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嘌呤霉素和6-二甲基氨基嘌呤影响下小鼠卵母细胞不同成熟阶段的染色质行为

Chromatin behaviour under influence of puromycin and 6-DMAP at different stages of mouse oocyte maturation.

作者信息

Szöllösi M S, Debey P, Szöllösi D, Rime H, Vautier D

机构信息

I.N.R.A., Unité de Biologie de la Fécondation, Jouy-en-Josas, France.

出版信息

Chromosoma. 1991 Jun;100(5):339-54. doi: 10.1007/BF00360533.

Abstract

Preovulatory mouse oocytes were cultured in vitro up to each subsequent stages of maturation: germinal vesicle (GV), germinal vesicle breakdown (GVBD), groups of not yet individualized bivalents, circular bivalents, late prometaphase I, metaphase I, anaphase I and telophase I. The stages were identified in living oocytes by fluorescence microscopy using Hoechst 33342 as a specific vital dye. Oocytes from each stage of development developed in vitro and ovulated metaphase II oocytes were subsequently cultured in the presence of puromycin or 6-dimethylaminopurine (6-DMAP), an inhibitor of protein phosphorylation. The effects on chromatin of these drugs were studied during and at the end of culture by fluorescence and electron microscopy. We found that puromycin and 6-DMAP stop meiosis when applied at all stages of oocyte maturation, except for metaphase II. Oocytes at this stage are activated by puromycin. Reaction of the oocytes to the two drugs is different at GV and at metaphase II. All of the other stages react to the drugs by chromatin compaction, which can be followed by chromatin decondensation to form a nucleus. Our results suggest that late prophase chromatin condensation, bivalent individualization and retention of their individuality, as well as individualization of monovalents from telophase and retention of their individuality at metaphase II, are dependent on protein phosphorylation. The events occurring between metaphase I and telophase I are independent of protein synthesis and phosphorylation. The events occurring between metaphase II and formation of the nucleus are independent of protein synthesis.

摘要

将排卵前的小鼠卵母细胞在体外培养至成熟的各个后续阶段

生发泡(GV)、生发泡破裂(GVBD)、尚未分离的二价体组、环状二价体、晚前期I、中期I、后期I和末期I。使用Hoechst 33342作为特异性活体染料,通过荧光显微镜在活卵母细胞中识别这些阶段。来自每个发育阶段的卵母细胞在体外发育,随后将排出的中期II卵母细胞在嘌呤霉素或蛋白磷酸化抑制剂6-二甲基氨基嘌呤(6-DMAP)存在下进行培养。在培养期间和结束时,通过荧光显微镜和电子显微镜研究了这些药物对染色质的影响。我们发现,嘌呤霉素和6-DMAP在卵母细胞成熟的所有阶段(中期II除外)应用时会阻止减数分裂。处于此阶段的卵母细胞会被嘌呤霉素激活。卵母细胞在GV期和中期II对这两种药物的反应不同。所有其他阶段对药物的反应是染色质浓缩,随后染色质可能解聚形成一个细胞核。我们的结果表明,晚前期染色质浓缩、二价体分离及其个体性的保留,以及末期单价体的分离及其在中期II的个体性保留,均依赖于蛋白磷酸化。在中期I和末期I之间发生的事件独立于蛋白质合成和磷酸化。在中期II和细胞核形成之间发生的事件独立于蛋白质合成。

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