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疟原虫两种红细胞结合抗原的遗传结构揭示了选择的对比模式。

Genetic structure of two erythrocyte binding antigens of Plasmodium falciparum reveals a contrasting pattern of selection.

机构信息

Department of Biochemistry, University of Calcutta, 35, Ballygunge Circular Road, Kolkata 700 019, West Bengal, India.

Mitra Tower, Lake Town, Block-A, Kolkata 700 089, India.

出版信息

Infect Genet Evol. 2018 Jan;57:64-74. doi: 10.1016/j.meegid.2017.11.006. Epub 2017 Nov 8.

Abstract

Erythrocyte binding antigens 175 (EBA-175) and 140 (EBA-140) play key roles in erythrocyte invasion by binding to glycophorin A (GPA) and C (GPC) respectively in human malaria. Since antigenic variation in malaria endemic region is a major barrier to development of effective vaccine, we explore the nature and pattern of sequence diversity of these two vaccine candidates in Kolkata, India. Population genetic parameters based on parasite sequences representing region II of Pfeba-175 and Pfeba-140 genes were estimated using DnaSP V.5.10 and MEGA version 6.0. A novel molecular docking approach was implemented to assess the binding affinities of Kolkata Pfeba-175 variants with GPA. P. falciparum Kolkata isolates experienced a recent population expansion as documented by negative Tajima's D, Fu & Li's statistics, unimodal mismatch distribution and star-like median-joining network for both loci. Positive selection seemed to play a major role in shaping the diversity of Pfeba-175 (d/d=2.45, and McDonald-Kreitman P-value=0.04) with successive accumulation of Q584K/E, E592A and R664S deriving high frequency haplotypes designated here as F2KH3 and F2KH1. In silico molecular docking demonstrated that polypeptides encoded by F2KH1 and F2KH3 were capable of engaging the parasite ligand into energetically favorable interaction with GPA. Our data demonstrated emergence of Pfeba-175 sequences harboring selectively advantageous nonsynonymous substitutions on Pf3D7 sequence background in the Kolkata parasite isolates. A contrasting pattern of Pf3D7-centric expansion of parasite sequences was noted for Pfeba-140. Together, this study provides a firm genetic and biological support favoring a dominant role of EBA-175 in erythrocyte invasion.

摘要

红细胞结合抗原 175(EBA-175)和 140(EBA-140)在人类疟疾中分别通过与糖蛋白 A(GPA)和 C(GPC)结合,在红细胞入侵中发挥关键作用。由于疟疾流行地区的抗原变异是开发有效疫苗的主要障碍,我们在印度加尔各答探索了这两种疫苗候选物的性质和序列多样性模式。使用 DnaSP V.5.10 和 MEGA 版本 6.0 基于代表 Pfeba-175 和 Pfeba-140 基因区域 II 的寄生虫序列估计了种群遗传参数。一种新的分子对接方法被用于评估加尔各答 Pfeba-175 变体与 GPA 的结合亲和力。如两个基因座的负 Tajima 的 D、Fu 和 Li 的统计、单峰不匹配分布和星状中值连接网络所示,P. falciparum 加尔各答分离株经历了近期的种群扩张。正选择似乎在塑造 Pfeba-175 的多样性方面发挥了主要作用(d/d=2.45,McDonald-Kreitman P 值=0.04),连续积累 Q584K/E、E592A 和 R664S 导致高频率单倍型指定为 F2KH3 和 F2KH1。体内分子对接表明,由 F2KH1 和 F2KH3 编码的多肽能够使寄生虫配体与 GPA 进行能量有利的相互作用。我们的数据表明,在加尔各答寄生虫分离株中,Pf3D7 序列背景下出现了携带选择性有利非同义突变的 Pfeba-175 序列。对于 Pfeba-140,观察到以 Pf3D7 为中心的寄生虫序列扩张的对比模式。总之,这项研究提供了有力的遗传和生物学支持,支持 EBA-175 在红细胞入侵中发挥主导作用。

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