肿瘤突变负荷在非小细胞肺癌中具有部位特异性，且在肺腺癌脑转移中最高。

Tumor Mutational Burden Is Site Specific in Non-Small-Cell Lung Cancer and Is Highest in Lung Adenocarcinoma Brain Metastases.

作者信息

Stein Matthew K, Pandey Manjari, Xiu Joanne, Tae Hongseok, Swensen Jeff, Mittal Sandeep, Brenner Andrew J, Korn W Michael, Heimberger Amy B, Martin Mike G

机构信息

West Cancer Center, University of Tennessee Health Science Center, Memphis, TN.

Caris Life Science, Phoenix, AZ.

出版信息

JCO Precis Oncol. 2019 Dec;3:1-13. doi: 10.1200/PO.18.00376.

DOI:10.1200/PO.18.00376

PMID:35100709

Abstract

PURPOSE

Tumor mutational burden (TMB) is a developing biomarker in non-small-cell lung cancer (NSCLC). Little is known regarding differences between TMB and sample location, histology, or other biomarkers.

METHODS

A total of 3,424 unmatched NSCLC samples, including 2,351 lung adenocarcinomas (LUADs) and 1,073 lung squamous cell carcinomas (LUSCs), underwent profiling, including next-generation sequencing of 592 cancer-related genes, programmed death ligand 1 immunohistochemistry, and TMB. The rate TMB of 10 mutations per megabase (Mb) or greater was compared between primary and metastatic LUAD and LUSC. Molecular alteration frequency was compared at a cutoff of 10 mutations/Mb.

RESULTS

LUAD metastases were more likely to have a TMB of 10 mutations/Mb or greater compared with primary LUADs (38% 25%; < .001), and this difference was most pronounced with brain metastases (61% 35% for other metastases; < .001). The median TMB for LUAD brain metastases was 13 mutations/Mb compared with six mutations/Mb for primary LUADs. Variability existed for other LUAD metastasis sites, with adrenal metastases most likely to meet the cutoff of 10 mutations/Mb (51%) and bone metastases least likely to meet the cutoff (19%). TMB was more commonly 10 mutations/Mb or greater for LUSC primary tumors than for LUAD primary tumors (35% 25%, respectively; < .001). LUSC metastases were more likely to have a TMB of 10 mutations/Mb or greater than LUSC primary tumors. Poorly differentiated disease was more likely have a TMB of 10 mutations/Mb or greater when stratified by histology and primary tumor or metastasis. Site-specific molecular differences existed at this TMB cutoff including programmed death ligand 1 positivity and and mutation rate.

CONCLUSION

TMB is a site-specific biomarker in NSCLC with important spatial and histologic differences. TMB is more frequently 10 mutations/Mb or greater in LUAD and LUSC metastases and highest in LUAD brain metastases. Along this TMB cutoff, clinically informative distinctions exist in other tumor profiling characteristics. Further investigation is needed to expand on these findings.

摘要

目的

肿瘤突变负荷（TMB）是一种正在发展的非小细胞肺癌（NSCLC）生物标志物。关于TMB与样本位置、组织学或其他生物标志物之间的差异，目前所知甚少。

方法

共对3424份不匹配的NSCLC样本进行分析，其中包括2351例肺腺癌（LUAD）和1073例肺鳞状细胞癌（LUSC），分析内容包括对592个癌症相关基因进行二代测序、程序性死亡配体1免疫组化以及TMB检测。比较原发性和转移性LUAD及LUSC中TMB≥10个突变/Mb的比例。分子改变频率以10个突变/Mb为界值进行比较。

结果

与原发性LUAD相比，LUAD转移灶更有可能出现TMB≥10个突变/Mb（38%对25%；P<0.001），这种差异在脑转移中最为明显（脑转移为61%，其他转移为35%；P<0.001）。LUAD脑转移灶的TMB中位数为13个突变/Mb，而原发性LUAD为6个突变/Mb。其他LUAD转移部位存在差异，肾上腺转移最有可能达到10个突变/Mb的界值（51%），骨转移最不可能达到该界值（19%）。LUSC原发性肿瘤的TMB≥10个突变/Mb比LUAD原发性肿瘤更常见（分别为35%和25%；P<0.001）。LUSC转移灶比LUSC原发性肿瘤更有可能出现TMB≥10个突变/Mb。当按组织学以及原发性肿瘤或转移灶分层时，低分化疾病更有可能出现TMB≥10个突变/Mb。在该TMB界值处存在部位特异性分子差异，包括程序性死亡配体1阳性以及某些基因突变率。