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Major histocompatibility complex alleles associated with parasite susceptibility in wild giant pandas

机译:野生大熊猫与寄生虫敏感性相关的主要组织相容性复杂等位基因

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摘要

Major histocompatibility complex (MHC) polymorphism is thought to be driven by antagonistic coevolution between pathogens and hosts, mediated through either overdominance or frequency-dependent selection. However, investigations under natural conditions are still rare for endangered mammals which often exhibit depleted variation, and the mechanism of selection underlying the maintenance of characteristics remains a considerable debate. In this study, 87 wild giant pandas were used to investigate MHC variation associated with parasite load. With the knowledge of the MHC profile provided by the genomic data of the giant panda, seven DRB1, seven DQA1 and eight DQA2 alleles were identified at each single locus. Positive selection evidenced by a significantly higher number of non-synonymous substitutions per non-synonymous codon site relative to synonymous substitutions per synonymous codon site could only be detected at the DRB1 locus, which leads to the speculation that DRB1 may have a more important role in dealing with parasite infection for pandas. Coprological analyses revealed that 55.17% of individuals exhibited infection with 1–2 helminthes and 95.3% of infected pandas carried Baylisascaris shroederi. Using a generalized linear model, we found that Aime-DRB1*10 was significantly associated with parasite infection, but no resistant alleles could be detected. MHC heterozygosity of the pandas was found to be uncorrelated with the infection status or the infection intensity. These results suggested that the possible selection mechanisms in extant wild pandas may be frequency dependent rather than being determined by overdominance selection. Our findings could guide the candidate selection for the ongoing reintroduction or translocation of pandas.
机译:主要的组织相容性复合体(MHC)多态性被认为是由病原体和宿主之间的拮抗协同进化驱动的,通过过度控制或频率依赖性选择介导。然而,在自然条件下对濒临灭绝的哺乳动物的研究仍然很少,这些哺乳动物通常表现出枯竭的变异性,而维持特征的选择机制仍然是一个颇有争议的问题。在这项研究中,使用了87只野生大熊猫来研究与寄生虫负荷相关的MHC变化。借助大熊猫基因组数据提供的MHC谱图知识,在每个单个基因座上鉴定了七个DRB1,七个DQA1和八个DQA2等位基因。相对于每个同义密码子位点的同义替换,每个非同义密码子位点的非同义替换数量明显更多,这表明只能在DRB1基因座处检测到阳性选择,这导致人们推测DRB1可能在处理大熊猫的寄生虫感染。细菌学分析表明,有55.17%的人表现出被1-2蠕虫感染,而95.3%的被感染的大熊猫携带了Baylisascaris shroederi。使用广义线性模型,我们发现Aime-DRB1 * 10与寄生虫感染显着相关,但未检测到抗性等位基因。发现大熊猫的MHC杂合性与感染状况或感染强度无关。这些结果表明,现存野生大熊猫的可能选择机制可能与频率有关,而不是由过度选择所决定。我们的研究结果可以指导正在进行的大熊猫重新引入或易位的候选人选择。

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