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Evidence for additive and interaction effects of host genotype and infection in malaria.


ABSTRACT: The host mechanisms responsible for protection against malaria remain poorly understood, with only a few protective genetic effects mapped in humans. Here, we characterize a host-specific genome-wide signature in whole-blood transcriptomes of Plasmodium falciparum-infected West African children and report a demonstration of genotype-by-infection interactions in vivo. Several associations involve transcripts sensitive to infection and implicate complement system, antigen processing and presentation, and T-cell activation (i.e., SLC39A8, C3AR1, FCGR3B, RAD21, RETN, LRRC25, SLC3A2, and TAPBP), including one association that validated a genome-wide association candidate gene (SCO1), implicating binding variation within a noncoding regulatory element. Gene expression profiles in mice infected with Plasmodium chabaudi revealed and validated similar responses and highlighted specific pathways and genes that are likely important responders in both hosts. These results suggest that host variation and its interplay with infection affect children's ability to cope with infection and suggest a polygenic model mounted at the transcriptional level for susceptibility.

SUBMITTER: Idaghdour Y 

PROVIDER: S-EPMC3479498 | biostudies-literature | 2012 Oct

REPOSITORIES: biostudies-literature

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Evidence for additive and interaction effects of host genotype and infection in malaria.

Idaghdour Youssef Y   Quinlan Jacklyn J   Goulet Jean-Philippe JP   Berghout Joanne J   Gbeha Elias E   Bruat Vanessa V   de Malliard Thibault T   Grenier Jean-Christophe JC   Gomez Selma S   Gros Philippe P   Rahimy Mohamed Chérif MC   Sanni Ambaliou A   Awadalla Philip P  

Proceedings of the National Academy of Sciences of the United States of America 20120904 42


The host mechanisms responsible for protection against malaria remain poorly understood, with only a few protective genetic effects mapped in humans. Here, we characterize a host-specific genome-wide signature in whole-blood transcriptomes of Plasmodium falciparum-infected West African children and report a demonstration of genotype-by-infection interactions in vivo. Several associations involve transcripts sensitive to infection and implicate complement system, antigen processing and presentati  ...[more]

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