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BG1 has a major role in MHC-linked resistance to malignant lymphoma in the chicken

机译:BG1在MHC相关的鸡恶性淋巴瘤耐药中起主要作用

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摘要

Pathogen selection is postulated to drive MHC allelic diversity at loci for antigen presentation. However, readily apparent MHC infectious disease associations are rare in most species. The strong link between MHC-B haplotype and the occurrence of virally induced tumors in the chicken provides a means for defining the relationship between pathogen selection and MHC polymorphism. Here, we verified a significant difference in resistance to gallid herpesvirus-2 (GaHV-2)-induced lymphomas (Marek's disease) conferred by two closely-related recombinant MHC-B haplotypes. We mapped the crossover breakpoints that distinguish these haplotypes to the highly polymorphic BG1 locus. BG1 encodes an Ig-superfamily type I transmembrane receptor-like protein that contains an immunoreceptor tyrosine-based inhibition motif (ITIM), which undergoes phosphorylation and is recognized by Src homology 2 domain-containing protein tyrosine phosphatase (SHP-2). The recombinant haplotypes are identical, except for differences within the BG1 3′-untranslated region (3′-UTR). The 3′-UTR of the BG1 allele associated with increased lymphoma contains a 225-bp insert of retroviral origin and showed greater inhibition of luciferase reporter gene translation compared to the other allele. These findings suggest that BG1 could affect the outcome of GaHV-2 infection through modulation of the lymphoid cell responsiveness to infection, a condition that is critical for GaHV-2 replication and in which the MHC-B haplotype has been previously implicated. This work provides a mechanism by which MHC-B region genetics contributes to the incidence of GaHV-2-induced malignant lymphoma in the chicken and invites consideration of the possibility that similar mechanisms might affect the incidence of lymphomas associated with other oncogenic viral infections.
机译:假定病原体选择可在基因座上驱动MHC等位基因多样性以进行抗原呈递。但是,在大多数物种中,很容易发现明显的MHC传染病关联。 MHC-B单倍型与鸡中病毒诱导的肿瘤的发生之间的紧密联系为定义病原体选择和MHC多态性之间的关系提供了一种手段。在这里,我们验证了由两个密切相关的重组MHC-B单倍型赋予的对鸡胆疱疹病毒2(GaHV-2)诱导的淋巴瘤(马立克氏病)的抵抗力的显着差异。我们将区分这些单倍型的交叉断点映射到高度多态的BG1基因座。 BG1编码一个Ig超家族I型跨膜受体样蛋白,该蛋白包含基于免疫受体酪氨酸的抑制基序(ITIM),该基序经过磷酸化作用,并被包含Src同源2域的蛋白酪氨酸磷酸酶(SHP-2)识别。重组单倍型是相同的,除了BG1 3'非翻译区(3'-UTR)内的差异。与其他淋巴瘤相关的BG1等位基因的3'-UTR包含一个225 bp的逆转录病毒插入片段,与其他等位基因相比,对荧光素酶报道基因的翻译显示出更大的抑制作用。这些发现表明,BG1可能通过调节淋巴样细胞对感染的反应性来影响GaHV-2感染的结果,这种情况对于GaHV-2复制至关重要,并且以前曾涉及过MHC-B单倍型。这项工作提供了一种机制,通过该机制,MHC-B区遗传学有助于鸡中GaHV-2诱导的恶性淋巴瘤的发生,并提请考虑类似机制可能影响与其他致癌病毒感染相关的淋巴瘤发生率的可能性。

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