Department of Biochemistry and Molecular Biology, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.
J Biol Chem. 2010 Mar 12;285(11):8316-29. doi: 10.1074/jbc.M109.062521. Epub 2010 Jan 7.
In addition to regulating receptor activity, non-visual arrestins function as scaffolds for numerous intracellular signaling cascades and as regulators of gene transcription. Here we report that the two non-visual arrestins, arrestin2 and arrestin3, localize to the centrosome, a key organelle involved in microtubule nucleation and bipolar mitotic spindle assembly. Both arrestins co-localized with the centrosomal marker gamma-tubulin during interphase and mitosis and were found in purified centrosome preparations. In vitro binding assays demonstrated that both arrestins directly interact with gamma-tubulin. Knockdown of either arrestin by RNA interference resulted in multinucleation, centrosome amplification, and mitotic defects, although only the loss of arrestin2 triggered aberrant microtubule nucleation. Importantly, overexpression of wild type arrestin rescued the multinucleation phenotype and restored normal centrosome number in arrestin siRNA-transfected cells. Moreover, overexpression of arrestin2 or -3 rescued the multinucleation defect observed in MDA-MB-231 breast cancer cells. Taken together, our data reveal that non-visual arrestins are novel centrosomal components and regulate normal centrosome function.
除了调节受体活性外,非视觉 arrestin 还作为许多细胞内信号级联反应的支架,并作为基因转录的调节剂。在这里,我们报告说,两种非视觉 arrestin,arrestin2 和 arrestin3,定位于中心体,这是一个参与微管起始和双极有丝分裂纺锤体组装的关键细胞器。在间期和有丝分裂过程中,两种 arrestin 都与中心体标记物γ-微管蛋白共定位,并在纯化的中心体制剂中发现。体外结合实验表明,两种 arrestin 都直接与γ-微管蛋白相互作用。通过 RNA 干扰敲低任一种 arrestin 都会导致多核化、中心体扩增和有丝分裂缺陷,尽管只有 arrestin2 的缺失会引发异常的微管起始。重要的是,野生型 arrestin 的过表达挽救了多核化表型,并在 arrestin siRNA 转染的细胞中恢复了正常的中心体数量。此外,arrestin2 或 -3 的过表达挽救了 MDA-MB-231 乳腺癌细胞中观察到的多核化缺陷。总之,我们的数据表明,非视觉 arrestin 是新型的中心体成分,并调节正常的中心体功能。
