3 months at 30C and 75% humidity Known to be light labile Sensitive to light Cytotoxic Generic name Sibutramine Simvastatin Sotalol Sotalol Spironolactone Spironolactone Spironolactone/ furosemide Stavudine Sulfasalazine Sulpiride Sulpiride Tacrolimus Tamoxifen Tamoxifen Tamoxifen Tamsulosin Tegafur with uracil Terazosin Terbinafine Terbutaline sulphate Testosterone Zerit Salazopyrin/EN/EC Dolmatil Sulpitil Prograf Nolvadex Flomax SR Uftoral Hytrin Lamisil Bricanyl Restandol BMS Pfizer SS Pfizer Fujisawa AstraZeneca APS Generics (UK) Yamanouchi BMS Abbott Novartis AstraZeneca Organon 2 2 2 2 5 3 2 3 2 1 2 2 2 1 Very sensitive to moisture and becomes sticky if removed from packaging Xenazine 25 Slo-Phyllin Uniphyllin Nuelin SA Franol/Plus Melleril Benerva Gabitril Skelid Betim Prestim Cambridge Merck Napp 3M SS Novartis Roche Cephalon UK SS Valeant Valeant 2 2 2 2 2 2 4 2 2 2 2 Hygroscopic; hydroxylates and becomes unstable with water Zanaflex Detrusitol/ XL Topamax Zydol Gopten Cyklokapron Molipaxin Surmontil De-Noltab Bextra Epilim Epilim chrono Depakote Diovan Zeneus Pharma Pfizer Janssen-Cilag Pfizer Abbott Pfizer Sanofi Aventis Sanofi Aventis Yamanouchi Pfizer SS SS SS Novartis 4 2 1 2 2 2 2 2 2 2 1 1 2 2 Hygroscopic Hygroscopic Tetrabenazine Theophylline Theophylline Theophylline Theophylline/ephedrine Thioridazine Thiamine Tiagabine Tiludronic acid Timolol maleate Timolol maleate/ bendroflumethiazide Tizanidine HCl Tolterodine Topiramate Tramadol Trandolapril Tranexamic acid Trazodone Trimipramine Tri-potassium di-citratobismuthate Valdecoxib Valproate sodium EC/ crushable tablets Valproate sodium chrono Valproic acid Valsartan
The stability of drugs in compliance aids, based on information provided by manufacturers (paracetamol/metoclopramide to valsartan)
Company SS
2 2 1
Articles
4 4 2 2 1 4
Unstable light sensitive and extremely hygroscopic (notably the 50g strength) Probably stable for 8 days Probably stable for 8 days
Moisture sensitive May absorb water; probably stable in an airtight compliance aid for 14 days
Arythmol Inderal/Half Inderal Mestinon Seroquel Accupro Kinidin Pariet Evista Tritace
Abbott AstraZeneca Celltech Valeant AstraZeneca Pfizer AstraZeneca Alpharma Janssen-Cilag Lilly Sanofi Aventis
2 2 2 1 4 2 2 4 1 2 2
Pravastatin Prazosin Prednisolone Prednisolone EC Prochlorperazine maleate Propafenone Propranolol HCl Propylthiouracil Pyridostigmine Quetiapine Quinapril Quinidine bisulphate Quinine sulphate Rabeprazole Raloxifene Ramipril tablets and capsules Ranitidine Ranitidine Reboxetine Ribavirin Risedronate sodium Risperidone
1 1 2 2 2 2
Hygroscopic and may turn brown Hygroscopic and degrades in the presence of water
Ritonavir Ropinirole
Norvir Requip
Abbott GSK
2 5
Not known to be hygroscopic or need a drying agent during storage Refrigeration by patient not required if used within 30 days Stable for up to 28 days below 25C and at 60% relative humidity
2 1 4 3 3
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Hygroscopic Probably stable for 4 weeks Store in the dark Probably stable for 3 months out of the refrigerato; store in the dark Hygroscopic Can absorb moisture Very light sensitive
The stability of drugs in compliance aids, based on information provided by manufacturers (vancomycin to zuclopenthixol)
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Generic name Vancomycin Vardenafil Venlafaxine Venlafaxine XL Verapamil HCl Verapamil HCl
Brand name Vancocin Matrigel Levitra Efexor Efexor XL Univer Securon/SR/ Half Securon SR Tarka
Code 4 4 1 4 4 2
Additional information Probably stable for up to 4 weeks Should be stable for 7 days Moisture sensitive* Probably stable for 7 days*
Abbott
Verapamil HCl/ trandolapril Warfarin Zafirlukast Zaleplon Zidovudine Zidovudine/lamivudine Zolmitriptan Zolpidem Zopiclone Zopiclone Zuclopenthixol
Goldshield AstraZeneca Wyeth GSK GSK AstraZeneca SS Sanofi Aventis IVAX Lundbeck
2 5 2 2 2 2 2 2 3 4
1. Do not put into a compliance aid. 2. No stability data available, therefore company does not recommend putting in a compliance aid. (Refer to SPC for additional stability information.) 3. No stability data available, therefore company does not recommend putting in a compliance aid. Reason for concern is stated, eg, light-sensitive. Individual pharmacists must accept responsibility for putting in a compliance aid. Risks can be minimised by additional safeguards, eg, use of a black bag. 4. No stability data available, but it is probably suitable to put in a compliance aid. 5. Stability data available in an alternative container, but not necessarily in a compliance aid. 6. Stability data available which state that it is suitable to put in a compliance aid.
KEY TO MANUFACTURERS: BI, Boehringer Ingelheim; BSM, Bristol-Myers Squibb; GSK, GlaxoSmithKline; MSD, Merck Sharp & Dohme; P&G, Procter & Gamble; SS, Sanofi Synthelabo
Protect from light 2mg stable for 14 days; other strengths stable for 4 weeks
DISCLAIMERS: It is important to note that the individual manufacturers do not endorse the practice of transferring medicines from the original packs to compliance aids as it may be outside the terms of their product licences. For the majority of manufacturers any information they provide is based on anecdotal evidence or in-house studies as no formal studies would have been carried out. *The product information provided in this article has been provided by the marketing authorisation holders for these products. The marketing authorisation holders only recommend that their products are stored in accordance with the summary of product characteristics for each product and that storage of products in any other way is entirely at the pharmacists own risk.
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