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Fast forward to new genes in mammalian reproduction

机译:快进哺乳动物繁殖中的新基因

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摘要

The study of reproductive genetics in mammals has lagged behind that of simpler and more tractable model organisms, such as D. melanogaster, C. elegans and various yeast models. Although much valuable information has been generated using these organisms, they do not model the genetic and biological complexity of mammalian reproduction. Thus, the majority of genes required for gametogenesis in mammals remain unidentified. To expand on the existing knowledge of mammalian reproductive genetics, we have carried out forward genetic screens in mice to identify infertility mutants and the underlying mutant genes. Two different approaches were used: mutagenesis of the germline in whole mice, and mutagenesis of embryonic stem cells. This was followed by two- or three-generation breeding schemes to identify pedigrees segregating infertility mutations, which were then phenotypically characterized, genetically mapped, and in some cases, positionally cloned. This whole-genome approach has generated a wide collection of mutants with defects ranging from problems with germ cell development to abnormal sperm morphology. These models have allowed us to study the genetics, as well as the physiology, of reproduction in mammals. This review focuses on describing some of the genes identified in these screens and the ongoing effort to characterize additional mutants.
机译:对哺乳动物生殖遗传学的研究落后于诸如D. melanogaster,秀丽隐杆线虫和各种酵母菌模型等更简单易处理的模型生物。尽管使用这些生物已经产生了许多有价值的信息,但是它们并不能模拟哺乳动物繁殖的遗传和生物学复杂性。因此,哺乳动物配子发生所需的大多数基因仍未确定。为了扩展哺乳动物生殖遗传学的现有知识,我们在小鼠中进行了正向遗传筛选,以鉴定不育突变体和潜在的突变基因。使用了两种不同的方法:对整个小鼠的种系进行诱变,以及对胚胎干细胞进行诱变。接下来是两代或三代育种方案,以鉴定出分离不育突变的家谱,然后对其进行表型鉴定,遗传定位以及在某些情况下进行定位克隆。这种全基因组方法已产生了许多突变体,其缺陷范围从生殖细胞发育问题到精子形态异常。这些模型使我们能够研究哺乳动物繁殖的遗传学以及生理学。这篇综述的重点是描述在这些筛选中鉴定出的一些基因,以及为表征其他突变体所做的持续努力。

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