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抗原致敏后诱导产生的抗独特型抑制性T细胞(Tsid)的特性分析。

Characterization of anti-idiotypic suppressor T cells (Tsid) induced after antigen priming.

作者信息

Sherr D H, Dorf M E

出版信息

J Immunol. 1984 Sep;133(3):1142-50.

PMID:6205068
Abstract

The induction and fine specificity of idiotype-specific suppressor T cells (Tsid) were studied. Spleen cells from C57BL/6 mice, immunized 4 wk previously with NP-KLH, failed to express NPb3 idiotype-bearing PFC when challenged in vitro with NP-Ficoll or NP-Brucella abortus. After treatment of NP-primed responder cultures with anti-Thy-1.2 anti-serum + C, NPb idiotype-bearing B cells could be detected. This B cell subset was preferentially suppressed by the addition of T cells from NP-primed mice. With this reconstitution protocol, it was determined that suppression of the NPb idiotype-bearing portion of the B cell response was mediated by a specifically induced T cell population (Tsid) that directly suppressed NPb-bearing B cells. As with a previously described suppressor population induced with hapten-modified syngeneic spleen cells (Ts2), the Tsid population bound and was lysed by NPb idiotype-bearing serum antibodies. However, the Tsid could be distinguished from the Ts2 population because it lacked I-J determinants and functioned as an effector T cell, not an intermediary suppressor cell. Furthermore, fine specificity studies with monoclonal NP-specific antibodies expressing various levels of serologically detectable NPb idiotypic determinants indicated that unlike the Ts2, the Tsid population reacts with conventional, serologically detected members of the NPb family. The combined idiotype binding studies for the Tsid and Ts2 populations demonstrate that the fine specificity of suppressor T cell populations reflects their independent mechanisms of regulation.

摘要

对独特型特异性抑制性T细胞(Tsid)的诱导及其精细特异性进行了研究。4周前用NP-KLH免疫的C57BL/6小鼠的脾细胞,在体外用NP-菲可或流产布鲁氏菌攻击时,未能表达带有NPb3独特型的PFC。在用抗Thy-1.2抗血清+C处理NP致敏的反应细胞培养物后,可检测到带有NPb独特型的B细胞。通过添加来自NP致敏小鼠的T细胞,可优先抑制该B细胞亚群。采用这种重建方案,确定B细胞反应中带有NPb独特型部分的抑制是由特异性诱导的T细胞群体(Tsid)介导的,该群体直接抑制带有NPb的B细胞。与先前描述的用半抗原修饰的同基因脾细胞诱导的抑制性群体(Ts2)一样,Tsid群体与带有NPb独特型的血清抗体结合并被裂解。然而,Tsid可与Ts2群体区分开来,因为它缺乏I-J决定簇,并且作为效应T细胞发挥作用,而不是中间抑制细胞。此外,用表达不同水平血清学可检测的NPb独特型决定簇的单克隆NP特异性抗体进行的精细特异性研究表明,与Ts2不同,Tsid群体与NPb家族的常规血清学检测成员发生反应。对Tsid和Ts2群体的联合独特型结合研究表明,抑制性T细胞群体的精细特异性反映了它们独立的调节机制。

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