Interaction between Allopurinol and Azathioprine
Major Metabolism

ID DDInter48 and DDInter150
Interaction Allopurinol may potentiate the pharmacologic effects of orally administered thiopurines. Severe bone marrow suppression and other toxicity have been associated with concomitant use of allopurinol and mercaptopurine (6-MP) or azathioprine, the latter of which is metabolized to 6-MP in vivo. The mechanism is thought to be allopurinol inhibition of 6-MP first-pass metabolism via hepatic or intestinal xanthine oxidase, the enzyme that catalyzes the inactivation of 6-MP. In one study, allopurinol pretreatment resulted in a nearly 500% increase in peak plasma concentration (Cmax) and area under the concentration-time curve (AUC) of oral 6-MP. No effect was observed on the pharmacokinetics of intravenous 6-MP. In a retrospective study of 24 heart and/or lung transplant patients receiving azathioprine, investigators found that 46% became leukopenic, 30% moderately anemic, and 22% thrombocytopenic within 3 months after starting allopurinol despite general compliance with thiopurine dosage reduction guidelines. Thus, decreasing the dosage by two-thirds or greater as often recommended does not abolish the risk of myelotoxicity.
renal tubular acidosis agranulocytoses anaemia Anemia aplastic Anorexia arteriosclerosis Aching joints Arthritis rheumatoid asthenia atelectasis More
Management Caution is advised if allopurinol must be used concomitantly with oral thiopurines. Most authorities recommend that thiopurine dosage be reduced to approximately 1/4 to 1/3 the usual dosage, and the patient closely monitored for hematologic and other toxicity. Subsequent doses should be adjusted based on therapeutic response and appearance of adverse effects. Patients should be advised to consult their physician if they develop signs and symptoms suggestive of thiopurine toxicity such as fever, chills, sore throat, fatigue, lethargy, pallor, anorexia, jaundice, dark urine, nausea, vomiting, signs of local infection, and unusual bleeding or bruising.
References
Alternative for Allopurinol M04A
Sulfinpyrazone
Probenecid
Rasburicase
Pegloticase
Lesinurad
Alternative for Azathioprine L04A
Muromonab
Tofacitinib
Teriflunomide
Alemtuzumab
Certolizumab pegol
Siponimod
Pomalidomide
Vedolizumab
Ocrelizumab
Brodalumab
Ozanimod
More

Potential Metabolism Interactions

Substrate-Substrate Interaction:If more than one drug is metabolized by the same CYP, it is possible that its metabolism is inhibited because of the competition between the drugs. That means, it can be useful to lower the dosage of the drugs in the drug-cocktail because they remain longer in the organism than in monotherapy.
Inhibitor-Inhibitor Interaction:Combining two or more inhibitors of one CYP, should be compensated by lowering the dosage of these drugs because the metabolism is reduced and the drugs remain longer in the organism than in monotherapy. Not adapting the dosage bears the risk of even more side effects.
Inhibitor-Substrate Interaction:Combining drugs that have inhibitory effect and are substrates of one particular CYP, should be compensated by lowering the dosage. They rest longer in the organism than in monotherapy. Not adapting the dosage bears the risk of even more side effects.