Attenuation of Hypertension and protection of vascular inflammation in hyperaldosteronism: GPER1 as potential therapeutic candidate when MR antagonist is less satisfying?

IF 3.7 3区 医学 Q2 Medicine Endocrine Pub Date : 2024-11-20 DOI:10.1007/s12020-024-04106-6
Yulian Lai, Ziwei Tang, Zhipeng Du, Qinglian Zeng, Yu Xia, Shangbin Chen, Xun Li, Qingfeng Cheng, Mei Mei, Wenwen He
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Abstract

Background: Hyperaldosteronism is an endocrine disorder leading to persistent and severe hypertension. G protein-coupled estrogen receptor 1(GPER1) is regarded as a potential receptor of aldosterone (ALDO).

Objective: This study aimed to investigate the effects of GPER1 on aldosterone (ALDO)-induced hypertension and inflammation in mice.

Methods: GPER1-knockout (KO) and wild-type (WT) C57BL/6j mice were divided into control (CON, normal saline treatment), ALDO (subcutaneous injections of 600 g/kg/d ALDO), and ALDO + eplerenone (EPL) (subcutaneous injections of 600 g/kg/d ALDO and 100 mg/kg/d EPL) groups (n = 5 per group). Fourteen days after drug administration, the heart rate and tail blood pressure of the mice in the different groups were measured. S100A8 and IL-1β protein expression in arterial tissues were detected by western blotting, NLRP3 expression was assessed using immunofluorescence, and CD68 expression was investigated using immunohistochemistry.

Results: GPER1 deficiency alleviated ALDO-induced diastolic blood pressure (P< 0.05). In addition, the protein expression levels of IL-1β, S100A8, and CD68 showed significant decreases in the arterial tissues of GPER1-KO mice after combination treatment with ALDO and EPL (all P < 0.05).

Conclusion: We discovered attenuation of hypertension and vascular inflammation of GPER1 KO mice only on the basis of mineralocorticoid receptor (MR) blocking. Collectively, our study indicates that GPER1 might become a therapeutic target of hyperaldosteronism in controlling the residual risk of cardiovascular disease when MR antagonist alone is not satisfying.

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减轻高醛固酮症患者的高血压和保护血管炎症:当 MR 拮抗剂不那么令人满意时,GPER1 可作为潜在的候选治疗药物?
背景:高醛固酮症是一种导致持续性严重高血压的内分泌疾病。G蛋白偶联雌激素受体1(GPER1)被认为是醛固酮(ALDO)的潜在受体:本研究旨在探讨 GPER1 对醛固酮(ALDO)诱导的小鼠高血压和炎症的影响:方法:将 GPER1 基因敲除(KO)和野生型(WT)C57BL/6j 小鼠分为对照组(CON,正常生理盐水处理)、ALDO 组(皮下注射 600 g/kg/d ALDO)和 ALDO + 依普利酮(EPL)组(皮下注射 600 g/kg/d ALDO 和 100 mg/kg/d EPL)(每组 n = 5)。给药 14 天后,测量不同组小鼠的心率和尾部血压。用 Western 印迹法检测动脉组织中 S100A8 和 IL-1β 蛋白的表达,用免疫荧光法评估 NLRP3 的表达,用免疫组化法检测 CD68 的表达:结果:GPER1的缺乏减轻了ALDO诱导的舒张压(P< 0.05)。此外,联合使用 ALDO 和 EPL 治疗后,GPER1-KO 小鼠动脉组织中 IL-1β、S100A8 和 CD68 的蛋白表达水平显著下降(均为 P 结论:GPER1-KO 小鼠动脉组织中 IL-1β、S100A8 和 CD68 的蛋白表达水平显著下降:我们发现 GPER1-KO 小鼠的高血压和血管炎症仅在矿物质皮质激素受体(MR)阻断的基础上有所减轻。总之,我们的研究表明 GPER1 有可能成为高醛固酮血症的治疗靶点,在单用 MR 拮抗剂无法控制心血管疾病残余风险的情况下发挥作用。
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来源期刊
Endocrine
Endocrine 医学-内分泌学与代谢
CiteScore
6.40
自引率
5.40%
发文量
0
期刊介绍: Well-established as a major journal in today’s rapidly advancing experimental and clinical research areas, Endocrine publishes original articles devoted to basic (including molecular, cellular and physiological studies), translational and clinical research in all the different fields of endocrinology and metabolism. Articles will be accepted based on peer-reviews, priority, and editorial decision. Invited reviews, mini-reviews and viewpoints on relevant pathophysiological and clinical topics, as well as Editorials on articles appearing in the Journal, are published. Unsolicited Editorials will be evaluated by the editorial team. Outcomes of scientific meetings, as well as guidelines and position statements, may be submitted. The Journal also considers special feature articles in the field of endocrine genetics and epigenetics, as well as articles devoted to novel methods and techniques in endocrinology. Endocrine covers controversial, clinical endocrine issues. Meta-analyses on endocrine and metabolic topics are also accepted. Descriptions of single clinical cases and/or small patients studies are not published unless of exceptional interest. However, reports of novel imaging studies and endocrine side effects in single patients may be considered. Research letters and letters to the editor related or unrelated to recently published articles can be submitted. Endocrine covers leading topics in endocrinology such as neuroendocrinology, pituitary and hypothalamic peptides, thyroid physiological and clinical aspects, bone and mineral metabolism and osteoporosis, obesity, lipid and energy metabolism and food intake control, insulin, Type 1 and Type 2 diabetes, hormones of male and female reproduction, adrenal diseases pediatric and geriatric endocrinology, endocrine hypertension and endocrine oncology.
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