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首页> 外文期刊>Cell structure and function >Complementation by a Cloned Human Ubiquitin-Activating Enzyme E1 of the S-Phase-Arrested Mouse FM3A Cell Mutant with Thermolabile E1
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Complementation by a Cloned Human Ubiquitin-Activating Enzyme E1 of the S-Phase-Arrested Mouse FM3A Cell Mutant with Thermolabile E1

机译:S阶段逮捕的小鼠FM3A细胞突变体与不耐热E1的克隆的人类泛素激活酶E1的补充。

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摘要

References(49) Cited-By(7) A temperature-sensitive growth mutant tsFS20 isolated from mouse FM3A cells was identified as a mutant with thermolabile ubiquitin-activating enzyme E1 by transfection with a full-length cDNA encoding the human E1 enzyme and cell-cell hybridization with an authentic E1 mutant ts85 previously isolated from FM3A cells. The resulting transformants produced thermoresistant E1 activity. Upon shift-up of temperature, asynchronously growing tsFS20 cells showed multiple points of cell-cycle arrest. At the nonpermissive temperature, tsFS20 cells that had been synchronized at the G1-S-phase progressed and accumulated in the mid-S-phase, as evidenced by the absence of G2-specific cdc2 kinase activity, while ts85 mutant cells, the widely used E1 mutant, reached the G2-phase and were arrested. Thus, the E1 mutation seemed to be involved in progression in the S-phase as well as in the G2-phase in the cell cycle. Degradation of short-lived abnormal proteins in tsFS20 cells was decreased to about 50% at the nonpermissive temperature, while the block was fully restored to the wildtype level in the transformant cells. Relevance of the unusually high incidence of the temperature-sensitive E1 mutation was discussed in terms of the E1 as a determinant of heat tolerance of cells.
机译:参考文献(49)被引(7)从小鼠FM3A细胞中分离出的对温度敏感的生长突变体tsFS20通过转染全长编码人E1酶的全长cDNA被鉴定为具有不耐热泛素激活酶E1的突变体,并且与先前从FM3A细胞中分离出的真实E1突变ts85进行细胞杂交。所得的转化体产生耐热的E1活性。温度升高后,异步生长的tsFS20细胞显示出多个细胞周期停滞点。在非容许温度下,已在G1-S期同步化的tsFS20细胞在S期中进行并积累,这由缺乏G2特异性cdc2激酶活性所证明,而ts85突变细胞则被广泛使用。 E1突变体,到达G2期并被捕。因此,E1突变似乎与细胞周期的S期以及G2期有关。在不允许的温度下,tsFS20细胞中短寿命异常蛋白的降解降低至约50%,而该块在转化细胞中已完全恢复至野生型水平。关于E1突变异常高发的相关性,以E1作为细胞耐热性的决定因素进行了讨论。

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