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4-1BB配体在共刺激T淋巴细胞生长中的作用及其被环磷酸腺苷上调表达于M12 B淋巴瘤细胞上的情况。

Role of 4-1BB ligand in costimulation of T lymphocyte growth and its upregulation on M12 B lymphomas by cAMP.

作者信息

DeBenedette M A, Chu N R, Pollok K E, Hurtado J, Wade W F, Kwon B S, Watts T H

机构信息

Department of Immunology, University of Toronto, Ontario, Canada.

出版信息

J Exp Med. 1995 Mar 1;181(3):985-92. doi: 10.1084/jem.181.3.985.

Abstract

K46J B lymphomas express a T cell costimulatory activity that is not inhibited by CTLA-4Ig, anti-B7-1, anti-B7-2, anti-intercellular adhesion molecule 1 or antibodies to heat stable antigen. In this paper we report that this costimulatory activity is mediated at least in part by 4-1BB ligand, a member of the tumor necrosis factor (TNF) gene family that binds to 4-1BB, a T cell activation antigen with homology to the TNF/nerve growth factor receptor family. A fusion protein between 4-1BB and alkaline phosphatase (4-1BB-AP) blocks T cell activation by K46J lymphomas in both an antigen-specific system and with polyclonally (anti-CD3) activated T cells. 4-1BB-AP also blocks antigen presentation by normal spleen cells. When the antigen-presenting cells express B7 molecules as well as 4-1BB ligand, we find that B7 molecules and 4-1BB-AP both contribute to T cell activation. These data suggest that 4-1BB ligand plays an important role in costimulation of IL-2 production and proliferation by T cells. The B lymphoma M12 expresses low levels of 4-1BB-L but can be induced to express higher levels by treatment of the B cells with cAMP, which also induces B7-1 and B7-2 in these cells. Thus cAMP appears to coordinately induce several costimulatory molecules on B cells.

摘要

K46J B淋巴瘤表达一种T细胞共刺激活性,该活性不受CTLA-4Ig、抗B7-1、抗B7-2、抗细胞间黏附分子1或抗热稳定抗原抗体的抑制。在本文中,我们报道这种共刺激活性至少部分由4-1BB配体介导,4-1BB配体是肿瘤坏死因子(TNF)基因家族的成员,它与4-1BB结合,4-1BB是一种与TNF/神经生长因子受体家族具有同源性的T细胞活化抗原。4-1BB与碱性磷酸酶的融合蛋白(4-1BB-AP)在抗原特异性系统和多克隆(抗CD3)活化的T细胞中均能阻断K46J淋巴瘤对T细胞的活化。4-1BB-AP还能阻断正常脾细胞的抗原呈递。当抗原呈递细胞同时表达B7分子和4-1BB配体时,我们发现B7分子和4-1BB-AP都有助于T细胞活化。这些数据表明4-1BB配体在T细胞IL-2产生和增殖的共刺激中起重要作用。B淋巴瘤M12表达低水平的4-1BB-L,但用cAMP处理B细胞可诱导其表达更高水平,cAMP也能诱导这些细胞中的B7-1和B7-2表达。因此,cAMP似乎能协同诱导B细胞上的几种共刺激分子。

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