Efficacy of NSCLC Rechallenge with Immune Checkpoint Inhibitors following Disease Progression or Relapse

Immune checkpoint inhibitors (ICIs) are at the forefront of advanced non-small-cell lung cancer (NSCLC) treatment. Still, only 27-46% of patients respond to initial therapy with ICIs, and of those, up to 65% develop resistance within four years. After disease progression (PD), treatment options are...

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Veröffentlicht in:	Cancers 2024-03, Vol.16 (6), p.1196
Hauptverfasser:	Livanou, Maria Effrosyni, Nikolaidou, Vasiliki, Skouras, Vasileios, Fiste, Oraianthi, Kotteas, Elias
Format:	Artikel
Sprache:	eng
Schlagworte:	Analysis Biology Cancer Cancer therapies Chemotherapy Clinical trials Development and progression Disease control FDA approval Immune checkpoint inhibitors Immunotherapy Lung cancer Lung cancer, Non-small cell Medical research Medicine, Experimental Non-small cell lung carcinoma Patients Review Small cell lung carcinoma Toxicity Tumors
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creator	Livanou, Maria Effrosyni Nikolaidou, Vasiliki Skouras, Vasileios Fiste, Oraianthi Kotteas, Elias
description	Immune checkpoint inhibitors (ICIs) are at the forefront of advanced non-small-cell lung cancer (NSCLC) treatment. Still, only 27-46% of patients respond to initial therapy with ICIs, and of those, up to 65% develop resistance within four years. After disease progression (PD), treatment options are limited, with 10% Objective Response Rate (ORR) to second or third-line chemotherapy. In this context, ICI rechallenge is an appealing option for NSCLC. Most data on the efficacy of ICI rechallenge are based on retrospective real-world studies of small, heavily pretreated, and heterogeneous patient groups. Despite these limitations, these studies suggest that ICI monotherapy rechallenge in unselected NSCLC patient populations who discontinued initial ICI due to PD is generally ineffective, with a median Progression-Free Survival (PFS) of 1.6-3.1 months and a Disease Control Rate (DCR) of 21.4-41.6%. However, there is a subpopulation that benefits from this strategy, and further characterization of this subgroup is essential. Furthermore, immunotherapy rechallenge in patients who discontinued initial immunotherapy following treatment protocol completion and progressed after an immunotherapy-free interval showed promising efficacy, with a DCR of 75-81%, according to post hoc analyses of several clinical trials. Future research on ICI rechallenge for NSCLC should focus on better patient stratification to reflect the underlying biology of immunotherapy resistance more accurately. In this review, we summarize evidence regarding rechallenge immunotherapy efficacy following NSCLC disease progression or relapse, as well as ongoing trials on immunotherapy rechallenge.
doi_str_mv	10.3390/cancers16061196
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Furthermore, immunotherapy rechallenge in patients who discontinued initial immunotherapy following treatment protocol completion and progressed after an immunotherapy-free interval showed promising efficacy, with a DCR of 75-81%, according to post hoc analyses of several clinical trials. Future research on ICI rechallenge for NSCLC should focus on better patient stratification to reflect the underlying biology of immunotherapy resistance more accurately. 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Furthermore, immunotherapy rechallenge in patients who discontinued initial immunotherapy following treatment protocol completion and progressed after an immunotherapy-free interval showed promising efficacy, with a DCR of 75-81%, according to post hoc analyses of several clinical trials. Future research on ICI rechallenge for NSCLC should focus on better patient stratification to reflect the underlying biology of immunotherapy resistance more accurately. 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subjects	Analysis Biology Cancer Cancer therapies Chemotherapy Clinical trials Development and progression Disease control FDA approval Immune checkpoint inhibitors Immunotherapy Lung cancer Lung cancer, Non-small cell Medical research Medicine, Experimental Non-small cell lung carcinoma Patients Review Small cell lung carcinoma Toxicity Tumors
title	Efficacy of NSCLC Rechallenge with Immune Checkpoint Inhibitors following Disease Progression or Relapse
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