Genetic Markers of Methotrexate Treatment Failure in Psoriasis
Maria N. Vikhreva, Lavrenty G. Danilov, Andrey A. Martynov, Olga A. Levashova, Svetlana N. Tuchkova, Sherzod P. Abdullaev, Karin B. Mirzaev, Andrey S. Glotov, Oleg S. Glotov, Dmitry A. Sychev

TL;DR
The study identifies genetic markers linked to methotrexate treatment failure in psoriasis patients, suggesting possible genetic predictors for treatment switching.
Contribution
The study discovers novel genetic polymorphisms associated with methotrexate intolerance or reduced efficacy in psoriasis patients.
Findings
SLC19A1 rs1051266 and COL18A1 rs9977268 polymorphisms are associated with the need to switch from methotrexate to biologics.
Carriers of the T allele in these genes show higher frequency among patients requiring biologic therapy.
The C allele in these genes may indicate increased risk of methotrexate intolerance.
Abstract
Background: Pharmacogenetic markers associated with the need to switch patients from methotrexate (MTX) to biologic agents in moderate-to-severe psoriasis remain insufficiently studied. The pharmacokinetics of MTX depend on the individual characteristics of the patient, as well as on the function of specific transporters and enzymes involved in its absorption, distribution, metabolism, and elimination; therefore, polymorphisms in genes encoding these proteins may be considered pharmacogenetic predictors of MTX intolerance or insufficient efficacy. This study aimed to investigate genetic variants associated with MTX intolerance or insufficient efficacy leading to therapy switch. Methods: A total of 80 patients with moderate-to-severe psoriasis were included: 43 who required switching from MTX to biologics and 37 who continued MTX therapy. Twelve polymorphisms in transporter and…
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Taxonomy
TopicsPsoriasis: Treatment and Pathogenesis · Glutathione Transferases and Polymorphisms · Acute Lymphoblastic Leukemia research
