矿质皮质激素受体和醛固酮：混合队列中 NR3C2 基因变异、性别和年龄之间的相互作用。

IF 5 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Journal of Clinical Endocrinology & Metabolism Pub Date : 2024-12-18 DOI:10.1210/clinem/dgae127

Mahyar Heydarpour, Wasita W Parksook, Luminita H Pojoga, Gordon H Williams, Jonathan S Williams

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引用次数: 0

摘要

背景：高血压是一种普遍存在的心血管风险，通常涉及醛固酮失调及其与矿质皮质激素受体（MR）的相互作用。在动物模型和人类队列中进行的实验设计证明了醛固酮分泌的性别和年龄依赖性，这拓展了我们对病理生理学的理解：本研究探讨了编码 MR 的 NR3C2 的遗传变异与醛固酮的关系，同时考虑了年龄、性别和种族因素：我们纳入了来自 HyperPATH 队列的 720 名白种人和 145 名非洲人，研究了单核苷酸风险等位基因变异 rs4835490 对醛固酮水平和血管的影响：值得注意的是，rs4835490 与欧洲血统个体在宽盐条件下的血浆醛固酮之间存在明显关联（P=0.0002）。风险等位基因 A 的等位基因携带者表现出血浆醛固酮水平升高（AA=8.1±0.9 vs GG=4.9±0.5 ng/dl）。此外，通过姿势激活醛固酮（P=0.025）和尿液排泄醛固酮（P=0.0122）也有显著关联。此外，还观察到遗传与种族、性别和年龄的相互作用。与 50 岁以上女性相比，50 岁以下白种女性的 AA 基因型血浆醛固酮、尿液醛固酮和体位醛固酮更高，这表明可能与更年期或雌激素的影响有关。结论：我们的研究强调了 NR3C2 基因变异及其与年龄、性别和种族在醛固酮激活中相互作用的重要性。研究结果表明，雌激素对 MR 激活有调节作用，尤其是在女性中，这强调了醛固酮失调在高血压发病中的作用。这一见解有助于我们理解高血压的复杂性，并为个性化干预开辟了道路。

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Mineralocorticoid Receptor and Aldosterone: Interaction Between NR3C2 Genetic Variants, Sex, and Age in a Mixed Cohort.

Context: Hypertension, a prevalent cardiovascular risk, often involves dysregulated aldosterone and its interaction with the mineralocorticoid receptor (MR). Experimental designs in animal models and human cohorts have demonstrated a sex and age dependency of aldosterone secretion that expands our pathophysiologic understanding.

Objective: This study explores the genetic variation of NR3C2, which encodes MR, in relation to aldosterone, considering age, sex, and race.

Methods: Incorporating 720 Caucasians and 145 Africans from the HyperPATH cohort, we investigated the impact of rs4835490, a single nucleotide risk allele variant, on aldosterone levels and vasculature.

Results: Notably, a significant association between rs4835490 and plasma aldosterone under liberal salt conditions emerged in individuals of European ancestry (P = .0002). Homozygous carriers of the risk A allele exhibited elevated plasma aldosterone levels (AA = 8.1 ± .9 vs GG = 4.9 ± .5 ng/dL). Additionally, aldosterone activation through posture (P = .025) and urinary excretion (P = .0122) showed notable associations. Moreover, genetic interactions with race, sex, and age were observed. Caucasian females under 50 years displayed higher plasma aldosterone, urine aldosterone, and posture aldosterone with the AA genotype compared to females over 50 years, suggesting a potential connection with menopausal or estrogen influences. Interestingly, such age-dependent interactions were absent in the African cohort.

Conclusion: Our study highlights the significance of the NR3C2 genetic variation and its interplay with age, sex, and race in aldosterone activation. The findings point toward an estrogen-modulating effect on MR activation, particularly in women, underlining the role of aldosterone dysregulation in hypertension development. This insight advances our comprehension of hypertension's complexities and opens avenues for personalized interventions. Clinical Trial Registration Number: NCT03029806 (registered January 24, 2017).

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来源期刊

Journal of Clinical Endocrinology & Metabolism 医学-内分泌学与代谢

CiteScore

11.40

自引率

5.20%

发文量

673

审稿时长

1 months

期刊介绍： The Journal of Clinical Endocrinology & Metabolism is the world"s leading peer-reviewed journal for endocrine clinical research and cutting edge clinical practice reviews. Each issue provides the latest in-depth coverage of new developments enhancing our understanding, diagnosis and treatment of endocrine and metabolic disorders. Regular features of special interest to endocrine consultants include clinical trials, clinical reviews, clinical practice guidelines, case seminars, and controversies in clinical endocrinology, as well as original reports of the most important advances in patient-oriented endocrine and metabolic research. According to the latest Thomson Reuters Journal Citation Report, JCE&M articles were cited 64,185 times in 2008.