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在非哺乳动物脊椎动物中鉴定前 T 细胞受体 α 链挑战了该分子的结构-功能。

Identification of the pre-T-cell receptor alpha chain in nonmammalian vertebrates challenges the structure-function of the molecule.

机构信息

Université Pierre et Marie Curie, Unité Mixte de Recherche-Centre National de la Recherche Scientifique 7622, 75252 Paris Cedex 05, France.

出版信息

Proc Natl Acad Sci U S A. 2010 Nov 16;107(46):19991-6. doi: 10.1073/pnas.1010166107. Epub 2010 Nov 2.

Abstract

In humans and mice, the early development of αβ T cells is controlled by the pre-T-cell receptor α chain (pTα) that is covalently associated with the T-cell receptor β (TCRβ) chain to form the pre-T-cell receptor (pre-TCR) at the thymocyte surface. Pre-TCR functions in a ligand-independent manner through self-oligomerization mediated by pTα. Using in silico and gene synteny-based approaches, we identified the pTα gene (PTCRA) in four sauropsid (three birds and one reptile) genomes. We also identified 25 mammalian PTCRA sequences now covering all mammalian lineages. Gene synteny around PTCRA is remarkably conserved in mammals but differences upstream of PTCRA in sauropsids suggest chromosomal rearrangements. PTCRA organization is highly similar in sauropsids and mammals. However, comparative analyses of the pTα functional domains indicate that sauropsids, monotremes, marsupials, and lagomorphs display a short pTα cytoplasmic tail and lack most residues shown to be critical for human and murine pre-TCR self-oligomerization. Chicken PTCRA transcripts similar to those in mammals were detected in immature double-negative and double-positive thymocytes. These findings give clues about the evolution of this key molecule in amniotes and suggest that the ancestral function of pTα was exclusively to enable expression of the TCRβ chain at the thymocyte surface and to allow binding of pre-TCR to the CD3 complex. Together, our data provide arguments for revisiting the current model of pTα signaling.

摘要

在人类和小鼠中,αβ T 细胞的早期发育受前 T 细胞受体α 链(pTα)的控制,该链与 T 细胞受体β(TCRβ)链共价结合,在胸腺细胞表面形成前 T 细胞受体(pre-TCR)。pre-TCR 通过 pTα 介导的自身寡聚化以非配体依赖的方式发挥作用。我们通过计算机模拟和基因同线性方法,在四个蜥形目动物(三种鸟类和一种爬行动物)基因组中鉴定出 pTα 基因(PTCRA)。我们还鉴定了 25 种哺乳动物 PTCRA 序列,现在涵盖了所有哺乳动物谱系。哺乳动物中 PTCRA 周围的基因同线性非常保守,但在蜥形目中 PTCRA 上游的差异表明存在染色体重排。PTCRA 的组织在蜥形目动物和哺乳动物中非常相似。然而,对 pTα 功能域的比较分析表明,蜥形目动物、单孔目动物、有袋类动物和兔形目动物显示出短的 pTα 细胞质尾巴,并且缺乏对人类和小鼠 pre-TCR 自身寡聚化至关重要的大多数残基。在未成熟的双阴性和双阳性胸腺细胞中检测到类似于哺乳动物的鸡 PTCRA 转录本。这些发现为研究有胎盘动物中这个关键分子的进化提供了线索,并表明 pTα 的祖先功能是专门使 TCRβ 链在胸腺细胞表面表达,并允许 pre-TCR 与 CD3 复合物结合。总之,我们的数据为重新审视 pTα 信号的当前模型提供了依据。

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