Phosphatidylserine Exposure is Required for ADAM17 Sheddase Function

Overview

Journal Nat Commun

Specialty Biology

Date 2016 May 11

PMID 27161080

Citations 97

Authors

Anselm Sommer

Felix Kordowski

Joscha Buch

Thorsten Maretzky

Astrid Evers

Jorg Andra

Stefan Dusterhoft

Matthias Michalek

Inken Lorenzen

Prasath Somasundaram

Andreas Tholey

Frank D Sonnichsen

Karl Kunzelmann

Lena Heinbockel

Christian Nehls

Thomas Gutsmann

Joachim Grotzinger

Sucharit Bhakdi

Karina Reiss

Affiliations

Soon will be listed here.

Abstract

ADAM17, a prominent member of the 'Disintegrin and Metalloproteinase' (ADAM) family, controls vital cellular functions through cleavage of transmembrane substrates. Here we present evidence that surface exposure of phosphatidylserine (PS) is pivotal for ADAM17 to exert sheddase activity. PS exposure is tightly coupled to substrate shedding provoked by diverse ADAM17 activators. PS dependency is demonstrated in the following: (a) in Raji cells undergoing apoptosis; (b) in mutant PSA-3 cells with manipulatable PS content; and (c) in Scott syndrome lymphocytes genetically defunct in their capacity to externalize PS in response to intracellular Ca(2+) elevation. Soluble phosphorylserine but not phosphorylcholine inhibits substrate cleavage. The isolated membrane proximal domain (MPD) of ADAM17 binds to PS but not to phosphatidylcholine liposomes. A cationic PS-binding motif is identified in this domain, replacement of which abrogates liposome-binding and renders the protease incapable of cleaving its substrates in cells. We speculate that surface-exposed PS directs the protease to its targets where it then executes its shedding function.

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