Scientific Reports (Dec 2020)

Predictors for clinical effectiveness of baricitinib in rheumatoid arthritis patients in routine clinical practice: data from a Japanese multicenter registry

  • Nobunori Takahashi,
  • Shuji Asai,
  • Tomonori Kobayakawa,
  • Atsushi Kaneko,
  • Tatsuo Watanabe,
  • Takefumi Kato,
  • Tsuyoshi Nishiume,
  • Hisato Ishikawa,
  • Yutaka Yoshioka,
  • Yasuhide Kanayama,
  • Tsuyoshi Watanabe,
  • Yuji Hirano,
  • Masahiro Hanabayashi,
  • Yuichiro Yabe,
  • Yutaka Yokota,
  • Mochihito Suzuki,
  • Yasumori Sobue,
  • Kenya Terabe,
  • Naoki Ishiguro,
  • Toshihisa Kojima

DOI
https://doi.org/10.1038/s41598-020-78925-8
Journal volume & issue
Vol. 10, no. 1
pp. 1 – 10

Abstract

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Abstract This study aimed to evaluate the short-term effectiveness and safety profiles of baricitinib and explore factors associated with improved short-term effectiveness in patients with rheumatoid arthritis (RA) in clinical settings. A total of 113 consecutive RA patients who had been treated with baricitinib were registered in a Japanese multicenter registry and followed for at least 24 weeks. Mean age was 66.1 years, mean RA disease duration was 14.0 years, 71.1% had a history of use of biologics or JAK inhibitors (targeted DMARDs), and 48.3% and 40.0% were receiving concomitant methotrexate and oral prednisone, respectively. Mean DAS28-CRP significantly decreased from 3.55 at baseline to 2.32 at 24 weeks. At 24 weeks, 68.2% and 64.1% of patients achieved low disease activity (LDA) and moderate or good response, respectively. Multivariate logistic regression analysis revealed that no previous targeted DMARD use and lower DAS28-CRP score at baseline were independently associated with achievement of LDA at 24 weeks. While the effectiveness of baricitinib was similar regardless of whether patients had a history of only one or multiple targeted DMARDs use, patients with previous use of non-TNF inhibitors or JAK inhibitors showed lower rates of improvement in DAS28-CRP. The overall retention rate for baricitinib was 86.5% at 24 weeks, as estimated by Kaplan–Meier analysis. The discontinuation rate due to adverse events was 6.5% at 24 weeks. Baricitinib significantly improved RA disease activity in clinical practice. Baricitinib was significantly more effective when used as a first-line targeted DMARDs.