首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Human T-cell receptor (TCR) alpha/beta + CD4-CD8- T cells express oligoclonal TCRs share junctional motifs across TCR V beta-gene families and phenotypically resemble memory T cells.
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Human T-cell receptor (TCR) alpha/beta + CD4-CD8- T cells express oligoclonal TCRs share junctional motifs across TCR V beta-gene families and phenotypically resemble memory T cells.

机译:人T细胞受体(TCR)α/β+ CD4-CD8- T细胞表达寡克隆TCR在TCR Vβ基因家族中共有连接基序并且在表型上类似于记忆T细胞。

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摘要

Most human T cells express the TCR alpha/beta and either CD4 or CD8 molecules (single positive, SP); however, small numbers lack CD4 and CD8. In inbred mice, alpha/beta CD4-CD8- (double negative, DN) T cells preferentially express certain beta variable region (V beta) families and may arise via unique developmental pathways. Increased percentages of alpha/beta DN T cells have been identified in some human and murine autoimmune and immunodeficiency diseases. However, their contribution to disease pathology or normal immunity is unknown. To study the cell surface phenotype and TCR diversity of human alpha/beta DN T cells, these cells were isolated from the peripheral blood of healthy adults. The proportion of alpha/beta DN T cells expressing molecules associated with activation (HLA-DR), previous exposure to antigen (CD45RO), and cytotoxic function (CD56, CD57, and CD11b) was increased relative to SP T cells. The TCR V beta repertoire of alpha/beta DN T cells was different from that of alpha/beta SP T cells, although most major gene families were present. For example, higher proportions of V beta 11, a minor gene family in peripheral blood leukocytes, were found in most alpha/beta DN T-cell samples. In contrast to mice, no dominant V beta family was used consistently in different human individuals. Within an individual alpha/beta DN T cells possessed an oligoclonal TCR beta repertoire with conservation of several distinct junctional amino acid motifs with one joined to three different V beta genes in two individuals, suggesting that these cells have undergone a selection process driven by a limited set of ligands. The possibility that they may represent, at least in part, originally SP T cells anergized by down-modulation of CD4 or CD8 must also be entertained. Overall, this study demonstrates that human peripheral blood alpha/beta DN T cells possess unique phenotypic and TCR beta repertoire characteristics when compared with the major alpha/beta SP T cell populations and thus may serve specialized immunologic functions and/or have an unusual origin.
机译:大多数人类T细胞都表达TCR alpha / beta和CD4或CD8分子(单阳性,SP);但是,少数人缺少CD4和CD8。在近交小鼠中,α/βCD4-CD8-(双阴性,DN)T细胞优先表达某些β可变区(Vβ)家族,并可能通过独特的发育途径而产生。在某些人类和鼠类自身免疫性疾病和免疫缺陷疾病中,已经确定了增加的α/βDN T细胞百分比。但是,它们对疾病病理或正常免疫的作用尚不清楚。为了研究人类α/βDN T细胞的细胞表面表型和TCR多样性,从健康成年人的外周血中分离了这些细胞。相对于SP T细胞,表达与激活(HLA-DR),先前暴露于抗原(CD45RO)和细胞毒性功能(CD56,CD57和CD11b)相关的分子的α/βDN T细胞的比例有所增加。尽管存在大多数主要基因家族,但α/βDN T细胞的TCR Vβ组成与α/βSP T细胞不同。例如,在大多数α/βDN T细胞样品中发现较高比例的Vβ11(一种外周血白细胞中的次要基因家族)。与小鼠不同,没有在不同的人类个体中一致使用显性的V beta家族。在单个α/βDN T细胞内,具有一个寡克隆TCRβ组成部分,保留了几个不同的连接氨基酸基序,其中一个与两个个体中的三个不同Vβ基因相连,这表明这些细胞经历了有限的驱动选择过程一组配体。还必须考虑它们可能至少部分代表通过CD4或CD8的下调而变质的原始SP T细胞的可能性。总体而言,这项研究表明,与主要的alpha / beta SP T细胞群体相比,人外周血alpha / beta DN T细胞具有独特的表型和TCR beta的库特征,因此可能具有特殊的免疫功能和/或具有异常的起源。

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