The Cross-talk Between p27~(kip1) and Its Interacting Molecules in Breast Cancer Cells

Weiwei HE; Xiaoxiang Guan; Longbang Chen

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The Cross-talk Between p27~(kip1) and Its Interacting Molecules in Breast Cancer Cells

VernacularTitle:乳腺癌细胞中p27~(kip1)分子相互作用蛋白质谱的改变
Author: Weiwei HE ; Xiaoxiang GUAN ; Longbang CHEN
Publication Type:Journal Article
Keywords: breast cancer, p27kip1, down expression and cytoplasm mislocalization, phosphorylation, signal transduction pathway, interacting protein profiling
From: Progress in Biochemistry and Biophysics 2006;0(06):-
CountryChina
Language:Chinese
Abstract: p27kip1 is an important negatively regulator of cell cycle progression and plays a central role in the pathogenesis of a member of tumors including breast cancer. In breast cancer cells, the level of p27kip1 expression usually decreases during tumor development and progression, in addition, cytoplasm mislocalization of p27kip1 has been reported, but less is known about the exact molecular mechanisms. Studies have indicated that phosphorylation is the key regulation way, several signal transduction pathways are involved in the regulation of the expression and distribution of p27kip1. To further understand the mechanism, the disparity of the interacting protein profiling between tumor cells and normal cells must be identified first. Including cyclins, cyclin-depend kinases, CRM1, jab1, SKP2, p27kip1 has various interacting molecules. There are also several interacting molecules especially for breast cancer cells. It seems that different protein profiling cause the different expression and intracellular distribution in different cell cycle phase. So, disparity of the p27kip1 protein profiling may be the main mechanism of its down-expression and mislocalization in breast cancer cells.