Shen Jiang-Cheng, Unoki Motoko, Ythier Damien, Duperray Alain, Varticovski Lyuba, Kumamoto Kensuke, Pedeux Remy, Harris Curtis C
Laboratory of Human Carcinogenesis, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, Maryland 20892-4258, USA.
Cancer Res. 2007 Mar 15;67(6):2552-8. doi: 10.1158/0008-5472.CAN-06-3870.
Inhibitor of growth 4 (ING4) is a candidate tumor suppressor that plays a major role in gene regulation, cell cycle control, apoptosis, and angiogenesis. ING4 expression is down-regulated in glioblastoma cells and head and neck squamous cell carcinoma. Here, we identified liprin alpha1/PPFIA1, a cytoplasmic protein necessary for focal adhesion formation and axon guidance, as a novel interacting protein with ING4. ING4 and liprin alpha1 colocalized at lamellipodia in the vicinity of vinculin. Overexpressed ING4 suppressed cell spreading and cell migration. In contrast, overexpressed liprin alpha1 enhanced cell spreading and cell migration. Knockdown of endogenous ING4 with RNA interference induced cell motility, whereas knockdown of endogenous liprin alpha1 suppressed cell motility. ING4 also suppressed cell motility that was enhanced by liprin alpha1. However, ING4 did not further suppress cell motility when liprin alpha1 was suppressed with RNA interference, suggesting a functional and mechanistic interdependence between these proteins. In addition to its nuclear functions, cytoplasmic ING4 interacts with liprin alpha1 to regulate cell migration and, with its known antiangiogenic function, may prevent invasion and metastasis.
生长抑制因子4(ING4)是一种候选肿瘤抑制因子,在基因调控、细胞周期控制、细胞凋亡和血管生成中起主要作用。ING4在胶质母细胞瘤细胞以及头颈部鳞状细胞癌中表达下调。在此,我们鉴定出脂磷素α1/PPFIA1,一种粘着斑形成和轴突导向所必需的胞质蛋白,为与ING4相互作用的新型蛋白。ING4和脂磷素α1在纽蛋白附近的片状伪足中共定位。过表达的ING4抑制细胞铺展和细胞迁移。相反,过表达的脂磷素α1增强细胞铺展和细胞迁移。用RNA干扰敲低内源性ING4可诱导细胞运动,而敲低内源性脂磷素α1则抑制细胞运动。ING4还可抑制由脂磷素α1增强的细胞运动。然而,当用RNA干扰抑制脂磷素α1时,ING4并未进一步抑制细胞运动,这表明这些蛋白之间存在功能和机制上的相互依赖性。除了其核功能外,胞质中的ING4与脂磷素α1相互作用以调节细胞迁移,并且凭借其已知的抗血管生成功能,可能会阻止侵袭和转移。
