| Literature DB >> 25030168 |
Matthew J Paszek1, Christopher C DuFort2, Olivier Rossier3, Russell Bainer2, Janna K Mouw4, Kamil Godula5, Jason E Hudak6, Jonathon N Lakins4, Amanda C Wijekoon2, Luke Cassereau2, Matthew G Rubashkin2, Mark J Magbanua7, Kurt S Thorn8, Michael W Davidson9, Hope S Rugo7, John W Park7, Daniel A Hammer10, Grégory Giannone3, Carolyn R Bertozzi11, Valerie M Weaver12.
Abstract
Malignancy is associated with altered expression of glycans and glycoproteins that contribute to the cellular glycocalyx. We constructed a glycoprotein expression signature, which revealed that metastatic tumours upregulate expression of bulky glycoproteins. A computational model predicted that these glycoproteins would influence transmembrane receptor spatial organization and function. We tested this prediction by investigating whether bulky glycoproteins in the glycocalyx promote a tumour phenotype in human cells by increasing integrin adhesion and signalling. Our data revealed that a bulky glycocalyx facilitates integrin clustering by funnelling active integrins into adhesions and altering integrin state by applying tension to matrix-bound integrins, independent of actomyosin contractility. Expression of large tumour-associated glycoproteins in non-transformed mammary cells promoted focal adhesion assembly and facilitated integrin-dependent growth factor signalling to support cell growth and survival. Clinical studies revealed that large glycoproteins are abundantly expressed on circulating tumour cells from patients with advanced disease. Thus, a bulky glycocalyx is a feature of tumour cells that could foster metastasis by mechanically enhancing cell-surface receptor function.Entities:
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Year: 2014 PMID: 25030168 PMCID: PMC4487551 DOI: 10.1038/nature13535
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962