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TGF beta-induced growth inhibition in primary fibroblasts requires the retinoblastoma protein

被引:68
作者
Herrera, RE
Makela, TP
Weinberg, RA
机构
[1] WHITEHEAD INST BIOMED RES,CAMBRIDGE,MA 02139
[2] MIT,DEPT BIOL,CAMBRIDGE,MA 02139
来源
MOLECULAR BIOLOGY OF THE CELL | 1996年 / 7卷 / 09期
关键词
CELL-CYCLE ARREST; DEPENDENT KINASE; MAMMALIAN-CELLS; GENE-PRODUCT; TRANSFORMING GROWTH-FACTOR-BETA-1; EXTRACELLULAR-MATRIX; SUSCEPTIBILITY GENE; PROSTATE-CANCER; TUMOR-GROWTH; EXPRESSION;
D O I
10.1091/mbc.7.9.1335
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Transforming growth factor beta (TGF beta) inhibits cell proliferation by inducing a G(1) cell-cycle arrest. Cyclin/CDK complexes have been implicated in this arrest, because TGF beta treatment leads to inhibition of cyclin/CDK activity. We have investigated the role of the retinoblastoma protein (pRb) in TGF beta-induced growth arrest by using RE(+/+) and RB(-/-) primary mouse embryo fibroblasts. In both of these cell types, TGF beta inhibits CDK4-associated kinase activity. However, whereas CDK2-associated kinase activity was completely inhibited by TGF beta in the wild-type cells, it was reduced only slightly in the RB mutant cells. In addition, at high-cell density the growth-inhibitory effects of TGF beta are no longer observed in the RB(-/-) cells; on the contrary, TGF beta treatment promotes the growth of these mutant fibroblasts. Thus, under certain cellular growth conditions, elimination of pRb transforms the growth-inhibitory effects of TGF beta into growth-stimulatory effects. These observations could help to explain why TGF beta is often found to enhance tumorigenicity in vivo and why inactivation of the RB gene leads to tumorigenesis.
引用
收藏
页码:1335 / 1342
页数:8
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