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免疫生物标志物与 BRAF 和非 BRAF V600 改变型肺癌对检查点抑制的反应。

Immune biomarkers and response to checkpoint inhibition of BRAF and BRAF non-V600 altered lung cancers.

机构信息

Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, NY, USA.

Department of Pharmacy, Memorial Sloan Kettering Cancer Center, New York, NY, USA.

出版信息

Br J Cancer. 2022 Apr;126(6):889-898. doi: 10.1038/s41416-021-01679-1. Epub 2021 Dec 28.

DOI:10.1038/s41416-021-01679-1
PMID:34963703
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8927094/
Abstract

BACKGROUND

While 2-4% of lung cancers possess alterations in BRAF, little is known about the immune responsiveness of these tumours.

METHODS

Clinical and genomic data were collected from 5945 patients with lung cancers whose tumours underwent next-generation sequencing between 2015 and 2018. Patients were followed through 2020.

RESULTS

In total, 127 patients with metastatic BRAF-altered lung cancers were identified: 29 tumours had Class I mutations, 59 had Class II/III alterations, and 39 had variants of unknown significance (VUS). Tumour mutation burden was higher in Class II/III than Class I-altered tumours (8.8 mutations/Mb versus 4.9, P < 0.001), but this difference was diminished when stratified by smoking status. The overall response rate to immune checkpoint inhibitors (ICI) was 9% in Class I-altered tumours and 26% in Class II/III (P = 0.25), with median time on treatment of 1.9 months in both groups. Among patients with Class I-III-altered tumours, 36-month HR for death in those who ever versus never received ICI was 1.82 (1.17-6.11). Nine patients were on ICI for >2 years (two with Class I mutations, two with Class II/III alterations, and five with VUS).

CONCLUSIONS

A subset of patients with BRAF-altered lung cancers achieved durable disease control on ICI. However, collectively no significant clinical benefit was seen.

摘要

背景

虽然 2-4%的肺癌存在 BRAF 改变,但对于这些肿瘤的免疫反应性知之甚少。

方法

收集了 5945 名接受了下一代测序的肺癌患者的临床和基因组数据,这些患者的肿瘤在 2015 年至 2018 年间进行了测序。患者的随访时间截至 2020 年。

结果

共发现 127 名转移性 BRAF 改变的肺癌患者:29 个肿瘤存在 I 类突变,59 个存在 II/III 类改变,39 个存在未知意义的变异(VUS)。II/III 类改变的肿瘤比 I 类改变的肿瘤具有更高的肿瘤突变负担(8.8 个突变/Mb 比 4.9 个突变/Mb,P<0.001),但在按吸烟状态分层时,这种差异减小。I 类改变的肿瘤对免疫检查点抑制剂(ICI)的总体反应率为 9%,而 II/III 类改变的肿瘤为 26%(P=0.25),两组的中位治疗时间均为 1.9 个月。在 I 类-III 类改变的肿瘤患者中,曾接受过与从未接受过 ICI 的患者的 36 个月死亡风险比为 1.82(1.17-6.11)。有 9 名患者接受 ICI 治疗>2 年(2 名 I 类突变患者,2 名 II/III 类改变患者,5 名 VUS 患者)。

结论

少数 BRAF 改变的肺癌患者接受 ICI 治疗后可获得持久的疾病控制。然而,总体上并未观察到显著的临床获益。

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