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体内T细胞介导免疫的同型样抑制。I. 引发接触性超敏反应的抗原结合T细胞因子诱导的T细胞抑制的迟发型超敏反应特异性。

Isotype-like suppression of T cell-mediated immunity in vivo. I. Delayed-type hypersensitivity specificity of T cell suppression induced by antigen-binding T cell factors that initiate contact sensitivity.

作者信息

Ptak W, Bereta M, Ptak M, Askenase P W

出版信息

J Immunol. 1986 Mar 1;136(5):1554-63.

PMID:2419404
Abstract

A new form of immunoregulation is described that is based on the recent suggestion that the effector phase of delayed-type hypersensitivity (DTH) responses consists of a cascade of steps that are dependent on the sequential action of two types of antigen-specific Ly-1+ effector cells. According to this formulation, which is based on analysis of contact sensitivity (CS) in mice, DTH consists of at least two T cell-dependent steps that must occur in sequence. The first of these steps occurs within 2 hr of challenge and depends on DTH-initiating, antigen-binding, antigen-specific T cell factors that sensitize the tissues for an obligatory initial vasoactive step, which allows the antigen/major histocompatibility complex (MHC)-restricted, Ly-1+ effector T cells of classic 24 to 48 hr DTH responses to enter the tissues and produce chemoattractant lymphokines. We have now found that nonspecific suppression of CS responses can be induced by i.v. injection of these antigen-binding, CS-initiating T cell factors. Injection of the antigen-binding T cell factor induces Ly-2+, I-J-, cyclophosphamide sensitive, seemingly nonspecific suppressor T cells to inhibit initiation of CS responses. These suppressor cells do not affect the late-acting lymphokine-producing T cells, but probably act by preventing production of antigen-specific factors of the type that are required to initiate DTH responses. Furthermore, injection of CS-initiating antigen-binding T cell factors also induces suppression of sheep red blood cell (SRBC)-specific DTH, but does not affect classic anti-SRBC B cell responses, which are dependent on antigen/MHC-restricted Ly-1+ helper T cells; skin allograft rejection responses are also not affected. Thus, the suppression is DTH-specific. In addition, suppression induced by antigen-binding T cell factors is Igh and not MHC/H-2 restricted. These findings and data in the companion manuscript showing that these suppressor T cells act by production of soluble suppressor factors that bind to antigen-specific T cell factors of different antigenic specificities, cause us to suggest that the antigen-binding T cell factors are T cell isotype-like. Therefore, an isotype-like suppression is induced by these factors. This isotype-like suppression affects factor-producing cells of various antigenic specificities, may be mediated by T cell isotype-binding factors that are Igh restricted and block initiation of DTH responses, but does not affect conventional, antigen/MHC-restricted T cells, which may therefore have antigen receptors of a different isotype.

摘要

本文描述了一种新的免疫调节形式,该形式基于最近的一项建议,即迟发型超敏反应(DTH)的效应阶段由一系列步骤组成,这些步骤依赖于两种抗原特异性Ly-1 +效应细胞的顺序作用。根据基于对小鼠接触敏感性(CS)分析的这一表述,DTH至少由两个必须依次发生的T细胞依赖性步骤组成。这些步骤中的第一步发生在攻击后2小时内,依赖于启动DTH、结合抗原的抗原特异性T细胞因子,这些因子使组织对一个必需的初始血管活性步骤敏感,该步骤允许经典的24至48小时DTH反应中抗原/主要组织相容性复合体(MHC)限制的Ly-1 +效应T细胞进入组织并产生趋化性淋巴因子。我们现在发现,静脉注射这些结合抗原、启动CS的T细胞因子可诱导对CS反应的非特异性抑制。注射结合抗原的T细胞因子会诱导Ly-2 +、I-J -、环磷酰胺敏感、看似非特异性的抑制性T细胞抑制CS反应的启动。这些抑制性细胞不影响后期产生淋巴因子的T细胞,但可能通过阻止产生启动DTH反应所需类型的抗原特异性因子来发挥作用。此外,注射启动CS的结合抗原的T细胞因子也会诱导对绵羊红细胞(SRBC)特异性DTH的抑制,但不影响经典的抗SRBC B细胞反应,后者依赖于抗原/MHC限制的Ly-1 +辅助性T细胞;皮肤同种异体移植排斥反应也不受影响。因此,这种抑制是DTH特异性的。此外,结合抗原的T细胞因子诱导的抑制是Igh限制而非MHC/H-2限制的。这些发现以及配套论文中的数据表明,这些抑制性T细胞通过产生与不同抗原特异性的抗原特异性T细胞因子结合的可溶性抑制因子来发挥作用,这使我们认为结合抗原的T细胞因子类似于T细胞同种型。因此,这些因子可诱导类似同种型的抑制。这种类似同种型的抑制影响各种抗原特异性的因子产生细胞,可能由Igh限制的T细胞同种型结合因子介导,并阻断DTH反应的启动,但不影响传统的、抗原/MHC限制的T细胞,因此这些T细胞可能具有不同同种型的抗原受体。

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