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雄性褐家鼠的生殖衰老:人类的一个模型。

Reproductive aging in the male brown-Norway rat: a model for the human.

作者信息

Wang C, Leung A, Sinha-Hikim A P

机构信息

Division of Endocrinology/Metabolism, Cedars-Sinai Medical Center, Los Angeles, California 90048.

出版信息

Endocrinology. 1993 Dec;133(6):2773-81. doi: 10.1210/endo.133.6.8243304.

Abstract

Previous studies in the Sprague-Dawley rat have demonstrated that male reproductive aging is primarily a neuroendocrine dysfunction characterized by decreased pulsatile LH secretion leading to low serum testosterone (T) levels, whereas sperm production is relatively well maintained. In contrast to the Sprague-Dawley rat, the Brown-Norway (BN) rat has a longer life span, does not become obese, and experiences fewer age-related tumors of the endocrine or reproductive system, thus providing a disease-free model for studying male reproductive aging. We studied the changes in serum hormone levels and related these alterations to testicular T production, Leydig cell morphometry, and spermatogenesis in young (6 months), aging (22 months), and old (30 months) BN rats. Low serum T levels were associated with decreased LH levels in the 22-month-old (T, 0.58 +/- 0.08 ng/ml; LH, 0.45 +/- 0.06 ng/ml) and 30-month-old rats (T, 0.63 +/- 0.10 ng/ml; LH, 0.34 +/- 0.04 ng/ml) compared to those in young rats (T, 1.35 +/- 0.30 ng/ml; LH, 0.79 +/- 0.10 ng/ml). In vitro Leydig cell T production, basally and after stimulation by LH, was similar in young and old rats. The total testicular T content was lower in 30- than in 6-month-old rats. Testicular morphometry showed smaller Leydig cell volume in the old (857 +/- 97 microns3) than in the young rats (1387 +/- 103 microns3), although their number per testis remained unchanged (6 months, 22.7 +/- 1.6 x 10(6)/testis; 30 months, 25.2 +/- 3.1 x 10(6)/testis). In contrast, a marked (68.4%) reduction in the total number of Sertoli cell per testis was noted in the 30-month-old rats. The proportion of the testis occupied by seminiferous tubules was also reduced in the old rats. Significant (P < 0.05) age-related reductions occurred in tubule diameter, length of tubules, and volume of tubules and their lumens. The testicular sperm concentration and total sperm production were significantly reduced in the 22- and 30-month-old rats. These changes in seminiferous tubule function in the old rats were associated with low serum and testicular inhibin and high serum FSH levels. We conclude that aging in the reproductive axis of the BN rat is manifested by 1) lower serum T levels due to decreased pituitary LH stimulation of endogenous T production, and 2) decreased seminiferous tubule function accompanied by elevated FSH levels indicative of a primary testicular disorder.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

先前对斯普拉格-道利大鼠的研究表明,雄性生殖衰老主要是一种神经内分泌功能障碍,其特征是促黄体生成素(LH)脉冲式分泌减少,导致血清睾酮(T)水平降低,而精子生成相对保持良好。与斯普拉格-道利大鼠不同,棕色挪威(BN)大鼠寿命更长,不会肥胖,且内分泌或生殖系统与年龄相关的肿瘤较少,因此为研究雄性生殖衰老提供了一个无疾病模型。我们研究了年轻(6个月)、衰老(22个月)和老年(30个月)BN大鼠血清激素水平的变化,并将这些变化与睾丸T生成、睾丸间质细胞形态计量学和精子发生相关联。与年轻大鼠(T,1.35±0.30 ng/ml;LH,0.79±0.10 ng/ml)相比,22个月大(T,0.58±0.08 ng/ml;LH,0.45±0.06 ng/ml)和30个月大的大鼠(T,0.63±0.10 ng/ml;LH,0.34±0.04 ng/ml)的低血清T水平与LH水平降低有关。年轻和老年大鼠的睾丸间质细胞基础状态下以及LH刺激后的体外T生成相似。30个月大的大鼠睾丸总T含量低于6个月大的大鼠。睾丸形态计量学显示,老年大鼠(857±97立方微米)的睾丸间质细胞体积小于年轻大鼠(1387±103立方微米),尽管每个睾丸中的细胞数量保持不变(6个月,22.7±1.6×10⁶/睾丸;30个月,25.2±3.1×10⁶/睾丸)。相反,30个月大的大鼠每个睾丸中支持细胞的总数显著减少(68.4%)。老年大鼠曲细精管占据睾丸的比例也降低。曲细精管直径、长度、曲细精管及其管腔体积出现了与年龄相关的显著(P<0.05)减少。22个月和30个月大的大鼠睾丸精子浓度和总精子生成显著降低。老年大鼠曲细精管功能的这些变化与低血清和睾丸抑制素以及高血清促卵泡激素(FSH)水平有关。我们得出结论,BN大鼠生殖轴的衰老表现为:1)由于垂体LH对内源性T生成的刺激减少,血清T水平降低;2)曲细精管功能降低,同时FSH水平升高,表明存在原发性睾丸疾病。(摘要截短至400字)

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