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Dynamics and molecular interactions of GPI-anchored CD59

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Title: Dynamics and molecular interactions of GPI-anchored CD59
Authors: Voisin, TB
Couves, EC
Tate, EW
Bubeck, D
Item Type: Journal Article
Abstract: CD59 is a GPI-anchored cell surface receptor that serves as a gatekeeper to controlling pore formation. It is the only membrane-bound inhibitor of the complement membrane attack complex (MAC), an immune pore that can damage human cells. While CD59 blocks MAC pores, the receptor is co-opted by bacterial pore-forming proteins to target human cells. Recent structures of CD59 in complexes with binding partners showed dramatic differences in the orientation of its ectodomain relative to the membrane. Here, we show how GPI-anchored CD59 can satisfy this diversity in binding modes. We present a PyLipID analysis of coarse-grain molecular dynamics simulations of a CD59-inhibited MAC to reveal residues of complement proteins (C6:Y285, C6:R407 C6:K412, C7:F224, C8β:F202, C8β:K326) that likely interact with lipids. Using modules of the MDAnalysis package to investigate atomistic simulations of GPI-anchored CD59, we discover properties of CD59 that encode the flexibility necessary to bind both complement proteins and bacterial virulence factors.
Issue Date: Jul-2023
Date of Acceptance: 26-Jun-2023
URI: http://hdl.handle.net/10044/1/109789
DOI: 10.3390/toxins15070430
ISSN: 2072-6651
Publisher: MDPI AG
Journal / Book Title: Toxins
Volume: 15
Issue: 7
Copyright Statement: © 2023 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
Publication Status: Published
Article Number: 430
Online Publication Date: 2023-06-30
Appears in Collections:Chemistry
Biological and Biophysical Chemistry
Faculty of Natural Sciences



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