Clinical study of genomic drivers in pancreatic ductal adenocarcinoma

被引:29
作者
Barrett, Michael T. [1 ]
Deiotte, Ray [2 ]
Lenkiewicz, Elizabeth [1 ]
Malasi, Smriti [1 ]
Holley, Tara [1 ]
Evers, Lisa [1 ]
Posner, Richard G. [3 ,4 ]
Jones, Timothy [2 ]
Han, Haiyong [4 ]
Sausen, Mark [5 ]
Velculescu, Victor E. [5 ]
Drebin, Jeffrey [6 ]
O'Dwyer, Peter [6 ]
Jameson, Gayle [7 ]
Ramanathan, Ramesh K. [8 ]
Von Hoff, Daniel D. [4 ,7 ]
机构
[1] Mayo Clin Arizona, Scottsdale, AZ 85259 USA
[2] ISSAC Corp, Colorado Springs, CO 80919 USA
[3] No Arizona Univ, Flagstaff, AZ 86011 USA
[4] Translat Genom Res Inst, Phoenix, AZ 85004 USA
[5] Johns Hopkins Univ, Baltimore, MD 21218 USA
[6] Univ Penn, Philadelphia, PA 19104 USA
[7] Honor Hlth, Virginia G Piper Canc Ctr, Scottsdale, AZ 85258 USA
[8] Mayo Clin, Canc Ctr, Phoenix, AZ 85054 USA
来源
BRITISH JOURNAL OF CANCER | 2017年 / 117卷 / 04期
关键词
pancreatic cancer; flow sorting; CNVs; homozygous deletions; focal amplicons; KRAS mutations; CYCLIN-DEPENDENT KINASES; ADJUVANT CHEMOTHERAPY; CANCER; GEMCITABINE; SUBTYPES; TUMOR; CDK6; PROGRESSION; INHIBITION; SURVIVAL;
D O I
10.1038/bjc.2017.209
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: Pancreatic ductal adenocarcinoma (PDA) is a lethal cancer with complex genomes and dense fibrotic stroma. This study was designed to identify clinically relevant somatic aberrations in pancreatic cancer genomes of patients with primary and metastatic disease enrolled and treated in two clinical trials. Methods: Tumour nuclei were flow sorted prior to whole genome copy number variant (CNV) analysis. Targeted or whole exome sequencing was performed on most samples. We profiled biopsies from 68 patients enrolled in two Stand Up to Cancer (SU2C)sponsored clinical trials. These included 38 resected chemoradiation naive tumours (SU2C 20206-003) and metastases from 30 patients who progressed on prior therapies (SU2C 20206-001). Patient outcomes including progression-free survival (PFS) and overall survival (OS) were observed. Results: We defined: (a) CDKN2A homozygous deletions that included the adjacent MTAP gene, only its' 30 region, or excluded MTAP; (b) SMAD4 homozygous deletions that included ME2; (c) a pancreas-specific MYC super-enhancer region; (d) DNA repair-deficient genomes; and (e) copy number aberrations present in PDA patients with long-term (>= 40 months) and short-term (<= 12 months) survival after surgical resection. Conclusions: We provide a clinically relevant framework for genomic drivers of PDA and for advancing novel treatments.
引用
收藏
页码:572 / 582
页数:11
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