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雌二醇诱导中国仓鼠细胞的有丝分裂抑制和染色体移位。

Mitotic inhibition and chromosome displacement induced by estradiol in Chinese hamster cells.

作者信息

Wheeler W J, Hsu T C, Tousson A, Brinkley B R

出版信息

Cell Motil Cytoskeleton. 1987;7(3):235-47. doi: 10.1002/cm.970070306.

Abstract

We tested diethylstilbestrol (DES) and 17 beta-estradiol as mitotic arrestants to determine their effects on chromosome distribution, spindle microtubules, and the cytoplasmic microtubule complex (CMTC) in the Chinese hamster strain Don. Cytological experiments assessed micronuclei induction, chromosome displacement, and anaphase recovery. Indirect immunofluorescence microscopy with antibody to tubulin and electron microscopy were used to illustrate effects on microtubules. Both DES and estradiol were potent inhibitors of mitosis when applied to cells in vitro. Estradiol induced micronuclei at a greater frequency than did DES. Estradiol-arrested metaphases often contained misaligned chromosomes despite the presence of a bipolar spindle and an equatorial plate. Equatorial plates were not observed in DES-arrested cells. Cells recovered quickly from estradiol exposure upon removal of the steroid. The frequency of abnormal metaphases and abnormal anaphases declined as the recovery period increased. Microtubule experiments showed that DES inhibited spindle assembly and disassembled the CMTC, whereas estradiol, at similar concentrations, arrested mitosis in a manner that allowed spindle assembly. A definite effect on the CMTC by estradiol could not be determined. However, changes in cell morphology were observed. In the presence of estradiol, centrosomes organized microtubules that joined with kinetochores of chromosomes at the equatorial plate as well as with those of misaligned chromosomes. Misaligned chromosomes appeared predominantly at polar regions of mitotic cells. Following drug removal, the pole-oriented chromosomes reoriented at the equatorial plate. The unique arresting properties of estradiol may prove useful in studies of chromosome migration and segregation during mitosis.

摘要

我们测试了己烯雌酚(DES)和17β-雌二醇作为有丝分裂阻滞剂,以确定它们对中国仓鼠唐恩品系的染色体分布、纺锤体微管和细胞质微管复合体(CMTC)的影响。细胞学实验评估了微核诱导、染色体移位和后期恢复情况。使用抗微管蛋白抗体的间接免疫荧光显微镜和电子显微镜来说明对微管的影响。当将DES和雌二醇应用于体外培养的细胞时,它们都是有丝分裂的有效抑制剂。雌二醇诱导微核的频率高于DES。尽管存在双极纺锤体和赤道板,但雌二醇阻滞的中期细胞常常含有排列不齐的染色体。在DES阻滞的细胞中未观察到赤道板。去除类固醇后,细胞从雌二醇暴露中迅速恢复。随着恢复期延长,异常中期和异常后期的频率下降。微管实验表明,DES抑制纺锤体组装并使CMTC解体,而在相似浓度下,雌二醇以允许纺锤体组装的方式阻滞有丝分裂。无法确定雌二醇对CMTC有明确影响。然而,观察到了细胞形态的变化。在雌二醇存在的情况下,中心体组织微管,这些微管与赤道板上染色体的动粒以及排列不齐的染色体的动粒相连。排列不齐的染色体主要出现在有丝分裂细胞的两极区域。去除药物后,两极定向的染色体在赤道板重新定向。雌二醇独特的阻滞特性可能在有丝分裂期间染色体迁移和分离的研究中有用。

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