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伊朗间日疟原虫分离株顶端膜抗原-1(AMA-1)的遗传多样性及自然选择效应

Genetic diversity and effect of natural selection at apical membrane antigen-1 (AMA-1) among Iranian Plasmodium vivax isolates.

作者信息

Esmaeili Rastaghi Ahmad Reza, Nedaei Fatemeh, Nahrevanian Hossein, Hoseinkhan Nazanin

机构信息

Department of Parasitology, Pasteur Institute or Iran, Tehran, Iran.

出版信息

Folia Parasitol (Praha). 2014 Oct;61(5):385-93.

Abstract

Apical membrane antigen-1 (AMA-1) of Plasmodium vivax Grassi et Feletti, 1890 is a promising malaria vaccine candidate. However, antigenic variation is a major problem to design a universal malaria vaccine. Hence, detailed understanding of the pvama-1 gene polymorphism can provide conductive information on this potential vaccine component. Therefore, this study investigated the extent of genetic polymorphisms at domain I (DI), DII and partial DIII of AMA-1 among Iranian P. vivax isolates. Out of 107 blood samples, 92 were analysed based on the quality of the sequencing data. The sequences were classified into 53 haplotypes. Amino acid changes were observed at 31 positions that 17 were located at DI, 11 were at DII and the rest of them (3 positions) were at DIII. Thus, codon polymorphisms at DI were found to be higher than DII. Also, five of these polymorphic codons (D242E, T374P, S389R, Y391F, I395F) were novel and have not been reported yet. Neutrality analysis by using the dN-dS difference (the difference between the rate of non-synonymous and synonymous mutations) showed a negative diversifying selection at DI, DII and across the length of both domains. The potential B-cell epitopes were found in 5 regions of the PvAMA-1 with 10 mutation sites (E145A, K188N, E189N/K/D, K190Q/E, P210S, E227V, D242E, R249H, G253E, K352E), whereas only one mutation (G288E) has been detected in intrinsically unstructured/disordered regions. Fixation index (Fst) estimation between Iranian and Indian isolates (0.0131) indicated a significant low genetic differentiation. Distribution of the polymorphic sites and IURs mapped on a three dimensional structure of PvAMA-1 showed that these regions were located at two opposite faces of the molecule. In conclusion, the results have significant value in the design and development of a malaria vaccine based on this antigen.

摘要

间日疟原虫(Plasmodium vivax Grassi et Feletti, 1890)的顶端膜抗原-1(AMA-1)是一种很有前景的疟疾疫苗候选物。然而,抗原变异是设计通用疟疾疫苗的一个主要问题。因此,详细了解间日疟原虫AMA-1(pvama-1)基因多态性可为这种潜在疫苗成分提供有益信息。为此,本研究调查了伊朗间日疟原虫分离株中AMA-1结构域I(DI)、DII和部分DIII的基因多态性程度。在107份血样中,基于测序数据质量对92份进行了分析。这些序列被分为53个单倍型。在31个位置观察到氨基酸变化,其中17个位于DI,11个位于DII,其余3个位于DIII。因此,发现DI处的密码子多态性高于DII。此外,这些多态密码子中的5个(D242E、T374P、S389R、Y391F、I395F)是新发现的,尚未见报道。通过非同义突变率与同义突变率之差(dN-dS差异)进行的中性分析显示,在DI、DII以及两个结构域的全长范围内存在负向多样化选择。在PvAMA-1的5个区域发现了潜在的B细胞表位,有10个突变位点(E145A、K188N、E189N/K/D、K190Q/E、P210S、E227V、D242E、R249H、G253E、K352E),而在内在无序区域仅检测到1个突变(G288E)。伊朗和印度分离株之间的固定指数(Fst)估计值(0.0131)表明遗传分化显著较低。多态性位点和内在无序区域(IURs)在PvAMA-1三维结构上的分布图显示,这些区域位于分子的两个相对面上。总之,这些结果对于基于该抗原的疟疾疫苗的设计和开发具有重要价值。

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