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Protein Paucimannosylation Is an Enriched N‐Glycosylation Signature of Human Cancers
Authors:Sayantani Chatterjee  Ling Y Lee  Rebeca Kawahara  Jodie L Abrahams  Barbara Adamczyk  Merrina Anugraham  Christopher Ashwood  Zeynep Sumer‐Bayraktar  Matthew T Briggs  Jenny H L Chik  Arun Everest‐Dass  Sarah Frster  Hannes Hinneburg  Katia R M Leite  Ian Loke  Uwe Mginger  Edward S X Moh  Miyako Nakano  Saulo Recuero  Manveen K Sethi  Miguel Srougi  Kathrin Stavenhagen  Vignesh Venkatakrishnan  Katherine Wongtrakul‐Kish  Simone Diestel  Peter Hoffmann  Niclas G Karlsson  Daniel Kolarich  Mark P Molloy  Michael H Muders  Martin K Oehler  Nicolle H Packer  Giuseppe Palmisano  Morten Thaysen‐Andersen
Institution:Sayantani Chatterjee,Ling Y. Lee,Rebeca Kawahara,Jodie L. Abrahams,Barbara Adamczyk,Merrina Anugraham,Christopher Ashwood,Zeynep Sumer‐Bayraktar,Matthew T. Briggs,Jenny H. L. Chik,Arun Everest‐Dass,Sarah Förster,Hannes Hinneburg,Katia R. M. Leite,Ian Loke,Uwe Möginger,Edward S. X. Moh,Miyako Nakano,Saulo Recuero,Manveen K. Sethi,Miguel Srougi,Kathrin Stavenhagen,Vignesh Venkatakrishnan,Katherine Wongtrakul‐Kish,Simone Diestel,Peter Hoffmann,Niclas G. Karlsson,Daniel Kolarich,Mark P. Molloy,Michael H. Muders,Martin K. Oehler,Nicolle H. Packer,Giuseppe Palmisano,Morten Thaysen‐Andersen
Abstract:While aberrant protein glycosylation is a recognized characteristic of human cancers, advances in glycoanalytics continue to discover new associations between glycoproteins and tumorigenesis. This glycomics‐centric study investigates a possible link between protein paucimannosylation, an under‐studied class of human N‐glycosylation Man1‐3GlcNAc2Fuc0‐1], and cancer. The paucimannosidic glycans (PMGs) of 34 cancer cell lines and 133 tissue samples spanning 11 cancer types and matching non‐cancerous specimens are profiled from 467 published and unpublished PGC‐LC‐MS/MS N‐glycome datasets collected over a decade. PMGs, particularly Man2‐3GlcNAc2Fuc1, are prominent features of 29 cancer cell lines, but the PMG level varies dramatically across and within the cancer types (1.0–50.2%). Analyses of paired (tumor/non‐tumor) and stage‐stratified tissues demonstrate that PMGs are significantly enriched in tumor tissues from several cancer types including liver cancer (p = 0.0033) and colorectal cancer (p = 0.0017) and is elevated as a result of prostate cancer and chronic lymphocytic leukaemia progression (p < 0.05). Surface expression of paucimannosidic epitopes is demonstrated on human glioblastoma cells using immunofluorescence while biosynthetic involvement of N‐acetyl‐β‐hexosaminidase is indicated by quantitative proteomics. This intriguing association between protein paucimannosylation and human cancers warrants further exploration to detail the biosynthesis, cellular location(s), protein carriers, and functions of paucimannosylation in tumorigenesis and metastasis.
Keywords:cancer  glycan  glycomics  paucimannosidic glycan  protein paucimannosylation
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