Biochemical and functional characterization of glycosylation-associated mutational landscapes in colon cancer

糖基化 生物 糖基转移酶 基因 结直肠癌 表型 突变体 癌症研究 突变 聚糖 癌症 遗传学 糖蛋白
作者
Srividya Venkitachalam,Leslie Revoredo,Vinay Varadan,Ryan E. Fecteau,Lakshmeswari Ravi,James Lutterbaugh,Sanford D. Markowitz,Joseph Willis,Thomas Gerken,Kishore Guda
出处
期刊:Scientific Reports [Nature Portfolio]
卷期号:6 (1) 被引量:53
标识
DOI:10.1038/srep23642
摘要

Abstract The molecular basis of aberrant protein glycosylation, a pathological alteration widespread in colorectal cancers (CRC) and the mechanisms by which it contributes to tumor progression remain largely unknown. We performed targeted re-sequencing of 430 glycosylation-associated genes in a series of patient-derived CRC cell lines (N = 31) and matched primary tumor tissues, identifying 12 new significantly mutated glycosylation-associated genes in colon cancer. In particular, we observed an enrichment of mutations in genes ( B3GNT2 , B4GALT 2, ST6GALNAC2 ) involved in the biosynthesis of N - and Cores 1–3 O -linked glycans in the colon, accounting for ~16% of the CRCs tested. Analysis of independent large-scale tumor tissue datasets confirmed recurrent mutations within these genes in colon and other gastrointestinal cancers. Systematic biochemical and phenotypic characterization of the candidate wild-type and mutant glycosyltransferases demonstrated these mutations as either markedly altering protein localization, post-translational modification, encoded enzymatic activities and/or the migratory potential of colon carcinoma cells. These findings suggest that functionally deleterious mutations in glycosyltransferase genes in part underlie aberrant glycosylation and contribute to the pathogenesis of molecular subsets of colon and other gastrointestinal malignancies.

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