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具有不同结合特性的抗B7-DC抗体发挥相反的作用。

Antibodies against B7-DC with differential binding properties exert opposite effects.

作者信息

Ritprajak Patcharee, Hashiguchi Masaaki, Akiba Hisaya, Yagita Hideo, Okumura Ko, Azuma Miyuki

机构信息

Department of Molecular Immunology, Graduate School, Tokyo Medical and Dental University, Tokyo, Japan.

出版信息

Hybridoma (Larchmt). 2012 Feb;31(1):40-7. doi: 10.1089/hyb.2011.0087.

Abstract

Programmed cell death 1 (PD-1) is an immunoregulatory receptor on T cells that binds two ligands, B7-H1 and B7-DC. Although accumulating reports suggest a critical role for the B7-H1:PD-1 pathway in peripheral tolerance, the actual involvement of B7-DC has not been well confirmed. Here, we established a new MAb against mouse B7-DC (MIH37) and compared its functional properties with a previously established anti-B7-DC MAb (TY25). Binding analyses using flow cytometry demonstrated that MIH37 showed an approximately four-fold higher binding affinity to B7-DC and stronger inhibitory effects on B7-DC:PD-1 binding. In contrast to the effects of TY25, treatment with MIH37 at both sensitization and challenge inhibited hapten-induced contact hypersensitivity reactions. Furthermore, the addition of MIH37 inhibited OVA-specific T cell responses in vitro. The inhibitory effects of MIH37 were counteracted by co-blockade with PD-1 and absent in PD-1-deficient mice, suggesting PD-1-dependent action of MIH37. Our present results suggest that greater complexities of PD-1-mediated functions are induced via ligand binding for controlling immunity and tolerance.

摘要

程序性细胞死亡蛋白1(PD-1)是T细胞上的一种免疫调节受体,可与两种配体B7-H1和B7-DC结合。尽管越来越多的报道表明B7-H1:PD-1通路在外周免疫耐受中起关键作用,但B7-DC的实际参与情况尚未得到充分证实。在此,我们制备了一种针对小鼠B7-DC的新型单克隆抗体(MIH37),并将其功能特性与先前制备的抗B7-DC单克隆抗体(TY25)进行了比较。使用流式细胞术进行的结合分析表明,MIH37对B7-DC的结合亲和力高出约四倍,对B7-DC:PD-1结合的抑制作用更强。与TY25的作用相反,在致敏和激发阶段用MIH37处理均能抑制半抗原诱导的接触性超敏反应。此外,添加MIH37可在体外抑制卵清蛋白特异性T细胞反应。MIH37的抑制作用可被与PD-1共同阻断所抵消,且在PD-1缺陷小鼠中不存在,这表明MIH37的作用依赖于PD-1。我们目前的结果表明,通过配体结合诱导PD-1介导的功能具有更大的复杂性,以控制免疫和耐受。

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