Abstract 2193P
Background
In 1st-line setting in MPM CheckMate-743 trial demonstrated better outcomes for IT over chemotherapy in p with no-epithelioid histology. However, another trials (MAPS2, DREAM) demonstrated efficacy of IT in all tumors. The objective of this study is to characterize the impact of IT according to histology in p with MPM.
Methods
Clinical records of MPM p treated with IT (anti-PD1/L1) at Vall d´Hebron University Hospital were reviewed. Associations between clinical variables and outcome were assessed with multivariate time-dependent Cox regression models to adjust for inmortal-time bias and histology. Survival data were calculated by the Kaplan-Meier method.
Results
228 p were reviewed: median age 68 years (29-88), males: 70%, performance status (PS)1: 69%, epithelioid: 82%. Median overall survival (OS) of the entire cohort was 21.4 months (m) (CI95% 18-23.8). Epithelioid histology, PS 0, stage 1-2 and treatment with cisplatin were associated with significant improvements in OS (p<0.001). Thirty-six p (16%) were treated with antiPD1/L1 (13 p in 1st line, 23 p in 2nd or further lines). In the multivariable time-dependent model, both histology (HR=0.51) and exposure to IT (HR=0.66) had significant impact on OS (P-values <0.1). Patients with epithelioid tumors treated with anti-PD1/L1 at any line had a median OS of 33.1 m (vs 23.8 m for p without IT), while p with non-epithelioid tumors exposed to anti-PD1/L1 had median OS of 19.5 m (vs 14.1 m without IT). In p exposed to IT in 2nd or further lines, median OS for p with epithelioid tumors treated with IT was 24.2 m (vs 13.7 m in p without IT), and for non-epithelioid cases median OS was 6.6 m and 10.0 m for p treated with or without IT respectively.
Conclusions
In our series of real-word MPM treated with IT we did demonstrate a benefit of IT for MPM p. Considering the prognostic effect of histology and the potential immortal time bias for IT exposure, we demonstrated improved OS for p receiving IT with a trend of higher benefit in epithelioid tumors. Ongoing studies combining checkpoint inhibitors plus chemotherapy are evaluating the impact of histology in the outcomes.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
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