Molecular architecture of a complex between an adhesion protein from the malaria parasite and intracellular adhesion molecule 1

Alan Brown; Louise Turner; Stig Christoffersen; Katrina A Andrews; Tadge Szestak; Yuguang Zhao; Sine Larsen; Alister G Craig; Matthew K Higgins

doi:10.1074/jbc.M112.416347

Molecular architecture of a complex between an adhesion protein from the malaria parasite and intracellular adhesion molecule 1

Alan Brown, Louise Turner, Stig Christoffersen, Katrina A Andrews, Tadge Szestak, Yuguang Zhao, Sine Larsen, Alister G Craig, Matthew K Higgins

30 Citations (Scopus)

Abstract

Background: PfEMP1 proteins cause Plasmodium falciparum-infected erythrocytes to bind human tissues during malaria. Results: The IT4VAR13 ectodomain is rigid, elongated, and monomeric, presenting a binding site for its ligand, ICAM-1. Conclusion: The IT4VAR13 ectodomain is unlike that of VAR2CSA, a PfEMP1 that adopts a compact structure with multiple domains contributing to ligand binding. Significance: PfEMP1 proteins have evolved diverse architectures to facilitate ligand recognition.

Original language	English
Journal	Journal of Biological Chemistry
Volume	288
Issue number	8
Pages (from-to)	5992-6003
Number of pages	12
ISSN	0021-9258
DOIs	https://doi.org/10.1074/jbc.M112.416347
Publication status	Published - 22 Feb 2013

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abstract = "Background: PfEMP1 proteins cause Plasmodium falciparum-infected erythrocytes to bind human tissues during malaria. Results: The IT4VAR13 ectodomain is rigid, elongated, and monomeric, presenting a binding site for its ligand, ICAM-1. Conclusion: The IT4VAR13 ectodomain is unlike that of VAR2CSA, a PfEMP1 that adopts a compact structure with multiple domains contributing to ligand binding. Significance: PfEMP1 proteins have evolved diverse architectures to facilitate ligand recognition.",

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AU - Brown, Alan

AU - Turner, Louise

AU - Christoffersen, Stig

AU - Andrews, Katrina A

AU - Szestak, Tadge

AU - Zhao, Yuguang

AU - Larsen, Sine

AU - Craig, Alister G

AU - Higgins, Matthew K

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N2 - Background: PfEMP1 proteins cause Plasmodium falciparum-infected erythrocytes to bind human tissues during malaria. Results: The IT4VAR13 ectodomain is rigid, elongated, and monomeric, presenting a binding site for its ligand, ICAM-1. Conclusion: The IT4VAR13 ectodomain is unlike that of VAR2CSA, a PfEMP1 that adopts a compact structure with multiple domains contributing to ligand binding. Significance: PfEMP1 proteins have evolved diverse architectures to facilitate ligand recognition.

AB - Background: PfEMP1 proteins cause Plasmodium falciparum-infected erythrocytes to bind human tissues during malaria. Results: The IT4VAR13 ectodomain is rigid, elongated, and monomeric, presenting a binding site for its ligand, ICAM-1. Conclusion: The IT4VAR13 ectodomain is unlike that of VAR2CSA, a PfEMP1 that adopts a compact structure with multiple domains contributing to ligand binding. Significance: PfEMP1 proteins have evolved diverse architectures to facilitate ligand recognition.

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Molecular architecture of a complex between an adhesion protein from the malaria parasite and intracellular adhesion molecule 1

Abstract

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