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在年轻小鼠的精子发生过程中,突变频率下降,但在老年小鼠中则增加。

Mutation frequency declines during spermatogenesis in young mice but increases in old mice.

作者信息

Walter C A, Intano G W, McCarrey J R, McMahan C A, Walter R B

机构信息

Department of Cellular and Structural Biology, The University of Texas Health Science Center at San Antonio, 7703 Floyd Curl Drive, San Antonio, TX 78284-7762, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Aug 18;95(17):10015-9. doi: 10.1073/pnas.95.17.10015.

Abstract

Five percent of live-born human offspring will have a genetic disorder. Of these, 20% are because of germ-line de novo mutations. Several genetic diseases, such as neurofibromatosis and Duchenne muscular dystrophy, are associated with a high percentage of de novo germ-line mutations. Until recently, a direct analysis of spontaneous mutation frequencies in mammalian germ cells has been prevented by technical limitations. We have measured spontaneous mutation frequencies in a lacI transgene by using enriched populations of specific spermatogenic cell types. Similar to previously published results, we observed a lower mutation frequency for seminiferous tubule cell preparations, which contain all stages of spermatogenesis, relative to somatic tissues. We made the unexpected observation of a decline in mutation frequency during spermatogenesis, such that the mutation frequencies of type B spermatogonia and all subsequent stages of spermatogenesis are lower than the frequency for primitive type A spermatogonia. In addition, spermatogenic cells from old mice have significantly increased mutation frequencies compared with spermatogenic cells from young or middle-aged mice. Finally, the mutation frequency was observed to increase during spermiogenesis in postreplicative cell types when spermatogenic cells were obtained from old mice.

摘要

5%的活产人类后代会患有遗传疾病。其中,20%是由于生殖系新生突变。几种遗传疾病,如神经纤维瘤病和杜兴氏肌营养不良症,与较高比例的生殖系新生突变有关。直到最近,技术限制一直阻碍着对哺乳动物生殖细胞中自发突变频率的直接分析。我们通过使用特定生精细胞类型的富集群体来测量lacI转基因中的自发突变频率。与之前发表的结果相似,我们观察到,相对于体细胞组织,包含所有生精阶段的生精小管细胞制剂的突变频率较低。我们意外地观察到,在精子发生过程中突变频率下降,因此B型精原细胞和所有后续精子发生阶段的突变频率低于原始A型精原细胞的频率。此外,与年轻或中年小鼠的生精细胞相比,老年小鼠的生精细胞的突变频率显著增加。最后,当从老年小鼠获得生精细胞时,观察到在复制后细胞类型的精子形成过程中突变频率增加。

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