Genetic diversity and natural selection on the thrombospondin-related adhesive protein (TRAP) gene of Plasmodium falciparum on Bioko Island, Equatorial Guinea and global comparative analysis

Author:

Lin Li-Yun,Huang Hui-Ying,Liang Xue-Yan,Xie Dong-De,Chen Jiang-Tao,Wei Hua-Gui,Huang Wei-Yi,Ehapo Carlos Salas,Eyi Urbano Monsuy,Li Jian,Wang Jun-Li,Zheng Yu-Zhong,Zha Guang-Cai,Wang Yu-Ling,Chen Wei-Zhong,Liu Xiang-Zhi,Mo Huan-Tong,Chen Xin-Yao,Lin MinORCID

Abstract

Abstract Background Thrombospondin-related adhesive protein (TRAP) is a transmembrane protein that plays a crucial role during the invasion of Plasmodium falciparum into liver cells. As a potential malaria vaccine candidate, the genetic diversity and natural selection of PfTRAP was assessed and the global PfTRAP polymorphism pattern was described. Methods 153 blood spot samples from Bioko malaria patients were collected during 2016–2018 and the target TRAP gene was amplified. Together with the sequences from database, nucleotide diversity and natural selection analysis, and the structural prediction were preformed using bioinformatical tools. Results A total of 119 Bioko PfTRAP sequences were amplified successfully. On Bioko Island, PfTRAP shows its high degree of genetic diversity and heterogeneity, with π value for 0.01046 and Hd for 0.99. The value of dN–dS (6.2231, p < 0.05) hinted at natural selection of PfTRAP on Bioko Island. Globally, the African PfTRAPs showed more diverse than the Asian ones, and significant genetic differentiation was discovered by the fixation index between African and Asian countries (Fst > 0.15, p < 0.05). 667 Asian isolates clustered in 136 haplotypes and 739 African isolates clustered in 528 haplotypes by network analysis. The mutations I116T, L221I, Y128F, G228V and P299S were predicted as probably damaging by PolyPhen online service, while mutations L49V, R285G, R285S, P299S and K421N would lead to a significant increase of free energy difference (ΔΔG > 1) indicated a destabilization of protein structure. Conclusions Evidences in the present investigation supported that PfTRAP gene from Bioko Island and other malaria endemic countries is highly polymorphic (especially at T cell epitopes), which provided the genetic information background for developing an PfTRAP-based universal effective vaccine. Moreover, some mutations have been shown to be detrimental to the protein structure or function and deserve further study and continuous monitoring.

Funder

Key scientific research projects of Guangdong Provincial Department of Education

Guangxi Key Research and Development Foundation

Special technology program of Chaozhou for novel coronavirus infection control

Special research project of Guangdong for Novel coronavirus pneumonia epidemic prevention and contro

Publisher

Springer Science and Business Media LLC

Subject

Infectious Diseases,Parasitology

Reference36 articles.

1. WHO. World Malaria Report 2019. Geneva: World Health Organization; 2019. https://www.who.int/malaria/publications/world_malaria_report/en/.

2. Bioko Island Malaria Elimination Project. https://www.mcdinternational.org/bimep.

3. Bioko Island Malaria Control Project. https://www.mcdinternational.org/bimcp.

4. Equatorial Guinea Malaria Vaccine Initiative. https://www.mcdinternational.org/egmvi/en/

5. Muller HM, Scarselli E, Crisanti A. Thrombospondin related anonymous protein (TRAP) of Plasmodium falciparum in parasite-host cell interactions. Parassitologia. 1993;35(Suppl):69–72.

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