Department of Public Health, Section of Epidemiology, University of Copenhagen, Copenhagen, Denmark.
Faculty of Science, Research Unit of Mathematical Sciences, University of Oulu, Oulu, Finland.
BMC Med. 2023 Apr 26;21(1):158. doi: 10.1186/s12916-023-02867-x.
C-type natriuretic peptide (CNP) is a known target for promoting growth and has been implicated as a therapeutic opportunity for the prevention and treatment of cardiovascular disease (CVD). This study aimed to explore the effect of CNP on CVD risk using the Mendelian randomization (MR) framework.
Instrumental variables mimicking the effects of pharmacological intervention on CNP were identified as uncorrelated genetic variants located in the genes coding for its primary receptors, natriuretic peptide receptors-2 and 3 (NPR2 and NPR3), that associated with height. We performed MR and colocalization analyses to investigate the effects of NPR2 signalling and NPR3 function on CVD outcomes and risk factors. MR estimates were compared to those obtained when considering height variants from throughout the genome.
Genetically-proxied reduced NPR3 function was associated with a lower risk of CVD, with odds ratio (OR) 0.74 per standard deviation (SD) higher NPR3-predicted height, and 95% confidence interval (95% CI) 0.64-0.86. This effect was greater in magnitude than observed when considering height variants from throughout the genome. For CVD subtypes, similar MR associations for NPR3-predicted height were observed when considering the outcomes of coronary artery disease (0.75, 95% CI 0.60-0.92), stroke (0.69, 95% CI 0.50-0.95) and heart failure (0.77, 95% CI 0.58-1.02). Consideration of CVD risk factors identified systolic blood pressure (SBP) as a potential mediator of the NPR3-related CVD risk lowering. For stroke, we found that the MR estimate for NPR3 was greater in magnitude than could be explained by a genetically predicted SBP effect alone. Colocalization results largely supported the MR findings, with no evidence of results being driven by effects due to variants in linkage disequilibrium. There was no MR evidence supporting effects of NPR2 on CVD risk, although this null finding could be attributable to fewer genetic variants being identified to instrument this target.
This genetic analysis supports the cardioprotective effects of pharmacologically inhibiting NPR3 receptor function, which is only partly mediated by an effect on blood pressure. There was unlikely sufficient statistical power to investigate the cardioprotective effects of NPR2 signalling.
C 型利钠肽(CNP)是一种已知的促进生长的靶点,被认为是预防和治疗心血管疾病(CVD)的治疗机会。本研究旨在使用孟德尔随机化(MR)框架探讨 CNP 对 CVD 风险的影响。
模拟 CNP 药理学干预效果的工具变量被鉴定为位于编码其主要受体,即利钠肽受体 2 和 3(NPR2 和 NPR3)的基因中的无关遗传变异体,这些变异体与身高相关。我们进行了 MR 和共定位分析,以研究 NPR2 信号传导和 NPR3 功能对 CVD 结局和危险因素的影响。MR 估计值与考虑整个基因组中身高变异体时获得的估计值进行了比较。
遗传上介导的 NPR3 功能降低与 CVD 风险降低相关,NPR3 预测身高每增加一个标准差(SD),比值比(OR)为 0.74,95%置信区间(95%CI)为 0.64-0.86。这种效应的幅度大于考虑整个基因组中身高变异体时观察到的效应。对于 CVD 亚型,当考虑冠心病(0.75,95%CI 0.60-0.92)、中风(0.69,95%CI 0.50-0.95)和心力衰竭(0.77,95%CI 0.58-1.02)的结局时,观察到 NPR3 预测身高的类似 MR 关联。考虑 CVD 危险因素时,发现收缩压(SBP)可能是 NPR3 相关 CVD 风险降低的潜在中介物。对于中风,我们发现 NPR3 的 MR 估计值大于仅由 SBP 效应遗传预测所能解释的幅度。共定位结果在很大程度上支持了 MR 研究结果,没有证据表明结果是由于与连锁不平衡相关的变异引起的。没有 MR 证据支持 NPR2 对 CVD 风险的影响,尽管这一无效发现可能归因于鉴定出的用于干预该靶点的遗传变异体较少。
这项遗传分析支持药理学抑制 NPR3 受体功能的心脏保护作用,这种作用部分是通过对血压的影响介导的。可能没有足够的统计能力来研究 NPR2 信号的心脏保护作用。
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