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恶喹酸对成年和老年Wistar大鼠精子发生无影响。

Lack of effects of oxolinic acid on spermatogenesis in young adult and aged Wistar rats.

作者信息

Yoshida M, Kitani T, Takenaka A, Kudoh K, Katsuda S I, Taya K, Kurokawa Y, Maekawa A

机构信息

Department of Pathology, Sasaki Institute, 2-2, Kanda-Surugadai, Chiyoda-ku, Tokyo 101-0062, Japan.

出版信息

Food Chem Toxicol. 2002 Dec;40(12):1815-25. doi: 10.1016/s0278-6915(02)00168-0.

Abstract

Prolonged treatment with oxolinic acid is known to elevate serum luteinizing hormone (LH) levels, resulting in induction of Leydig cell tumors in rats. In a carcinogenicity study of the compound, tubular atrophy of the testis was also increased, suggesting that oxolinic acid might affect spermatogenesis. The present study was therefore performed using rats of different ages with a particular focus on seminiferous tubule alteration and its relation to Leydig cell proliferation. Young adult (7 weeks of age) and aged (52 weeks of age) males of the Wistar strain were administered oxolinic acid at dietary concentrations of 0 (basal diet), 300, 1000 or 3000 ppm for 4 (all groups), 13 (0 and 3000 ppm groups), 26 (0 and 3000 ppm groups), or 52 weeks (0 and 3000 ppm groups of aged rats). Serum LH levels were elevated in both young adult and aged animals treated with 3000 ppm at most examined time points. While testosterone levels were also increased at the early time points in young adult, this was not the case in older animals. Elevation of the incidences of foci and/or focal hyperplasia of Leydig cells was noted but was only slight limited to aged rats treated with 3000 ppm after 26 weeks. Furthermore, it did not appear to be related to seminiferous tubular alteration. No treatment-related histopathological abnormalities could be detected in any treatment group, and morphometrical stage analysis of spermatogenesis conducted for the control and 3000 ppm-treated groups demonstrated no lesions. These results provide strong evidence that prolonged oxolinic treatment does not directly induce testicular toxicity or altered spermatogenesis in either young adult or aged rats, except for slight increase of Leydig cell proliferative lesions caused by elevated serum LH levels. Aged rats might have higher sensitivity than young adults to the effects of oxolinic acid on proliferative lesions of Leydig cells.

摘要

已知用恶喹酸进行长期治疗会提高血清促黄体生成素(LH)水平,从而在大鼠中诱发睾丸间质细胞瘤。在该化合物的致癌性研究中,睾丸的管状萎缩也有所增加,这表明恶喹酸可能会影响精子发生。因此,本研究使用不同年龄的大鼠进行,特别关注生精小管的改变及其与睾丸间质细胞增殖的关系。将Wistar品系的年轻成年(7周龄)和老年(52周龄)雄性大鼠分别给予饮食浓度为0(基础饮食)、300、1000或3000 ppm的恶喹酸,持续4周(所有组)、13周(0和3000 ppm组)、26周(0和3000 ppm组)或52周(老年大鼠的0和3000 ppm组)。在大多数检测时间点,给予3000 ppm恶喹酸的年轻成年和老年动物的血清LH水平均升高。虽然年轻成年动物在早期时间点的睾酮水平也有所升高,但老年动物并非如此。睾丸间质细胞灶和/或灶性增生的发生率有所升高,但仅轻微升高,仅限于26周后接受3000 ppm恶喹酸治疗的老年大鼠。此外,这似乎与生精小管的改变无关。在任何治疗组中均未检测到与治疗相关的组织病理学异常,对对照组和3000 ppm治疗组进行的精子发生形态学阶段分析也未发现病变。这些结果提供了有力证据,表明长期使用恶喹酸治疗不会直接诱导年轻成年或老年大鼠的睾丸毒性或精子发生改变,除了血清LH水平升高导致睾丸间质细胞增殖性病变略有增加外。老年大鼠可能比年轻成年大鼠对恶喹酸对睾丸间质细胞增殖性病变的影响更敏感。

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