Geographical and temporal dynamics of genetic diversity of Plasmodium falciparum merozoite surface proteins 1/2 in India.

Q3 Immunology and Microbiology Journal of Parasitic Diseases Pub Date : 2024-09-01 Epub Date: 2024-06-28 DOI:10.1007/s12639-024-01698-8
Loick Pradel Kojom Foko, Jahnvi Jakhan, Geetika Narang, Vineeta Singh
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Abstract

The high genetic diversity of Plasmodium falciparum (Pf) is a big obstacle to successful vaccine development programs. Here, the geographical and temporal dynamics of the genetic diversity of Indian Pf isolates from patients living in Ranchi, Raipur, Mewat, and Rourkela were analyzed. Typing and frequency of merozoite surface protein 1 and 2 genes (pfmsp1/2), their genotypes, clonality, heterozygosity, multiplicity of infection, and neutral evolution metrics were computed. A phylogenetic analysis was also performed for these two genes. The dominant allelic types were K1 (55%) and MAD20 (55%) for msp1, and FC27 (64.7%) for msp2. Infections were mainly monoclonal in Ranchi and Mewat while polyclonal in Raipur and Rourkela. Polyclonal infections dropped from 57.1 to 71.3% in 2013 to 33.3-33.4% in 2016 in Raipur. K1 and MAD20 sequences were highly diverse due to the organization of the amino acid units SGG, SVA, SVT, and SGN. The IC/3D7-related G,S,A-rich region showed a large variation of four to eight amino acid repeats, including mostly GAVASA (81.8%), GSGA (54.5%), and GASGSA (45.5%). The 32-amino acid sequence of the FC27 type was present in all isolates with several mutations. The msp1/2 sequences were not under neutral evolution, except the K1 family, which is under balancing selection. The msp1/2 sequences are phylogenetically closer to previous Indian sequences than those from Africa, Asia, the Americas, and Oceania. This study outlines a high genetic diversity of Pf infections with complex structure, and evolutionary signature changed with time.

Supplementary information: The online version contains supplementary material available at 10.1007/s12639-024-01698-8.

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印度恶性疟原虫裂殖体表面蛋白 1/2遗传多样性的地域和时间动态。
恶性疟原虫(Plasmodium falciparum,Pf)的高度遗传多样性是疫苗开发计划取得成功的一大障碍。在此,研究人员分析了来自兰契、赖普尔、梅瓦特和鲁尔克勒患者的印度恶性疟原虫分离株遗传多样性的地理和时间动态。计算了裂殖体表面蛋白 1 和 2 基因(pfmsp1/2)的类型和频率、基因型、克隆性、杂合性、感染倍数和中性进化指标。还对这两个基因进行了系统进化分析。msp1的显性等位基因类型为K1(55%)和MAD20(55%),msp2为FC27(64.7%)。兰契和梅瓦特的感染主要是单克隆感染,而赖普尔和鲁克拉则是多克隆感染。莱普尔的多克隆感染率从 2013 年的 57.1% 到 71.3% 下降到 2016 年的 33.3%-33.4%。由于氨基酸单位 SGG、SVA、SVT 和 SGN 的组织结构,K1 和 MAD20 序列具有高度多样性。与IC/3D7相关的富含G、S、A的区域出现了4至8个氨基酸重复的较大变化,主要包括GAVASA(81.8%)、GSGA(54.5%)和GASGSA(45.5%)。FC27型的32个氨基酸序列在所有分离株中都存在,并有几种变异。除 K1 家族处于平衡选择外,其他 msp1/2 序列均未发生中性进化。与非洲、亚洲、美洲和大洋洲的 msp1/2 序列相比,印度的 msp1/2 序列在系统发育上更接近于以前的印度序列。这项研究概述了 Pf 感染的高度遗传多样性,其结构复杂,进化特征随时间而变化:在线版本包含补充材料,可查阅 10.1007/s12639-024-01698-8。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Parasitic Diseases
Journal of Parasitic Diseases Immunology and Microbiology-Parasitology
CiteScore
2.60
自引率
0.00%
发文量
86
期刊介绍: The primary constituency of the Journal of Parasitic Diseases is parasitology. It publishes original research papers (pure, applied and clinical), which contribute significantly to any area of parasitology. Research papers on various aspects of cellular and molecular parasitology are welcome.
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