医学
甲氨蝶呤
类风湿性关节炎
阿达木单抗
内科学
胃肠病学
不利影响
关节炎
临床试验
药理学
体质指数
外科
作者
H. Tamai,Kei Ikeda,Toshiaki Miyamoto,Hiroaki Taguchi,Chang‐Fu Kuo,Kichul Shin,Shintaro Hirata,Yutaka Okano,Shinji Sato,Hidekata Yasuoka,Masataka Kuwana,Tomonori Ishii,Hideto Kameda,Toshihisa Kojima,Yurie Nishi,Masahiko Mori,Hideaki Miyagishi,Genta Toshima,Yasunori Sato,Wen‐Chan Tsai,Tsutomu Takeuchi,Yuko Kaneko
标识
DOI:10.1136/ard-2024-226350
摘要
Objectives The usefulness of methotrexate-polyglutamates (MTX-PGs) concentration for management of rheumatoid arthritis has been debated. We aimed to clarify the association of MTX-PGs concentration with efficacy and safety in MTX-naïve patients initiating MTX in a prospective interventional clinical trial. Methods The MIRACLE trial enrolled 300 MTX-naïve patients. Oral MTX was initiated and increased to the maximum tolerated dose by week 12. Patients who did not achieve remission according to the Simplified Disease Activity Index at week 24 were randomised to either the continued dose or reduced dose group and were started on subcutaneous adalimumab. We measured the concentrations of MTX-PGs in erythrocytes using liquid chromatography-tandem mass spectrometry and analysed the association of these concentrations with efficacy and safety. Results The mean concentration of total MTX-PGs increased with an increasing dose of MTX and continued to elevate for another 12 weeks after the dose was fixed. At week 24, the total MTX-PGs concentration was 110.5 (SD 43.8) nmol/L with MTX dose of 12.6 (3.0) mg/week (0.23 (0.07) mg/kg/week). During MTX monotherapy, the higher MTX-PGs concentration was an independent factor for lower disease activity; however, this association disappeared after adalimumab initiation in patients with continued MTX dose. Hepatotoxicity was related to the higher MTX-PGs concentration regardless of adalimumab use. The total MTX-PGs concentration was significantly elevated by lower estimated glomerular filtration rate, serum albumin and body mass index. Conclusions The MIRACLE trial demonstrated that higher total MTX-PGs concentration in erythrocytes is related to the higher efficacy and lower safety of MTX. Trial registration number NCT03505008 .
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