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甲磺酸乙酯对雄性小鼠生殖细胞中DNA和鱼精蛋白的乙基化作用以及这些分子靶点与显性致死诱导的相关性。

Ethylation of DNA and protamine by ethyl methanesulfonate in the germ cells of male mice and the relevancy of these molecular targets to the induction of dominant lethals.

作者信息

Sega G A, Owens J G

出版信息

Mutat Res. 1978 Oct;52(1):87-106. doi: 10.1016/0027-5107(78)90098-2.

Abstract

The molecular dosimetry of ethyl methanesulfonate (EMS) in the germ cells of male mice has been investigated. The mice were injected i.p. with 200 mg/kg of [3H]EMS and the ethylations per sperm head, per deoxynucleotide, and per unit of protamine were then determined over a 2-week period. The ethylations per sperm head closely paralleled the dominant-lethal frequency curve for EMS, reaching a maximum of 5 to 6.5 million ethylations per vas sperm head at 8 to 10 days after treatment. Ethylation of sperm DNA was greatest at 4 h after treatment, with 5.7 ethylations/10(5) deoxynucleotides, and gradually decreased to 2.2 ethylations/10(5) deoxynucleotides at 15 days after treatment. The ethylation of sperm DNA did not increase in the germ-cell stages most sensitive to EMS, and was not correlated with the dominant-lethal frequency curve for EMS. However, ethylation of sperm protamine did increase in the germ-cell stages most sensitive to EMS, and showed an excellent correlation with the incidence of dominant lethals produced by EMS in the germ cells. A model is presented to explain, at a molecular level, how dominant lethals may be induced in mouse germ cells by EMS. Ethylation of cysteine sulfhydryl groups contained in mouse-sperm protamine could block normal disulfide-bond formation, preventing proper chromatin condensation in the sperm nucleus. Stresses in the chromatin structure could then eventually lead to chromosome breakage, with resultant dominant lethality.

摘要

对雄性小鼠生殖细胞中甲基磺酸乙酯(EMS)的分子剂量学进行了研究。给小鼠腹腔注射200mg/kg的[³H]EMS,然后在2周时间内测定每个精子头部、每个脱氧核苷酸和每个鱼精蛋白单位的乙基化程度。每个精子头部的乙基化程度与EMS的显性致死频率曲线密切平行,在处理后8至10天,每个输精管精子头部的乙基化程度最高达到500万至650万次。精子DNA的乙基化在处理后4小时最高,为5.7次乙基化/10⁵个脱氧核苷酸,并在处理后15天逐渐降至2.2次乙基化/10⁵个脱氧核苷酸。精子DNA的乙基化在对EMS最敏感的生殖细胞阶段并未增加,且与EMS的显性致死频率曲线无关。然而,精子鱼精蛋白的乙基化在对EMS最敏感的生殖细胞阶段确实增加了,并且与EMS在生殖细胞中产生的显性致死发生率显示出极好的相关性。提出了一个模型,从分子水平解释EMS如何在小鼠生殖细胞中诱导显性致死。小鼠精子鱼精蛋白中含有的半胱氨酸巯基的乙基化可能会阻止正常的二硫键形成,从而防止精子核中染色质的正常凝聚。染色质结构的压力最终可能导致染色体断裂,从而产生显性致死。

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