Sustainability of response to upadacitinib as monotherapy or in combination among patients with rheumatoid arthritis and prior inadequate response to conventional synthetic dmards

Kavanaugh, Arthur; Buch, Maya; Combe, Bernard; Bessette, Louis; Song, In-Ho; Song, Yanna; Suboticki, Jessica; Nash, Peter

Author(s)

Kavanaugh, Arthur

Buch, Maya

Combe, Bernard

Bessette, Louis

Song, In-Ho

Song, Yanna

Suboticki, Jessica

Nash, Peter

Griffith University Author(s)

Nash, Peter

Year published

2021

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Abstract

Aim: To assess long-term sustainability of responses to upadacitinib (UPA), a JAK inhibitor, with or without background csDMARD(s) in patients (pts) with rheumatoid arthritis (RA). Methods: Data are from two phase 3 trials of UPA in RA pts: SELECT-NEXT enrolled pts with inadequate response (IR) to csDMARD(s) on background stable csDMARD(s) receiving UPA 15 or 30 mg once daily or placebo for 12 wks; SELECT-MONOTHERAPY enrolled methotrexate (MTX)-IR pts receiving UPA 15 or 30 mg monotherapy or blinded MTX for 14 wks. After 12/14 wks, pts could receive UPA 15 or 30 mg up to 5 years in a blinded long-term extension. This post ...
View more >Aim: To assess long-term sustainability of responses to upadacitinib (UPA), a JAK inhibitor, with or without background csDMARD(s) in patients (pts) with rheumatoid arthritis (RA). Methods: Data are from two phase 3 trials of UPA in RA pts: SELECT-NEXT enrolled pts with inadequate response (IR) to csDMARD(s) on background stable csDMARD(s) receiving UPA 15 or 30 mg once daily or placebo for 12 wks; SELECT-MONOTHERAPY enrolled methotrexate (MTX)-IR pts receiving UPA 15 or 30 mg monotherapy or blinded MTX for 14 wks. After 12/14 wks, pts could receive UPA 15 or 30 mg up to 5 years in a blinded long-term extension. This post hoc analysis evaluated clinical remission (REM:CDAI ≤2.8; SDAI ≤3.3), low disease activity (LDA:CDAI≤10; SDAI≤11), and DAS28(CRP) < 2.6/≤3.2 at first occurrence before Wk 84. Results: Through Wk 84, CDAI REM/LDA was achieved in 43%/79% of pts receiving UPA 15 mg with background csDMARD(s) (SELECT-NEXT) and 37%/76% without background csDMARD(s) (SELECT-MONOTHERAPY). 35%/25% of pts randomised to UPA 15 mg with background csDMARD(s) and 27%/23% without background csDMARD(s) achieved sustained CDAI REM through 6/12 months after first occurrence. 64%/56% of pts randomised to UPA 15 mg with background csDMARD(s) and 61%/56% without background csDMARD(s) achieved sustained CDAI LDA through 6/12 months after first occurrence. Time to initial clinical REM/LDA did not appear to be associated with sustained disease control. Similar results were observed across other disease activity measures (SDAI REM/LDA and DAS28(CRP) < 2.6/≤3.2). Conclusion: More than a quarter and more than a half of pts with RA and prior IR to csDMARD(s) receiving UPA with or without background csDMARD therapy achieved sustained clinical REM and LDA, respectively, across disease activity measures. Sustainability of responses appeared comparable among pts receiving UPA with or without background csDMARDs through up to 84 wks.
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