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Poster Session B

Rheumatoid arthritis (RA)

Session: (1308–1344) RA – Treatment Poster II

1328: Switching Biologics or Janus Kinase Inhibitors Is Effective in Difficult-to-treat Rheumatoid Arthritis, Regardless of Inflammation

Monday, November 13, 2023
9:00 AM – 11:00 AM PT
Location: Poster Hall
On Demand In Person

    Abstract Poster Presenter(s)

  • ko

    katsuaki onishi, -None-

    Osaka Metropolitan Univ. Graduate School of Medicine, Baba Memorial Hospital
    Osaka, Japan

    Disclosure information not submitted.

Katsuaki Onishi1, Yutaro Yamada2, Tadashi Okano2, Kenji Mamoto2, Shohei Anno3, Tatsuya Koike4 and Hiroaki Nakamura2, 1Baba Memorial Hospital, Osaka, Japan, 2Osaka Metropolitan University, Osaka, Japan, 3Yodogawa Christian Hospital, Osaka, Japan, 4Search Institute for Bone and Arthritis Disease (SINBAD), Shirahama Foundation for Health and Welfare, Shirahama, Japan

Background/Purpose: Although biologics (BIO) or Janus kinase inhibitors (JAKi) have improved treatment for rheumatoid arthritis (RA), there are patients with difficult disease activity control even after using several BIO/JAKi, that is difficult-to-treat rheumatoid arthritis (D2TRA). D2TRA can be divided to two groups by mechanism: persistent inflammatory refractory RA (PIRRA) and non-inflammatory refractory RA with only persistent pain (NIRRA). We investigated these two different types of D2TRA.

Methods: Total of 147 patients switched to another BIO/JAKi because of inadequate response to previous BIO/JAKi and considered as D2TRA in our institution as of 2021. Patients with negative CRP and tender joint count > swollen joint count was defined as NIRRA, otherwise was defined as PIRRA. We investigated clinical characteristics and efficacy of following BIO/JAKi in both types of D2TRA for 52 weeks.

Results: Compared to NIRRA (n=33), PIRRA (n=114) showed significantly low hemoglobin (12.9 vs 12.0, p=0.02) and high DAS28ESR (4.43 vs 5.25, p=0.003) at the time of switching (baseline). There was no significant difference in MMP3 and CDAI. Retention rate at 52w also showed no difference (51.5% vs 45.6%, p=0.48). MMP3 and CDAI significantly improved during 52w in NIRRA, whereas CRP, MMP3, DAS28ESR, CDAI, and HAQ significantly improved in PIRRA. Switched BIO/JAKi consisted of IL6 inhibitors (n=7) and JAKi (n=15) in NIRRA, IL6 inhibitors (n=24) and JAKi (n=70) in PIRRA. Efficacy of switched BIO/JAKi showed no difference regardless of mechanism in both NIRRA and PIRRA.

Conclusion: MMP3 and CDAI improved after switching both in NIRRA and PIRRA. This tendency was similar whichever following BIO/JAKi was IL6 inhibitors and JAKi. Switching BIO/JAKi was effective in both types of D2TRA.


The clinical characteristics and efficacy of BIO/JAKi after switching in two types of D2TRA


K. Onishi: None; Y. Yamada: None; T. Okano: None; K. Mamoto: None; S. Anno: None; T. Koike: None; H. Nakamura: None.