Instructing Mouse Germ Cells to Adopt a Female Fate.

IF 2.4 4区 医学 Q2 DEVELOPMENTAL BIOLOGY
Cassy Spiller, Josephine Bowles
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引用次数: 5

Abstract

Background: Germ cells are critical for the survival of our species. They are the only cells that undergo meiosis - the reductive form of cell division that is necessary for genetic reassortment of chromosomes and production of the haploid gametes, the sperm and eggs. Remarkably, the initial female/male fate decision in fetal germ cells does not depend on whether they are chromosomally XX or XY; rather, initial sexual fate is imposed by influences from the surrounding tissue. In mammals, the female germline is particularly precious: despite recent suggestions that germline stem cells exist in the ovary, it is still generally accepted that the ovarian reserve is finite, and its size is dependant on germ cells of the fetal ovary initiating meiosis in a timely manner.

Summary: Prior to 2006, evidence suggested that gonadal germ cells initiate meiotic prophase I by default, but more recent data support a key role for the signalling molecule retinoic acid (RA) in instructing female germ cell fate. Newer findings also support a key meiosis-inducing role for another signalling molecule, bone morphogenic protein (BMP). Nonetheless, many questions remain.

Key messages: Here, we review knowledge thus far regarding extrinsic and intrinsic determinants of a female germ cell fate, focusing on the mouse model.

引导小鼠生殖细胞接受雌性命运。
背景:生殖细胞对人类的生存至关重要。它们是唯一经历减数分裂的细胞,减数分裂是染色体基因重组和产生单倍体配子、精子和卵子所必需的细胞分裂的减数形式。值得注意的是,胎儿生殖细胞最初的雌雄命运决定并不取决于它们是XX染色体还是XY染色体;相反,最初的性命运是由周围组织的影响强加的。在哺乳动物中,雌性生殖系尤为珍贵:尽管最近有人认为卵巢中存在生殖系干细胞,但人们仍然普遍认为卵巢储备是有限的,其大小取决于胎儿卵巢生殖细胞是否及时开始减数分裂。摘要:在2006年之前,有证据表明性腺生殖细胞默认启动减数分裂前期I,但最近的数据支持信号分子维甲酸(RA)在指导女性生殖细胞命运方面的关键作用。最新的发现也支持另一种信号分子骨形态发生蛋白(BMP)在减数分裂诱导中的关键作用。尽管如此,许多问题依然存在。关键信息:在这里,我们回顾了迄今为止关于雌性生殖细胞命运的外在和内在决定因素的知识,重点是小鼠模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Sexual Development
Sexual Development 生物-发育生物学
CiteScore
4.00
自引率
4.30%
发文量
25
审稿时长
>12 weeks
期刊介绍: Recent discoveries in experimental and clinical research have led to impressive advances in our knowledge of the genetic and environmental mechanisms governing sex determination and differentiation, their evolution as well as the mutations or endocrine and metabolic abnormalities that interfere with normal gonadal development. ‘Sexual Development’ provides a unique forum for this rapidly expanding field. Its broad scope covers all aspects of genetics, molecular biology, embryology, endocrinology, evolution and pathology of sex determination and differentiation in humans and animals. It publishes high-quality original research manuscripts, review articles, short reports, case reports and commentaries. An internationally renowned and multidisciplinary editorial team of three chief editors, ten prominent scientists serving as section editors, and a distinguished panel of editorial board members ensures fast and author-friendly editorial processing and peer reviewing.
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