首页> 美国卫生研究院文献>The EMBO Journal >Cytotoxicity-dependent APO-1 (Fas/CD95)-associated proteins form a death-inducing signaling complex (DISC) with the receptor.
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Cytotoxicity-dependent APO-1 (Fas/CD95)-associated proteins form a death-inducing signaling complex (DISC) with the receptor.

机译:细胞毒性依赖性APO-1(Fas / CD95)相关蛋白与受体形成死亡诱导信号复合物(DISC)。

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摘要

APO-1 (Fas/CD95), a member of the tumor necrosis factor receptor superfamily, induces apoptosis upon receptor oligomerization. In a search to identify intracellular signaling molecules coupling to oligomerized APO-1, several cytotoxicity-dependent APO-1-associated proteins (CAP) were immunoprecipitated from the apoptosis-sensitive human leukemic T cell line HUT78 and the lymphoblastoid B cell line SKW6.4. CAP1-3 (27-29 kDa) and CAP4 (55 kDa), instantly detectable after the crosslinking of APO-1, were associated only with aggregated (the signaling form of APO-1) and not with monomeric APO-1. CAP1 and CAP2 were identified as serine phosphorylated MORT1/FADD. The association of CAP1-4 with APO-1 was not observed with C-terminally truncated non-signaling APO-1. In addition, CAP1 and CAP2 did not associate with an APO-1 cytoplasmic tail carrying the lprcg amino acid replacement. Moreover, no APO-1-CAP association was found in the APO-1+, anti-APO-1-resistant pre-B cell line Boe. Our data suggest that in vivo CAP1-4 are the APO-1 apoptosis-transducing molecules.
机译:APO-1(Fas / CD95)是肿瘤坏死因子受体超家族的成员,在受体寡聚时诱导细胞凋亡。为了鉴定与寡聚化的APO-1偶联的细胞内信号分子,从凋亡敏感的人类白血病T细胞系HUT78和淋巴母细胞B细胞系SKW6.4中免疫沉淀了几种细胞毒性依赖性APO-1相关蛋白(CAP)。 。 CAP1-3(27-29 kDa)和CAP4(55 kDa),在APO-1交联后立即可检测到,仅与聚集体(APO-1的信号传导形式)相关,与单体APO-1不相关。 CAP1和CAP2被鉴定为丝氨酸磷酸化MORT1 / FADD。 C端截短的非信号APO-1未观察到CAP1-4与APO-1的缔合。此外,CAP1和CAP2与携带lprcg氨基酸替代物的APO-1细胞质尾巴不相关。此外,在抗APO-1的APO-1 +前B细胞系Boe中未发现APO-1-CAP缔合。我们的数据表明,体内CAP1-4是APO-1细胞凋亡分子。

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