MRC Centre for Reproductive Health, The Queen's Medical Research Institute, University of Edinburgh, Edinburgh, UK.
Warwick Medical School, Coventry, UK.
Clin Endocrinol (Oxf). 2017 Dec;87(6):748-756. doi: 10.1111/cen.13445. Epub 2017 Sep 5.
Patients with mutations of neurokinin B (NKB) and its receptor show hypogonadotrophic hypogonadism, but there is little evidence for the importance of this pathway in reproductive function in normal men, or its functional hierarchy with kisspeptin.
An open label study wherein men (n = 6) were administered the NK3R antagonist MLE4901 40 mg orally twice a day for 7 days. Kisspeptin-10 (0.3 μg/kg iv bolus) was given before and on day 7 of NK3R antagonist treatment.
Subjects were healthy men.
Reproductive hormones were measured before and during the NK3R antagonist administration, including frequent sampling on two occasions for analysis of pulsatile LH secretion.
LH, FSH and testosterone secretion were decreased during NK3R antagonist administration. LH showed a biphasic response, being reduced after 24 hours of treatment (4.5 ± 0.6 IU/L pretreatment to 1.7 ± 0.2 IU/L, P < .05), with partial recovery thereafter, but it was again decreased on day 7 (2.5 ± 0.6 IU/L, P < .05 vs pretreatment). FSH secretion was also suppressed, with a similar temporal pattern to that of LH. Testosterone secretion was decreased from 24 hours (18.4 ± 1.6 pretreatment vs 5.6 ± 1.5 nmol/L, P < .01) and remained suppressed throughout the treatment period. Analysis of LH pulsatility showed that both basal and pulsatile LH secretion were markedly suppressed but there was no detected change in LH pulse frequency. Kisspeptin-10 stimulated LH secretion, with similar responses before and during NK3R antagonist administration.
These data demonstrate a central role for NKB/NK3R in the physiological regulation of reproductive function in men, and that this is functionally upstream of kisspeptin-mediated GnRH secretion.
神经激肽 B(NKB)及其受体发生突变的患者表现为促性腺激素缺乏性性腺功能减退症,但在正常男性生殖功能中,该途径的重要性及其与 kisspeptin 的功能层次关系的证据很少。
一项开放性标签研究,其中 6 名男性(n=6)每天口服两次 NK3R 拮抗剂 MLE490140mg,共 7 天。在 NK3R 拮抗剂治疗前和第 7 天给予 kisspeptin-10(0.3μg/kg 静脉推注)。
研究对象为健康男性。
在 NK3R 拮抗剂给药前后测量生殖激素,包括两次频繁采样分析 LH 脉冲分泌。
NK3R 拮抗剂给药期间,LH、FSH 和睾酮分泌减少。LH 呈双相反应,治疗 24 小时后降低(预处理时为 4.5±0.6IU/L,降至 1.7±0.2IU/L,P<.05),此后部分恢复,但第 7 天再次降低(2.5±0.6IU/L,P<.05 与预处理相比)。FSH 分泌也受到抑制,与 LH 的时间模式相似。睾酮分泌从 24 小时开始下降(预处理时为 18.4±1.6,降至 5.6±1.5nmol/L,P<.01),并在整个治疗期间持续抑制。LH 脉冲分析显示,基础和脉冲 LH 分泌均明显受抑制,但 LH 脉冲频率无变化。Kisspeptin-10 刺激 LH 分泌,NK3R 拮抗剂给药前后反应相似。
这些数据表明,NKB/NK3R 在男性生殖功能的生理调节中起中枢作用,其功能位于 kisspeptin 介导的 GnRH 分泌的上游。
