癌蛋白 BCL-3 的抑制功能需要 CtBP,而其多泛素化和降解则涉及 E3 连接酶 TBLR1。
The repressing function of the oncoprotein BCL-3 requires CtBP, while its polyubiquitination and degradation involve the E3 ligase TBLR1.
机构信息
Interdisciplinary Cluster for Applied Genoproteomics (GIGA-Research), University of Liege, CHU, Sart-Tilman, Liege, Belgium.
出版信息
Mol Cell Biol. 2010 Aug;30(16):4006-21. doi: 10.1128/MCB.01600-09. Epub 2010 Jun 14.
Abstract
The nuclear and oncogenic BCL-3 protein activates or represses gene transcription when bound to NF-kappaB proteins p50 and p52, yet the molecules that specifically interact with BCL-3 and drive BCL-3-mediated effects on gene expression remain largely uncharacterized. Moreover, GSK3-mediated phosphorylation of BCL-3 triggers its degradation through the proteasome, but the proteins involved in this degradative pathway are poorly characterized. Biochemical purification of interacting partners of BCL-3 led to the identification of CtBP as a molecule required for the ability of BCL-3 to repress gene transcription. CtBP is also required for the oncogenic potential of BCL-3 and for its ability to inhibit UV-mediated cell apoptosis in keratinocytes. We also defined the E3 ligase TBLR1 as a protein involved in BCL-3 degradation through a GSK3-independent pathway. Thus, our data demonstrate that the LSD1/CtBP complex is required for the repressing abilities of an oncogenic I kappaB protein, and they establish a functional link between the E3 ligase TBLR1 and NF-kappaB.
摘要
核转录因子和致癌蛋白 BCL-3 与 NF-κB 家族的 p50 和 p52 蛋白结合后,能激活或抑制基因转录,然而,能与 BCL-3 特异性相互作用并驱动 BCL-3 对基因表达产生影响的分子在很大程度上仍未被阐明。此外,GSK3 介导的 BCL-3 磷酸化触发其通过蛋白酶体降解,但参与该降解途径的蛋白质的特征描述较差。BCL-3 相互作用伙伴的生化纯化导致鉴定出 CtBP 是 BCL-3 抑制基因转录能力所必需的分子。CtBP 也需要 BCL-3 的致癌潜力及其在角质细胞中抑制 UV 介导的细胞凋亡的能力。我们还定义了 E3 连接酶 TBLR1 作为通过非 GSK3 依赖途径参与 BCL-3 降解的蛋白质。因此,我们的数据表明,LSD1/CtBP 复合物是致癌 IκB 蛋白抑制能力所必需的,并且它们在 E3 连接酶 TBLR1 和 NF-κB 之间建立了功能联系。
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