遗传预测的雄激素特征与不良心脏标志物:一项性别特异性孟德尔随机化研究。
Genetically predicted androgenic profiles and adverse cardiac markers: a sex-specific Mendelian randomization study.
机构信息
National Heart and Lung Institute, Imperial College London, London, UK.
British Heart Foundation Cardiovascular Epidemiology Unit, Department of Public Health and Primary Care, University of Cambridge, Cambridge, UK.
出版信息
ESC Heart Fail. 2023 Dec;10(6):3525-3537. doi: 10.1002/ehf2.14527. Epub 2023 Sep 22.
AIMS
Observational evidence suggests associations between sex hormone levels and heart failure (HF). We used sex-specific genetic variants associated with androgenic sex hormone profiles to investigate the causal relevance of androgenic sex hormone profiles on cardiac structure and function and HF using Mendelian randomization (MR).
METHODS AND RESULTS
Sex-specific uncorrelated genome-wide significant (P < 5 × 10 ) variants predicting sex hormone-binding globulin (SHBG), total testosterone, and bioavailable testosterone were extracted from summary statistics of genome-wide association study (GWAS) on 425 097 participants in the UK Biobank. Sex-specific gene-outcome association estimates were computed for left ventricular ejection fraction (LVEF), left ventricular end-diastolic and end-systolic volumes (LVEDV and LVESV, respectively), left ventricular stroke volume (LVSV), cardiac index, and cardiac output in 11 528 female and 14 356 male UK Biobank Imaging Study participants and for incident or prevalent HF in an external cohort of 47 309 cases and 930 014 controls. Inverse-variance weighted MR was the primary analysis method. In females, higher genetically predicted bioavailable testosterone was associated with lower LVEDV [β per nmol/L = -0.11 (-0.19 to -0.03), P = 0.006], lower LVESV [β = -0.09 (-0.17 to -0.01), P = 0.022], lower LVSV [β = -0.11 (-0.18 to -0.03), P = 0.005], lower cardiac output [β = -0.08 (-0.16 to 0.00), P = 0.046], and lower cardiac index [β = -0.08 (-0.16 to -0.01), P = 0.034] and a higher risk of HF [odds ratio 1.10 (1.01-1.19), P = 0.026] on external validation analysis in larger scale, sex-adjusted GWAS data. Higher genetically predicted SHBG was associated with higher LVEDV [β per nmol/L = 0.17 (0.08-0.25), P = 2 × 10 ], higher LVESV [β = 0.13 (0.05-0.22), P = 0.003], and higher LVSV [β = 0.18 (0.08-0.28), P = 2 × 10 ]. In males, higher genetically predicted total and bioavailable testosterone was associated with lower LVESV [β = -0.07 (-0.12 to -0.02), P = 0.007] and LVEF [β = -0.11 (-0.18 to -0.04), P = 0.003], respectively.
CONCLUSIONS
This study supports a causal effect of pro-androgenic sex hormone profiles in females on adverse markers of left ventricular structure and function typically associated with HF with preserved ejection fraction and with HF. There was weaker evidence of association in males.
目的
观察性证据表明,性激素水平与心力衰竭(HF)之间存在关联。我们使用与雄激素性激素谱相关的特定性别的遗传变异,通过孟德尔随机化(MR)研究雄激素性激素谱对心脏结构和功能以及 HF 的因果相关性。
方法和结果
从英国生物库中 425097 名参与者的全基因组关联研究(GWAS)汇总统计数据中提取了与性激素结合球蛋白(SHBG)、总睾酮和生物可利用睾酮相关的特定性别的无相关性的全基因组显著(P<5×10)变异。对于 11528 名女性和 14356 名男性英国生物库成像研究参与者的左心室射血分数(LVEF)、左心室舒张末期和收缩末期容积(LVEDV 和 LVESV,分别)、左心室每搏量(LVSV)、心指数和心输出量,以及在外部队列的 47309 例病例和 930014 例对照中进行了与 HF 事件或 HF 发生相关的特定性别的基因-结果关联估计。逆方差加权 MR 是主要分析方法。在女性中,较高的遗传预测生物可利用睾酮与较低的 LVEDV[每 nmol/L 的β值=-0.11(-0.19 至-0.03),P=0.006]、较低的 LVESV[β值=-0.09(-0.17 至-0.01),P=0.022]、较低的 LVSV[β值=-0.11(-0.18 至-0.03),P=0.005]、较低的心输出量[β值=-0.08(-0.16 至 0.00),P=0.046]和较低的心指数[β值=-0.08(-0.16 至-0.01),P=0.034]和 HF 的风险增加[比值比 1.10(1.01-1.19),P=0.026]相关,在更大规模、性别调整的 GWAS 数据的外部验证分析中具有更高的相关性。较高的遗传预测 SHBG 与较高的 LVEDV[每 nmol/L 的β值=0.17(0.08-0.25),P=2×10]、较高的 LVESV[β值=0.13(0.05-0.22),P=0.003]和较高的 LVSV[β值=0.18(0.08-0.28),P=2×10]相关。在男性中,较高的遗传预测总睾酮和生物可利用睾酮与较低的 LVESV[β值=-0.07(-0.12 至-0.02),P=0.007]和 LVEF[β值=-0.11(-0.18 至-0.04),P=0.003]相关。
结论
本研究支持了女性雄激素性激素谱对射血分数保留性心力衰竭和心力衰竭的左心室结构和功能不良标志物的因果效应。在男性中,相关性的证据较弱。
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