Raoul Santucci scite author profile

Methotrexate is an antifolate agent used in the treatment of various cancers and some autoimmune diseases. In oncology, methotrexate is frequently administered at a high dose (>1 g/m(2)) and comes with various procedures to reduce the occurrence of toxicity and particularly to ensure optimal renal elimination. Drug-drug interactions involving methotrexate are the origin of severe side effects owing to delayed elimination of the antifolate and, more rarely, of decreased efficacy in relation to suboptimal exposure. Most of these interactions are driven by membrane drug transporters whose activity/expression can be inhibited by the interacting medication. In the last 10 years, research on drug transporters has permitted retrospective identification of the molecular mechanisms underlying drug-drug interactions with methotrexate. This article summarizes reported drug-drug interactions involving methotrexate in clinical oncology with reference to the role of drug transporters that control the disposition of the antifolate agent.

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Contamination fongique des habitations : bilan de 10 années d’analyses

Santucci

Meunier

Ott

et al. 2007

Revue Française d'Allergologie et d'Immunologie Clinique

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Cola beverage and delayed elimination of methotrexate

Santucci¹,

Levêque²,

Herbrecht

2010

Brit J Clinical Pharma

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AIMSTo report a case of severe delayed methotrexate elimination attributable to consumption of a cola beverage. METHODSTo investigate unexplained low urinary pH in a lymphoma patient treated with high-dose methotrexate. RESULTSUnexpected urinary acidity, despite administration of large amounts of sodium bicarbonate, could be attributed to repeated consumption of a cola beverage. It resulted in a delayed elimination of methotrexate and acute renal failure. Discontinuation of cola drinks, increase in calcium folinate rescue and in sodium bicarbonate allowed satisfactory elimination of methotrexate on day 12 after infusion and recovery from renal impairment without other severe toxicity. No other cause of delay in methotrexate elimination could be identified. CONCLUSIONSCola beverages have a low pH due to their phosphoric acid content that is excreted by renal route. We recommend patients receiving high dose methotrexate abstain from any cola drink within 24 h before and during methotrexate administration and until complete elimination of the drug.

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Mécanismes des interactions médicamenteuses d’origine pharmacocinétique

Levêque¹,

Lemachatti²,

Nivoix³

et al. 2010

La Revue de Médecine Interne

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Paralytic ileus possibly associated with interaction between ritonavir/lopinavir and vincristine

et al. 2009

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We speculate that an interaction between ritonavir/lopinavir and vincristine was responsible for this severe toxicity. Vincristine is transported by P-gp and is metabolized via CYP3A5. Ritonavir is a potent CYP3A5 isoenzyme and P-gp inhibitor. Lopinavir is also a P-gp inhibitor. Ritonavir and lopinavir might have delayed vincristine elimination. Clinicians should be aware of this possible interaction.

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Raoul Santucci

Pharmacokinetic drug–drug interactions with methotrexate in oncology

Contamination fongique des habitations : bilan de 10 années d’analyses

Cola beverage and delayed elimination of methotrexate

Mécanismes des interactions médicamenteuses d’origine pharmacocinétique

Paralytic ileus possibly associated with interaction between ritonavir/lopinavir and vincristine

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