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用三亚乙基三聚氰胺(TEM)处理的小鼠粗线期精母细胞中染色体畸变的延迟形成。

Delayed formation of chromosome aberrations in mouse pachytene spermatocytes treated with triethylenemelamine (TEM).

作者信息

Generoso W M, Krishna M, Sotomayor R E, Cacheiro N L

出版信息

Genetics. 1977 Jan;85(1):65-72. doi: 10.1093/genetics/85.1.65.

Abstract

Induction of chromosome aberrations in pachytene spermatocytes of mice by 2 mg/kg TEM was compared with induction by 400 R X rays. These doses induced comparably high dominant lethal effects in pachytene spermatocytes of mice. Cytological analysis at diakinesis-metaphase I stage showed that whereas 76.4% of the cells treated with X rays at pachytene stage had aberrations, the frequencies observed in two TEM experiments were only 0.8 and 2.2%. On the other hand, 5% of the progeny from TEM-treated pachytene spermatocytes were found to be translocation heterozygotes. This is the first report on the recovery of heritable translocations from treated spermatocytes of mice. The aberration frequencies observed for TEM in diakinesis-metaphase I were much too low to account for all the lethal mutations and heritable translocations. Thus, the formation of the bulk of aberrations induced by TEM in pachytene spermatocytes was delayed--a marked contrast to the more immediate formation of X-ray-induced aberrations. It is postulated that the formation of the bulk of TEM-induced aberrations in pachytene spermatocytes and in certain postmeiotic stages occurs sometime during spermiogenesis, and not through the operation of postfertilization pronuclear DNA synthesis.

摘要

将2mg/kg的三乙撑密胺(TEM)对小鼠粗线期精母细胞染色体畸变的诱导作用与400伦琴(R)的X射线诱导作用进行了比较。这些剂量在小鼠粗线期精母细胞中诱导出相当高的显性致死效应。在终变期-中期I阶段的细胞学分析表明,在粗线期用X射线处理的细胞中,有76.4%出现了畸变,而在两个TEM实验中观察到的频率分别仅为0.8%和2.2%。另一方面,发现来自经TEM处理的粗线期精母细胞的后代中有5%是易位杂合子。这是关于从小鼠经处理的精母细胞中恢复可遗传易位的首次报道。在终变期-中期I观察到的TEM诱导的畸变频率过低,无法解释所有的致死突变和可遗传易位。因此,TEM在粗线期精母细胞中诱导的大部分畸变的形成被延迟了——这与X射线诱导的畸变形成更为迅速形成了显著对比。据推测,TEM在粗线期精母细胞和某些减数分裂后阶段诱导的大部分畸变是在精子发生的某个时候形成的,而不是通过受精后原核DNA合成的作用。

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1
X-ray sensitivity of primary spermatocytes of the mouse.int.小鼠初级精母细胞的X射线敏感性。国际
Int J Radiat Biol Relat Stud Phys Chem Med. 1960 Apr;2:196-209. doi: 10.1080/09553006014550211.

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