What question did this study set out to answer?

This study aims to investigate the clinicogenomic characteristics and treatment outcomes of advanced ALK+ squamous and adenosquamous non-small cell lung cancers.

April 1, 2026

Clinicogenomic Characteristics and Treatment Outcomes of Patients With Advanced ALK -Rearranged Squamous and Adenosquamous Non–Small Cell Lung Cancers

Puntos clave

This study aims to investigate the clinicogenomic characteristics and treatment outcomes of advanced ALK+ squamous and adenosquamous non-small cell lung cancers.
Conducted a multi-institutional retrospective analysis
Compared advanced ALK+ squamous and adenosquamous NSCLCs with ALK+ adenocarcinoma
Analyzed overall survival, time to progression, and time to treatment discontinuation using Kaplan-Meier methodology
Among 177 patients, 29 had squamous or adenosquamous NSCLCs
Overall survival was significantly shorter for squamous (27.0 months) and adenosquamous (31.0 months) compared to adenocarcinoma (median not reached)
Time to progression was shorter for squamous (8.0 months) compared to adenocarcinoma (19.0 months)
Genomic profiling showed more frequent TP53 and other coalterations in squamous/adenosquamous cohort

Resumen

PURPOSE Anaplastic lymphoma kinase (ALK) is an established therapeutic target in non–small cell lung cancer (NSCLC), predominantly identified in adenocarcinomas. However, ALK rearrangements also occur in de novo squamous and adenosquamous NSCLCs and their clinicogenomic features remain poorly defined. METHODS This multi-institutional retrospective analysis included patients with advanced ALK+ NSCLC. Patients with de novo ALK+ squamous and adenosquamous NSCLCs were identified and compared with an ALK+ adenocarcinoma cohort treated with first-line (1L) alectinib. Overall survival (OS), time to progression (TTP), and time to treatment discontinuation (TTD) were analyzed using the Kaplan-Meier methodology. RESULTS Among 177 patients, 29 had ALK+ squamous (n = 17) and adenosquamous (n = 12) NSCLCs and 148 had ALK+ adenocarcinoma treated with 1L alectinib. Among patients receiving 1L alectinib, OS was significantly shorter for patients with adenosquamous (median, 31. 0 months 95% CI, 17. 0 to not reached NR) and squamous (27. 0 months 95% CI, 5. 0 to 35. 0) tumors compared with that for patients with adenocarcinoma (median NR; median follow-up 51. 2 months; P <. 001). TTP was shorter for squamous (median, 8. 0 months 95% CI, 2. 0 to 12. 0) versus adenocarcinoma (median, 19. 0 months 95% CI, 12. 6 to 25. 0) cohorts (P <. 001), although the adenosquamous cohort had comparable TTP (median, 20. 0 months 95% CI, 9. 4 to 30. 6) with the adenocarcinoma cohort (P =. 70). TTD was significantly shorter for squamous (median, 9. 5 months 95% CI, 1. 5 to 13. 0) and adenosquamous (median, 20. 0 months 95% CI, 3. 0 to 24. 0) versus adenocarcinoma cohorts (52. 3 months 95% CI, 40. 5 to 57. 5; P <. 001). Genomic profiling revealed more frequent TP53 (53% v 25%; P =. 026), PDGFRA (16% v 0%; P =. 009), KIT (11% v 0%; P =. 045), PIK3CA (11% v 0%; P =. 045), and MYC (11% v 0%; P =. 045) coalterations in the squamous/adenosquamous cohort. CONCLUSION ALK+ squamous and adenosquamous NSCLCs are rare, but biologically distinct, with inferior outcomes on 1L ALK TKI, highlighting the need for further research to develop effective treatment strategies.

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Clinicogenomic Characteristics and Treatment Outcomes of Patients With Advanced ALK -Rearranged Squamous and Adenosquamous Non–Small Cell Lung Cancers

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