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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >RhoB induces apoptosis via direct interaction with TNFAIP1 in HeLa cells.
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RhoB induces apoptosis via direct interaction with TNFAIP1 in HeLa cells.

机译:RhoB通过与HeLa细胞中的TNFAIP1直接相互作用诱导凋亡。

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RhoB, a tumor suppressor, has emerged as an interesting cancer target, and extensive studies aimed at understanding its role in apoptosis have been performed. In our study, we investigated the involvement of RhoB-interacting molecules in apoptosis. To identify RhoB-interacting proteins, we performed yeast-two hybrid screening assays using RhoB as a bait and isolated TNFAIP1, a TNFalpha-induced protein containing the BTB/POZ domain. The interaction between RhoB and TNFAIP1 was demonstrated in vivo through coimmunoprecipitation studies and in vitro binding assays. RFP-TNFAIP1 was found to be partially colocalized with EGFP-RhoB. The partial colocalization of RhoB and TNFAIP1 in endosomes suggests that RhoB-TNFAIP1 interactions may have a functional role in apoptosis. TNFAIP1 elicited proapoptotic activity, while simultaneous expression of RhoB and TNFAIP1 resulted in a dramatic increase in apoptosis in HeLa cells. Furthermore, knockdown of RhoB using siRNA clearly rescued cells from apoptosis induced by TNFAIP1. This finding suggests that interactions between RhoB and TNFAIP1 are crucial for induction of apoptosis in HeLa cells. The observation of increased SAPK/JNK phosphorylation in apoptotic cells and the finding that a JNK inhibitor suppressed apoptosis indicates that SAPK/JNK signaling may be involved in apoptosis induced by RhoB-TNFAIP1 interactions. In conclusion, we found that RhoB interacts with TNFAIP1 to regulate apoptosis via a SAPK/JNK-mediated signal transduction mechanism.
机译:RhoB是一种肿瘤抑制因子,已成为一种有趣的癌症靶标,并且已经进行了广泛的研究,旨在了解其在凋亡中的作用。在我们的研究中,我们调查了RhoB相互作用分子参与细胞凋亡。为了鉴定与RhoB相互作用的蛋白,我们使用RhoB作为诱饵并分离了TNFAIP1(一种由TNFalpha诱导的包含BTB / POZ域的蛋白),进行了两次酵母杂交筛选测定。 RhoB和TNFAIP1之间的相互作用已通过体内共免疫沉淀研究和体外结合试验得以证明。发现RFP-TNFAIP1与EGFP-RhoB部分共定位。 RhoB和TNFAIP1在内体中的部分共定位表明RhoB-TNFAIP1相互作用可能在细胞凋亡中具有功能性作用。 TNFAIP1引起促凋亡活性,而RhoB和TNFAIP1的同时表达导致HeLa细胞凋亡的急剧增加。此外,使用siRNA敲低RhoB可以使细胞从TNFAIP1诱导的细胞凋亡中解救出来。这一发现表明,RhoB与TNFAIP1之间的相互作用对于诱导HeLa细胞凋亡具有至关重要的作用。观察到凋亡细胞中SAPK / JNK磷酸化增加,并且发现JNK抑制剂抑制凋亡,这表明SAPK / JNK信号可能参与RhoB-TNFAIP1相互作用诱导的凋亡。总之,我们发现RhoB与TNFAIP1相互作用以通过SAPK / JNK介导的信号转导机制调节细胞凋亡。

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