Intercellular transfer of cancer cell invasiveness via endosome-mediated protease shedding

Author:

Wenzel Eva MariaORCID,Pedersen Nina Marie,Elfmark Liv Anker,Wang Ling,Kjos IngridORCID,Stang Espen,Malerød Lene,Brech Andreas,Stenmark HaraldORCID,Raiborg CamillaORCID

Abstract

AbstractOverexpression of the transmembrane matrix metalloproteinase MT1-MMP/MMP14 promotes cancer cell invasion. Here we show that MT1-MMP-positive cancer cells turn MT1-MMP-negative cells invasive by transferring a soluble catalytic ectodomain of MT1-MMP. Surprisingly, this effect depends on the presence of TKS4 and TKS5 in the donor cell, adaptor proteins previously implicated in invadopodia formation. In endosomes of the donor cell, TKS4/5 promote ADAM-mediated cleavage of MT1-MMP by bridging the two proteases, and cleavage is stimulated by the low intraluminal pH of endosomes. The bridging depends on the PX domains of TKS4/5, which coincidently interact with the cytosolic tail of MT1-MMP and endosomal phosphatidylinositol 3-phosphate. MT1-MMP recruits TKS4/5 into multivesicular endosomes for their subsequent co-secretion in extracellular vesicles, together with the enzymatically active ectodomain. The shed ectodomain converts non-invasive recipient cells into an invasive phenotype. Thus, TKS4/5 promote intercellular transfer of cancer cell invasiveness by facilitating ADAM-mediated shedding of MT1-MMP in acidic endosomes.

Funder

Kreftforeningen

Ministry of Health and Care Services | Helse Sør-Øst RHF

Norges Forskningsråd

EC | Horizon 2020 Framework Programme

InvaCell Trond Paulsen

Publisher

Springer Science and Business Media LLC

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