There are four dynamically and functionally distinct populations of E-cadherin in cell junctions
Author(s) -
Zahra Erami,
Paul Timpson,
Wu Yao,
Ronen ZaidelBar,
Kurt I. Anderson
Publication year - 2015
Publication title -
biology open
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.936
H-Index - 41
ISSN - 2046-6390
DOI - 10.1242/bio.014159
Subject(s) - cadherin , adhesive , adhesion , cell adhesion , cytoskeleton , biology , microbiology and biotechnology , intracellular , actin cytoskeleton , cell junction , cell–cell interaction , cell , actin , biophysics , materials science , nanotechnology , biochemistry , layer (electronics) , composite material
E-cadherin is a trans-membrane tumor suppressor responsible for epithelial cell adhesion. E-cadherin forms adhesive clusters through combined extra-cellular cis- and trans-interactions and intracellular interaction with the actin cytoskeleton. Here we identify four populations of E-cadherin within cell junctions based on the molecular interactions which determine their mobility and adhesive properties. Adhesive and non-adhesive populations of E-cadherin each consist of mobile and immobile fractions. Up to half of the E-cadherin immobilized in cell junctions is non-adhesive. Incorporation of E-cadherin into functional adhesions require all three adhesive interactions, with deletion of any one resulting in loss of effective cell-cell adhesion. Interestingly, the only interaction which could independently slow the diffusion of E-cadherin was the tail-mediated intra-cellular interaction. The adhesive and non-adhesive mobile fractions of E-cadherin can be distinguished by their sensitivity to chemical cross-linking with adhesive clusters. Our data define the size, mobility, and adhesive properties of four distinct populations of E-cadherin within cell junctions, and support association with the actin cytoskeleton as the first step in adhesion formation.
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