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A role for the anaphase-promoting complex inhibitor Emi2/XErp1, a homolog of early mitotic inhibitor 1, in cytostatic factor arrest of Xenopus eggs

机译:促后期复合抑制剂Emi2 / XErp1(早期有丝分裂抑制剂1的同源物)在非洲爪蟾卵细胞抑制细胞因子阻滞中的作用

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摘要

Unfertilized vertebrate eggs are arrested in metaphase of meiosis II with high cyclin B/Cdc2 activity to prevent parthenogenesis. Until fertilization, exit from metaphase is blocked by an activity called cytostatic factor (CSF), which stabilizes cyclin B by inhibiting the anaphase-promoting complex (APC) ubiquitin ligase. The APC inhibitor early mitotic inhibitor 1 (Emi1) was recently found to be required for maintenance of CSF arrest. We show here that exogenous Emi1 is unstable in CSF-arrested Xenopus eggs and is destroyed by the SCFβTrCP ubiquitin ligase, suggesting that endogenous Emi1, an apparent 44-kDa protein, requires a stabilizing factor. However, anti-Emi1 antibodies crossreact with native Emi2/Erp1/FBXO43, a homolog of Emi1 and conserved APC inhibitor. Emi2 is stable in CSF-arrested eggs, is sufficient to prevent CSF release, and is rapidly degraded in a Polo-like kinase 1-dependent manner in response to calcium-mediated egg activation. These results identify Emi2 as a candidate CSF maintenance protein.
机译:未受精的脊椎动物卵被捕获在减数分裂II中期,具有高的细胞周期蛋白B / Cdc2活性,以防止孤雌生殖。在受精之前,被称为细胞生长抑制因子(CSF)的活性阻止了中期的退出,该活性通过抑制促后期复合物(APC)泛素连接酶来稳定细胞周期蛋白B。最近发现维持ASF抑制剂需要APC抑制剂早期有丝分裂抑制剂1(Emi1)。我们在此处显示,外源Emi1在CSF被捕的非洲爪蟾卵中不稳定,并被SCFβTrCP泛素连接酶破坏,表明内源性Emi1,一种明显的44 kDa蛋白,需要稳定因子。但是,抗Emi1抗体会与天然Emi2 / Erp1 / FBXO43(Emi1的同系物和保守的APC抑制剂)发生交叉反应。 Emi2在被CSF捕获的卵中稳定,足以阻止CSF释放,并响应钙介导的卵活化而以Polo样激酶1依赖性方式迅速降解。这些结果确定Emi2为候选CSF维持蛋白。

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