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锂:长期给药后小鼠循环睾酮水平降低的证据。

Lithium: evidence for reduction in circulating testosterone levels in mice following chronic administration.

作者信息

Collins T J, Chatterjee S, LeGate L S, Banerji T K

机构信息

Department of Anatomy and Neurosciences, University of Texas Medical Branch, Galveston 77550.

出版信息

Life Sci. 1988;43(19):1501-5. doi: 10.1016/0024-3205(88)90397-9.

Abstract

Lithium, the widely-used antipsychotic drug, is known to exert adverse effects on a number of endocrine organs. In the present investigations, the effects of chronic lithium administration on circulating levels of testosterone and plasma and pituitary levels of luteinizing hormone (LH) were evaluated in order to examine whether or not the pituitary-gonadal axis is a probable target of lithium action. Adult male C57BL/6 mice, maintained on a fixed photoperiodism (LD 14:10), were administered lithium orally, by being fed on a specially prepared chow containing 0.4% lithium chloride for 15 or 30 days, while their matched controls were maintained on standard laboratory chow. At the termination of the respective experimental schedules, the animals were decapitated, their blood collected, and plasma was separated and stored frozen. Pituitaries were quickly removed, weighed, homogenized, centrifuged and their supernatants were stored frozen. Testosterone in plasma and LH in pituitary and plasma were quantitated by standard RIA methods. Plasma Li concentration was determined by using flame photometric methods. A significant suppression in testosterone levels was noted after both 15 (p less than .01) and 30 (p less than .05) days of lithium treatment, but both pituitary and plasma LH levels remained unchanged at both the periods. It is, therefore, suggested that lithium exerts its effect directly at the level of the Leydig cells rather than through the pituitary-gonadal axis. Since the noted lithium-induced reduction of testosterone was manifested when the plasma lithium levels were within (or around) the therapeutic range, these results may have important clinical implications.

摘要

锂作为一种广泛使用的抗精神病药物,已知会对多个内分泌器官产生不良影响。在本研究中,评估了长期给予锂对睾酮循环水平以及黄体生成素(LH)的血浆和垂体水平的影响,以检查垂体 - 性腺轴是否可能是锂作用的靶点。将成年雄性C57BL / 6小鼠维持在固定的光周期(LD 14:10)下,通过喂食含有0.4%氯化锂的特制饲料口服给予锂15天或30天,而其配对的对照组则维持在标准实验室饲料上。在各自实验计划结束时,将动物断头,采集血液,分离血浆并冷冻保存。迅速取出垂体,称重,匀浆,离心,其上清液冷冻保存。通过标准放射免疫分析方法对血浆中的睾酮以及垂体和血浆中的LH进行定量。使用火焰光度法测定血浆锂浓度。锂治疗15天(p小于0.01)和30天(p小于0.05)后均观察到睾酮水平有显著抑制,但在这两个时期垂体和血浆LH水平均保持不变。因此,提示锂直接在睾丸间质细胞水平发挥作用,而非通过垂体 - 性腺轴。由于在血浆锂水平处于(或接近)治疗范围内时就出现了锂诱导的睾酮降低,这些结果可能具有重要的临床意义。

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