O-mannosylation and N-glycosylation: Two coordinated mechanisms regulating the tumour suppressor functions of E-cadherin in cancer

Dysregulation of tumor suppressor protein E-cadherin is an early molecular event in cancer. O-mannosylation profile of E-cadherin is a newly-described posttranslational modification crucial for its adhesive functions in homeostasis. However, the role of O-mannosyl glycans in E-cadherin-mediated cell...

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Bibliographic Details
Main Author: Carvalho, S (author)
Other Authors: Oliveira, T (author), Bartels, M (author), Miyoshi, E (author), Pierce, M (author), Taniguchi, N (author), Carneiro, F (author), Seruca, R (author), Reis, CA (author), Strahl, S (author), Pinho, SS (author)
Format: article
Language:eng
Published: 2016
Subjects:
Adenocarcinoma/metabolism
Adenocarcinoma/pathology
Animals
Cadherins/metabolism
Glycosylation
Humans
Mannose/metabolism
Mice
Mice, Transgenic
Polysaccharides
Protein Processing, Post-Translational/physiology
Stomach Neoplasms/metabolism
Stomach Neoplasms/pathology
Tumor Suppressor Proteins/metabolism
Online Access:https://repositorio-aberto.up.pt/handle/10216/118210
Country:Portugal
Oai:oai:repositorio-aberto.up.pt:10216/118210
Description
Summary:Dysregulation of tumor suppressor protein E-cadherin is an early molecular event in cancer. O-mannosylation profile of E-cadherin is a newly-described posttranslational modification crucial for its adhesive functions in homeostasis. However, the role of O-mannosyl glycans in E-cadherin-mediated cell adhesion in cancer and their interplay with N-glycans remains largely unknown. We herein demonstrated that human gastric carcinomas exhibiting a non-functional E-cadherin display a reduced expression of O-mannosyl glycans concomitantly with increased modification with branched complex N-glycans. Accordingly, overexpression of MGAT5-mediated branched N-glycans both in gastric cancer cells and transgenic mice models led to a significant decrease of O-mannosyl glycans attached to E-cadherin that was associated with impairment of its tumour suppressive functions. Importantly, overexpression of protein O-mannosyltransferase 2 (POMT2) induced a reduced expression of branched N-glycans which led to a protective effect of E-cadherin biological functions. Overall, our results reveal a newly identified mechanism of (dys)regulation of E-cadherin that occur through the interplay between O-mannosylation and N-glycosylation pathway.

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