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中国仓鼠卵巢细胞中中心粒形成与DNA合成起始的独立性

Independence of centriole formation and initiation of DNA synthesis in Chinese hamster ovary cells.

作者信息

Kuriyama R, Dasgupta S, Borisy G G

出版信息

Cell Motil Cytoskeleton. 1986;6(4):355-62. doi: 10.1002/cm.970060402.

Abstract

The relationship between centriole formation and DNA synthesis was investigated by examining the effect of taxol on the centriole cycle and the initiation of DNA synthesis in synchronized cells. The centriole cycle was monitored by electron microscopy of whole-mount preparations [Kuriyama and Borisy, J. Cell Biol., 1981, 91:814-821]. A short daughter centriole appeared in perpendicular orientation to each parent during late G1 or early S and elongated slowly during S to G2. Addition of 5-20 micrograms/ml taxol to a synchronous population of cells in S phase did not inhibit centriole elongation; rather, elongation was accelerated. In contrast, when taxol was added to M phase or early G1 cells, centriole duplication was completely inhibited. The taxol block was reversible since nucleation and elongation of centrioles resumed as soon as the drug was removed. Cells exposed to taxol progressed through the cell cycle and became blocked in mitosis, as indicated by an increase in the mitotic index, but eventually the mitotic arrest was overcome, resulting in formation of multinucleated cells. A peak in mitotic index was seen in the following generation, indicating that chromosomes duplicated in the presence of taxol. Incorporation of 3H-thymidine followed by autoradiography confirmed that DNA synthesis was initiated in the presence of taxol even though formation of daughter centrioles was inhibited. It seems, therefore, that centriole duplication is not a prerequisite for entry into S phase. Since DNA synthesis has already been demonstrated not to be necessary for centriole duplication, these two events, normally coordinated in time, appear to be independent of each other.

摘要

通过研究紫杉醇对同步化细胞中心粒周期和DNA合成起始的影响,探讨了中心粒形成与DNA合成之间的关系。通过对整装标本进行电子显微镜观察来监测中心粒周期[栗山和博里西,《细胞生物学杂志》,1981年,91:814 - 821]。在G1晚期或S早期,每个母中心粒垂直方向会出现一个短的子中心粒,并在S期至G2期缓慢延长。向处于S期的同步化细胞群体中添加5 - 20微克/毫升的紫杉醇,并不抑制中心粒延长;相反,延长加速。相比之下,当紫杉醇添加到M期或G1早期细胞时,中心粒复制被完全抑制。紫杉醇的阻断是可逆的,因为一旦去除药物,中心粒的成核和延长就会恢复。暴露于紫杉醇的细胞通过细胞周期并在有丝分裂中受阻,有丝分裂指数增加表明了这一点,但最终有丝分裂停滞被克服,导致多核细胞形成。在下一代中观察到有丝分裂指数峰值,表明在紫杉醇存在的情况下染色体进行了复制。3H - 胸腺嘧啶核苷掺入后进行放射自显影证实,即使子中心粒的形成受到抑制,在紫杉醇存在的情况下DNA合成仍会起始。因此,似乎中心粒复制不是进入S期的先决条件。由于已经证明DNA合成对于中心粒复制不是必需的,这两个通常在时间上协调的事件似乎相互独立。

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