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TRAF2的泛素化和易位是JNK激活所必需的,但不是p38或NF-κB激活所必需的。

Ubiquitination and translocation of TRAF2 is required for activation of JNK but not of p38 or NF-kappaB.

作者信息

Habelhah Hasem, Takahashi Shoichi, Cho Ssang-Goo, Kadoya Takayuki, Watanabe Toshiki, Ronai Ze'ev

机构信息

Ruttenberg Cancer Center, Mount Sinai School of Medicine, New York, NY, USA.

出版信息

EMBO J. 2004 Jan 28;23(2):322-32. doi: 10.1038/sj.emboj.7600044. Epub 2004 Jan 8.

DOI:10.1038/sj.emboj.7600044
PMID:14713952
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1271753/
Abstract

TRAF2 is a RING finger protein that regulates the cellular response to stress and cytokines by controlling JNK, p38 and NF-kappaB signaling cascades. Here, we demonstrate that TRAF2 ubiquitination is required for TNFalpha-induced activation of JNK but not of p38 or NF-kappaB. Intact RING and zinc finger domains are required for TNFalpha-induced TRAF2 ubiquitination, which is also dependent on Ubc13. TRAF2 ubiquitination coincides with its translocation to the insoluble cellular fraction, resulting in selective activation of JNK. Inhibition of Ubc13 expression by RNAi resulted in inhibition of TNFalpha-induced TRAF2 translocation and impaired activation of JNK but not of IKK or p38. TRAF2 aggregates in the cytoplasm, as seen in Hodgkin-Reed-Sternberg lymphoma cells, resulting in constitutive NF-kappaB activity but failure to activate JNK. These findings demonstrate that the TRAF2 RING is required for Ubc13-dependent ubiquitination, resulting in translocation of TRAF2 to an insoluble fraction and activation of JNK, but not of p38 or NF-kappaB. Altogether, our findings highlight a novel mechanism of TRAF2-dependent activation of diverse signaling cascades that is impaired in Hodgkin-Reed-Sternberg cells.

摘要

TRAF2是一种具有RING结构域的蛋白质,它通过控制JNK、p38和NF-κB信号级联反应来调节细胞对应激和细胞因子的反应。在此,我们证明TRAF2的泛素化是TNFα诱导JNK激活所必需的,但不是p38或NF-κB激活所必需的。完整的RING和锌指结构域是TNFα诱导TRAF2泛素化所必需的,这也依赖于Ubc13。TRAF2的泛素化与其向不溶性细胞组分的易位同时发生,导致JNK的选择性激活。通过RNAi抑制Ubc13表达导致TNFα诱导的TRAF2易位受到抑制,JNK激活受损,但IKK或p38的激活不受影响。在霍奇金-里德-斯腾伯格淋巴瘤细胞中观察到TRAF2在细胞质中聚集,导致组成型NF-κB活性,但未能激活JNK。这些发现表明,TRAF2的RING结构域是Ubc13依赖性泛素化所必需的,导致TRAF2易位至不溶性组分并激活JNK,但不激活p38或NF-κB。总之,我们的发现突出了一种TRAF2依赖性激活多种信号级联反应的新机制,这种机制在霍奇金-里德-斯腾伯格细胞中受损。

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