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果蝇 BRUCE 通过非赖氨酸泛素化 IAP 拮抗剂 REAPER 抑制细胞凋亡。

Drosophila BRUCE inhibits apoptosis through non-lysine ubiquitination of the IAP-antagonist REAPER.

机构信息

Department of Cell Biology, New York University School of Medicine, 550 First Avenue, New York, NY 10016, USA.

出版信息

Cell Death Differ. 2012 Mar;19(3):470-7. doi: 10.1038/cdd.2011.116. Epub 2011 Sep 2.

DOI:10.1038/cdd.2011.116
PMID:21886178
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3235231/
Abstract

Active caspases execute apoptosis to eliminate superfluous or harmful cells in animals. In Drosophila, living cells prevent uncontrolled caspase activation through an inhibitor of apoptosis protein (IAP) family member, dIAP1, and apoptosis is preceded by the expression of IAP-antagonists, such as Reaper, Hid and Grim. Strong genetic modifiers of this pathway include another IAP family gene encoding an E2 ubiquitin conjugating enzyme domain, dBruce. Although the genetic effects of dBruce mutants are well documented, molecular targets of its encoded protein have remained elusive. Here, we report that dBruce targets Reaper for ubiquitination through an unconventional mechanism. Specifically, we show that dBruce physically interacts with Reaper, dependent upon Reaper's IAP-binding (IBM) and GH3 motifs. Consistently, Reaper levels were elevated in a dBruce -/- background. Unexpectedly, we found that dBruce also affects the levels of a mutant form of Reaper without any internal lysine residues, which normally serve as conventional ubiquitin acceptor sites. Furthermore, we were able to biochemically detect ubiquitin conjugation on lysine-deficient Reaper proteins, and knockdown of dBruce significantly reduced the extent of this ubiquitination. Our results indicate that dBruce inhibits apoptosis by promoting IAP-antagonist ubiquitination on unconventional acceptor sites.

摘要

活性胱天蛋白酶通过凋亡执行来消除动物体内多余或有害的细胞。在果蝇中,活细胞通过凋亡抑制蛋白(IAP)家族成员 dIAP1 来防止不受控制的胱天蛋白酶激活,凋亡之前会表达 IAP 拮抗剂,如 Reaper、Hid 和 Grim。该途径的强遗传修饰因子包括另一个编码 E2 泛素连接酶结构域的 IAP 家族基因 dBruce。尽管 dBruce 突变体的遗传效应已有详细记录,但它编码的蛋白的分子靶标仍然难以捉摸。在这里,我们报告 dBruce 通过一种非传统的机制将 Reaper 靶向泛素化。具体来说,我们表明 dBruce 依赖于 Reaper 的 IAP 结合(IBM)和 GH3 基序与 Reaper 物理相互作用。一致地,Reaper 的水平在 dBruce-/-背景中升高。出乎意料的是,我们发现 dBruce 还会影响没有任何内部赖氨酸残基的 Reaper 突变体的水平,这些赖氨酸残基通常作为常规泛素受体位点。此外,我们能够在生化上检测到缺乏赖氨酸的 Reaper 蛋白上的泛素缀合,并且 dBruce 的敲低显著降低了这种泛素化的程度。我们的结果表明,dBruce 通过促进非常规受体位点上的 IAP 拮抗剂泛素化来抑制凋亡。

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本文引用的文献

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Systematic in vivo RNAi analysis identifies IAPs as NEDD8-E3 ligases.系统的体内 RNAi 分析鉴定 IAPs 为 NEDD8-E3 连接酶。
Mol Cell. 2010 Dec 10;40(5):810-22. doi: 10.1016/j.molcel.2010.11.011.
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Drosophila IAP antagonists form multimeric complexes to promote cell death.果蝇 IAP 拮抗剂形成多聚体复合物以促进细胞死亡。
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Antagonists of IAP proteins as cancer therapeutics.IAP 蛋白拮抗剂作为癌症治疗药物。
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