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首页> 外文期刊>Molecular and Cellular Biology >4-1BB and Ox40 Are Members of a Tumor Necrosis Factor (TNF)-Nerve Growth Factor Receptor Subfamily That Bind TNF Receptor-Associated Factors and Activate Nuclear Factor κB
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4-1BB and Ox40 Are Members of a Tumor Necrosis Factor (TNF)-Nerve Growth Factor Receptor Subfamily That Bind TNF Receptor-Associated Factors and Activate Nuclear Factor κB

机译:4-1BB和Ox40是与TNF受体相关因子结合并激活核因子κB的肿瘤坏死因子(TNF)-神经生长因子受体亚家族的成员

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Members of the tumor necrosis factor (TNF)-nerve growth factor (NGF) receptor family have been shown to be important costimulatory molecules for cellular activation. 4-1BB and Ox40 are two recently described members of this protein family which are expressed primarily on activated T cells. To gain insight into the signaling pathways employed by these factors, yeast two-hybrid library screens were performed with the cytoplasmic domains of 4-1BB and Ox40 as baits. TNF receptor-associated factor 2 (TRAF2) was identified as an interacting protein in both screens. The ability of both 4-1BB and Ox40 to interact with TRAF2 was confirmed in mammalian cells by coimmunoprecipitation studies. When the binding of the receptors to other TRAF proteins was investigated, 4-1BB and Ox40 displayed distinct binding patterns. While 4-1BB bound TRAF2 and TRAF1, Ox40 interacted with TRAF3 and TRAF2. Using deletion and alanine scanning analysis, we defined the elements in the cytoplasmic domains of both receptors that mediate these interactions. The 4-1BB receptor was found to have two independent stretches of acidic residues that can mediate association of the TRAF molecules. In contrast, a single TRAF binding domain was identified in the cytoplasmic tail of Ox40. The cytoplasmic domains of both receptors were shown to activate nuclear factor κB in a TRAF-dependent manner. Taken together, our results indicate that 4-1BB and Ox40 bind TRAF proteins to initiate a signaling cascade leading to activation of nuclear factor κB.
机译:肿瘤坏死因子(TNF)-神经生长因子(NGF)受体家族的成员已被证明是重要的细胞激活共刺激分子。 4-1BB和Ox40是该蛋白家族的两个最近描述的成员,它们主要在活化的T细胞上表达。为了深入了解这些因子采用的信号传导途径,以4-1BB和Ox40的胞质结构域为诱饵,进行了酵母双杂交文库筛选。在两个筛选中,TNF受体相关因子2(TRAF2)被确定为相互作用蛋白。通过共免疫沉淀研究在哺乳动物细胞中证实了4-1BB和Ox40与TRAF2相互作用的能力。当研究受体与其他TRAF蛋白的结合时,4-1BB和Ox40表现出独特的结合模式。当4-1BB结合TRAF2和TRAF1时,Ox40与TRAF3和TRAF2相互作用。使用删除和丙氨酸扫描分析,我们定义了介导这些相互作用的两个受体的胞质域中的元素。发现4-1BB受体具有两个独立的酸性残基链段,可以介导TRAF分子的缔合。相反,在Ox40的细胞质尾部鉴定出单个TRAF结合域。两种受体的胞质结构域均以TRAF依赖性方式激活核因子κB。两者合计,我们的结果表明4-1BB和Ox40结合TRAF蛋白以启动信号传导级联反应,导致核因子κB活化。

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