Mineralocorticoid Receptor and Aldosterone-Related Biomarkers of End-Organ Damage in Cardiometabolic Disease

Gorini, Stefania; Marzolla, Vincenzo; Mammi, Caterina; Armani, Andrea M.; Caprio, Massimiliano

doi:10.3390/biom8030096

Cited by 25 publications

(20 citation statements)

References 169 publications

(209 reference statements)

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“…NK1R antagonists like aprepitant may thus represent a valuable therapeutic option to reduce obesity-and SAS-associated hyperaldosteronism, manage low renin hypertension and limit aldosterone breakthrough. In fact, it is now well demonstrated that aldosterone exerts profibrotic and inflammation actions in the cardiovascular system and kidney, and counteracting its effects has proved its efficacy to reduce the progression of heart failure and chronic nephropathy 36,37 . Especially, NK1R antagonists may constitute an alternative to both mineralocorticoid receptor antagonists whose utilisation is hampered by their antiandrogenic properties 38,39 , and aldosterone synthase inhibitors whose administration leads to accumulation of steroid precursors with mineralocorticoid activity 40 , a phenomenon which may reduce their clinical benefits.…”

Section: Discussionmentioning

confidence: 99%

The neuropeptide substance P regulates aldosterone secretion in human adrenals

et al. 2020

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Aldosterone, produced by the adrenals and under the control of plasma angiotensin and potassium levels, regulates hydromineral homeostasis and blood pressure. Here we report that the neuropeptide substance P (SP) released by intraadrenal nerve fibres, stimulates aldosterone secretion via binding to neurokinin type 1 receptors (NK1R) expressed by aldosterone-producing adrenocortical cells. The action of SP is mediated by the extracellular signal-regulated kinase pathway and involves upregulation of steroidogenic enzymes. We also conducted a prospective proof-of-concept, double blind, placebo-controlled clinical trial aimed to investigate the impact of the NK1R antagonist aprepitant on aldosterone secretion in healthy male volunteers (EudraCT: 2008-003367-40, ClinicalTrial.gov: NCT00977223). Participants received during two 7-day treatment periods aprepitant (125 mg on the 1 st day and 80 mg during the following days) or placebo in a random order at a 2-week interval. The primary endpoint was plasma aldosterone levels during posture test. Secondary endpoints included basal aldosterone alterations, plasma aldosterone variation during metoclopramide and hypoglycaemia tests, and basal and stimulated alterations of renin, cortisol and ACTH during the three different stimulatory tests. The safety of the treatment was assessed on the basis of serum transaminase measurements on days 4 and 7. All pre-specified endpoints were achieved. Aprepitant decreases aldosterone production by around 30% but does not influence the aldosterone response to upright posture. These results indicate that the autonomic nervous system exerts a direct stimulatory tone on mineralocorticoid synthesis through SP, and thus plays a role in the maintenance of hydromineral homeostasis. This regulatory mechanism may be involved in aldosterone excess syndromes.

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Section: Discussionmentioning

confidence: 99%

The neuropeptide substance P regulates aldosterone secretion in human adrenals

et al. 2020

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“…The RAAS plays a very important role in regulating cardiovascular function, but it may also lead to the occurrence and development of various cardiovascular diseases, including cardiac hypertrophy and heart failure [33,34]. More and more evidence has shown that ALDO plays an important role in the pathological development of cardiovascular disease [33][34][35]. Calvier et al [36] proved that in PAH, ALDO was considered to be a potential tandem biomarker.…”

Section: Discussionmentioning

confidence: 99%

Aldosterone Contributed to Pulmonary Arterial Hypertension Development via Stimulating Aquaporin Expression and Pulmonary Arterial Smooth Muscle Cells Proliferation

Wang

Zhong

et al. 2020

Pharmacology

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Introduction and Objective: The regulatory network of aquaporin (AQP) 1 and renin-angiotensin-aldosterone (ALDO) system are not quite clear in pulmonary arterial hypertension (PAH). Thus, we explored the role of AQP1, ALDO and spirolactone (SP) in the PAH animal model and pulmonary arterial smooth muscle cells (PASMCs). Method: PAH rat model was established by monocrotaline (MCT) via intraperitoneal in SD rat. Hemodynamic measurement was conducted via the external jugular vein cannula. PASMCs were extracted from normal SD rat and cultured in SmGM medium. α-Actin expression was identified by immunocytochemistry. Protein levels were assessed by Western blot. Cell viability was assayed using the MTT method. Apoptosis rate was evaluated by flow cytometry. ALDO level was measured by ELISA. Result: SP decreased AQP1 and β-catenin expressions in PAH rat model induced successfully by MCT. Moreover, ALDO increased AQP1 expression and cell viability in PASMCs, which were extracted from rat and identified by α-actin expression. AQP1 downregulation decreased β-catenin expression, and SP lowered AQP1 and β-catenin expressions elevated by ALDO in PASMCs. SP offset ALDO's effect on the upregulation of cell viability as well as AQP1 and β-catenin expressions in PASMCs. In addition, AQP1 downregulation and SP have a negative effect on Ki-67 and proliferating cell nuclear antigen expressions as well as cell viability after ALDO treatment in PASMCs. Conclusion: ALDO might contribute to PAH development via stimulating AQP1 expression and PASMCs proliferation. However, SP could be considered an effective drug regulating PASMCs proliferation through modulating AQP1 and β-catenin expressions in PAH.

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“…В последние годы получены неоспоримые доказательства, что спектр действия альдостерона лежит далеко за пределами узкого перечня «почечных» эффектов. Системная или локальная гиперпродукция гормона вызывает целый ряд патологических реакций [19][20][21][22][23][24]…”

Section: обмен и роль альдостерона в организмеunclassified

The role of aldosterone in the development of atrial fibrillation: modern understanding of problem

Ватутин

Шевелёк

Кравченко³

2019

Arhivʺ vnutrennej mediciny

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В обзоре литературы изложены современные представления о роли альдостерона в развитии и поддержании фибрилляции предсердий. Показано, что гормон принимает участие во всех этапах электрофизиологического и структурного ремоделирования предсердий, способствуя формированию субстрата аритмии. Отмечено, что неблагоприятные эффекты гормона в миокарде реализуются не только за счет его системной гиперпродукции, но и ввиду непосредственного синтеза гормона в тканях предсердий. Немаловажную роль в развитии фибрилляции предсердий играет повышенная экспрессия минералокортикоидных рецепторов кардиомиоцитов. Продемонстрировано, что гиперальдостеронемия может являться не только причиной, но и следствием фибрилляции предсердий. Эпизод аритмии характеризуется выраженной нейрогормональной активацией, сопровождающейся повышением интрамиокардиального синтеза альдостерона и экспрессии рецепторов к нему. Это способствует дальнейшему прогрессированию ремоделирования предсердий, создавая условия для рецидивирования аритмии и замыкая тем самым порочный круг.

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Mineralocorticoid Receptor and Aldosterone-Related Biomarkers of End-Organ Damage in Cardiometabolic Disease

Cited by 25 publications

References 169 publications

The neuropeptide substance P regulates aldosterone secretion in human adrenals

The neuropeptide substance P regulates aldosterone secretion in human adrenals

Aldosterone Contributed to Pulmonary Arterial Hypertension Development via Stimulating Aquaporin Expression and Pulmonary Arterial Smooth Muscle Cells Proliferation

The role of aldosterone in the development of atrial fibrillation: modern understanding of problem

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