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TCR-CD3复合物触发的人T细胞中外切腺苷脱氨酶和CD26的表达。腺苷脱氨酶作为共刺激分子的可能作用。

Expression of ecto-adenosine deaminase and CD26 in human T cells triggered by the TCR-CD3 complex. Possible role of adenosine deaminase as costimulatory molecule.

作者信息

Martín M, Huguet J, Centelles J J, Franco R

机构信息

Department of Biochemistry and Molecular Biology, University of Barcelona, Catalonia, Spain.

出版信息

J Immunol. 1995 Nov 15;155(10):4630-43.

PMID:7594462
Abstract

The expression of surface adenosine deaminase (ADA) and CD26 in activated human T cells was studied by flow cytometry. PBLs and CD3+ or CD4+ cells, when subjected to a variety of stimuli (anti-CD3 Abs plus IL-2 or phorbol esters), presented two structurally different cell populations, which differed in size and cellular complexity (populations B1 and B2). In PBLs triggered by an anti-CD3 mAb there was no significant increase of expression of either surface ADA or CD26 in cells of population B1, whose structure is similar to that of nonstimulated cells. In contrast, there was a significant increase in the percentage of expression of ADA and CD26 in the population B2, which corresponds to structurally more complex and larger cells. In the case of activation via TCR-CD3 but in the presence of IL-2 or via phorbol esters, the increase was found in cells from both populations, but B2 cells always showed a higher percentage of expression than B1 cells. The results of increased expression of surface ADA and CD26 were similar in whole T cells or in purer preparations such as CD3+ or CD4+ lymphocytes. Polyclonal Abs against ADA were not able to induce an activation response in T cells even when cross-linked by a secondary Ab. Interestingly, these Abs produced anergy in CD4+ cells subjected to an anti-CD3 stimulus. In contrast, addition of ADA produced an enzyme-independent synergism in the response through the TCR-CD3 complex. In T cells, ADA and CD26 colocalized on the surface of T cells; thus, the effect of exogenous ADA seems to be mediated by CD26 molecules that are not interacting with endogenous ADA (spare CD26 molecules). The presence of spare CD26 molecules on the surface of CD4+ cells was demonstrated by flow cytometry in the presence of exogenous ADA and also by confocal microscopy. The set of results strongly indicates that ADA binding to CD26 produces a costimulatory response in T cell activation events.

摘要

通过流式细胞术研究了活化的人T细胞表面腺苷脱氨酶(ADA)和CD26的表达。外周血淋巴细胞(PBLs)以及CD3⁺或CD4⁺细胞在受到多种刺激(抗CD3抗体加白细胞介素-2或佛波酯)时,呈现出两个结构不同的细胞群体,它们在大小和细胞复杂性上存在差异(群体B1和B2)。在由抗CD3单克隆抗体触发的PBLs中,群体B1细胞的表面ADA或CD26表达均无显著增加,其结构与未刺激细胞相似。相反,群体B2中ADA和CD26的表达百分比显著增加,该群体对应于结构上更复杂且更大的细胞。在通过TCR - CD3但存在白细胞介素-2或通过佛波酯激活的情况下,两个群体的细胞中均发现了增加,但B2细胞的表达百分比始终高于B1细胞。表面ADA和CD26表达增加的结果在全T细胞或更纯的制剂(如CD3⁺或CD4⁺淋巴细胞)中相似。抗ADA的多克隆抗体即使通过二抗交联也无法在T细胞中诱导激活反应。有趣的是,这些抗体在受到抗CD3刺激的CD4⁺细胞中产生无反应性。相反,添加ADA在通过TCR - CD3复合物的反应中产生了不依赖酶的协同作用。在T细胞中,ADA和CD26共定位于T细胞表面;因此,外源性ADA的作用似乎是由不与内源性ADA相互作用的CD26分子介导的(备用CD26分子)。在外源性ADA存在的情况下,通过流式细胞术以及共聚焦显微镜证实了CD4⁺细胞表面存在备用CD26分子。这一系列结果有力地表明,ADA与CD26的结合在T细胞激活事件中产生共刺激反应。

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