Abstract
BackgroundThe high proportion of human cases due to the simian malaria parasite Plasmodium knowlesi in Malaysia is a cause of concern, as they can be severe and even fatal. Merozoite surface protein 7 (MSP7) is a multigene family which forms a non-covalent complex with MSP-1 prior to receptor-ligand recognition in Plasmodium falciparum and thus an important antigen for vaccine development. However, no study has been done in any of the ortholog family members in P. knowlesi from clinical samples. This study investigates the level of polymorphism, haplotypes, and natural selection acting at the pkmsp-7D gene in clinical samples from Malaysia.MethodsThirty-six full-length pkmsp7D gene sequences (along with the reference H-strain: PKNH_1266000) obtained from clinical isolates of Malaysia, which were orthologous to pvmsp7H (PVX_082680) were downloaded from public databases. Population genetic, evolutionary and phylogenetic analyses were performed to determine the level of genetic diversity, polymorphism, recombination and natural selection.ResultsAnalysis of 36 full-length pkmsp7D sequences identified 147 SNPs (91 non-synonymous and 56 synonymous substitutions). Nucleotide diversity across the full-length gene was higher than its ortholog in Plasmodium vivax (msp7H). Region-wise analysis of the gene indicated that the nucleotide diversity at the central region was very high (π = 0.14) compared to the 5′ and 3′ regions. Most hyper-variable SNPs were detected at the central domain. Multiple test for natural selection indicated the central region was under strong positive natural selection however, the 5′ and 3′ regions were under negative/purifying selection. Evidence of intragenic recombination were detected at the central region of the gene. Phylogenetic analysis using full-length msp7D genes indicated there was no geographical clustering of parasite population.ConclusionsHigh genetic diversity with hyper-variable SNPs and strong evidence of positive natural selection at the central region of MSP7D indicated exposure of the region to host immune pressure. Negative selection at the 5′ and the 3′ regions of MSP7D might be because of functional constraints at the unexposed regions during the merozoite invasion process of P. knowlesi. No evidence of geographical clustering among the clinical isolates from Malaysia indicated uniform selection pressure in all populations. These findings highlight the further evaluation of the regions and functional characterization of the protein as a potential blood stage vaccine candidate for P. knowlesi.
Highlights
The high proportion of human cases due to the simian malaria parasite Plasmodium knowlesi in Malay‐ sia is a cause of concern, as they can be severe and even fatal
Within the full-length pkmsp7D sequences (n = 36), there were 203 (17.13%) polymorphic sites leading to 34 haplotypes (Table 1)
Within the full-length gene, there were 147 SNPs which could be analyzed by DnaSP (91 non-synonymous substitutions and 56 synonymous substitutions) (Table 2) and 75 nonsynonymous complex codons were excluded from analysis by the DnaSP software
Summary
The high proportion of human cases due to the simian malaria parasite Plasmodium knowlesi in Malay‐ sia is a cause of concern, as they can be severe and even fatal. Plasmodium knowlesi is a simian malaria parasite which can infect humans and is an emerging infection in Southeast Asian countries [2,3,4,5,6]. Studies on mitochondrial and ssrRNA genes in P. knowlesi from patients and wild macaques identified two distinct sub-populations which clustered geographically to Peninsular Malaysia and Malaysian Borneo [23]. Genetic and genomic studies from Malaysia identified 3 distinct sub-populations; two originating from Sarawak and one from Peninsular Malaysia [24,25,26,27], highlighting the complexity of infections in humans and the challenges for control and vaccine design
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