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精子发生过程中线粒体DNA拷贝数的调控。

Regulation of mitochondrial DNA copy number during spermatogenesis.

作者信息

Rantanen A, Larsson N G

机构信息

Department of Molecular Medicine, Center for Molecular Medicine, Karolinska Hospital, Stockholm, Sweden.

出版信息

Hum Reprod. 2000 Jul;15 Suppl 2:86-91. doi: 10.1093/humrep/15.suppl_2.86.

DOI:10.1093/humrep/15.suppl_2.86
PMID:11041516
Abstract

The nuclear genome is physically compacted during spermatogenesis by replacing histones with protamines and transition proteins. This altered nuclear protein context may make gene regulation at the transcriptional level less efficient and could explain why post-transcriptional regulation is prominent in haploid male germ cells. Mitochondria and mitochondrial (mt) DNA are maternally inherited, whereas the transmission of paternal mtDNA is blocked in mammals. The paternal mtDNA enters the oocyte but is no longer detectable in the preimplantation embryo. Several mechanisms could be responsible for preventing the transmission of paternal mtDNA, including the down-regulation of mtDNA copy number during spermatogenesis, specific elimination of paternal mitochondria in fertilized oocytes, and the suspension of mtDNA replication in the fertilized oocyte. It is the first of these that is the subject of the present review. Mitochondrial transcription factor A (mtTFA, or Tfam) is a key regulator of mtDNA copy number in mammals. Germ cell-specific Tfam transcript isoforms are expressed during spermatogenesis in mice and humans. These alternative Tfam transcript isoforms have a structure that could prevent protein translation; their expression coincides with down-regulation of the mitochondrial Tfam protein values. We propose that this down-regulation of mitochondrial Tfam protein levels in turn down-regulates mtDNA copy number during mammalian spermatogenesis.

摘要

在精子发生过程中,核基因组通过用鱼精蛋白和过渡蛋白取代组蛋白而在物理上被压缩。这种改变的核蛋白环境可能会使转录水平的基因调控效率降低,并可以解释为什么转录后调控在单倍体雄性生殖细胞中很突出。线粒体和线粒体(mt)DNA是母系遗传的,而父系mtDNA在哺乳动物中的传递被阻断。父系mtDNA进入卵母细胞,但在植入前胚胎中不再可检测到。有几种机制可能负责阻止父系mtDNA的传递,包括精子发生过程中mtDNA拷贝数的下调、受精卵中父系线粒体的特异性消除以及受精卵中mtDNA复制的暂停。本文综述的正是其中的第一种机制。线粒体转录因子A(mtTFA,或Tfam)是哺乳动物中mtDNA拷贝数的关键调节因子。生殖细胞特异性的Tfam转录本异构体在小鼠和人类的精子发生过程中表达。这些替代性的Tfam转录本异构体具有可能阻止蛋白质翻译的结构;它们的表达与线粒体Tfam蛋白值的下调相一致。我们提出,哺乳动物精子发生过程中线粒体Tfam蛋白水平的这种下调反过来会下调mtDNA拷贝数。

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