| Literature DB >> 29276373 |
Julia Krushkal1, Yingdong Zhao1, Curtis Hose2, Anne Monks2, James H Doroshow3, Richard Simon1.
Abstract
Cellular glycosylation processes are vital to cell functioning. In malignant cells, they are profoundly altered. We used time-course gene expression data from the NCI-60 cancer cell lines treated with 11 antitumor agents to analyze expression changes of genes involved in glycosylation pathways, genes encoding glycosylation targets or regulators, and members of cancer pathways affected by glycosylation. We also identified glycosylation genes for which pretreatment expression levels or changes after treatment were correlated with drug sensitivity. Their products are involved in N-glycosylation and O-glycosylation, fucosylation, biosynthesis of poly-N-acetyllactosamine, removal of misfolded proteins, binding to hyaluronic acid and other glycans, and cell adhesion. Tumor cell sensitivity to multiple agents was correlated with transcriptional response of C1GALT1C1, FUCA1, SDC1, MUC1; members of the MGAT, GALNT, B4GALT, B3GNT, MAN, and EDEM families; and other genes. These genes may be considered as potential candidates for drug targeting in combination therapy to enhance treatment response.Entities:
Keywords: Cancer drug treatment; gene expression; glycoprotein; glycosylation; microarray analysis
Year: 2017 PMID: 29276373 PMCID: PMC5734428 DOI: 10.1177/1176935117747259
Source DB: PubMed Journal: Cancer Inform ISSN: 1176-9351