Detection of ALK fusion variants by RNA-based NGS and clinical outcome correlation in NSCLC patients treated with ALK-TKI sequences

克里唑蒂尼 间变性淋巴瘤激酶 铈替尼 肺癌 医学 肿瘤科 靶向治疗 融合基因 癌症 内科学 生物 基因 生物化学 恶性胸腔积液
作者
Fabrizio Tabbò,Lucia Anna Muscarella,Élisa Gobbini,Domenico Trombetta,Stefano Castellana,Angelica Rigutto,Domenico Galetta,Evaristo Maiello,Olga Martelli,Marcello Tiseo,Vieri Scotti,Laura Ghilardi,Vanesa Gregorc,Concetta Sergi,Sara Pilotto,Alessandro Del Conte,Federico Cappuzzo,Diego Cortinovis,Giorgia Osman,Claudia Bareggi
出处
期刊:European Journal of Cancer [Elsevier BV]
卷期号:174: 200-211 被引量:12
标识
DOI:10.1016/j.ejca.2022.07.026
摘要

Abstract

Introduction

Anaplastic lymphoma kinase (ALK) fusions identify a limited subset of non–small cell lung cancer (NSCLC) patients, whose therapeutic approach have been radically changed in recent years. However, diagnostic procedures and clinical-radiological responses to specific targeted therapies remain heterogeneous and intrinsically resistant or poor responder patients exist.

Methods

A total of 290 patients with advanced NSCLC defined as ALK+ by immunohistochemistry (IHC) and/or fluorescent in situ hybridisation (FISH) test and treated with single or sequential multiple ALK inhibitors (ALKi) from 2011 to 2017 have been retrospectively retrieved from a multicentre Italian cancer network database. In 55 patients with enough leftover tumour tissue, specimens were analysed with both targeted and customised next generation sequencing panels. Identified fusion variants have been correlated with clinical outcomes.

Results

Of the 55 patients, 24 received crizotinib as first-line therapy, 1 received ceritinib, while 30 received chemotherapy. Most of the patients (64%) received ALKi in sequence. An ALK fusion variant was identified in 73% of the cases, being V3 variant (E6A20) the most frequent, followed by V1 (E13A20) and more rare ones (e.g. E6A19). In three specimens, four new EML4-ALK fusion breakpoints have been reported. Neither fusion variants nor brain metastases were significantly associated with overall survival (OS), while it was predictably longer in patients receiving a sequence of ALKi. The presence of V1 variant was associated with progression-free survival (PFS) improvement when crizotinib was used (p = 0.0073), while it did not affect cumulative PFS to multiple ALKi.

Conclusion

Outcomes to sequential ALKi administration were not influenced by fusion variants. Nevertheless, in V1+ patients a prolonged clinical benefit was observed. Fusion variant identification by NGS technology may add relevant information about rare chromosomal events that could be potentially correlated to worse outcomes.
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