-Glycoproteomics Study of Putative -Glycoprotein Biomarkers of Drug Resistance in MCF-7/ADR Cells.

Phenomics

Shanghai Key Laboratory of Chemical Assessment and Sustainability, School of Chemical Science and Engineering, Tongji University, Shanghai, 200092 China.

Published: December 2021

Unlabelled: Currently, drug resistance of anti-cancer therapy has become the main cause of low survival rate and poor prognosis. Full understanding of drug resistance mechanisms is an urgent request for further development of anti-cancer therapy and improvement of prognosis. Here we present our -glycoproteomics study of putative -glycoprotein biomarkers of drug resistance in doxorubicin resistance breast cancer cell line michigan cancer foundation-7 (MCF-7/ADR) relative to parental michigan cancer foundation-7 (MCF-7) cells. Intact -glycopeptides (IDs) from MCF-7/ADR and MCF-7 cells were enriched with zwitterionic hydrophilic interaction liquid chromatography (ZIC-HILIC), labeled with stable isotopic diethylation (SIDE), and analyzed with C18-RPLC-MS/MS (HCD with stepped normalized collision energies); these IDs were identified with database search engine GPSeeker, and the differentially expressed intact -glycopeptides (DEGPs) were quantified with GPSeekerQuan. With target-decoy searches and control of spectrum-level FDR ≤ 1%, 322 intact -glycopeptides were identified; these intact -glycopeptides come from the combination of 249 unique peptide backbones (corresponding to 234 intact -glycoproteins) and 90 monosaccharide compositions (corresponding to 248 putative -glycosites). The sequence structures of 165 IDs were confirmed with structure-diagnostic fragment ions. With the criteria of observation at least twice among the three technical replicates, ≥ 1.5-fold change and value < 0.05, 20 DEGPs were quantified, where five of them were up-regulated and 15 of them were down-regulated; the corresponding intact -glycoproteins as putative markers of drug resistance were discussed.

Supplementary Information: The online version contains supplementary material available at 10.1007/s43657-021-00029-8.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9590513PMC
http://dx.doi.org/10.1007/s43657-021-00029-8DOI Listing

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