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利用小鼠cdc2突变细胞系tsFT210通过生物测定法从微生物代谢产物中筛选细胞周期抑制剂。

Screening of cell cycle inhibitors from microbial metabolites by a bioassay using a mouse cdc2 mutant cell line, tsFT210.

作者信息

Osada H, Cui C B, Onose R, Hanaoka F

机构信息

Institute of Physical and Chemical Research (RIKEN), Saitama, Japan.

出版信息

Bioorg Med Chem. 1997 Jan;5(1):193-203. doi: 10.1016/s0968-0896(96)00207-6.

Abstract

We have established a bioassay system using a mouse cdc2 mutant cell line, tsFT210, to detect inhibitors of the mammalian cell cycle. When cultured at the high temperature, restrictive temperature at 39.4 degrees C, tsFT210 cells can be arrested at G2 phase and are large in size. Four hours after release from G2 arrest, the cells entered into the G1 phase. At this time, G1 phase cells were easily discriminated from the G2/M-cells by their size under microscopic observation. The cell-morphology-based bioassay utilizing tsFT210 cells is very simple and sensitive for detecting cdc2 kinase inhibitors and also G2/M-phase inhibitors of the mammalian cell cycle. To demonstrate the merits of this bioassay, the effects of protein kinase inhibitors isolated from actinomycetes were investigated. RK-286C and RK-1409, which are structurally related to staurosporine, inhibited cell cycle progression at the G2 phase in both G2-synchronized and nonsynchronized cultures of tsFT210 cells. Another kinase inhibitor, sangivamycin, inhibited cell cycle progression at the G2 phase of cells released from temperature arrest but did not inhibit that of the exponentially growing cells. Using the bioassay system, we carried out screening of the cell cycle inhibitors from the microbial metabolites and have discovered several new inhibitors, including novel compounds such as tryprostatins A, B and acetophthalidin. Thus, this bioassay allowed for the detection of cell cycle inhibitors and provided a convenient and useful method for the screening of new inhibitors from the microbial metabolites.

摘要

我们建立了一种生物测定系统,使用小鼠cdc2突变细胞系tsFT210来检测哺乳动物细胞周期的抑制剂。当在高温(39.4摄氏度的限制温度)下培养时,tsFT210细胞可停滞在G2期且体积较大。从G2期阻滞中释放4小时后,细胞进入G1期。此时,在显微镜观察下,通过细胞大小很容易将G1期细胞与G2/M期细胞区分开来。利用tsFT210细胞基于细胞形态的生物测定对于检测cdc2激酶抑制剂以及哺乳动物细胞周期的G2/M期抑制剂非常简单且灵敏。为了证明这种生物测定的优点,研究了从放线菌中分离出的蛋白激酶抑制剂的作用。与星形孢菌素结构相关的RK - 286C和RK - 1409在tsFT210细胞的G2期同步化和非同步化培养中均抑制细胞周期进程。另一种激酶抑制剂桑吉瓦霉素抑制从温度阻滞中释放的细胞在G2期的细胞周期进程,但不抑制指数生长细胞的进程。利用该生物测定系统,我们对微生物代谢产物中的细胞周期抑制剂进行了筛选,并发现了几种新的抑制剂,包括诸如曲普他汀A、B和乙酰苯酞等新型化合物。因此,这种生物测定能够检测细胞周期抑制剂,并为从微生物代谢产物中筛选新抑制剂提供了一种方便且有用的方法。

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