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Extracellular vesicles adhere to cells primarily by interactions of integrins and GM1 with laminin

Tatsuki Isogai, Koichiro M. Hirosawa, Miki Kanno, Ayano Sho, Rinshi S. Kasai, Naoko Komura, Hiromune Ando, Keiko Furukawa, Yuhsuke Ohmi, Koichi Furukawa, Yasunari Yokota, Kenichi Suzuki

2025The Journal of Cell Biology13 citationsDOIOpen Access PDF

Abstract

Tumor-derived extracellular vesicles (EVs) have attracted significant attention, yet the molecular mechanisms that govern their specific binding to recipient cells remain elusive. Our in vitro study utilizing single-particle tracking demonstrated that integrin heterodimers comprising α6β4 and α6β1 and ganglioside, GM1, are responsible for the binding of small EV (sEV) subtypes to laminin. EVs derived from four distinct tumor cell lines, regardless of size, exhibited high binding affinities for laminin but not for fibronectin, although fibronectin receptors are abundant in EVs and have functional roles in EV-secreting cells. Our findings revealed that integrins in EVs bind to laminin via the conventional molecular interface, facilitated by CD151 rather than by inside-out signaling of talin-1 and kindlin-2. Super-resolution movie observation revealed that sEV integrins bind only to laminin on living recipient cells. Furthermore, sEVs bound to HUVEC and induced cell branching morphogenesis in a laminin-dependent manner. Thus, we demonstrated that EVs predominantly bind to laminin on recipient cells, which is indispensable for cell responses.

Topics & Concepts

LamininIntegrinFibronectinCell biologyBiologyCell adhesionCellMorphogenesisExtracellular matrixBiochemistryGeneExtracellular vesicles in diseaseCell Adhesion Molecules ResearchPlatelet Disorders and Treatments
Extracellular vesicles adhere to cells primarily by interactions of integrins and GM1 with laminin | Litcius