Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites

Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites

Abstract Background The most severe form of human malaria is caused by the protozoan parasite Plasmodium falciparum. This unicellular organism is a member of a subgenus of Plasmodium called the Laverania that infects apes, with P. falciparum being the only member that infects humans. The exceptional...

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Main Authors: Mackensie R. Gross, Rosie Hsu, Kirk W. Deitsch
Format: Article
Language:English
Published: BMC 2021-07-01
Series:BMC Ecology and Evolution
Subjects:
Cytoadherence
Transcriptional regulation
Mutually exclusive expression
Pathogenesis
Online Access:https://doi.org/10.1186/s12862-021-01872-z
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spelling doaj-a089d59e5fbf4d54b1ac4c2eb58309d02021-08-29T11:05:24ZengBMCBMC Ecology and Evolution2730-71822021-07-0121111510.1186/s12862-021-01872-zEvolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasitesMackensie R. Gross0Rosie Hsu1Kirk W. Deitsch2Department of Microbiology and Immunology, Weill Cornell Medical CollegeDepartment of Microbiology and Immunology, Weill Cornell Medical CollegeDepartment of Microbiology and Immunology, Weill Cornell Medical CollegeAbstract Background The most severe form of human malaria is caused by the protozoan parasite Plasmodium falciparum. This unicellular organism is a member of a subgenus of Plasmodium called the Laverania that infects apes, with P. falciparum being the only member that infects humans. The exceptional virulence of this species to humans can be largely attributed to a family of variant surface antigens placed by the parasites onto the surface of infected red blood cells that mediate adherence to the vascular endothelium. These proteins are encoded by a large, multicopy gene family called var, with each var gene encoding a different form of the protein. By changing which var gene is expressed, parasites avoid immune recognition, a process called antigenic variation that underlies the chronic nature of malaria infections. Results Here we show that the common ancestor of the branch of the Laverania lineage that includes the human parasite underwent a remarkable change in the organization and structure of elements linked to the complex transcriptional regulation displayed by the var gene family. Unlike the other members of the Laverania, the clade that gave rise to P. falciparum evolved distinct subsets of var genes distinguishable by different upstream transcriptional regulatory regions that have been associated with different expression profiles and virulence properties. In addition, two uniquely conserved var genes that have been proposed to play a role in coordinating transcriptional switching similarly arose uniquely within this clade. We hypothesize that these changes originated at a time of dramatic climatic change on the African continent that is predicted to have led to significant changes in transmission dynamics, thus selecting for patterns of antigenic variation that enabled lengthier, more chronic infections. Conclusions These observations suggest that changes in transmission dynamics selected for significant alterations in the transcriptional regulatory mechanisms that mediate antigenic variation in the parasite lineage that includes P. falciparum. These changes likely underlie the chronic nature of these infections as well as their exceptional virulence.https://doi.org/10.1186/s12862-021-01872-zCytoadherenceTranscriptional regulationMutually exclusive expressionPathogenesis
collection DOAJ
language English
format Article
sources DOAJ
author Mackensie R. Gross
Rosie Hsu
Kirk W. Deitsch
spellingShingle Mackensie R. Gross
Rosie Hsu
Kirk W. Deitsch
Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
BMC Ecology and Evolution
Cytoadherence
Transcriptional regulation
Mutually exclusive expression
Pathogenesis
author_facet Mackensie R. Gross
Rosie Hsu
Kirk W. Deitsch
author_sort Mackensie R. Gross
title Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
title_short Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
title_full Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
title_fullStr Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
title_full_unstemmed Evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
title_sort evolution of transcriptional control of antigenic variation and virulence in human and ape malaria parasites
publisher BMC
series BMC Ecology and Evolution
issn 2730-7182
publishDate 2021-07-01
description Abstract Background The most severe form of human malaria is caused by the protozoan parasite Plasmodium falciparum. This unicellular organism is a member of a subgenus of Plasmodium called the Laverania that infects apes, with P. falciparum being the only member that infects humans. The exceptional virulence of this species to humans can be largely attributed to a family of variant surface antigens placed by the parasites onto the surface of infected red blood cells that mediate adherence to the vascular endothelium. These proteins are encoded by a large, multicopy gene family called var, with each var gene encoding a different form of the protein. By changing which var gene is expressed, parasites avoid immune recognition, a process called antigenic variation that underlies the chronic nature of malaria infections. Results Here we show that the common ancestor of the branch of the Laverania lineage that includes the human parasite underwent a remarkable change in the organization and structure of elements linked to the complex transcriptional regulation displayed by the var gene family. Unlike the other members of the Laverania, the clade that gave rise to P. falciparum evolved distinct subsets of var genes distinguishable by different upstream transcriptional regulatory regions that have been associated with different expression profiles and virulence properties. In addition, two uniquely conserved var genes that have been proposed to play a role in coordinating transcriptional switching similarly arose uniquely within this clade. We hypothesize that these changes originated at a time of dramatic climatic change on the African continent that is predicted to have led to significant changes in transmission dynamics, thus selecting for patterns of antigenic variation that enabled lengthier, more chronic infections. Conclusions These observations suggest that changes in transmission dynamics selected for significant alterations in the transcriptional regulatory mechanisms that mediate antigenic variation in the parasite lineage that includes P. falciparum. These changes likely underlie the chronic nature of these infections as well as their exceptional virulence.
topic Cytoadherence
Transcriptional regulation
Mutually exclusive expression
Pathogenesis
url https://doi.org/10.1186/s12862-021-01872-z
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AT kirkwdeitsch evolutionoftranscriptionalcontrolofantigenicvariationandvirulenceinhumanandapemalariaparasites
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