Haddad Rudy M, Kennedy Cassie C, Caples Sean M, Tracz Michal J, Boloña Enrique R, Sideras Kostandinos, Uraga Maria V, Erwin Patricia J, Montori Victor M
Knowledge and Encounter Research Unit, Mayo Clinic College of Medicine, Rochester, Minn 55905, USA.
Mayo Clin Proc. 2007 Jan;82(1):29-39. doi: 10.4065/82.1.29.
To conduct a systematic review and meta-analysis of randomized trials that assessed the effect of testosterone use on cardiovascular events and risk factors in men with different degrees of androgen deficiency.
Librarian-designed search strategies were used to search the MEDLINE (1966 to October 2004), EMBASE (1988 to October 2004), and Cochrane CENTRAL (inception to October 2004) databases. The database search was performed again in March 2005. We also reviewed reference lists from included studies and content expert files. Eligible studies were randomized trials that compared any formulation of commercially available testosterone with placebo and that assessed cardiovascular risk factors (lipid fractions, blood pressure, blood glucose), cardiovascular events (cardiovascular death, nonfatal myocardial infarction, angina or claudication, revascularization, stroke), and cardiovascular surrogate end points (ie, laboratory tests indicative of cardiac or vascular disease). Using a standardized data extraction form, we collected data on participants, testosterone administration, and outcome measures. We assessed study quality with attention to allocation concealment, blinding, and loss to follow-up.
The 30 trials included 1642 men, 808 of whom were treated with testosterone. Overall, the trials had limited reporting of methodological features that prevent biased results (only 6 trials reported allocation concealment), enrolled few patients, and were of brief duration (only 4 trials followed up patients for > 1 year). The median loss to follow-up across all 30 trials was 9%. Testosterone use in men with low testosterone levels led to inconsequential changes in blood pressure and glycemia and in all lipid fractions (total cholesterol: odds ratio [OR], -0.22; 95% confidence interval [CI], -0.71 to 0.27; high-density lipoprotein cholesterol: OR, -0.04; 95% CI, -0.39 to 0.30; low-density lipoprotein cholesterol: OR, 0.06; 95% CI, -0.30 to 0.42; and triglycerides: OR, -0.27; 95% CI, -0.61 to 0.08); results were similar in patients with low-normal to normal testosterone levels. The OR between testosterone use and any cardiovascular event pooled across trials that reported these events (n = 6) was 1.82 (95% CI, 0.78 to 4.23). Several trials failed to report data on measured outcomes. For reasons we could not explain statistically, the results were inconsistent across trials.
Currently available evidence weakly supports the inference that testosterone use in men is not associated with important cardiovascular effects. Patients and clinicians need large randomized trials of men at risk for cardiovascular disease to better inform the safety of long-term testosterone use.
对评估睾酮治疗对不同程度雄激素缺乏男性心血管事件及危险因素影响的随机试验进行系统评价和荟萃分析。
采用图书馆员设计的检索策略,检索MEDLINE(1966年至2004年10月)、EMBASE(1988年至2004年10月)和Cochrane CENTRAL(创刊至2004年10月)数据库。2005年3月再次进行数据库检索。我们还查阅了纳入研究的参考文献列表和内容专家档案。符合条件的研究为随机试验,比较了任何市售睾酮制剂与安慰剂,并评估了心血管危险因素(血脂成分、血压、血糖)、心血管事件(心血管死亡、非致死性心肌梗死、心绞痛或间歇性跛行、血运重建、中风)以及心血管替代终点(即指示心脏或血管疾病的实验室检查)。使用标准化的数据提取表格,我们收集了关于参与者、睾酮给药和结局指标的数据。我们评估研究质量时关注分配隐藏、盲法和失访情况。
30项试验纳入了1642名男性,其中808名接受了睾酮治疗。总体而言,这些试验在防止偏倚结果的方法学特征方面报告有限(仅6项试验报告了分配隐藏),纳入患者较少,且持续时间较短(仅4项试验对患者随访超过1年)。所有30项试验的中位失访率为9%。睾酮水平低的男性使用睾酮导致血压、血糖和所有血脂成分的变化不显著(总胆固醇:比值比[OR],-0.22;95%置信区间[CI],-0.71至0.27;高密度脂蛋白胆固醇:OR,-0.04;95%CI,-0.39至0.30;低密度脂蛋白胆固醇:OR,0.06;95%CI,-0.30至0.42;甘油三酯:OR,-0.27;95%CI,-0.61至0.08);睾酮水平低至正常的患者结果相似。在报告了这些事件的试验(n = 6)中,汇总的睾酮使用与任何心血管事件之间的OR为1.82(95%CI,0.78至4.23)。几项试验未报告测量结局的数据。由于我们无法从统计学上解释的原因,各试验结果不一致。
现有证据微弱支持男性使用睾酮与重要心血管影响无关的推断。患者和临床医生需要对有心血管疾病风险的男性进行大型随机试验,以更好地了解长期使用睾酮的安全性。
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