Specific activation of the alternative cardiac promoter of Cacna1c by the mineralocorticoid receptor / Activation spécifique du promoteur cardiaque alternatif du Cacna1c par le récepteur aux minéralocorticoïdes

Ribeiro mesquita, Thássio Ricardo

13 December 2017

Les antagonistes des récepteurs aux minéralocorticoïdes (MR) appartiennent à l'arsenal thérapeutique pour le traitement de diverses maladies cardiovasculaires, mais les mécanismes conférant leurs effets bénéfiques sont encore mal compris. Une partie de ces effets peuvent être liée à la régulation de l'expression du canal Ca2+ de type L Cav1.2, largement impliqué dans l'insuffisance cardiaque et l'hypertension. Nous montrons que MR fonctionne comme un facteur de transcription transformant le signal de l'aldostérone dans l'utilisation du 'cardiaque' promoteur alternatif P1, dirigeant l'expression du long N-terminal transcrit (Cav1.2-LNT. L'aldostérone augmente de façon concentration- et de temps dépendente l'expression de Cav1.2-LNT dans les cardiomyocytes en raison de l'activation du promoteur P1, par interactions des MR avec des séquences spécifiques de l'ADN sur le promoter P1. Ce mécanisme de cis-régulation induit l'activation de promoteur P1 dans les cellules vasculaires conduisant à une nouvelle signature moléculaire de Cav1.2-LNT associé à une sensibilité réduite aux bloqueurs des canaux Ca2+. Ces résultats révèlent Cav1.2-LNT comme une cible minéralocorticoïde spécifique qui pourrait influencer sur l'éfficacité thérapeutique dans les maladies cardiovasculaires. / The mineralocorticoid receptor (MR) antagonists belong to the current therapeutic armamentarium for the management of cardiovascular diseases, but the mechanisms conferring their beneficial effects are still poorly understood. Part of these MR effects might be related to the L-type Cav1.2 Ca2+ channel expression regulation, critically involved in heart failure and hypertension. Here, we show that MR acts as a transcription factor triggering aldosterone signal into specific alternative 'cardiac' P1-promoter usage, given rise to long (Cav1.2-LNT) N-terminal transcripts. Aldosterone increases Cav1.2-LNT expression in cardiomyocytes in a time- and dose-dependent manner due to MR-dependent P1-promoter activity, through specific DNA sequence-MR interactions. This cis-regulatory mechanism induced a MR-dependent P1-promoter switch in vascular cells leading to a new Cav1.2-LNT molecular signature with reduced Ca2+ channel blocker sensitivity. These findings uncover Cav1.2-LNT as a specific mineralocorticoid target that might influence the therapeutic outcome of cardiovascular diseases.

Canaux Ca2+ de type L

Aldostérone

Récepteur aux minéralocorticoïde

Cœur

Muscle lisse vasculaire

L-Type Ca2+ channel

Aldosterone

Mineralocorticoid receptor

Heart

Vascular smooth muscle cells

Bloqueio do receptor mineralocorticoide em hipertensos com síndrome metabólica: estudo da vasodilatação fluxo-mediada

Lovisi, Julio Cesar Moraes

09 September 2013

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No. of bitstreams: 1 juliocesarmoraeslovisi.pdf: 3660990 bytes, checksum: 9bfd65df440e1a934d906a3918e427d5 (MD5) Previous issue date: 2013-09-09 / INTRODUÇÃO: A epidemia de obesidade e de síndrome metabólica (SM) observada nos últimos anos se associa a uma série de agravos clínicos como neoplasias, diabetes mellitus e doenças cardiovasculares, notadamente a hipertensão arterial (HA). Diversos mecanismos etiopatogênicos têm sido descritos na HA associada à SM entre os quais citam-se a participação da aldosterona (ALDO) e da disfunção endotelial. OBJETIVOS: avaliar os efeitos do bloqueio do receptor mineralocorticoide (RMC) na função endotelial, na pressão arterial (PA) e em parâmetros inflamatórios e renais de indivíduos com SM. PACIENTES E MÉTODOS: Foram selecionados 42 pacientes elegíveis para o protocolo. Todos os voluntários foram submetidos a exame clínico, avaliação laboratorial com dosagens de mediadores inflamatórios e de excreção urinária de albumina, além de avaliação cardiológica, com monitorização ambulatorial da pressão arterial (MAPA), ecocardiograma e estudo da vasodilatação fluxo-mediada (VDFM), antes e após o tratamento. Destes, 28 indivíduos foram tratados com espironolactona (ESPIRO) na dose de 25-50 mg/dia e 14 com amlodipina (AMLO) na dose 5-10 mg/dia por 16 semanas (Resultados 1). Após essa avaliação, com objetivo de homogeneizar os grupos para melhor comparação dos parâmetros de VDFM, inflamatórios e renais, foram selecionados 27 indivíduos alocados em dois grupos por meio da aplicação da técnica do Propensity Score (PS). Deste modo foram constituídos dois grupos homogêneos, a saber: 16 pacientes em um grupo tratado com ESPIRO e 11 no grupo controle, tratados com AMLO, por um período de 16 semanas (Resultados 2). Resultados 1: Os dados iniciais mostraram que o tratamento da HA com ESPIRO e com AMLO resultou em redução significante da PA em ambos os grupos. No grupo ESPIRO foi observado aumento da VDFM, enquanto no grupo AMLO houve redução significativa desse parâmetro. Observamos ainda redução significativa da microalbuminúria e de mediadores inflamatórios no grupo ESPIRO, o que não ocorreu no grupo AMLO. Finalmente, observou- se aumento significativo do colesterol HDL no grupo ESPIRO o que não foi observado no grupo AMLO. Resultados 2: com a aplicação do PS e consequente maior homogeneidade entre os grupos houve a confirmação desses achados nos 2 grupos (ESPIRO e AMLO) e, adicionalmente, permitiu a subdivisão destes em inflamados (PCR>3,0 mg/dL) e não inflamados (PCR < 3,0 mg/dL). Quando se avaliaram a VDFM, o comportamento pressórico e de parâmetros metabólicos e renais observou-se aumento da VDFM, maior redução da PA, aumento do colesterol HDL e redução da albuminúria que foram significativas no grupo ESPIRO, notadamente no subgrupo não inflamado em comparação ao grupo inflamado. CONCLUSÃO: O bloqueio dos RMC em hipertensos com SM melhorou a função endotelial e reduziu a pressão arterial, com impacto favorável sobre marcadores metabólicos, inflamatórios e na excreção urinária de albumina. Estes achados apontam para efeitos benéficos adicionais à redução pressórica em pacientes portadores de SM tratados com bloqueadores dos RMC. / INTRODUCTION: The epidemic of obesity and metabolic syndrome (MS) described in recent years is associated with a series of clinical conditions such as malignancy, diabetes mellitus, and cardiovascular diseases, chiefly systemic arterial hypertension (AH). There are several mechanisms proposed to explain the development of MS-associated AH, among which the role of aldosterone and endothelial dysfunction are noteworthy. OBJECTIVES: assess the effects of mineralocorticoid receptor blockade (MRB) on endothelial function, blood pressure (BP) and inflammatory and renal parameters of individuals with the MS. PATIENTS AND METHODS: Forty-two eligible patients were selected. All volunteers underwent clinical examination, laboratory determination of inflammatory mediators and urinary albumin excretion, and cardiologic examination with 24-hour ambulatory blood pressure (24-h ABPM), echocardiography and assessment of the flow-mediated vasodilation (FMD) at baseline and after treatment. Twenty-eight individuals received spironolactone (SPIRO), 25-50mg/day, and 14 individuals received amlodipine (AMLO), 5-10mg/day, for 16 weeks (Results 1). In order to homogenize the groups and better compare the FMD and the inflammatory and renal parameters, 27 individuals were selected and allocated to two groups according to the propensity score (PS) technique: 16 individuals treated with SPIRO and 11 controls, treated with AMLO, for 16 weeks (Results 2). Results 1: Both SPIRO-treated and AMLO-treated groups had significant BP reductions. While the SPIRO-treated group had increased FMD, the AMLO-treated group had a significant reduction of this parameter. There was also a significant reduction of microalbuminuria and inflammatory mediators in the SPIRO-treated group, but not in the AMLO one. There was a significant increase of HDL-cholesterol in the SPIRO group, but not in the AMLO one. Results 2: With the PS technique, and consequent better homogenization of the groups, we confirmed these findings in the two groups (SPIRO and AMLO) and further subdivided them into those with inflammation (CRP>3.0mg/dl) and those without inflammation (CRP<3.0mg/dl). There were significantly increased FMV, greater BP reduction, increased HDL-cholesterol, and significant reduction of albuminuria in the SPIRO group, notably in the subgroup without inflammation, as compared with that with inflammation. CONCLUSION: MRB in hypertensive subjects with the MS improved endothelial function and reduced blood pressure, with a favorable impact on metabolic and inflammatory markers and on the urinary albumin excretion. These findings point to MRB as a new option for treatment of AH in individuals with the MS.

CNPQ::CIENCIAS DA SAUDE::MEDICINA

Síndrome X metabólica

Endotélio vascular

Hipertensão

Aldosterona

Sistema renina-angiotensina

Metabolic Syndrome X

Vascular endothelium

Hypertension

Aldosterone

Mineralocorticoid receptor antagonists

Renin-angiotensin system

L’impact de l’inhibition de l’aldostérone sur l’homéostasie du glucose et le risque de diabète chez les patients atteints d’insuffisance cardiaque

Korol, Sandra

12 1900

Le système rénine-angiotensine-aldostérone est impliqué dans la physiopathologie de l’insuffisance cardiaque (IC). L’inhibition de l’aldostérone par les antagonistes du récepteur aux minéralocorticoïdes (ARM), la spironolactone et l’éplérénone, est associée à une réduction de morbidité et mortalité. Or, la spironolactone est un antagoniste non sélectif, avec des effets hors-cibles sur d’autres récepteurs stéroïdiens. Des données suggèrent qu’elle pourrait avoir un effet défavorable sur l’homéostasie du glucose, avec une augmentation en hémoglobine glyquée (HbA1c), un marqueur de contrôle du glucose à long terme. Au contraire, l’éplérénone semble exercer un effet neutre. Les objectifs de cette thèse de doctorat sont les suivants : 1) Assembler toutes les connaissances dans la littérature au sujet de l’effet glycémique des ARM; 2) Évaluer le risque de développement de diabète avec la spironolactone chez les patients IC; 3) Analyser si la spironolactone peut moduler l’effet glycémique d’autres médicaments utilisés en IC; 4) Comparer la spironolactone à l’éplérénone sur des marqueurs de glucose chez les patients IC avec dérèglements glycémiques. Quatre projets ont été effectués afin de répondre à ces questions. Premièrement, une revue systématique a permis d’identifier toutes les études publiées contenant de l’information sur l’effet glycémique des ARM. Les résultats étaient hétérogènes, mais ont suggéré que l’effet est dépendant de la pathologie et serait potentiellement néfaste dans les maladies à haut risque d’évènements cardiovasculaires. Une méta-analyse d’études en diabète indique que l’effet à long terme serait non significatif. Le deuxième projet utilise une cohorte de patients IC de bases de données administratives entre 1995 et 2009 (suivi jusqu’en 2010). Nous n’avons pas détecté d’association significative entre l’utilisation de la spironolactone et le risque de diabète. Par contre, l’étude a démontré qu’un âge plus jeune, la digoxine, et les corticostéroïdes augmentent le risque de diabète. Le troisième projet est une sous-étude d’une étude clinique CANDIID-II (Effect of ACE inhibitor alone versus ACE inhibitor plus high dose candesartan on BNP, immune markers, inflammatory status, and urinary kinins in patients with symptomatic left ventricular systolic dysfunction) chez des patients IC traités avec un inhibiteur de l’enzyme de conversion à l’angiotensine et le candésartan, antagoniste du récepteur à l’angiotensine II. Ces classes pharmacologiques ont des effets bénéfiques sur la glycémie. En comparant les patients traités aussi avec la spironolactone versus les patients sans ARM, nous n’avons pas trouvé que la spironolactone module l’effet bénéfique du candésartan sur le métabolisme du glucose. Le dernier projet consiste d’une étude prospective, multicentrique, randomisée, contrôlée à double-insu : SNOW (A comparison of the effects of selective and non selective mineralocorticoid antagonism on glucose homeostasis and lipid profile of heart failure patients with glucose intolerance or type 2 diabetes). Elle compare, pendant 16 semaines, la spironolactone à l’éplérénone sur des marqueurs glycémiques, notamment, l’HbA1c, chez 62 patients IC avec diabète de type II ou intolérance au glucose. Aucune différence significative n’a été observée entre les groupes. En résumé, les résultats de cette thèse indiquent que les ARM ne présentent pas de risque de détérioration du contrôle du glucose sur une durée modérée à longue en IC. / The renin-angiotensin-aldosterone system is involved in the pathophysiology of heart failure (HF). The inhibition of aldosterone by mineralocorticoid receptor antagonists (MRAs), spironolactone and eplerenone, is associated with a reduction in morbidity and mortality. However, spironolactone is a non selective antagonist, with off-target effects on other steroid receptors. There is some evidence suggesting that it may have an unfavorable effect on glucose homeostasis, with an increase in glycated hemoglobin (HbA1c), a marker of long-term glucose control. On the contrary, eplerenone seems to exert a neutral effect. The objectives of this doctoral thesis were the following: 1) Compile all current knowledge in the literature on the subject of MRAs’ glycemic effects; 2) Evaluate the risk of developing diabetes with spironolactone in HF patients; 3) Analyze if spironolactone may modulate the glycemic effects of other medications used in HF; 4) Compare spironolactone to eplerenone on markers of glucose control in HF patients with glycemic disorders. Four projects were conducted in order to meet these objectives. Firstly, a systematic review allowed us to identify all published studies containing information on MRAs’ glycemic effects. The literature search yielded heterogenous results; however, it suggested that the effect was disease-specific and would be potentially harmful in diseases with a high risk of cardiovascular events. A meta-analysis of studies in diabetes insinuated that the effect is non significant on a long-term basis. The second project uses a cohort of HF patients from administrative databases between 1995 and 2009 (follow-up till 2010). We did not detect a significant association between the use of spironolactone and the risk of diabetes. On the other hand, the study demonstrated that younger age, digoxin, and corticosteroids increase the risk of diabetes. The third project is a substudy of a clinical trial CANDIID-II (Effect of ACE inhibitor alone versus ACE inhibitor plus high dose candesartan on BNP, immune markers, inflammatory status, and urinary kinins in patients with symptomatic left ventricular systolic dysfunction) among HF patients treated with an angiotensin converting enzyme inhibitor and candesartan, an angiotensin II receptor blocker. These pharmacological classes have beneficial effects on glycemia. By comparing patients also treated with spironolactone versus patients without an MRA, we did not find that spironolactone alters the effect of candesartan on glucose metabolism. The last project consisted of a prospective, multicenter, randomized, controlled, double-blind trial: SNOW (A comparison of the effects of selective and non selective mineralocorticoid antagonism on glucose homeostasis and lipid profile of heart failure patients with glucose intolerance or type 2 diabetes). It compares, for 16 weeks, spironolactone to eplerenone on glycemic markers, notably, HbA1c, among 62 HF patients with type II diabetes or glucose intolerance. There was no significant difference between groups. In summary, the research results from this thesis reveal that, in HF, MRAs do not present additional risks of deterioration in glucose control over a moderate to long period.

Insuffisance cardiaque

Aldostérone

Spironolactone

Éplérénone

Diabète

Glucose

Hémoglobine glyquée

Heart failure

Mineralocorticoid receptor antagonists

Spironolactone

Diabetes

Glycated hemoglobin

Aldosteron syntáza u arteriální hypertenze a možný vliv polymorfismu jejího genu na hypertrofii levé komory srdeční / Aldosterone synthase in arterial hypertension and possible influence of its genenetic polymorphism on left ventricular hypertrophy

Heller, Samuel

January 2013

Part I. The aldosterone synthase gene (CYP11B2) polymorphism T-344C in blood pressure and left ventricular hypertrophy. BACKGROUND: Aldosterone is a key cardovascular hormone, it significantly influences volume, pressure and electrolyte balance. Aldosterone plays an important role in development of left ventricular (LV) hypertrophy and myocardial fibrosis. The aldosterone synthase gene (CYP11B2) is an important candidate gene region in essential hypertension. DESIGN AND METHODS: We assessed the influence of the T-344C polymorphism of aldosterone synthase - the rate-limiting enzyme in aldosterone biosynthesis - on the structure of the left ventricle in young normotensive men. The population included 113 normotensive mid-European Caucasian men aged 18-40 years (mean 27 +/- 5 years). We also studied the association of -344T/C polymorphism of the CYP11B2 gene with the presence and severity of hypertension in 369 individuals, of whom 213 were hypertensive patients (139 controlled hypertensive, 74 resistant hypertensive) and 156 were healthy normotensive subjects. The genotype was assessed using polymerase chain reaction with subsequent cleavage with restriction enzyme HAEIII (restriction fragment length polymorphism method) and visualization with ethidium bromide. Plasma renin activity (PRA) and plasma...