Molecular analysis of lung adenocarcinomas from the SAFIR02-Lung cohort reveals new metastasis-associated copy-number alterations including frequent mutant-specific KRAS-allelic imbalance and identifies CDKN2A homozygous deletions as an independent biomarker of poor prognosis.

IF 6.8 1区医学 Q1 ONCOLOGY

British Journal of Cancer Pub Date : 2025-09-11 DOI:10.1038/s41416-025-03183-2

Abderaouf Hamza, Pierre Gestraud, Maryam Karimi, Alicia Tran-Dien, Laurène Syx, Sophie Vacher, Quentin Peretti, Ludovic Lacroix, Valery Attignon, Isabelle Soubeyran, Pascal Jézéquel, David Planchard, Samia Melaabi, Trenton Dailey-Chwalibóg, Marta Jimenez, Stefan Michiels, Nicolas Servant, Christophe Le Tourneau, Nicolas Girard, Fabrice André, Benjamin Besse, Maud Kamal, Fabrice Barlesi, Ivan Bièche

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引用次数: 0

Abstract

Background: Identifying molecular alterations specific to advanced lung adenocarcinomas could provide insights into tumour progression and dissemination mechanisms.

Method: We analysed tumour samples, either from locoregional lesions or distant metastases, from patients with advanced lung adenocarcinoma from the SAFIR02-Lung trial by targeted sequencing of 45 cancer genes and comparative genomic hybridisation array and compared them to early tumours samples from The Cancer Genome Atlas.

Results: Differences in copy-number alterations frequencies suggest the involvement in tumour progression of LAMB3, TNN/KIAA0040/TNR, KRAS, DAB2, MYC, EPHA3 and VIPR2, and in metastatic dissemination of AREG, ZNF503, PAX8, MMP13, JAM3, and MTURN. Conversely, no meaningful difference was found in pathogenic single-nucleotide variant frequencies, reinforcing the notion that they are early events in tumorigenesis. CDKN2A homozygous deletion was linked to poor clinical outcome in patients with early tumours (overall survival hazard ratio 2.17, 95% CI: 1.43-3.28, corrected p-value = 0.01). Furthermore, we found that KRAS mutant allele specific imbalance, i.e. focal amplification of the mutant allele, is more prevalent in locoregional or distant samples of metastatic patients than in early lesions (8.4%, 13% and 2.8% respectively). This observation was replicated in three public cohorts. Tumours with KRAS mutant allele specific imbalance show specific patterns of co-occurrence and mutual exclusion with alterations in key cancer genes like CDKN2A, TP53, STK11 and NKX2-1, often in a tumour type dependent manner.

Conclusion: Advanced LUAD tumours exhibit higher copy-number alteration burden, with distinct alterations associated with tumour progression and metastasis. CDKN2A homozygous deletions predict poor prognosis in early disease, while KRAS mutant allele-specific imbalance is enriched in advanced tumours.

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来自SAFIR02-Lung队列的肺腺癌分子分析揭示了新的转移相关拷贝数改变，包括频繁的突变特异性kras等位基因失衡，并将CDKN2A纯合缺失确定为预后不良的独立生物标志物。

背景：识别晚期肺腺癌特异性的分子改变可以为肿瘤进展和传播机制提供见解。方法：我们对来自SAFIR02-Lung试验的晚期肺腺癌患者的肿瘤样本，无论是局部病变还是远处转移，通过45个癌症基因的靶向测序和比较基因组杂交阵列进行分析，并将其与来自癌症基因组图谱的早期肿瘤样本进行比较。结果：拷贝数改变频率的差异提示LAMB3、TNN/KIAA0040/TNR、KRAS、DAB2、MYC、EPHA3和VIPR2参与肿瘤进展，以及AREG、ZNF503、PAX8、MMP13、JAM3和MTURN的转移性传播。相反，在致病性单核苷酸变异频率上没有发现有意义的差异，这加强了它们是肿瘤发生早期事件的概念。CDKN2A纯合子缺失与早期肿瘤患者临床预后差有关（总生存风险比2.17,95% CI: 1.43-3.28，校正p值= 0.01）。此外，我们发现KRAS突变等位基因特异性失衡，即突变等位基因的局部扩增，在转移患者的局部或远处样本中比在早期病变中更为普遍（分别为8.4%，13%和2.8%）。这一观察结果在三个公共队列中得到了重复。KRAS突变等位基因特异性失衡的肿瘤与CDKN2A、TP53、STK11和NKX2-1等关键癌症基因的改变显示出共同发生和相互排斥的特定模式，通常以肿瘤类型依赖的方式发生。结论：晚期LUAD肿瘤表现出较高的拷贝数改变负担，与肿瘤进展和转移相关。CDKN2A纯合缺失在早期疾病中预测预后不良，而KRAS突变等位基因特异性失衡在晚期肿瘤中富集。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

British Journal of Cancer 医学-肿瘤学

CiteScore

15.10

自引率

1.10%

发文量

383

审稿时长

6 months

期刊介绍： The British Journal of Cancer is one of the most-cited general cancer journals, publishing significant advances in translational and clinical cancer research.It also publishes high-quality reviews and thought-provoking comment on all aspects of cancer prevention,diagnosis and treatment.