Title of article
Structural Basis of Chemokine Sequestration by a Herpesvirus Decoy Receptor
Author/Authors
Jennifer M. Alexander، نويسنده , , Christopher A. Nelson، نويسنده , , Victor van Berkel، نويسنده , , Elaine K. Lau، نويسنده , , Joey M. Studts، نويسنده , , Tom J. Brett، نويسنده , , Samuel H. Speck، نويسنده , , Tracy M. Handel، نويسنده , , Herbert W. Virgin IV، نويسنده , , Daved H. Fremont، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2002
Pages
14
From page
343
To page
356
Abstract
The M3 protein encoded by murine γherpesvirus68 (γHV68) functions as an immune system saboteur by the engagement of chemoattractant cytokines, thereby altering host antiviral inflammatory responses. Here we report the crystal structures of M3 both alone and in complex with the CC chemokine MCP-1. M3 is a two-domain β sandwich protein with a unique sequence and topology, forming a tightly packed anti-parallel dimer. The stoichiometry of the MCP-1:M3 complex is 2:2, with two monomeric chemokines embedded at distal ends of the preassociated M3 dimer. Conformational flexibility and electrostatic complementation are both used by M3 to achieve high-affinity and broad-spectrum chemokine engagement. M3 also employs structural mimicry to promiscuously sequester chemokines, engaging conservative structural elements associated with both chemokine homodimerization and binding to G protein-coupled receptors.
Journal title
CELL
Serial Year
2002
Journal title
CELL
Record number
1017989
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