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新生大鼠植入胎儿视前区组织预防损伤诱导的雌性大鼠性早熟

Prevention of lesioning-induced precocious puberty in female rats by neonatal implantation of fetal preoptic tissue.

作者信息

Döcke F, Dörner G, Smollich A, Jensen C, Gruner B

出版信息

Exp Clin Endocrinol. 1985 Dec;86(3):353-6. doi: 10.1055/s-0029-1210508.

Abstract

Damage to the medial preoptic area (MPOA) was produced in one-day-old female rats by bilateral electrolytic lesions or by aspiration of preoptic tissue. Both procedures resulted in similar advancement of vaginal opening and the first ovulation. A further group of rats was lesioned or aspirated in the MPOA and immediately bilaterally implanted with medial preoptic tissue collected by the puncture method from 17-19-day-old female rat fetuses. After autopsy, tissue destruction and implants located in the MPOA could be identified in 5 females that showed significantly later onset of puberty than both the lesioned or aspirated and the untreated controls. The findings suggest that the elimination of neurones and not a stimulatory effect of electrolytic lesions on GnRH secretion is responsible for the acceleration of sexual maturation recorded after lesioning of the MPOA. Possible reasons for the failure to identify the grafts in most of the implanted females are discussed.

摘要

通过双侧电解损伤或视前组织抽吸术,对出生一天的雌性大鼠造成内侧视前区(MPOA)损伤。两种手术均导致阴道开口和首次排卵时间提前。另一组大鼠在MPOA处进行损伤或抽吸,并立即双侧植入从17 - 19日龄雌性大鼠胎儿通过穿刺法收集的内侧视前组织。尸检后,在5只雌性大鼠中可识别出位于MPOA的组织破坏和植入物,这些大鼠的青春期开始时间明显晚于损伤或抽吸组以及未处理的对照组。研究结果表明,神经元的消除而非电解损伤对促性腺激素释放激素(GnRH)分泌的刺激作用,是导致MPOA损伤后记录到的性成熟加速的原因。文中讨论了在大多数植入雌性大鼠中未能识别移植物的可能原因。

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