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双氢睾酮治疗的时间和持续时间会影响性二态性大鼠脊髓核中运动神经元数量和形态的发育。

Timing and duration of dihydrotestosterone treatment affect the development of motoneuron number and morphology in a sexually dimorphic rat spinal nucleus.

作者信息

Goldstein L A, Sengelaub D R

机构信息

Program in Neural Science, Indiana University, Bloomington 47405.

出版信息

J Comp Neurol. 1992 Dec 1;326(1):147-57. doi: 10.1002/cne.903260113.

Abstract

The spinal nucleus of the bulbocavernosus (SNB) is a sexually dimorphic motor nucleus in the rat lumbar spinal cord. SNB motoneurons and their perineal target muscles are present in adult males, but reduced or absent in adult females. This dimorphism is due to the presence of androgens during development. Perinatal treatment of females with testosterone (T), or a combination of dihydrotestosterone (DHT) and estrogen (E+D females) from embryonic (E) day 16 through postnatal (P) day 5, results in a masculine number of SNB motoneurons and the retention of the target muscles. Perinatal treatment with estrogen alone does not masculinize the SNB; prenatal treatment with DHT alone from E17-E22 results in a feminine number of SNB motoneurons and a significantly altered motoneuron morphology and connectivity. To determine if masculinization of the SNB involves the interaction of estrogen and DHT or results from a longer exposure to DHT alone, the number, morphology, and connectivity of SNB motoneurons in females treated with DHT both pre- and post-natally (from E16-P5) were examined. At E22, DHTP (E16-P5) females have SNB motoneuron numbers identical to E+D and normal females, but far fewer than normal males, thus indicating that T is essential for prenatal masculinization. After E22, SNB motoneuron number declines precipitously in normal females but remains stable in DHTP (E16-P5) females and E+D females, which do not differ from normal males at P10. These results demonstrate that DHT can completely masculinize SNB motoneuron number without any synergistic actions with estrogen, and suggest that the development of SNB motoneuron number is strictly an androgen-mediated event. In adulthood, horseradish peroxidase histochemistry reveals that the connectivity, dendritic length, and soma size of SNB motoneurons in DHTP (E16-P5) females are identical to those of normal males but differ significantly from those of DHTP (E17-E22) females. These data suggest that the altered connectivity in DHTP (E17-E22) females is not simply a hormone-specific effect, but the result of a truncated hormone exposure. Thus, DHT can fully masculinize SNB morphology and connectivity if given during the appropriate period of development. It is suggested that while T may be required to masculinize the SNB prenatally, DHT may be involved in masculinizing postnatal aspects of SNB development.

摘要

球海绵体肌脊髓核(SNB)是大鼠腰脊髓中的一个性别二态性运动核。SNB运动神经元及其会阴靶肌肉在成年雄性中存在,但在成年雌性中减少或缺失。这种二态性是由于发育过程中雄激素的存在。从胚胎(E)第16天到出生后(P)第5天,用睾酮(T)或二氢睾酮(DHT)与雌激素的组合(E + D雌性)对雌性进行围产期治疗,会导致SNB运动神经元数量呈男性化,并保留靶肌肉。单独用雌激素进行围产期治疗不会使SNB男性化;从E17 - E22单独用DHT进行产前治疗会导致SNB运动神经元数量呈女性化,并且运动神经元形态和连接性发生显著改变。为了确定SNB的男性化是否涉及雌激素和DHT的相互作用,或者是否仅由更长时间暴露于DHT导致,研究了在产前和产后(从E16 - P5)用DHT治疗的雌性中SNB运动神经元的数量、形态和连接性。在E22时,DHTP(E16 - P5)雌性的SNB运动神经元数量与E + D和正常雌性相同,但远少于正常雄性,因此表明T对产前男性化至关重要。在E22之后,正常雌性的SNB运动神经元数量急剧下降,但在DHTP(E16 - P5)雌性和E + D雌性中保持稳定,这两组在P10时与正常雄性没有差异。这些结果表明,DHT可以完全使SNB运动神经元数量男性化,而无需与雌激素有任何协同作用,并表明SNB运动神经元数量的发育严格是雄激素介导的事件。在成年期,辣根过氧化物酶组织化学显示,DHTP(E16 - P5)雌性中SNB运动神经元的连接性、树突长度和胞体大小与正常雄性相同,但与DHTP(E17 - E22)雌性有显著差异。这些数据表明,DHTP(E17 - E22)雌性中连接性的改变不仅仅是激素特异性效应,而是激素暴露截断的结果。因此,如果在适当的发育时期给予DHT,可以完全使SNB形态和连接性男性化。有人认为,虽然产前可能需要T使SNB男性化,但DHT可能参与使SNB发育的产后方面男性化。

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