Exome Sequencing and Digital PCR Analyses Reveal Novel Mutated Genes Related to the Metastasis of Pancreatic Ductal Adenocarcinoma

Overview

Journal Cancer Biol Ther

Specialties Oncology
Pharmacology

Date 2012 Jul 17

PMID 22797009

Citations 20

Authors

Bin Zhou

Astrid Irwanto

Yun-Miao Guo

Jin-Xin Bei

Qiao Wu

Ge Chen

Tai-Ping Zhang

Jin-Jv Lei

Qi-Sheng Feng

Li-Zhen Chen

Jianjun Liu

Yu-Pei Zhao

Affiliations

Soon will be listed here.

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is one of the most malignant cancers with more than 94% mortality rate mainly due to the widespread metastases. To find out the somatically mutated genes related to the metastasis of PDAC, we analyzed the matched tumor and normal tissue samples from a patient diagnosed with liver metastatic PDAC using intensive exome capture-sequencing analysis (> 170× coverage). Searching for the somatic mutations that drive the clonal expansion of metastasis, we identified 12 genes with higher allele frequencies (AFs) of functional mutations in the metastatic tumor, including known genes KRAS and TP53 for metastasis. Of the 10 candidate genes, 6 (ADRB1, DCLK1, KCNH2, NOP14, SIGLEC1, and ZC3H7A), together with KRAS and TP53, were clustered into a single network (p value = 1 × 10(-22)) that is related to cancer development. Moreover, these candidate genes showed abnormal expression in PDAC tissues and functional impacts on the migration, proliferation, and colony formation abilities of pancreatic cancer cell lines. Furthermore, through digital PCR analysis, we revealed potential genomic mechanisms for the KRAS and TP53 mutations in the metastatic tumor. Taken together, our study shows the possibility for such personalized genomic profiling to provide new biological insight into the metastasis of PDAC.

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