Selective expression of variant surface antigens enables Plasmodium falciparum to evade immune clearance in vivo

Author:

Chew Marvin,Ye Weijian,Omelianczyk Radoslaw IgorORCID,Pasaje Charisse FleridaORCID,Hoo Regina,Chen QingfengORCID,Niles Jacquin C.ORCID,Chen JianzhuORCID,Preiser PeterORCID

Abstract

AbstractPlasmodium falciparum has developed extensive mechanisms to evade host immune clearance. Currently, most of our understanding is based on in vitro studies of individual parasite variant surface antigens and how this relates to the processes in vivo is not well-understood. Here, we have used a humanized mouse model to identify parasite factors important for in vivo growth. We show that upregulation of the specific PfEMP1, VAR2CSA, provides the parasite with protection from macrophage phagocytosis and clearance in the humanized mice. Furthermore, parasites adapted to thrive in the humanized mice show reduced NK cell-mediated killing through interaction with the immune inhibitory receptor, LILRB1. Taken together, these findings reveal new insights into the molecular and cellular mechanisms that the parasite utilizes to coordinate immune escape in vivo. Identification and targeting of these specific parasite variant surface antigens crucial for immune evasion provides a unique approach for therapy.

Funder

National Research Foundation Singapore

Ministry of Health -Singapore

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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