Mercaptopurine (6MP) was approved by the Food and Drug Administration (FDA) for use in acute lymphoblastic leukemia in children and adults as part of combination therapy. However, there are several off-label uses for 6MP[1][2][3][4][5]:
Mercaptopurine and azathioprine are prodrugs of a purine analog hypoxanthine that works as an antagonist to endogenous purines required for DNA replication during the S-phase of the cell cycle and inhibition of RNA and protein synthesis. Azathioprine breaks down into 88% mercaptopurine and 12% other thiopurine metabolites. 6MP requires conversion into 6-thioguanine nucleotides (6TGN) to become active and exert antileukemic effects.[6]
The prodrug is metabolized in the liver, GI tract, and taken up by lymphocytes where mercaptopurine is metabolized via the purine salvage enzyme via hypoxanthine-guanine phosphoribosyltransferase (HGPRT) to thioguanine nucleotides 6TGN and thioinosine monophosphate (TIMP). Inosine triphosphate (ITPA) catalyzes the hydrolysis of thioinosine triphosphate (TITP) to thioinosine monophosphate (TIMP), which increases 6TGN levels.[7]
There is also a secondary pathway via thiopurine methyltransferase (TPMT), which produces inactive methylated bases, 6-methylmercaptopurine. The methylated metabolite, methyl-thioinosine monophosphate (Me-TIMP), is a potent inhibitor of the purine de novo synthesis. Me-TIMP further reduces purines available for incorporation in DNA synthesis.[7]
Deoxy-6-thioguanine triphosphate (6-dTGTP) incorporates into DNA, and 6-thioguanine triphosphate (6-TGTP) inserts into RNA. 6-TGTP also binds to Rac1, resulting in the inactivation of Vav-Rac1 signaling pathway in T-lymphocytes. This process further prevents the activation of Rac1 target genes such as nuclear factor kappa beta (NF-kB), which induces apoptosis of activated T-lymphocytes.[6]
The replacement of the endogenous purines with these synthetic thiopurine nucleotides results in purine deprivation within the cells, which halts DNA, RNA, and protein synthesis leading to decreased cell proliferation and cytotoxicity.[8][9][10]
Mercaptopurine comes as a 50 mg tablet that may be administered orally as either a tablet or suspension, preferably on an empty stomach at the same time each day.[11]
The dosage varies from 1 to 3 mg/kg or 50 to 150 mg/day for long term therapy.[12]
The therapeutic response is generally observable after three months of therapy, but it may take longer to observe results.
Dosages may need to be adjusted based on the patient's renal or hepatic impairments.
Patients may exhibit non-dose dependent or dose-dependent side effects while undergoing treatment with mercaptopurine. Allergic reactions such as nausea, fever, rash, flu-like symptoms, and arthralgias are considered non-dose dependent symptoms that may require changing the timing of dosing to night time administration or discontinuation of therapy.[13]
These symptoms may also reoccur in patients reintroduced to azathioprine or mercaptopurine after an initial adverse reaction. [14] To reduce these symptoms, administering 6MP at night may be required.[13]
Dose-dependent adverse reactions that are potentially observable with 6MP are[13]:
There are various forms of hepatotoxicity resulting from both acute and chronic mercaptopurine intake. Acute liver injury is usually observed as elevation in liver enzymes with fatigue and jaundice within one to six months after starting therapy. The liver biopsy depicts mixed hepatocellular-cholestatic injury with cholestasis, focal hepatocellular necrosis, bile duct injury, and variable inflammation.[12]
In chronic therapy, nodular regenerative hyperplasia (NRH) and symptomatic portal hypertension with ascites and varices were observed from six months to several years after starting therapy. This condition physically presented itself in patients as ascites, varices, and mild liver enzyme abnormalities and jaundice and is concerning because it can progress to hepatic failure if 6MP therapy is not discontinued.[15][12]
Hepatosplenic T-cell lymphoma (HSTCL) is a rare complication with high mortality rate reported in men with inflammatory bowel disease who have been immunosuppressed long term with thiopurines such as mercaptopurine with or without anti-tumor necrosis factor therapy. They present with fatigue, fever, hepatosplenomegaly, and pancytopenia. Diagnosis is from either bone marrow or liver biopsy showing marked infiltration with malignant T cells.[12]
Also, NUDT15 correlates with thiopurine-induced myelosuppression.[16]
It is important to note that switching from 6MP to AZA does not reduce the risk of side effects.[17]
If patients are previously known to have severe allergic or hypersensitivity reactions, they are required to discontinue use of the medication immediately. Mercaptopurine is also contraindicated for use in patients who have previously shown resistance to the drug.
There should be at least a two-month window between the cessation of mercaptopurine treatment and vaccination with live viral or bacterial vaccines to prevent severe and fatal infections.[18]
Approximately 2 to 4% of patients receiving treatment with thiopurines develop thiopurine-induced pancreatitis. This condition is an absolute contraindication to the reintroduction of thiopurines.[19]
All patients require complete blood count and liver enzymes every two weeks for six to eight weeks since starting azathioprine or mercaptopurine treatment. The testing should be followed by changes or adjustments in treatment as well.[20]
Monitoring 6TG level concentrations to be maintained between 230 and 400 proves to be related to sufficient bone marrow suppression and reduces the chances of liver toxicity.[21]
Research has found some medications to increase mercaptopurine levels in the plasma. Allopurinol and febuxostat inhibit the first-pass metabolism of 6MP via enzyme xanthine oxidase (XO), which resulted in a fivefold increase in plasma 6MP concentrations and a threefold increase in steady-state erythrocyte 6-TGN concentrations.[22] This effect may be useful in inducing shunting of 6MMP metabolites towards 6TG in patients with 6MP resistance.[23][24][25]
Methotrexate can also increase 6MP plasma levels through the formation of active metabolites via XO inhibition and other mechanisms.[22]
In patients with IBD, vigilant monitoring of CBC counts is necessary when they are receiving combined therapy that includes mercaptopurine. 5-aminosalicylates cause in vitro inhibition of TPMT. Combining 6MP with mesalazine or sulfasalazine induced mild to moderate leukopenia.[26]
Concurrent treatment of warfarin while being treated with 6MP is known to diminish the anticoagulant effects. Also, discontinuing 6MP with an adjusted warfarin dose can lead to bleeding in a previously stable patient.[27]
NSAIDs such as naproxen, mefenamic acid, tolfenamic acid exhibit noncompetitive inhibition of TPMT activity in vitro and thus require monitoring while the patient receives treatment with mercaptopurine.[13]
Mercaptopurine therapy should be reduced by 50% of the current dose or discontinued if the patient exhibits leukopenia (WBC =< 4000 cells/mm^3) or thrombocytopenia (platelet count < 150,000/microL). If the patient continues to show persistent cytopenia with the dosage reduction, then the medication should be permanently discontinued.[28]
If mild hepatitis (transaminitis) is present, it is reversible by lowering the dose of 6MP. If ALT and AST levels continue to remain elevated, a further dose reduction by 33-50% will be needed. Liver function tests require monitoring and evaluation every two weeks. ALT and AST levels should not exceed two times the upper limit of normal. If such an event occurs, the medication should be discontinued until the liver enzyme levels normalize, at which point 6MP may be reintroduced cautiously at a lower dose.[12]
Macrocytosis should have close monitoring, with CBC every two weeks for one month to exclude other causes such as vitamin B12 or folate deficiencies.
Mercaptopurine may be used during pregnancy with close monitoring. There is no known risk of teratogenicity or higher rates of pregnancy complications with the use of this medication. Concentrations of 6MP have not been detected in breast milk.[13]
It is important to maintain a constant dose titration to maintain steady thiopurine exposure while minimizing toxicity. There have been observations that in patients with nonfunctional variant alleles of TPMT or with reduced TPMT enzyme activity, there is a resulting accumulation of 6TGN in hematopoietic tissues causing toxicity.[16]
Mercaptopurine, due to its narrow therapeutic index, requires continuous monitoring for toxicity in patients due to enzyme activity levels and interactions with other medications. This medication is listed in the Institute for Safe Medication Practices (ISMP), where it is among a list of drugs classified as having a heightened risk of causing significant patient harm when used in error. Because 6MP is a maintenance treatment for inflammatory disorders and leukemia with other disease-modifying agents or chemotherapy, adjustments may be needed frequently or intermittently throughout the time of administration. Most, if. not all, of the diseases that require mercaptopurine therapy are chronic conditions requiring long term treatment. Pharmacists need to ensure that dosage levels are appropriately administered based on side effects and contraindications. The patients will require both inpatient and at-home care throughout the course of their treatment. Also, to ensure the efficacy of the treatment, patient compliance will need to be taken into account because this is a slow-acting medication. There will need to be communication with the specialists, general practitioners, nurses, and care staff involved in the patient's care. There is also a long-term risk of secondary leukemia or malignancies occurring with mercaptopurine therapy, which will require follow up and screening among patients undergoing such treatment.[29] [Level 3]
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