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在使用他达拉非进行药物治疗之前或之后,基线雌激素和睾酮水平是否会影响下尿路症状(LUTS)?

Do baseline estrogen and testosterone affect lower urinary tract symptoms (LUTS) prior to or after pharmacologic treatment with tadalafil?

作者信息

Egan K B, Miner M M, Suh M, McVary K, Ni X, Roehrborn C G, Wittert G, Wong D G, Rosen R C

机构信息

New England Research Institutes, Inc., Watertown, MA, USA.

Men's Health Center, The Miriam Hospital, Providence, RI, USA.

出版信息

Andrology. 2015 Nov;3(6):1165-72. doi: 10.1111/andr.12114. Epub 2015 Oct 9.

Abstract

Little is known about how total testosterone and estradiol-17β influence lower urinary tract symptoms (LUTS) in men with benign prostatic hypertrophy (BPH). We analyzed data from a subset of men aged ≥18 years randomized to tadalafil 5 mg once-daily or placebo who had ≥6 month history of LUTS and an International Prostate Symptom Score (IPSS)≥13 enrolled in one of three randomized, placebo-controlled tadalafil clinical trials (N = 958). Three specific aims were addressed, as follows: (i) To characterize enrolled men by treatment randomization and testosterone level; (ii) to assess cross-sectional associations of estradiol-17β, testosterone, and LUTS prior to treatment with tadalafil; and, (iii) to assess longitudinal associations between baseline estradiol-17β and testosterone and improvements or worsening of LUTS during a 12-week period of tadalafil or placebo administration. LUTS were assessed by total IPSS, IPSS voiding sub-score (IPSS-V) and IPSS storage sub-score (IPSS-S) for cross-sectional analyses, and change in total IPSS (ΔIPSS), ΔIPSS-V, and ΔIPSS-S between baseline and 12-week visit for longitudinal analyses. Correlation analyses and linear regression examined associations. Baseline testosterone was not significantly associated with IPSS. In contrast, estradiol-17β was inversely correlated with IPSS (r = -0.08; p < 0.05) and IPSS-S (r = -0.14; p < 0.05). Tadalafil treatment resulted in greater IPSS improvements in men with lower baseline estradiol-17β versus those with higher baseline estradiol-17β. Lower baseline estradiol-17β was significantly associated with modestly improved ΔIPSS-V (p = 0.04) and Δtotal IPSS (p = 0.05) but not with ΔIPSS-S, following treatment which may substantiate the role of bladder dysfunction because of nerve and smooth muscle changes in the bladder in addition to benign prostatic enlargement in LUTS. Circulating baseline testosterone did not predict ΔIPSS. Men with lower baseline estradiol-17β levels showed greater responsiveness to tadalafil 5 mg treatment than those with higher baseline estradiol-17β levels when responsiveness was measured using total IPSS and IPSS-V.

摘要

关于总睾酮和雌二醇 - 17β 如何影响良性前列腺增生(BPH)男性的下尿路症状(LUTS),目前所知甚少。我们分析了来自年龄≥18岁的男性亚组的数据,这些男性被随机分配至每日一次服用5毫克他达拉非或安慰剂组,他们有≥6个月的LUTS病史且国际前列腺症状评分(IPSS)≥13,这些数据来自三项随机、安慰剂对照的他达拉非临床试验之一(N = 958)。研究了三个具体目标,如下:(i)根据治疗随机分组和睾酮水平对入选男性进行特征描述;(ii)评估在服用他达拉非治疗前雌二醇 - 17β、睾酮与LUTS的横断面关联;以及,(iii)评估基线雌二醇 - 17β和睾酮与在12周他达拉非或安慰剂给药期间LUTS改善或恶化之间的纵向关联。横断面分析通过总IPSS、IPSS排尿子评分(IPSS - V)和IPSS储尿子评分(IPSS - S)评估LUTS,纵向分析通过基线和12周访视之间总IPSS(ΔIPSS)、ΔIPSS - V和ΔIPSS - S的变化来评估。相关性分析和线性回归用于检验关联。基线睾酮与IPSS无显著关联。相比之下,雌二醇 - 17β与IPSS(r = - 0.08;p < 0.05)和IPSS - S(r = - 0.14;p < 0.05)呈负相关。与基线雌二醇 - 17β较高的男性相比,他达拉非治疗使基线雌二醇 - 17β较低的男性IPSS改善更大。较低的基线雌二醇 - 17β与治疗后适度改善的ΔIPSS - V(p = 0.04)和Δ总IPSS(p = 0.05)显著相关,但与ΔIPSS - S无关,这可能证实了除良性前列腺增生外,膀胱神经和平滑肌变化导致的膀胱功能障碍在LUTS中的作用。循环基线睾酮不能预测ΔIPSS。当使用总IPSS和IPSS - V测量反应性时,基线雌二醇 - 17β水平较低的男性比基线雌二醇 - 17β水平较高的男性对5毫克他达拉非治疗反应更大。

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