The genome of the zoonotic malaria parasite Plasmodium simium reveals adaptations to host-switching

Author:

Mourier TobiasORCID,de Alvarenga Denise Anete Madureira,Kaushik Abhinav,de Pina-Costa Anielle,Douvropoulou Olga,Guan Qingtian,Guzmán-Vega Francisco J.,Forrester Sarah,de Abreu Filipe Vieira Santos,Júnior Cesare Bianco,de Souza Junior Julio Cesar,Moreira Silvia Bahadian,Hirano Zelinda Maria Braga,Pissinatti Alcides,de Fátima Ferreira-da-Cruz Maria,de Oliveira Ricardo Lourenço,Arold Stefan T.,Jeffares Daniel C.,Brasil Patrícia,de Brito Cristiana Ferreira Alves,Culleton Richard,Daniel-Ribeiro Cláudio Tadeu,Pain ArnabORCID

Abstract

AbstractBackgroundPlasmodium simium, a malaria parasite of non-human primates (NHP) was recently shown to cause zoonotic infections in humans in Brazil. We sequenced the P. simium genome to investigate its evolutionary history and to identify any genetic adaptions that may underlie the ability of this parasite to switch between host species.ResultsPhylogenetic analyses based on whole genome sequences of P. simium from humans and NHPs reveals that P. simium is monophyletic within the broader diversity of South American Plasmodium vivax, suggesting P. simium first infected NHPs as a result of a host-switch of P. vivax from humans. The P. simium isolates show the closest relationship to Mexican P. vivax isolates. Analysis of erythrocyte invasion genes reveals differences between P. vivax and P. simium, including large deletions in the Duffy Binding Protein 1 (DBP1) and Reticulocyte Binding Protein 2a genes of P. simium. Analysis of P. simium isolated from NHPs and humans revealed a deletion of 38 amino acids in DBP1 present in all human-derived isolates, whereas NHP isolates were multi-allelic.ConclusionsAnalysis of the P. simium genome confirmed a close phylogenetic relationship between P. simium and P. vivax, and suggests a very recent American origin for P. simium. The presence of the DBP1 deletion in all human-derived isolates tested suggests that this deletion, in combination with other genetic changes in P. simium, may facilitate the invasion of human red blood cells and may explain, at least in part, the basis of the recent zoonotic infections.

Publisher

Cold Spring Harbor Laboratory

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