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XXY小鼠中的生殖细胞发育:X染色体重新激活独立于性别分化的证据。

Germ cell development in the XXY mouse: evidence that X chromosome reactivation is independent of sexual differentiation.

作者信息

Mroz K, Carrel L, Hunt P A

机构信息

Department of Genetics and Center for Human Genetics, Case Western Reserve University and University Hospitals of Cleveland, Cleveland, Ohio, 44106-4955, USA.

出版信息

Dev Biol. 1999 Mar 1;207(1):229-38. doi: 10.1006/dbio.1998.9160.

Abstract

Prior to entry into meiosis, XX germ cells in the fetal ovary undergo X chromosome reactivation. The signal for reactivation is thought to emanate from the genital ridge, but it is unclear whether it is specific to the developing ovary. To determine whether the signals are present in the developing testis as well as the ovary, we examined the expression of X-linked genes in germ cells from XXY male mice. To facilitate this analysis, we generated XXY and XX fetuses carrying X chromosomes that were differentially marked and subject to nonrandom inactivation. This pattern of nonrandom inactivation was maintained in somatic cells but, in XX as well as XXY fetuses, both parental alleles were expressed in germ cell-enriched cell populations. Because testis differentiation is temporally and morphologically normal in the XXY testis and because all germ cells embark upon a male pathway of development, these results provide compelling evidence that X chromosome reactivation in fetal germ cells is independent of the somatic events of sexual differentiation. Proper X chromosome dosage is essential for the normal fertility of male mammals, and abnormalities in germ cell development are apparent in the XXY testis within several days of X reactivation. Studies of exceptional germ cells that survive in the postnatal XXY testis demonstrated that surviving germ cells are exclusively XY and result from rare nondisjunctional events that give rise to clones of XY cells.

摘要

在进入减数分裂之前,胎儿卵巢中的XX生殖细胞会经历X染色体重新激活。重新激活的信号被认为源自生殖嵴,但尚不清楚它是否特定于发育中的卵巢。为了确定这些信号是否也存在于发育中的睾丸以及卵巢中,我们检测了XXY雄性小鼠生殖细胞中X连锁基因的表达。为便于此项分析,我们构建了携带经差异标记且会发生非随机失活的X染色体的XXY和XX胎儿。这种非随机失活模式在体细胞中得以维持,但在XX和XXY胎儿中,两个亲本等位基因在富含生殖细胞的细胞群体中均有表达。由于XXY睾丸中的睾丸分化在时间和形态上均正常,且所有生殖细胞都走上雄性发育途径,这些结果提供了令人信服的证据,表明胎儿生殖细胞中的X染色体重新激活独立于性分化的体细胞事件。适当的X染色体剂量对于雄性哺乳动物的正常生育能力至关重要,并且在X重新激活后的几天内,XXY睾丸中生殖细胞发育的异常就很明显。对出生后XXY睾丸中存活的特殊生殖细胞的研究表明,存活的生殖细胞均为XY型,是由罕见的不分离事件产生的XY细胞克隆。

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