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经血清睾酮预测,接受皮下睾酮埋植治疗长达 21 年的低雄激素血症男性会发展为红细胞增多症。

Trough serum testosterone predicts the development of polycythemia in hypogonadal men treated for up to 21 years with subcutaneous testosterone pellets.

机构信息

Department of Andrology, Concord Hospital and ANZAC Research Institute, University of Sydney, Sydney, New South Wales 2139, Australia.

出版信息

Eur J Endocrinol. 2010 Feb;162(2):385-90. doi: 10.1530/EJE-09-0717. Epub 2009 Nov 10.

Abstract

OBJECTIVES

Testosterone formulations that have more steady-state pharmacokinetics, such as subcutaneously implanted testosterone pellets, may cause less erythrocytosis than i.m. injections of shorter acting androgen esters. We, therefore, sought to define the prevalence, predictors, and proximate basis (role of erythropoietin) for polycythemia (hematocrit >0.50) in hypogonadal men receiving testosterone implants long term.

DESIGN

A cross-sectional study was conducted in an academic andrology center with a longitudinal subgroup analysis.

PATIENTS

A total of 158 hypogonadal men aged 14-84 years (mean age 46.7 years) treated on average for 8 years (range 0-21 years).

MEASUREMENTS

Trough blood testosterone and hematocrit. Serial serum erythropoietin concentrations were measured in 16 volunteers.

RESULTS

Positive univariate associations between polycythemia (hematocrit >0.50) and log(testosterone) (odds ratio (OR) 24.7, 95% confidence interval (CI): 4.3, 141.2, P<0.01) and age (OR 1.1, 95% CI: 1.0, 1.1, P=0.03) and a borderline relationship with current smoking (OR 4.2, 95% CI: 0.9, 20.0, P=0.08) were unveiled. A sensitivity analysis using alternate definitions of polycythemia was performed to capture all potential covariants. Multivariate regression analysis incorporating all potential covariants disclosed the independent OR of developing polycythemia (after adjusting for smoking and age) for log(testosterone) to be 15.0 (95% CI: 2.5, 90.8). Duration of testosterone therapy did not alter the risk of polycythemia. A direct relationship between testosterone and erythropoietin was observed (P=0.05).

CONCLUSIONS

Higher trough serum testosterone concentrations but not duration of treatment predict the development of polycythemia in men receiving long-acting depot testosterone treatment.

摘要

目的

具有更稳定药代动力学的睾酮制剂,如皮下植入的睾酮丸,可能比作用时间较短的肌肉注射雄激素酯引起的红细胞增多症更少。因此,我们试图确定长期接受睾酮植入物治疗的性腺功能减退男性红细胞增多症(血细胞比容>0.50)的患病率、预测因素和近似基础(促红细胞生成素的作用)。

设计

在一个学术男科中心进行了横断面研究,并进行了纵向亚组分析。

患者

共 158 名年龄在 14-84 岁(平均年龄 46.7 岁)的性腺功能减退男性,平均治疗时间为 8 年(范围 0-21 年)。

测量

最低点血液睾酮和血细胞比容。在 16 名志愿者中测量了血清促红细胞生成素的浓度。

结果

红细胞增多症(血细胞比容>0.50)与对数睾酮(比值比(OR)24.7,95%置信区间(CI):4.3,141.2,P<0.01)和年龄(OR 1.1,95% CI:1.0,1.1,P=0.03)呈正相关,与当前吸烟呈临界关系(OR 4.2,95% CI:0.9,20.0,P=0.08)。为了捕获所有潜在的协变量,我们进行了一项使用替代红细胞增多症定义的敏感性分析。纳入所有潜在协变量的多元回归分析显示,调整吸烟和年龄因素后,对数睾酮(log(testosterone))发生红细胞增多症的独立比值比(OR)为 15.0(95%CI:2.5,90.8)。睾酮治疗的持续时间并未改变红细胞增多症的风险。观察到睾酮与促红细胞生成素之间存在直接关系(P=0.05)。

结论

在接受长效睾酮 depot 治疗的男性中,较高的血清睾酮浓度(而非治疗持续时间)预测红细胞增多症的发生。

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