Nivolumab (NIVO) plus ipilimumab (IPI) vs chemotherapy (chemo) or NIVO monotherapy for microsatellite instability-high/mismatch repair-deficient (MSI-H/dMMR) metastatic colorectal cancer (mCRC): Expanded analyses from CheckMate 8HW.

无容量 医学 易普利姆玛 结直肠癌 微卫星不稳定性 内科学 肿瘤科 化疗 癌症 免疫疗法 生物化学 微卫星 基因 等位基因 化学
作者
Heinz‐Josef Lenz,Sara Lonardi,Elena Élez,Lars Henrik Jensen,Eric Van Cutsem,Yann Touchefeu,Rocio García‐Carbonero,David Tougeron,Guillermo Méndez,Michael Schenker,Christelle de la Fouchardière,María Luisa Limón,Takayuki Yoshino,Jin Li,F. Aubin,Elvis Cela,Li Li,Rachel Tam,Lixian Jin,Thierry André
出处
期刊:Journal of Clinical Oncology [Lippincott Williams & Wilkins]
卷期号:43 (16_suppl): 3501-3501 被引量:3
标识
DOI:10.1200/jco.2025.43.16_suppl.3501
摘要

3501 Background: In the phase 3 CheckMate 8HW study (NCT04008030), both dual primary endpoints of progression-free survival (PFS) for first-line (1L) NIVO + IPI vs chemo (HR 0.21; P < 0.0001) and NIVO + IPI vs NIVO across all lines (HR 0.62; P = 0.0003) in patients (pts) with centrally confirmed MSI-H/dMMR mCRC were met. We report expanded analyses of NIVO + IPI vs NIVO (all lines) and longer follow-up results for NIVO + IPI vs chemo (1L). Methods: The study design was described previously. Pts with MSI-H/dMMR per local testing were enrolled. After randomization, IHC and PCR based tests were used for central confirmation. PFS2 (time from randomization to progression after subsequent systemic therapy, start of second subsequent systemic therapy, or death) was a key exploratory endpoint. Results: In all randomized pts (all lines), 296 of 354 (84%) in the NIVO + IPI arm, 286 of 353 (81%) in the NIVO arm, and 113 of 132 (86%) in the chemo arm had centrally confirmed MSI-H/dMMR. In all randomized 1L pts, 171 of 202 (85%) in the NIVO + IPI arm and 84 of 101 (83%) in the chemo arm had centrally confirmed MSI-H/dMMR. Median follow-up was 47.0 mo (range 16.7–60.5). 1L NIVO + IPI continued to show PFS benefit vs chemo (Table). Subsequent systemic therapy was received by 27 (16%) and 61 (73%) pts after 1L NIVO + IPI and chemo, respectively; 10 (6%) and 21 (25%) received subsequent non-study immunotherapy. In the 1L chemo arm, 39 (46%) pts crossed over to NIVO + IPI on study. PFS2 continued to favor 1L NIVO + IPI vs chemo (Table). Across all lines, NIVO + IPI demonstrated superior PFS vs NIVO (Table). Subsequent systemic therapy was received by 54 (18%) pts in the NIVO + IPI arm and 83 (29%) in the NIVO arm; 20 (7%) and 31 (11%) received subsequent non-study immunotherapy. PFS2 favored NIVO + IPI vs NIVO across all lines of therapy (Table). In all treated pts, grade 3/4 treatment-related adverse events occurred in 78 (22%) and 50 (14%) pts in the NIVO + IPI and NIVO arms, respectively. Additional analyses will be presented. Conclusions: NIVO + IPI demonstrated sustained clinical benefit vs chemo (1L) and NIVO (all lines) despite use of subsequent therapy, as shown by improved PFS2 in pts with centrally confirmed MSI-H/dMMR mCRC. No new safety signals were observed. These results support NIVO + IPI as a standard of care treatment for MSI-H/dMMR mCRC. Clinical trial information: NCT04008030 . Centrally confirmed MSI-H/dMMR (1L) NIVO + IPI(n = 171) Chemo(n = 84) Median PFS (95% CI), mo 54.1 (54.1–NE) 5.9 (4.4–7.8) HR (95% CI) 0.21 (0.14–0.31) Median PFS2 (95% CI), mo NR (NE–NE) 30.3 (15.2–NE) HR (95% CI) 0.28 (0.18–0.44) Centrally confirmed MSI-H/dMMR (all lines) NIVO + IPI (n = 296) NIVO (n = 286) Median PFS (95% CI), mo NR (53.8–NE) 39.3 (22.1–NE) HR (95% CI) 0.62 (0.48-0.81); P = 0.0003 Median PFS2 (95% CI), mo NR (NE–NE) NR (NE–NE) HR (95% CI) 0.57 (0.42–0.78) NE, not evaluable; NR, not reached.
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