INSERM UMR1037, Cancer Research Center of Toulouse, Toulouse, France.
J Clin Invest. 2012 Mar;122(3):844-58. doi: 10.1172/JCI60376. Epub 2012 Feb 1.
p27(Kip1) (p27) acts as a tumor suppressor by inhibiting cyclin-cyclin-dependent kinase (cyclin-CDK) activity. However, mice expressing a form of p27 that is unable to bind or inhibit cyclin-CDK complexes (p27(CK-)) have increased incidence of tumor development as compared with wild-type and p27(-/-) mice, revealing an oncogenic role for p27. Here, we identified a phenotype of multinucleation and polyploidy in p27(CK-) mice not present in p27(-/-) animals, suggesting a role for p27 in G2/M that is independent of cyclin-CDK regulation. Further analysis revealed that p27(CK-) expression caused a cytokinesis and abscission defect in mouse embryonic fibroblasts. We identified the Rho effector citron kinase (citron-K) as a p27-interacting protein in vitro and in vivo and found that p27 and citron-K colocalized at the contractile ring and mid-body during telophase and cytokinesis. Moreover, overexpression of the minimal p27-binding domain of citron-K was sufficient to rescue the phenotype caused by p27(CK-). Conversely, expression of a mutant p27(CK-) unable to bind citron-K did not induce multinucleation. Finally, by binding to citron-K, p27 prevented the interaction of citron-K with its activator RhoA. Taken together, these data suggest a role for p27 during cytokinesis via the regulation of citron-K activity.
p27(Kip1)(p27)通过抑制细胞周期蛋白-细胞周期依赖性激酶(cyclin-CDK)活性发挥肿瘤抑制因子的作用。然而,与野生型和 p27(-/-)小鼠相比,表达一种无法结合或抑制细胞周期蛋白-CDK 复合物的 p27 形式(p27(CK-))的小鼠肿瘤发生率增加,这揭示了 p27 的致癌作用。在这里,我们在 p27(CK-)小鼠中发现了多核和多倍体的表型,而在 p27(-/-)动物中则没有,这表明 p27 在 G2/M 期具有独立于细胞周期蛋白-CDK 调节的作用。进一步的分析表明,p27(CK-)的表达导致了小鼠胚胎成纤维细胞的胞质分裂和分离缺陷。我们在体外和体内鉴定出 Rho 效应物 citron 激酶(citron-K)是 p27 的相互作用蛋白,并发现 p27 和 citron-K 在有丝分裂末期和胞质分裂期间在收缩环和中间体共定位。此外,citron-K 的最小 p27 结合域的过表达足以挽救 p27(CK-)引起的表型。相反,表达一种不能与 citron-K 结合的突变型 p27(CK-)不会诱导多核化。最后,通过与 citron-K 结合,p27 阻止了 citron-K 与其激活剂 RhoA 的相互作用。总之,这些数据表明 p27 通过调节 citron-K 活性在胞质分裂过程中发挥作用。
