BRCA相关癌症中的种系-体细胞相互作用:将ATM与TP53合成必需性联系起来的独特分子特征和临床结果
Germline-Somatic Interactions in BRCA-Associated Cancers: Unique Molecular Profiles and Clinical Outcomes Linking ATM to TP53 Synthetic Essentiality.
作者信息
Arafa Ali T, Yadav Siddhartha, Marshall Catherine H, Mauer Elizabeth, Huang Minxuan, Yilma Binyam, van der Pol Ymke, Fragkogianni Stamatina, Teslow Emily A, Kellen Samuel, Boytim Ella, Luo Christine, Ludwig Megan, Zhang Weijie, Jayaraj Arockia, Armstrong Deborah K, Isaacs William B, Drake Justin M, Nguyen Hai Dang, Huang R Stephanie, Chao Calvin Y, Lou Emil, Dehm Scott M, Couch Fergus J, Hwang Justin H, Antonarakis Emmanuel S
机构信息
Masonic Cancer Center, University of Minnesota, Minneapolis, Minnesota.
Department of Pharmacology, University of Minnesota, Minneapolis, Minnesota.
出版信息
Clin Cancer Res. 2025 May 1;31(9):1730-1745. doi: 10.1158/1078-0432.CCR-24-2058.
PURPOSE
Germline alterations in homologous recombination repair (gHRR) genes affect the pathogenesis, treatment options, and survival of patients with cancer. However, distinct gHRR gene alterations may differentially affect treatment response and oncogenic signaling. In this study, we interrogated genomic and transcriptomic data and assessed clinical outcomes of patients with gHRR mutations across four BRCA-associated cancers (breast, ovarian, pancreatic, and prostate cancers) to identify therapeutic vulnerabilities.
EXPERIMENTAL DESIGN
We assessed 24,309 patients undergoing matched tumor/normal next-generation DNA and RNA sequencing. Annotated gHRR gene variants [germline BRCA1, germline BRCA2, germline PALB2, germline ATM (gATM), and germline CHEK2] were analyzed. HRs were used to assess survival outcomes comparing germline versus sporadic groups. Somatic alterations and their frequencies were compared across gHRR-altered groups. Differential gene expression and gene set enrichment analysis were used to compare transcriptomic profiles.
RESULTS
Somatic TP53 mutations were depleted in gATM carriers (P < 0.05) across all four BRCA-associated cancers by up to 2.5-fold. Tumors with germline BRCA1/2 mutations were associated with improved survival in patients with ovarian cancer and had consistent enrichment of TP53 mutations in all four cancers. gATM mutations displayed elevated p53 transcriptional activity in all four cancers, with significance reached in breast and prostate cancers (P < 0.01). In breast, ovarian, and prostate cancers, gATM tumors demonstrated significantly increased inflammatory pathways (P < 0.001). Finally, using gene dependency data, we found that cell lines that were highly dependent on ATM were co-dependent on canonical p53 function.
CONCLUSIONS
gATM-associated cancers seem to require intact p53 activity and this synthetic essentiality may be used to guide targeted therapies that perturb canonical TP53 function.
目的
同源重组修复(gHRR)基因的种系改变会影响癌症患者的发病机制、治疗选择和生存情况。然而,不同的gHRR基因改变可能对治疗反应和致癌信号传导产生不同影响。在本研究中,我们分析了基因组和转录组数据,并评估了四种与BRCA相关癌症(乳腺癌、卵巢癌、胰腺癌和前列腺癌)中gHRR突变患者的临床结局,以确定治疗弱点。
实验设计
我们评估了24309例接受肿瘤/正常组织配对的下一代DNA和RNA测序的患者。分析了注释的gHRR基因变异(种系BRCA1、种系BRCA2、种系PALB2、种系ATM(gATM)和种系CHEK2)。使用风险比(HRs)评估种系组与散发组的生存结局。比较了gHRR改变组之间的体细胞改变及其频率。采用差异基因表达和基因集富集分析来比较转录组图谱。
结果
在所有四种与BRCA相关的癌症中,gATM携带者的体细胞TP53突变减少(P<0.05),最多减少2.5倍。种系BRCA1/2突变的肿瘤与卵巢癌患者的生存期改善相关,并且在所有四种癌症中TP53突变均持续富集。gATM突变在所有四种癌症中均显示p53转录活性升高,在乳腺癌和前列腺癌中达到显著水平(P<0.01)。在乳腺癌、卵巢癌和前列腺癌中,gATM肿瘤的炎症途径显著增加(P<0.001)。最后,利用基因依赖性数据,我们发现高度依赖ATM的细胞系同时依赖于经典p53功能。
结论
与gATM相关的癌症似乎需要完整的p53活性,这种合成必需性可用于指导干扰经典TP53功能的靶向治疗。
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