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抗原/抗体比例对巨噬细胞摄取、处理以及将与多克隆抗体复合的抗原呈递给T细胞的影响。

Effect of antigen/antibody ratio on macrophage uptake, processing, and presentation to T cells of antigen complexed with polyclonal antibodies.

作者信息

Manca F, Fenoglio D, Li Pira G, Kunkl A, Celada F

机构信息

Department of Immunology, University of Genoa, San Martino Hospital, Italy.

出版信息

J Exp Med. 1991 Jan 1;173(1):37-48. doi: 10.1084/jem.173.1.37.

Abstract

Activation of a galactosidase-specific murine T hybridoma clone and of a human tetanus toxoid-specific T clone by antigen-presenting cells (APC) was used to evaluate the regulatory function of antibodies complexed with the relevant antigen. Complexed antigen, in fact, is taken up with high efficiency thanks to Fc receptors borne by APC. Antibody/antigen ratio in the complexes proved to be a critical parameter in enhancing antigen presentation. Complexes in moderate antibody excess provided optimal T cell activation independently of the physical state of the complexes (precipitated by a second antibody or solubilized by complement). Complexes in extreme antibody excess, on the contrary, did not yield T cell activation although taken up by APC efficiently. The effect of antibodies at extreme excess was observed with substimulatory dose of antigen (loss of potentiation) and with optimal dose of antigen (loss of stimulation). An excess of specific polyclonal antibodies hampers proteolytic degradation of antigen in vitro, supporting the view that a similar mechanism may operate within the APC that have internalized immune complexes in extreme antibody excess. The possibility that immune complex forming in extreme antibody excess may turn off the T cell response is proposed as a regulatory mechanism.

摘要

利用抗原呈递细胞(APC)激活半乳糖苷酶特异性小鼠T杂交瘤克隆和破伤风类毒素特异性人T克隆,以评估与相关抗原复合的抗体的调节功能。事实上,由于APC携带的Fc受体,复合抗原能被高效摄取。复合物中的抗体/抗原比率被证明是增强抗原呈递的关键参数。适度抗体过量的复合物能提供最佳的T细胞激活,而与复合物的物理状态无关(由第二抗体沉淀或由补体溶解)。相反,尽管抗体极度过量的复合物能被APC有效摄取,但却不能产生T细胞激活。在亚刺激剂量的抗原(增强作用丧失)和最佳剂量的抗原(刺激作用丧失)情况下,均观察到了抗体极度过量的影响。过量的特异性多克隆抗体在体外会阻碍抗原的蛋白水解降解,这支持了一种观点,即在抗体极度过量的情况下内化了免疫复合物的APC内可能存在类似机制。有人提出,抗体极度过量时形成的免疫复合物可能会关闭T细胞反应,这是一种调节机制。

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