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PACSIN 2 represses cellular migration through direct association with cyclin D1 but not its alternate splice form cyclin D1b
Authors:Hui Meng  Lifeng Tian  Jie Zhou  Zhiping Li  Xuanmao Jiao  Wayne W Li  Markus Plomann  Zhishun Xu  Michael P Lisanti  Chenguang Wang  Richard G Pestell
Affiliation:1.Department of Cancer Biology; Thomas Jefferson University; Philadelphia, PA USA;2.Department of Stem Cell Biology & Regenerative Medicine; Thomas Jefferson University; Philadelphia, PA USA;3.Kimmel Cancer Center; Thomas Jefferson University; Philadelphia, PA USA;4.Department of Urology; QiLu Hospital of Shandong University; Ji''nan China;5.Institute for Biochemistry and Center for Molecular Medicine Cologne (CMMC); University of Cologne; Cologne, Germany
Abstract:Cyclin D1 overexpression is a common feature of many human malignancies. Genomic deletion analysis has demonstrated a key role for cyclin D1 in cellular proliferation, angiogenesis and cellular migration. To investigate the mechanisms contributing to cyclin D1 functions, we purified cyclin D1a-associated complexes by affinity chromatography and identified the PACSIN 2 (protein kinase C and casein kinase substrate in neurons 2) protein by mass spectrometry. The PACSIN 2, but not the related PACSIN 1 and 3, directly bound wild-type cyclin D1 (cyclin D1a) at the carboxyl terminus and failed to bind cyclin D1b, the alternative splicing variant of cyclin D1. PACSIN 2 knockdown induced cellular migration and reduced cell spreading in LNCaP cells expressing cyclin D1a. In cyclin D1−/− mouse embryonic fibroblasts (MEFs), cyclin D1a, but not cyclin D1b, reduced the cell spreading to a polarized morphology. siPACSIN 2 had no effect on cellular migration of cyclin D1−/− MEFs. Cyclin D1a restored the migratory ability of cyclin D1−/− MEFs, which was further enhanced by knocking down PACSIN 2 with siRNA. The cyclin D1-associated protein, PACSIN 2, regulates cell spreading and migration, which are dependent on cyclin D1 expression.Key words: PACSIN 2, cyclin D1, polymorphism, cellular migration, cell spreading, cancer
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