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转化生长因子β1对周期中上皮细胞p34cdc2合成的细胞周期依赖性抑制作用。

Cell cycle-dependent inhibition of p34cdc2 synthesis by transforming growth factor beta 1 in cycling epithelial cells.

作者信息

Eblen S T, Fautsch M P, Burnette R J, Joshi P, Leof E B

机构信息

Department of Cell Biology, Vanderbilt University, Nashville, Tennessee 37232.

出版信息

Cell Growth Differ. 1994 Feb;5(2):109-16.

PMID:8180123
Abstract

Cycling epithelial cells were shown to reversibly arrest in late G1 phase following treatment with transforming growth factor beta 1. Associated with this G1-S phase arrest was a decrease in the synthesis and histone H1 kinase activity of p34cdc2. Transforming growth factor beta 1 did not reduce p34cdc2 levels by modulating the turnover of newly synthesized p34cdc2. The decrease in p34cdc2 synthesis preceded any detectable effect on DNA synthesis. Moreover, the action of transforming growth factor beta 1 was regulated in a cell cycle-specific manner; epithelial cells were sensitive to transforming growth factor beta 1 only during the G1 phase. The results suggest that p34cdc2 might be a useful biochemical marker for investigating the mechanism(s) of transforming growth factor beta 1 signaling.

摘要

研究表明,在用转化生长因子β1处理后,循环上皮细胞会在G1期晚期发生可逆性停滞。与这种G1-S期停滞相关的是p34cdc2的合成及组蛋白H1激酶活性降低。转化生长因子β1并未通过调节新合成的p34cdc2的周转来降低p34cdc2水平。p34cdc2合成的减少先于对DNA合成的任何可检测到的影响。此外,转化生长因子β1的作用是以细胞周期特异性方式调节的;上皮细胞仅在G1期对转化生长因子β1敏感。这些结果表明,p34cdc2可能是研究转化生长因子β1信号传导机制的有用生化标志物。

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