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自然选择对新兴人畜共患疟原虫 Inui 属的顶膜抗原 1(AMA1)的影响。

Natural selection on apical membrane antigen 1 (AMA1) of an emerging zoonotic malaria parasite Plasmodium inui.

机构信息

Molecular Biology of Malaria and Opportunistic Parasites Research Unit, Department of Parasitology, Faculty of Medicine, Chulalongkorn University, Bangkok, Thailand.

Faculty of Health Science and Technology, Community Public Health Program, Southern College of Technology, Nakorn Si Thammarat, Thailand.

出版信息

Sci Rep. 2024 Oct 9;14(1):23637. doi: 10.1038/s41598-024-74785-8.

Abstract

Apical membrane antigen 1 (AMA1) of malaria parasites plays an important role in host cell invasion. Antibodies to AMA1 can inhibit malaria merozoite invasion of erythrocytes while vaccine-induced specific cytotoxic T cell responses to this protein are associated with clinical protection. Polymorphisms in AMA1 of Plasmodium falciparum (PfAMA1) and P. vivax (PvAMA1) are of concern for vaccine development. To date, little is known about sequence diversity in ama1 of P. inui (Piama1), an emerging zoonotic malaria parasite. In this study, 80 complete Piama1 coding sequences were obtained from 57 macaques in Thailand that defined 60 haplotypes clustering in two phylogenetic lineages. In total, 74 nucleotide substitutions were identified and distributed unevenly across the gene. Blockwise analysis of the rates of synonymous (d) and nonsynonymous (d) nucleotide substitutions did not show a significant deviation from neutrality among Thai isolates. However, significantly negative Tajima's D values were detected in domain I and the loop region of domain II, implying purifying selection. Codon-based analysis of d/d has identified 12 and 14 codons under positive and negative selections, respectively. Meanwhile, 85 amino acid substitutions were identified among 80 Thai and 11 non-Thai PiAMA1 sequences. Of these, 48 substituted residues had a significant alteration in physicochemical properties, suggesting positive selection. More than half of these positively selected amino acids (32 of 48) corresponded to the predicted B-cell or T-cell epitopes, suggesting that selective pressure could be mediated by host immunity. Importantly, 14 amino acid substitutions were singletons and predicted to be deleterious that could be subject to ongoing purifying selection or elimination. Besides genetic drift and natural selection, intragenic recombination identified in domain II could generate sequence variation in Piama1. It is likely that malarial ama1 exhibits interspecies differences in evolutionary histories. Knowledge of the sequence diversity of the Piama1 locus further provides an evolutionary perspective of this important malaria vaccine candidate.

摘要

疟原虫顶膜抗原 1(AMA1)在宿主细胞入侵中发挥重要作用。针对 AMA1 的抗体可抑制疟原虫裂殖子入侵红细胞,而针对该蛋白的疫苗诱导的特异性细胞毒性 T 细胞反应与临床保护相关。恶性疟原虫(PfAMA1)和间日疟原虫(PvAMA1)AMA1 的多态性是疫苗开发的关注点。迄今为止,人们对新出现的人畜共患疟原虫(Piama1)ama1 的序列多样性知之甚少。在这项研究中,从泰国的 57 只猕猴中获得了 80 个完整的 Piama1 编码序列,这些序列定义了 60 个聚类在两个系统发育分支中的单倍型。总共鉴定出 74 个核苷酸替换,并且在整个基因中分布不均匀。对泰国分离株进行的同义(d)和非同义(d)核苷酸替换率的分块分析表明,它们没有偏离中性。然而,在结构域 I 和结构域 II 的环区中检测到显著的负 Tajima 的 D 值,表明存在纯化选择。基于密码子的 d/d 分析确定了 12 个和 14 个分别受到正选择和负选择的密码子。同时,在 80 个泰国和 11 个非泰国 PiAMA1 序列中鉴定出 85 个氨基酸替换。其中,48 个取代残基在理化性质上有显著改变,表明存在正选择。这些被正选择的氨基酸(48 个中的 32 个)中有一半以上对应于预测的 B 细胞或 T 细胞表位,表明选择压力可能由宿主免疫介导。重要的是,14 个氨基酸替换是单倍体,预测为有害,可能受到持续的纯化选择或消除的影响。除了遗传漂变和自然选择之外,在结构域 II 中鉴定到的基因内重组可能会导致 Piama1 中的序列变异。疟原虫 ama1 的进化历史可能存在种间差异。了解 Piama1 基因座的序列多样性进一步为这一重要疟疾疫苗候选物提供了进化视角。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7283/11464719/205cc52daa2d/41598_2024_74785_Fig1_HTML.jpg

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