来曲唑治疗男性肥胖相关性低促性腺激素型性腺功能减退症的随机双盲 2b 期临床试验。

Leflutrozole in male obesity-associated hypogonadotropic hypogonadism: Ph 2b double-blind randomised controlled trial.

机构信息

Centre for Diabetes and Endocrinology, Barnsley Hospital NHS Trust, Barnsley, United Kingdom.

Department of Oncology and Metabolism, University of Sheffield Medical School, Sheffield, United Kingdom.

出版信息

Eur J Endocrinol. 2023 Sep 1;189(3):297-308. doi: 10.1093/ejendo/lvad099.

DOI:10.1093/ejendo/lvad099

PMID:37579053

Abstract

OBJECTIVE

Assessment of the efficacy and safety/tolerability of the aromatase inhibitor leflutrozole to normalise testosterone in Obesity-associated Hypogonadotropic Hypogonadism (OHH).

DESIGN

Placebo-controlled, double-blind, RCT, in 70 sites in Europe/USA.

METHODS

Patient inclusion criteria: men with BMI of 30-50 kg/m2, morning total testosterone (TT) < 10.41 nmol/L, and two androgen deficiency symptoms (at least one of sexual dysfunction). Patients randomised to weekly leflutrozole (0.1/0.3/1.0 mg) or placebo for 24 weeks. Primary endpoint: normalisation of TT levels in ≥75% of patients after 24 weeks. Secondary endpoints (included): time to TT normalisation and change in LH/FSH. Safety was assessed through adverse events and laboratory monitoring.

RESULTS AND CONCLUSIONS

Of 2103 screened, 271 were randomised, 81 discontinued. Demographic characteristics were similar across groups. Mean BMI was 38.1 kg/m2 and TT 7.97 nmol/L. The primary endpoint was achieved in all leflutrozole-treated groups by 24 weeks with a dose-tiered response; mean TT 15.89; 17.78; 20.35 nmol/L, for leflutrozole 0.1 mg, 0.3 mg, and 1.0 mg groups respectively, vs 8.04 nmol/L for placebo. LH/FSH significantly increased in leflutrozole vs placebo groups. No improvements in body composition or sexual dysfunction were observed. Semen volume/total motile sperm count improved with leflutrozole vs placebo. Treatment-emergent adverse events, more common in leflutrozole-treated groups included, raised haematocrit, hypertension, increased PSA, and headache. Some reduction in lumbar bone density was observed with leflutrozole (mean -1.24%, -1.30%, -2.09%) and 0.66% for 0.1 mg, 0.3 mg, 1.0 mg, and placebo, respectively, without change at the hip. This RCT of leflutrozole in OHH demonstrated normalisation of TT in obese men. FSH/LH and semen parameter changes support that leflutrozole may preserve/improve testicular function.

CLINICAL TRIAL REGISTRATION NUMBER

NCT02730169.

摘要

目的

评估芳香酶抑制剂来曲唑使肥胖相关性低促性腺激素性性腺功能减退症（OHH）患者的睾酮正常化的疗效和安全性/耐受性。

设计

在欧洲/美国的 70 个地点进行安慰剂对照、双盲、随机对照试验（RCT）。

方法

患者纳入标准：BMI 为 30-50kg/m2、早晨总睾酮（TT）<10.41nmol/L 且有两种雄激素缺乏症状（至少有一种性功能障碍）的男性。患者随机接受每周来曲唑（0.1/0.3/1.0mg）或安慰剂治疗 24 周。主要终点：24 周后≥75%的患者 TT 水平正常化。次要终点（包括）：TT 正常化时间和 LH/FSH 变化。安全性通过不良事件和实验室监测进行评估。

结果和结论

在 2103 名筛查患者中，271 名被随机分组，81 名退出。各组的人口统计学特征相似。平均 BMI 为 38.1kg/m2，TT 为 7.97nmol/L。所有来曲唑治疗组在 24 周时均达到主要终点，呈剂量分层反应；平均 TT 分别为 15.89、17.78、20.35nmol/L，来曲唑 0.1mg、0.3mg 和 1.0mg 组，安慰剂组为 8.04nmol/L。与安慰剂组相比，LH/FSH 在来曲唑组显著增加。未观察到身体成分或性功能障碍的改善。来曲唑组精液量/总活动精子计数改善。与来曲唑治疗组相比，治疗出现的不良事件更为常见，包括红细胞压积升高、高血压、PSA 升高和头痛。来曲唑治疗（平均 -1.24%、-1.30%、-2.09%）和 0.1mg、0.3mg、1.0mg 组的腰椎骨密度分别观察到一些减少，安慰剂组为 0.66%。髋部无变化。这项来曲唑治疗 OHH 的 RCT 显示，肥胖男性的 TT 正常化。FSH/LH 和精液参数变化支持来曲唑可能保留/改善睾丸功能。