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雄性和雌性小鼠在产前和新生儿期的性二态性睾丸素分泌独立于 kisspeptin-Kiss1r 和 GnRH 信号。

Sexually dimorphic testosterone secretion in prenatal and neonatal mice is independent of kisspeptin-Kiss1r and GnRH signaling.

机构信息

Department of Reproductive Medicine, University of California, San Diego, 9500 Gilman Drive, La Jolla, California 92093, USA.

出版信息

Endocrinology. 2012 Feb;153(2):782-93. doi: 10.1210/en.2011-1838. Epub 2011 Dec 27.

Abstract

Kisspeptin, encoded by the Kiss1 gene, stimulates GnRH secretion and is therefore critical for sex steroid secretion at puberty and in adulthood. However, kisspeptin's role in regulating sex steroid secretion earlier in development is unexplored. In rodents, testosterone (T) levels are higher in prenatal and newborn males than females. We determined whether kisspeptin-Kiss1r and GnRH signaling plays a role in sexually dimorphic perinatal T secretion in mice. Our results demonstrate that 1) T levels in newborn males are elevated at 4 h but not 20 h after birth, but hypothalamic Kiss1 and neurokinin B (NKB) levels in males are not different between these time points (and both are lower than in females); 2) serum T levels in newborn Kiss1r knockout (KO) males are higher than in newborn females and similar to wild-type (WT) males; 3) perinatal hypothalamic progesterone receptor (Pgr) expression, which is dependent on circulating levels of gonadally produced T, is significantly higher in prenatal and newborn Kiss1r KO and WT males than similarly aged females; 4) multiple measures of testicular growth and function are not different between developing Kiss1r KO and WT mice until after postnatal d 5; and 5) GnRH neurons of newborn males do not exhibit high c-fos coexpression, and newborn hypogonadal (hpg) male mice (lacking GnRH) secrete elevated T, similar to newborn WT males. We conclude that, unlike in puberty and adulthood, elevated T secretion in prenatal and neonatal mice is independent of both kisspeptin and GnRH signaling, and the necessity of kisspeptin-Kiss1r signaling for testicular function is first apparent after d 5.

摘要

Kisspeptin 由 Kiss1 基因编码,可刺激 GnRH 分泌,因此对青春期和成年期的性激素分泌至关重要。然而,kisspeptin 在早期发育过程中调节性激素分泌的作用尚未得到探索。在啮齿动物中,雄性胎儿和新生鼠的睾酮(T)水平高于雌性。我们确定 kisspeptin-Kiss1r 和 GnRH 信号是否在雄性鼠围产期性别二态性 T 分泌中起作用。我们的结果表明:1)新生雄性鼠的 T 水平在出生后 4 小时而非 20 小时升高,但此时雄性鼠下丘脑 Kiss1 和神经激肽 B(NKB)水平与这些时间点之间没有差异(且均低于雌性);2)新生 Kiss1r 敲除(KO)雄性鼠的血清 T 水平高于新生雌性鼠,与野生型(WT)雄性鼠相似;3)依赖于循环性腺产生的 T 水平的围产期下丘脑孕激素受体(Pgr)表达,在新生 Kiss1r KO 和 WT 雄性鼠中显著高于同龄雌性鼠;4)直到出生后第 5 天,发育中的 Kiss1r KO 和 WT 雄性鼠的睾丸生长和功能的多个指标均无差异;5)新生雄性鼠的 GnRH 神经元不表现出高 c-fos 共表达,且缺乏 GnRH 的新生 Hypogonadal(hpg)雄性鼠(缺乏 GnRH)分泌的 T 水平升高,类似于新生 WT 雄性鼠。我们得出结论,与青春期和成年期不同,围产期和新生期鼠 T 分泌升高与 kisspeptin 和 GnRH 信号均无关,而 kisspeptin-Kiss1r 信号对睾丸功能的必要性在第 5 天之后才首次显现。

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