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成人卵巢中的生殖系干细胞与新卵子生成

Germline stem cells and neo-oogenesis in the adult human ovary.

作者信息

Liu Yifei, Wu Chao, Lyu Qifeng, Yang Dongzi, Albertini David F, Keefe David L, Liu Lin

机构信息

College of Life Sciences, Sun Yat-Sen University, Guangzhou 510275, China.

出版信息

Dev Biol. 2007 Jun 1;306(1):112-20. doi: 10.1016/j.ydbio.2007.03.006. Epub 2007 Mar 12.

Abstract

It remains unclear whether neo-oogenesis occurs in postnatal ovaries of mammals, based on studies in mice. We thought to test whether adult human ovaries contain germline stem cells (GSCs) and undergo neo-oogenesis. Rather than using genetic manipulation which is unethical in humans, we took the approach of analyzing the expression of meiotic marker genes and genes for germ cell proliferation, which are required for neo-oogenesis, in adult human ovaries covering an age range from 28 to 53 years old, compared to testis and fetal ovaries served as positive controls. We show that active meiosis, neo-oogenesis and GSCs are unlikely to exist in normal, adult, human ovaries. No early meiotic-specific or oogenesis-associated mRNAs for SPO11, PRDM9, SCP1, TERT and NOBOX were detectable in adult human ovaries using RT-PCR, compared to fetal ovary and adult testis controls. These findings are further corroborated by the absence of early meiocytes and proliferating germ cells in adult human ovarian cortex probed with markers for meiosis (SCP3), oogonium (OCT3/4, c-KIT), and cell cycle progression (Ki-67, PCNA), in contrast to fetal ovary controls. If postnatal oogenesis is confirmed in mice, then this species would represent an exception to the rule that neo-oogenesis does not occur in adults.

摘要

基于对小鼠的研究,目前尚不清楚新生殖发生是否在哺乳动物出生后的卵巢中出现。我们试图测试成年人类卵巢中是否含有生殖系干细胞(GSCs)并发生新生殖。我们没有采用在人类身上不道德的基因操作方法,而是采用分析减数分裂标记基因以及新生殖所需的生殖细胞增殖相关基因的表达情况这种方法,将年龄范围在28至53岁的成年人类卵巢与作为阳性对照的睾丸和胎儿卵巢进行比较。我们发现,正常成年人类卵巢中不太可能存在活跃的减数分裂、新生殖和生殖系干细胞。与胎儿卵巢和成年睾丸对照相比,使用逆转录聚合酶链反应(RT-PCR)在成年人类卵巢中未检测到SPO11、PRDM9、SCP1、端粒酶逆转录酶(TERT)和无框蛋白(NOBOX)等早期减数分裂特异性或卵子发生相关的信使核糖核酸(mRNAs)。与胎儿卵巢对照相比,用减数分裂标记物(SCP3)、卵原细胞标记物(OCT3/4、原癌基因c-Kit)和细胞周期进程标记物(Ki-67、增殖细胞核抗原(PCNA))检测成年人类卵巢皮质中不存在早期减数分裂细胞和增殖的生殖细胞,这进一步证实了上述发现。如果在小鼠中证实了出生后卵子发生,那么这个物种将成为成年后不发生新生殖这一规则的例外。

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