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经HGG耐受脾细胞对免疫反应进行特异性、短暂性抑制。II. 效应细胞和靶细胞。

Specific, transient suppression of the immune response by HGG tolerant spleen cells. II. Effector cells and target cells.

作者信息

Doyle M V, Parks E, Weigle W O

出版信息

J Immunol. 1976 Oct;117(4):1152-8.

PMID:61992
Abstract

In a previous report, it was shown that spleen cells from mice made tolerant to human gamma-globulin (HGG)5 could specifically inhibit the immune response of normal spleen cells after adoptive transfer to lethally irradiated recipients. However, that report also showed that the suppressive activity was only transiently associated with tolerant spleen cell populations. It was concluded from those experiments that while suppressive activity could be demonstrated in tolerant spleen cells under certain conditions, such activity was not obligatory for the maintainance of the tolerant state. The experiments presented here were performed to determine the nature of the effector cell(s) and the target cell(s) involved in this system of suppression of the immune response. Treatment of cells from tolerant animals with anti-thymocyte serum and complement to remove thymus-derived (T) cells completely abrogated suppresive activity. Removal of adherent cells from tolerant spleen cells by passage over glass wool columns resulted in partial loss of the suppression. The inhibitory activity of the suppressor cells was resistant to 900 R irradiation regardless of whether the tolerant spleen cells were irradiated before or after adoptive transfer. The cellular target(s) for the supprssor cells was examined by using lipopolysaccharide (LPS) as an alternative source of helper activity for the response to HGG. LPS, injected at the time of the initial antigenic challenge of mice that had been reconstituted with tolerant and normal spleen cells, prevented the expression of suppression against bone marrow-derived (B) cells. However, when LPS was presented only at the time of secondary antigenic challenge, it was unable to overcome suppression of the immune response of reconstituted recipients. Thus, LPS could produce a state where the B cells were resistant to suppression, but LPS could not rescue the responsiveness of B cells once the cells in the reconstituted recipient had been suppressed. In addition, the immune response to both the hapten dinitrophenol (DNP) and the carrier (HGG) were suppressed when recipients of tolerant and normal spleen cells were challenged with DNP6HGG. This indicates that T helper cells are also a target for suppression. The results presented in this paper are discussed in relation to a possible mechanism of suppression which proposes that suppressive activity represents the induction of tolerance in immunologically competent cells by HCG which is closely associated with the tolerant spleen cells.

摘要

在之前的一份报告中显示,对人γ球蛋白(HGG)产生耐受的小鼠的脾细胞,在过继转移至致死剂量照射的受体后,能够特异性抑制正常脾细胞的免疫反应。然而,该报告还表明,抑制活性仅与耐受脾细胞群体短暂相关。从这些实验得出的结论是,虽然在某些条件下可以在耐受脾细胞中证明抑制活性,但这种活性对于维持耐受状态并非必需。进行此处展示的实验是为了确定参与该免疫反应抑制系统的效应细胞和靶细胞的性质。用抗胸腺细胞血清和补体处理来自耐受动物的细胞以完全去除胸腺来源(T)细胞,可完全消除抑制活性。通过玻璃棉柱传代从耐受脾细胞中去除贴壁细胞会导致抑制作用部分丧失。无论耐受脾细胞在过继转移之前还是之后接受照射,抑制细胞的抑制活性对900拉德辐射均具有抗性。通过使用脂多糖(LPS)作为对HGG反应的辅助活性的替代来源,来检测抑制细胞的细胞靶标。在用耐受和正常脾细胞重建的小鼠初次抗原攻击时注射LPS,可防止对骨髓来源(B)细胞的抑制作用的表达。然而,当仅在二次抗原攻击时给予LPS,它无法克服对重建受体免疫反应的抑制。因此,LPS可以产生一种状态,其中B细胞对抑制具有抗性,但一旦重建受体中的细胞被抑制,LPS就无法挽救B细胞的反应性。此外,当用二硝基苯酚(DNP)-6- HGG攻击耐受和正常脾细胞的受体时,对半抗原DNP和载体(HGG)的免疫反应均受到抑制。这表明T辅助细胞也是抑制的靶标。本文所呈现的结果将结合一种可能的抑制机制进行讨论,该机制提出抑制活性代表与耐受脾细胞密切相关的HCG在免疫活性细胞中诱导耐受。

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