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Role of the major histocompatibility complex in T cell activation of B cell subpopulations. Major histocompatibility complex-restricted and -unrestricted B cell responses are mediated by distinct B cell subpopulations

机译:主要组织相容性复合物在B细胞亚群的T细胞活化中的作用。主要的组织相容性复合物限制性和非限制性B细胞反应是由不同的B细胞亚群介导的

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摘要

The present study has evaluated the identity of the B cell subpopulations participating in T dependent antibody responses that differ in their requirements for major histocompatibility complex-restricted T cell recognition. In vitro responses of keyhole limpet hemocyanin (KLH)-primed T cells and trinitrophenyl (TNP)-primed B cells were studied to both low and high concentrations of the antigen TNP-KLH. It was first demonstrated that for responses to low concentrations of TNP-KLH, (A × B)F(1) {arrow} parent(A) chimeric helper T cells were restricted in their ability to recognize parent(A) but not parent(B) H-2 determinants expressed by both B cells and antigen-presenting cells (APC). In contrast, at higher antigen concentrations, helper T cells were not restricted in their interaction with B cells. It was then determined whether these observed differences in T cell recognition resulted from the activation of distinct B cell subpopulations with different activation requirements. At low concentrations of TNP-KLH it was demonstrated that Lyb-5(-) B cells were activated, and that it was thus the activation of the Lyb-5(-) subpopulation that required T cell recognition of B cell H-2 under these conditions. In contrast, responses to high concentration of antigen required the participation of Lyb-5(+) B cells, and these Lyb-5(+) B cells were activated by a pathway that required H-2- restricted T cell interaction with APC, but not with B cells. The findings presented here have demonstrated that Lyb-5(-) and Lyb-5(+) B cells constitute B cell subpopulations that differ significantly in their activation requirements for T cell-dependent antibody responses to TNP-KLH. In so doing, these findings have established that the function of genetic restrictions in immune response regulation is critically dependent upon the activation pathways employed by functionally distinct subpopulations of B, as well as T, lymphocytes.
机译:本研究评估了参与T依赖性抗体反应的B细胞亚群的身份,这些反应在主要组织相容性复合物限制T细胞识别的要求方面有所不同。研究了匙孔血蓝蛋白(KLH)引发的T细胞和三硝基苯基(TNP)引发的B细胞对低浓度和高浓度抗原TNP-KLH的体外反应。首次证明,对于低浓度的TNP-KLH的反应,(A×B)F(1){arrow}亲本(A)嵌合辅助T细胞在识别亲本(A)而非亲本( B)由B细胞和抗原呈递细胞(APC)表达的H-2决定簇。相反,在较高的抗原浓度下,辅助性T细胞与B细胞的相互作用不受限制。然后确定这些观察到的T细胞识别差异是否是由具有不同激活要求的不同B细胞亚群的激活引起的。在低浓度的TNP-KLH下,证明Lyb-5(-)B细胞被激活,因此Lyb-5(-)亚群的激活需要T细胞识别B细胞H-2。这些条件。相反,对高浓度抗原的反应需要Lyb-5(+)B细胞的参与,而这些Lyb-5(+)B细胞则通过一条需要H-2-限制T细胞与APC相互作用的途径激活,但不是B细胞此处提出的发现表明,Lyb-5(-)和Lyb-5(+)B细胞构成B细胞亚群,这些B细胞亚群在其对TNP-KLH的T细胞依赖性抗体应答的激活要求上存在显着差异。通过这样做,这些发现已经确定了遗传限制在免疫应答调节中的功能主要取决于B以及T淋巴细胞在功能上不同的亚群所采用的激活途径。

著录项

  • 作者

    Asano, Y; Singer, A; Hodes, RJ;

  • 作者单位
  • 年度 1981
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
  • 中图分类
  • 入库时间 2022-08-20 20:38:23

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