- Azathioprine
Drugbox
IUPAC_name = 6-(3-methyl-5-nitro-imidazol-4-yl)sulfanyl-7"H"-purine
width=200
CAS_number=446-86-6
ChemSpiderID=2178
ATC_prefix=L04
ATC_suffix=AX01
ATC_supplemental=
PubChem=2265
DrugBank=APRD00811
C=9 | H=7 | N=7 | O=2 | S=1
molecular_weight = 277.264 g/mol
bioavailability= Well absorbed
metabolism =xanthine oxidase
elimination_half-life= 3hr
excretion = renal, minimally
pregnancy_category = D
legal_status = Approved Drug
routes_of_administration= oralAzathioprine is an immunosuppressant used in
organ transplant ation,autoimmune disease such asrheumatoid arthritis andpemphigus or inflammatory bowel disease such asCrohn's disease andulcerative colitis as well asmultiple sclerosis . It is apro-drug , converted in the body to the active metabolites6-mercaptopurine and 6-thioinosinic acid. It is apurine synthesis inhibitor .Azathioprine is produced by a number of generic manufacturers and as branded names (Azasan by
Salix in the U.S., Imuran byGlaxoSmithKline in Canada and the U.S., Australia and UK, Azamun in Finland and Imurel in Scandinavia).History
Azathioprine was first introduced into clinical practice by Sir
Roy Calne , the British pioneer in transplantation. Following the work done by SirPeter Medawar in discovering the immunological basis of rejection of transplanted tissues and organs, Calne introduced 6-mercaptopurine as an experimental immunosuppressant for kidney transplants. When azathioprine was discovered, he then introduced it as a less toxic replacement for 6-mercaptopurine. For many years, dual therapy with azathioprine and steroids was the standard anti-rejection regime, until cyclosporine was introduced into clinical practice (also by Calne) in 1978.Mechanism of action
Azathioprine is a
purine synthesis inhibitor , inhibiting the proliferation of cells, especiallyleukocytes . It is an effective drug used alone in certain autoimmune diseases, or in combination with other immunosuppressants in organ transplantation. Side effects are uncommon, but include nausea, fatigue, hair loss, and rash. Because azathioprine suppresses the bone marrow, patients will be more susceptible to infection. Caution should be exercised when it is used in conjunction with purine analogues such asallopurinol . The enzyme thiopurine S-methyltransferase (TPMT) deactivates 6-mercaptopurine. Genetic polymorphisms of TPMT can lead to excessive drug toxicity, thus assay of serum TPMT may be useful to prevent this complication. cite journal | author=Konstantopoulou M, Belgi A, Griffiths K, Seale J, Macfarlane A | title=Azathioprine-induced pancytopenia in a patient with pompholyx and deficiency of erythrocyte thiopurine methyltransferase | journal=BMJ | volume=330 | issue=7487 | pages=350–1 | year=2005 | pmid=15705694 | doi=10.1136/bmj.330.7487.350]Mycophenolate mofetil is increasingly being used in place of azathioprine in organ transplantation as it is associated with lessbone marrow suppression , feweropportunistic infection s and a lower incidence of acute rejection. cite journal | author=Woodroffe R, Yao G, Meads C, Bayliss S, Ready A, Raftery J, Taylor R | title=Clinical and cost-effectiveness of newer immunosuppressive regimens in renal transplantation: a systematic review and modelling study | journal=Health Technol Assess | volume=9 | issue=21 | pages=1–194 | year=2005 | pmid=15899149] However azathioprine certainly still has a major role.Long term side effects
It is listed as a human
carcinogen in the 11th Report on Carcinogens of the U.S. Department of Health and Human Services, although they note that theInternational Agency for Research on Cancer (IARC) considered some of the animal studies to be inconclusive because oflimitations in the study design and inadequate reporting. cite book | author = National Toxicology Program | title = Substance Profiles, Report on Ccarcinogens | url = http://ntp.niehs.nih.gov/ntp/roc/toc11.html | edition = Eleventh Edition | publisher = U.S. Department of Health and Human Services | chapter = Azathioprine | chapterurl = http://ntp.niehs.nih.gov/ntp/roc/eleventh/profiles/s018azat.pdf] The risks involved seem to be related both to the duration and dosage used. People who have previously been treated with an alkylating agent may have an excessive risk of cancers if treated with azathioprine. Epidemiological studies have provided "sufficient" evidence of Azathioprine carcinogenicity in humans, cite web | author=International Agency for Research on Cancer (IARC) | authorlink =International Agency for Research on Cancer | year = 1987 | url=http://www.inchem.org/documents/iarc/vol26/azathioprine.html | title =Azathioprine - 5. Summary of Data Reported and Evaluation | work =Summaries & Evaluations | pages =VOL.: 26 (1981) (p. 47) | publisher=World Health Organization ] although the methodology of past studies and the possible underlying mechanisms are questioned. cite journal | author=Gombar V, Enslein K, Blake B, Einstein K | title=Carcinogenicity of azathioprine: an S-AR investigation | journal=Mutat Res | volume=302 | issue=1 | pages=7–12 | year=1993 | pmid=7683109 | doi=10.1016/0165-7992(93)90083-8] The various diseases requiring transplantation, and thus azathioprine, may in themselves increase the risks ofnon-Hodgkin's lymphoma ,squamous cell carcinoma s of the skin, hepatobiliary carcinomas and mesenchymal tumours to which azathioprine may add additional risks. Those receiving azathioprine for rheumatoid arthritis may have a lesser risk than those following transplantation. cite web | author=International Agency for Research on Cancer (IARC) | authorlink =International Agency for Research on Cancer | year = 1987 | url=http://www.inchem.org/documents/iarc/suppl7/azathioprine.html | title =Azathioprine - Evidence for carcinogenicity to humans (sufficient) | work =Summaries & Evaluations | pages =Supplement 7: (1987) (p. 119) | publisher=World Health Organization ]Azathioprine is not thought to cause fetal malformation (
teratogenesis ) and any risk to the offspring of treated women is small.British National Formulary "45" March 2003] A more recent product monograph produced by Glaxo Smith Kline and dated June 2005 does note that IMURAN can cause fetal harm when given to a pregnant woman. Their document also states that the drug should not be given during pregnancy or in patients of reproductive potential withoutcareful weighing of benefit versus the risks and should be avoided whenever possible in pregnant women. It goes on to say that when used in pregnancy the patient should be apprised of the potential hazard to the fetus. While stating that no adequate and well-controlled studies have taken place in humans, it notes that when given to animals in doses equivalent to human dosages teratogenesis was observed. Transplant patients already on this drug should not discontinue on becoming pregnant. This contrasts to the later developed drugstacrolimus and myophenolate which are contra-indicated by the manufacturers during pregnancy. As for all cytotoxic drugs, the manufacturer advises not to breastfeed whilst taking azathioprine. The Lactation Risk Category (LAC) reported by Thomas Hale in "Medications and Mothers' Milk" lists azathioprine as "L3", termed "moderately safe".Under FDA rules, this drug, like many others, excludes eligibility for blood donation.
References
External links
* [http://emc.medicines.org.uk/emc/assets/c/html/displaydoc.asp?documentid=3847 Imuran] (GlaxoSmithKline Patient Information Leaflet)
* [http://www.salix.com/products/products_azasan.asp Azasan] (manufacturer's website)
* [http://www.nlm.nih.gov/medlineplus/druginfo/medmaster/a682167.html Medline Plus advice on Imuran] ( A service of the National Institutes of Health)
* [http://www.gsk.ca/en/products/prescription/ GSK Product Monograph for Imuran (for Canadian patients only)]
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