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Unread 09-27-2013, 05:26 PM
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Default Mechanism of E-cadherin dimerization probed by NMR relaxation dispersion.

Mechanism of E-cadherin dimerization probed by NMR relaxation dispersion.

Mechanism of E-cadherin dimerization probed by NMR relaxation dispersion.

Proc Natl Acad Sci U S A. 2013 Sep 25;

Authors: Li Y, Altorelli NL, Bahna F, Honig B, Shapiro L, Palmer AG

Abstract
Epithelial cadherin (E-cadherin), a member of the classical cadherin family, mediates calcium-dependent homophilic cell-cell adhesion. Crystal structures of classical cadherins reveal an adhesive dimer interface featuring reciprocal exchange of N-terminal ?-strands between two protomers. Previous work has identified a putative intermediate (called the "X-dimer") in the dimerization pathway of wild-type E-cadherin EC1-EC2 domains, based on crystal structures of mutants not capable of strand swapping and on deceleration of binding kinetics by mutations at the X-dimer interface. In the present work, NMR relaxation dispersion spectroscopy is used to directly observe and characterize intermediate states without the need to disrupt the strand-swapped binding interface by mutagenesis. The results indicate that E-cadherin forms strand-swapped dimers predominantly by a mechanism in which formation of a weak and short-lived X-dimer-like state precedes the conformational changes required for formation of the mature strand-swapped dimeric structure. Disruption of this intermediate state through mutation reduces both association and dissociation rates by factors of ~10(4), while minimally perturbing affinity. The X-dimer interface lowers the energy barrier associated with strand swapping and enables E-cadherins to form strand-swapped dimers at a rate consistent with residence times in adherens junctions.


PMID: 24067646 [PubMed - as supplied by publisher]



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