Spatial N-glycan rearrangement on α5β1integrin nucleates galectin-3 oligomers to determine endocytic fate

Author:

Shafaq-Zadah MassiullahORCID,Dransart Estelle,Wunder Christian,Chambon Valérie,Valades-Cruz Cesar A.ORCID,Leconte Ludovic,Sarangi Nirod Kumar,Robinson Jack,Bai Siau-Kun,Regmi Raju,Cicco Aurélie Di,Hovasse Agnès,Bartels Richard,Nilsson Ulf J.,Cianférani-Sanglier Sarah,Leffler Hakon,Keyes Tia E.,Lévy Daniel,Raunser Stefan,Roderer Daniel,Johannes Ludger

Abstract

SummaryMembrane glycoproteins frequently adopt different conformations when altering between active and inactive states. Here, we discover a molecular switch that exploits dynamic spatial rearrangements of N-glycans during such conformational transitions to control protein function. For the conformationally switchable cell adhesion glycoprotein α5β1integrin, we find that only the bent-closed state arranges N-glycans to nucleate the formation of up to tetrameric oligomers of the glycan-binding protein galectin-3. We propose a structural model of how these galectin-3 oligomers are assembled and how they clamp the bent-closed state to prime it for endocytic uptake and subsequent retrograde trafficking to the Golgi for polarized distribution in cells. Our findings highlight an unexpectedly dynamic regulation of the glycan landscape at the cell surface to achieve oligomerization of galectin-3. Galectin-3 oligomers are thereby identified as decoders of defined spatial patterns of N-glycans and as functional extracellular interactors of specifically the bent- closed conformational state of α5β1integrin and possibly other family members.

Publisher

Cold Spring Harbor Laboratory

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