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全面分析和鉴定普通狨猴 TCRα 链序列。

Comprehensive analysis and characterization of the TCR alpha chain sequences in the common marmoset.

机构信息

Department of Rheumatology and Clinical Immunology, Clinical Research Center for Allergy and Rheumatology, Sagamihara National Hospital, National Hospital Organization, 18-1 Sakuradai, Sagamihara, Kanagawa, 228-0815, Japan.

出版信息

Immunogenetics. 2010 Jun;62(6):383-95. doi: 10.1007/s00251-010-0445-0. Epub 2010 Apr 20.

Abstract

The common marmoset (Callithrix jacchus) is useful as a nonhuman primate model of human diseases. Although the marmoset model has great potential for studying autoimmune diseases and immune responses against pathogens, little information is available regarding the genes involved in adaptive immunity. Here, we identified one TCR alpha constant (TRAC), 46 TRAJ (joining), and 35 TRAV (variable) segments from marmoset cDNA. Marmoset TRAC, TRAJ, and TRAV shared 80%, 68-100%, and 79-98% identity with their human counterparts at the amino acid level, respectively. The amino acid sequences were less conserved in TRAC than in TCRbeta chain constant (TRBC). Comparative analysis of TRAV between marmosets and humans showed that the rates of synonymous substitutions per site (d(S)) were not significantly different between the framework regions (FRs) and complementarity determining regions (CDRs), whereas the rates of nonsynonymous substitutions per site (d(N)) were significantly lower in the FRs than in CDRs. Interestingly, the d(N) values of the CDRs were greater for TRBV than TRAV. These results suggested that after the divergence of Catarrhini from Platyrrhini, amino acid substitutions were decreased in the FRs by purifying selection and occurred more frequently in CDRbeta than in CDRalpha by positive selection, probably depending on structural and functional constraints. This study provides not only useful information facilitating the investigation of adaptive immunity using the marmoset model but also new insight into the molecular evolution of the TCR heterodimer in primate species.

摘要

普通狨猴(Callithrix jacchus)是一种有用的非人类灵长类动物模型,可用于研究人类疾病。尽管狨猴模型在研究自身免疫性疾病和针对病原体的免疫反应方面具有巨大的潜力,但有关适应性免疫涉及的基因的信息却很少。在这里,我们从狨猴 cDNA 中鉴定出一个 TCR alpha 恒定(TRAC)、46 个 TRAJ(连接)和 35 个 TRAV(可变)片段。狨猴 TRAC、TRAJ 和 TRAV 在氨基酸水平上分别与人类同源物具有 80%、68-100%和 79-98%的同一性。TRAC 的氨基酸序列不如 TCRbeta 链恒定(TRBC)保守。狨猴和人类之间的 TRAV 比较分析表明,同义替换率(d(S))在框架区(FR)和互补决定区(CDR)之间没有显著差异,而非同义替换率(d(N))在 FR 中显著低于 CDR。有趣的是,CDR 中的 d(N)值在 TRBV 中大于 TRAV。这些结果表明,在类人猿与阔鼻猴类分化之后,通过纯化选择,FR 中的氨基酸替换减少,而 CDRbeta 中的正选择比 CDRalpha 中的正选择更频繁,这可能取决于结构和功能约束。这项研究不仅为使用狨猴模型研究适应性免疫提供了有用的信息,而且还为灵长类动物 TCR 异二聚体的分子进化提供了新的见解。

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