Survival outcomes of patients with metastatic non-small cell lung cancer receiving chemotherapy or immunotherapy as first-line in a real-life setting

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作者
Yaniss Belaroussi
Fanny Bouteiller
Carine Bellera
David Pasquier
Maurice Perol
Didier Debieuvre
Thomas Filleron
Nicolas Girard
Roland Schott
Simone Mathoulin-Pélissier
Anne-Laure Martin
Sophie Cousin
机构
[1] Univ. Bordeaux,UMR 1219
[2] Bordeaux Population Health Research Center,Inserm CIC1401, Clinical and Epidemiological Research Unit
[3] Epicene Team,Radiotherapy Department
[4] Institut Bergonié,Chest Disease Department
[5] Comprehensive Cancer Center,Medical Oncology Department
[6] Centre Oscar Lambret,Early Phase Trials Unit, Department of Medical Oncology
[7] Medical Oncology Department,undefined
[8] Centre Léon Bérard,undefined
[9] GHRMSA,undefined
[10] Biostatistic and Health Data Science Unit,undefined
[11] Institut Claudius Régaud IUTC-O,undefined
[12] Institut du Thorax Curie-Montsouris,undefined
[13] Medical Oncology Department,undefined
[14] Institut de Cancérologie Strasbourg Europe,undefined
[15] Health Data and Partnership Department,undefined
[16] Unicancer,undefined
[17] Institut Bergonié,undefined
[18] Comprehensive Cancer Center,undefined
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Treatment of metastatic non-small cell lung cancer (mNSCLC) has been modified due to the development of immunotherapy. We assessed survival outcomes (overall [OS] and progression-free [rwPFS] survivals, time-to-next-treatment [TNT]) in mNSCLC patients after first-line immunotherapy and chemotherapy in real-life settings. Association between rwPFS and TNT, two candidate surrogate endpoints (SE), with OS was assessed. This retrospective multi-center study uses data from patients included in the Epidemio-Strategy Medico-Economic program with mNSCLC over 2015–2019. The impact of treatment on rwPFS/OS was evaluated with Cox models. Individual-level associations between SE and OS were estimated with an iterative multiple imputation approach and joint survival models. The population included 5294 patients (63 years median age). Median OS in immunotherapy group was 16.4 months (95%CI [14.1–NR]) and was higher than in chemotherapy group (11.6 months; 95%CI [11.0–12.2]). Improved OS was observed for the immunotherapy group after 3 months for subjects with performance status 0–1 (HR = 0.59; 95%CI [0.42–0.83], p < 0.01). The associations between rwPFS and TNT with OS were close (τ\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$\uptau$$\end{document}=0.57). Results emphasized a survival improvement with immunotherapy for patients in good health condition. There was moderate evidence of individual-level association between candidate SE and OS.
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