Therapeutic Implications of Germline Testing in Patients With Advanced Cancers

PALB2 支票2 生殖系 医学 种系突变 基因型 卵巢癌 肿瘤科 PARP抑制剂 内科学 癌症 乳腺癌 遗传性癌症 基因检测 疾病 基因 突变 遗传学 生物 聚合酶 聚ADP核糖聚合酶
作者
Zsofia K. Stadler,Anna Maio,Debyani Chakravarty,Yelena Kemel,Margaret Sheehan,Erin Salo‐Mullen,Kaitlyn Tkachuk,Christopher J. Fong,Bastien Nguyen,Amanda Erakky,Karen A. Cadoo,Ying L. Liu,Maria I. Carlo,Alicia Latham,Hongxin Zhang,Ritika Kundra,Shaleigh Smith,Jesse Galle,Carol Aghajanian,Nadeem R. Abu‐Rustum,Anna M. Varghese,Eileen Mary O'Reilly,Michael J. Morris,Wassim Abida,Michael F. Walsh,Alexander Drilon,Gowtham Jayakumaran,Ahmet Zehir,Marc Ladanyi,Ozge Ceyhan‐Birsoy,David B. Solit,Nikolaus Schultz,Michael F. Berger,Diana Mandelker,Luis A. Díaz,Kenneth Offit,Mark E. Robson
出处
期刊:Journal of Clinical Oncology [American Society of Clinical Oncology]
卷期号:39 (24): 2698-2709 被引量:68
标识
DOI:10.1200/jco.20.03661
摘要

PURPOSE Tumor mutational profiling is increasingly performed in patients with advanced cancer. We determined the extent to which germline mutation profiling guides therapy selection in patients with advanced cancer. METHODS Patients with cancer undergoing tumor genomic profiling were prospectively consented for germline cancer predisposition gene analysis (2015-2019). In patients harboring germline likely pathogenic or pathogenic (LP/P) alterations, therapeutic actionability was classified using a precision oncology knowledge base. Patients with metastatic or recurrent cancer receiving germline genotype–directed therapy were determined. RESULTS Among 11,947 patients across > 50 malignancies, 17% (n = 2,037) harbored a germline LP/P variant. By oncology knowledge base classification, 9% (n = 1042) had an LP/P variant in a gene with therapeutic implications (4% level 1; 4% level 3B; < 1% level 4). BRCA1/2 variants accounted for 42% of therapeutically actionable findings, followed by CHEK2 (13%), ATM (12%), mismatch repair genes (11%), and PALB2 (5%). When limited to the 9,079 patients with metastatic or recurrent cancer, 8% (n = 710) harbored level 1 or 3B genetic findings and 3.2% (n = 289) received germline genotype–directed therapy. Germline genotype–directed therapy was received by 61% and 18% of metastatic cancer patients with level 1 and level 3B findings, respectively, and by 54% of BRCA1/2, 75% of mismatch repair, 43% of PALB2, 35% of RAD51C/D, 24% of BRIP1, and 19% of ATM carriers. Of BRCA1/2 patients receiving a poly(ADP-ribose) polymerase inhibitor, 45% (84 of 188) had tumors other than breast or ovarian cancer, wherein the drug, at time of delivery, was delivered in an investigational setting. CONCLUSION In a pan-cancer analysis, 8% of patients with advanced cancer harbored a germline variant with therapeutic actionability with 40% of these patients receiving germline genotype–directed treatment. Germline sequence analysis is additive to tumor sequence analysis for therapy selection and should be considered for all patients with advanced cancer.
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