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对主要组织相容性复合体(MHC)DRB 外显子 2 和 DRA 外显子 3 片段在原发性陆生狂犬病传播媒介(浣熊)中的特征分析。

Characterization of major histocompatibility complex (MHC) DRB exon 2 and DRA exon 3 fragments in a primary terrestrial rabies vector (Procyon lotor).

机构信息

Environmental and Life Sciences Gradate Program, Trent University, Peterborough, Ontario, Canada.

出版信息

PLoS One. 2010 Aug 10;5(8):e12066. doi: 10.1371/journal.pone.0012066.

Abstract

The major histocompatibility complex (MHC) presents a unique system to explore links between genetic diversity and pathogens, as diversity within MHC is maintained in part by pathogen driven selection. While the majority of wildlife MHC studies have investigated species that are of conservation concern, here we characterize MHC variation in a common and broadly distributed species, the North American raccoon (Procyon lotor). Raccoons host an array of broadly distributed wildlife diseases (e.g., canine distemper, parvovirus and raccoon rabies virus) and present important human health risks as they persist in high densities and in close proximity to humans and livestock. To further explore how genetic variation influences the spread and maintenance of disease in raccoons we characterized a fragment of MHC class II DRA exon 3 (250 bp) and DRB exon 2 (228 bp). MHC DRA was found to be functionally monomorphic in the 32 individuals screened; whereas DRB exon 2 revealed 66 unique alleles among the 246 individuals screened. Between two and four alleles were observed in each individual suggesting we were amplifying a duplicated DRB locus. Nucleotide differences between DRB alleles ranged from 1 to 36 bp (0.4-15.8% divergence) and translated into 1 to 21 (1.3-27.6% divergence) amino acid differences. We detected a significant excess of nonsynonymous substitutions at the peptide binding region (P = 0.005), indicating that DRB exon 2 in raccoons has been influenced by positive selection. These data will form the basis of continued analyses into the spatial and temporal relationship of the raccoon rabies virus and the immunogenetic response in its primary host.

摘要

主要组织相容性复合体 (MHC) 提供了一个独特的系统来探索遗传多样性与病原体之间的联系,因为 MHC 内部的多样性部分是由病原体驱动的选择维持的。虽然大多数野生动物 MHC 研究都调查了受到保护关注的物种,但在这里,我们描述了一种常见且广泛分布的物种——北美的浣熊(Procyon lotor)的 MHC 变异。浣熊宿主广泛分布的野生动物疾病(例如犬瘟热、细小病毒和浣熊狂犬病病毒),并且由于它们在高密度下持续存在并与人类和牲畜密切接触,因此对人类健康构成重要风险。为了进一步探讨遗传变异如何影响浣熊疾病的传播和维持,我们对 MHC 类 II DRA 外显子 3(250bp)和 DRB 外显子 2(228bp)进行了特征描述。在筛选的 32 个个体中,MHC DRA 被发现在功能上是单态的;而在筛选的 246 个个体中,DRB 外显子 2 显示了 66 个独特的等位基因。每个个体观察到 2 到 4 个等位基因,表明我们正在扩增一个重复的 DRB 基因座。DRB 等位基因之间的核苷酸差异范围为 1 到 36bp(0.4-15.8%的差异),并转化为 1 到 21 个(1.3-27.6%的差异)氨基酸差异。我们在肽结合区检测到明显的非同义替换过剩(P=0.005),表明浣熊的 DRB 外显子 2 受到了正选择的影响。这些数据将为继续分析浣熊狂犬病病毒的时空关系及其主要宿主的免疫遗传反应奠定基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b8c/2919397/2f4975adcaad/pone.0012066.g001.jpg

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