Contribution à l'étude de l'effet de la substance P sur la sécrétion d'aldostérone dans la glande surrénale humaine normale / Role of substance P in the regulation of aldosterone secretion in normal human adrenal gland

Wils, Julien

15 May 2018

La sécrétion d'aldostérone par la glande surrénale est principalement contrôlée par le système rénine-angiotensine circulant (SRA) et la kaliémie. La synthèse de l'aldostérone est également influencée par les facteurs paracrines intra-surrénaliens, y compris les neuropeptides. En particulier, les tachykinines, comme la substance P (SP), peuvent être libérées par les terminaisons nerveuses dans le cortex surrénalien. Le rôle de la SP dans la régulation de la fonction surrénalienne a été évalué chez l'animal mais rarement étudié chez l'homme. Le but de la présente étude est d'explorer le rôle de la SP dans le contrôle de la synthèse des minéralocorticoïdes dans la glande surrénale humaine. Des expériences in vitro conduites dans des échantillons surrénaliens normaux révèlent l'expression de SP codée par TAC1 qui est détecté par immunohistochimie dans des fibres nerveuses non-adrénergiques non-cholinergiques dans la zone glomérulée. Les fibres SP-positives établissent des contacts étroits avec des cellules productrices d'aldostérone qui expriment le récepteur NK1 (NK1R), récepteur de la SP. La SP stimule la production d'aldostérone à partir de cellules corticosurrénales cultivées, un effet qui est inhibé par l'aprépitant, antagoniste NK1R. L'action de la SP est relayée par la voie ERK et implique une régulation à la hausse de plusieurs gènes codant pour des enzymes de la stéroïdogénèse. Le rôle physiologique de la SP dans la régulation de la sécrétion d'aldostérone a été évalué à l'aide d'un essai clinique prospectif, contrôlé par placebo, de l'impact de l'aprépitant sur les concentrations plasmatiques et urinaires d'aldostérone chez des volontaires sains. L'aprépitant a réduit la production quotidienne d'aldostérone et la concentration plasmatique d'aldostérone (CPA) dans le décubitus, mais n'a pas modifié les CPA en position debout. Ces données montrent que la SP exerce un tonus stimulant sur la production d'aldostérone chez l'homme. / Aldosterone secretion by the adrenal gland is principally under control of the circulating renin-angiotensin system (RAS) and kalemia. Aldosterone synthesis is also influenced by intra-adrenal paracrine factors including neuropeptides. Especially, tachykinins, like substance P (SP), can be released by nerve endings in the adrenal cortex. The role of SP in the regulation of the adrenal function has been evaluated in animals but only scarcely investigated in humans. The aim of the present study is to explore the role of SP in the control of mineralocorticoid synthesis in the human adrenal gland. In vitro experiments conducted in normal adrenal samples reveal expression of the TAC1 encoding SP which is detected by immunohistochemistry in non adrenergic non cholinergic nerve fibres in the zona glomerulosa. SP-positive fibres establish close contacts with aldosterone-producing cells which express the SP receptor, i.e. the NK1 receptor (NK1R). SP stimulates aldosterone production from cultured adrenocortical cells, an effect which is inhibited by the NK1R antagonist aprepitant. The action of SP is mediated by the ERK pathway and involves upregulation of several genes encoding steroidogenic enzymes. The physiological role of SP in the regulation of aldosterone secretion was further assessed through a prospective clinical placebo-controlled trial investigating the impact of aprepitant on plasma and urine aldosterone levels in healthy volunteers. Aprepitant reduced daily aldosterone production and plasma aldosterone concentration (PAC) in recumbency but did not modify PAC in upright position. These data show that SP exerts a stimulatory tone on aldosterone production in man.

Aldostérone

Cortex surrénalien

Substance P

Régulation paracrine

Récepteur NK1

Aprépitant

Aldosterone

Adrenal cortex

Substance P

Paracrine regulation

NK1 receptor

Agrepitant

612.4

Contrôle post-transcriptionnel de l'expression rénale du récepteur minéralocorticoide par les variations de tonicité extracellulaire : conséquences physiopathologiques. / Posttrancriptional Regulation of Mineralocorticoid Receptor by Osmotic Stress : Pathophysiological Consequences

Lema, Ingrid

14 October 2016

L’aldostérone et le Récepteur Minéralocorticoïde (MR) participent au contrôle de la balance hydrosodée et de la pression artérielle. Les altérations de l’expression du MR ou de la signalisation minéralocorticoïde sont associées à de nombreuses pathologies chez l’Homme. Dans ce travail, nous avons démontré, le rôle majeur de protéines de liaison à l’ARN, Tis11b et HuR, dans le contrôle post-transcriptionnel de l’expression du MR en réponse aux variations de tonicité extracellulaire dans un modèle de cellules principales rénales et chez la souris. L’hypertonicité (500 mOsmol/L) induit l’expression de la protéine Tis11b, qui lie la région 3’-non traduite du transcrit MR afin d’accélérer sa dégradation, diminuant ainsi l’expression rénale de la protéine MR et de la signalisation minéralocorticoïde. A l’opposé, l’hypotonicité (150 mOsmol/L) stimule la translocation nucléo-cytoplasmique de HuR, qui stabilise le transcrit MR, augmentant ainsi l’expression du MR et la sensibilité rénale à l’aldostérone. De plus, HuR est responsable de l’édition d’un nouveau variant d’épissage du MR, le variant MR Δ6, obtenu par l’exclusion de l’exon 6.Ce variant d’épissage exerce un effet dominant négatif sur la signalisation minéralocorticoïde. Enfin, l’identification de microARN modulés par l’hypertonicité suggère leur rôle potentiel dans le contrôle de la signalisation minéralocorticoïde rénale. La caractérisation de ces mécanismes inédits modulant l’action du MR améliore notre compréhension de la physiopathologie de la signalisation minéralocorticoïde, et pourrait aboutir, à terme, à de nouvelles stratégies thérapeutiques. / Aldosterone and the Mineralocorticoid Receptor (MR) participate to the control of salt and water balance and the arterial pressure. Alteration of renal MR expression or mineralocorticoid signaling pathway contributes to the development of numerous human disorders. In this work, we have demonstrated the major role played by the RNA-Binding Proteins, Tis11b and HuR, in the control of MR expression in response to variations of extracellular tonicity in a model of principal tubular cells and in vivo. Hypertonicity (500 mOsmol/L) increases the expression ofTis11b, which binds the 3’-untranslated region of MR transcript and accelerates the degradation of MR transcript, leading to the reduction of the mineralocorticoid signaling. Conversely, hypotonicity (150 mOsmol/L) stimulates nuclear-cytoplasmic shuttling of HuR protein, which stabilizes MR transcript increasing its expression and renal sensitivity to aldosterone action. Furthermore, HuR participates to the editing of the novel MR Δ6 splice variant, which lacks exon 6, and exerts a dominant negative effect on mineralocorticoid signaling. Finally, we have provided evidence that hypertonicity modulates expression of microRNA, which may control mineralocorticoid signaling pathway. Characterization of these original mechanisms modulating MR action is pivotal for a better understanding of mineralocorticoid-related pathophysiology, and should ultimately lead to the development of new therapeutic strategies.

Récepteur Minéralocorticoïde

Aldostérone

Protéine de Liaison à l'ARN

Tonicité extracellulaire

Micro-ARN

Épissage alternatif

Mineralocorticoid Receptor

Aldosterone

RNA Binding Protein

Extracellular Tonicity

Micro-RNA

Splicing alternatif

Remodelace levé komory srdeční u pacientů s primárním hyperaldosteronismem a esenciální hypertenzí / Left ventricle remodeling in patients with primary aldosteronism and essential hypertension

Indra, Tomáš

January 2016

Myocardial damage is one of the most serious consequences of arterial hypertension. Changes in the heart structure and function develop not only due to pressure overload itself, but many other hemodynamic and neurohumoral factors contribute to their formation. Our work has compared echocardiohraphic strucutural anf functional changes of the left ventricle, caused by essential hypertension and hypertension associated with primary aldosteronism (PA) as the most common reason for secondary hypertension. The first part of our work focused on the differences in left ventricle geometry in men with PA and essential hypertension after separating it's low-renin form (where, similarly to PA, the plasma volume expansion was considered to have the dominant effect on left ventricle remodelation). In men with low-renin forms of hypertension including PA, we observed greater both endsystolic and enddiastolic diameter of the left ventricle, lower relative wall thickness and more frequent eccentric type of hypertrophy when compared to essential hypertensives with normal renin levels. Whereas left ventricle cavity diameters were positively correlated to aldosterone levels, wall thicknesses were associated mainly with hypertension severity expressed as an average 24hour blood pressure and number of antihypertensives....

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

Élucidation des mécanismes moléculaires impliqués dans l’expression aberrante du récepteur au peptide insulinotropique glucose-dépendant (GIP) dans les tumeurs du cortex de la glande surrénale

Lampron, Antoine

10 1900

Les tumeurs du cortex surrénalien sont variées et fréquentes dans la population. Bien que des mutations aient été identifiées dans certains syndromes familiaux, les causes génétiques menant à la formation de tumeur du cortex surrénalien ne sont encore que peu connues. Un sous-type de ces tumeurs incluent les hyperplasies macronodulaires et sont pressenties comme la voie d’entrée de la tumorigenèse du cortex surrénalien. L’événement génétique le plus fréquemment observé dans ces tumeurs est l’expression aberrante d’un ou plusieurs récepteurs couplés aux protéines G qui contrôle la production de stéroïdes ainsi que la prolifération cellulaire. L’événement génétique menant à l’expression aberrante de ces récepteurs est encore inconnu. En utilisant le récepteur au peptide insulinotropique dépendant du glucose (GIP) comme modèle, cette étude se propose d’identifier les mécanismes moléculaires impliqués dans l’expression aberrante du récepteur au GIP (GIPR) dans les tumeurs du cortex surrénalien. Une partie clinique de cette étude se penchera sur l’identification de nouveaux cas de tumeurs surrénaliennes exprimant le GIPR de façon aberrante. Les patients étudiés seront soumis à un protocole d’investigation in vivo complet et les tumeurs prélevées seront étudiées extensivement in vitro par RT-PCR en temps réel, culture primaire des tumeurs, immunohistochimie et biopuces. Le lien entre le GIP et la physiologie normal sera également étudiée de cette façon. Une autre partie de l’étude utilisera les nouvelles techniques d’investigation à grande échelle en identifiant le transcriptome de différents cas de tumeurs exprimant le GIPR de façon aberrante. L’importance fonctionnelle des gènes identifiée par ces techniques sera confirmée dans des modèles cellulaires. Cette étude présente pour la première des cas de tumeurs productrices d’aldostérone présentant des réponses aberrantes, auparavant confinées aux tumeurs productrice de cortisol ou d’androgènes surrénaliens. Le cas probant présenté avait une production d’aldostérone sensible au GIP, le GIPR était surexprimé au niveau de l’ARNm et un fort marquage a été identifié dans la tumeur spécifiquement. Dans les surrénales normales, cette étude démontre que le GIP est impliqué dans le contrôle de la production d’aldostérone. Ces résultats ont été confirmés in vitro. Finalement, le profilage à grande échelle des niveaux d’expression de tous les gènes du génome a permis d’isoler une liste de gènes spécifiquement liés à la présence du GIPR dans des hyperplasies du cortex surrénalien. Cette liste inclus la périlipine, une protéine de stockage des lipides dans les adipocytes et la glande surrénale, dont l’expression est fortement réprimée dans les cas GIP-dépendant. Des études dans un modèle cellulaire démontrent que la répression de ce gène par siRNA est suffisante pour induire l’expression du récepteur au GIP et que cette protéine est impliquée dans la stimulation de la stéroïdogénèse par le GIP. En alliant des méthodes d’investigation in vivo de pointe à des techniques in vitro avancée, cette étude offre de nouveaux regards sur les liens entre le GIP et la physiologie de la glande surrénale, que ce soit dans des conditions normales ou pathologiques. / Tumors of the adrenal cortex are varied and frequently found in the population. Aside from rare family cases in which mutations have been identified, the genetic events leading to the formation of adrenocortical tumors remain obscure. A subtype of these tumors includes macronodular hyperplasias, now percieved as the entry point of adrenocortical tumorigenesis. The most commonly observed molecular event in these cases is the presence of aberrantly expressed G-protein coupled receptor that drive steroid production and cellular proliferation. The genetic events leading to these aberrant levels of expression are unknown. This study will use the Glucose-dependent Insulinotropic Polypeptide (GIP) receptor as a model to identify the molecular mecanisms leading to the aberrant expression of the GIP receptor (GIPR) in adrenocortical tumors. The first part of the study will be a clinical investigation of new cases of adrenocortical tumors to screen for aberrant responses to GIP in various types of these tumors. The patients will be evaluated by a thorough clinical investigation protocol and the resected tumors will be extensively analysed in vitro, using real-time RT-PCR, immunohistochemistry, microarray and primary cultures of the tumors. The link between GIP and the normal physiology of the adrenal cortex will also be assessed in normal subjects. The second part of the study will use novel large-scale investigation techniques to determine the transcriptome of different cases of adrenocortical tumors expressing aberrant levels of the GIPR. The functional importance of identified genes will be assessed in cellular models. This study presents the first cases of aldosterone-producing tumors with aberrant responses to hormones, previously confined to cortisol- or androgen producing tumors. The case presented showed an aldosterone production sensitive, among others, to GIP. The GIPR’s mRNA was strongly over expressed and a specific staining was observed in immunohistochemistry. The responses were confirmed in primary cultures of the tumor. In normal adrenals, a role for the control of aldosterone by GIP was also demonstrated. Finally, large-scale profiling of the transcriptome led to the identification of a list of genes with expression levels strictly related to the presence of the GIPR in adrenocortical hyperplasias. One of these genes, perilipin, was strongly repressed specifically in GIP-dependent cases. siRNA techniques were used in a cellular model and confirmed that the repression of perilipin is sufficient to induce the expression of GIPR and that this protein is implicated in the GIP induced steroidogenesis. Allying state-of-the-art in vivo investigation methods to advanced in vitro techniques, the present study identifies novel insights on the link between GIP and the normal adrenal physiology, in normal and pathological conditions.

Glande surrénale

Adrenal gland

Récepteur couplé aux protéines G

GPCR

Tumeur

Tumor

Biopuce

Microarray

Aldostérone

Aldosterone

Syndrome de Cushing

Cushing's syndrome

Hyperaldosteronisme

Primary aldosteronism

GIP

GIP

Cortisol

Cortisol

Der Stellenwert von Biomarkern zur Prognoseabschätzung bei diastolischer Dysfunktion und HFpEF / The prognostic value of neuropeptides in diastolic dysfunction and HFpEF

Gonschior, Stefan

20 March 2017

No description available.

610

prognostic value

HFpEF

neuropeptides

diastolic dysfunction

NTproBNP

MRproADM

MRproANP

NTproANP

hsCRP

PIIINP

CTproET-1

CTproAVP

aldosterone

renin

hazard ratio

diastolic heart failure

prognose

mortality

Le rôle de l’aldostérone sur le remodelage structurel pulmonaire et la fonction ventriculaire droite en insuffisance cardiaque congestive

Chabot, Andréanne

08 1900

INTRODUCTION : L’insuffisance cardiaque congestive (ICC) induit remodelage pulmonaire et dysfonction ventriculaire droite (VD) qui contribuent de façon importante à la morbidité/mortalité. Malgré l’efficacité prouvée, l’antagonisme des récepteurs minéralocorticoïdes est sous-utilisé en ICC et ses mécanismes d’actions demeurent incompris. Nous avons évalué si l’Aldostérone contribue au remodelage pulmonaire et à la dysfonction VD en stimulant la prolifération des myofibroblastes (MYFs) pulmonaires. MÉTHODE ET RÉSULTATS : L’étude a été réalisée chez des rats avec infarctus du myocarde (IM) de taille modérée à grande permettant le développement de l’ICC. Deux semaines après l’IM, les rats ont été traités avec 100mg/kg/jour d’Aldactone ou non, pendant trois semaines et comparé à un groupe témoin (N=21;24;8). Comparativement au groupe témoin, les rats IM ont développé une ICC caractérisée par une réduction de la fraction de raccourcissement du VG (53±1%vs.16±2%, moyenne±ESM, P<0.0001), une hypertension pulmonaire (PSVD:27±1vs.40±3mmHg, P<0.01) et une hypertrophie VD (VD/(VG+Septum):24±1%vs.38±3%, P<0.05). L’Aldactone n’a eu aucun effet sur ces paramètres. Les rats IM ont développé un syndrome pulmonaire caractérisé par un abaissement de la courbe respiratoire pression-volume, un remodelage structurel pulmonaire avec doublement du poids poumon sec (P<0.01) et de la fibrose pulmonaire avec augmentation du taux de collagène dans les poumons (P<0.05). L’Aldactone n’a pas restauré la fonction pulmonaire. Enfin, les MYFs pulmonaires isolés n’ont pas proliféré avec l’exposition de 48h aux deux traitements d’Aldostérone (10-7M, 10-6M). CONCLUSION : L’Aldostérone ne contribue pas au remodelage pulmonaire et à la dysfonction VD associés à l’ICC. D’autres mécanismes d’actions sont responsables des effets bénéfiques de l’Aldactone. / BACKGROUND: Congestive heart failure (CHF) can induce pulmonary remodeling and RV dysfunction, which importantly contribute to morbidity and mortality. Despite proven efficacy, antagonism of mineralocorticoid receptors is underused in CHF and the mechanisms of its benefits still debated. We hypothesized that Aldosterone contributes to pulmonary remodeling and RV dysfunction by stimulating lung myofibroblasts (MYFs) proliferation. METHODS AND RESULTS: We studied rats with moderate to large myocardial infarcts (MI) to allow CHF development. Two weeks after MI, rats were treated with Aldactone 100mg/kg/day (N=21) or untreated (N=24) for three weeks and compared to a sham group (N=8). Five weeks after MI, infarct size was similar in the two MI groups, both by ultrasound and pathologic measures. Compared to sham, the MI-untreated group developed CHF with reduced LV fractional shortening (53±1%vs.16±2%; mean±SEM, P<0.0001), pulmonary hypertension (RVSP:27±1vs.40±3mmHg, P<0.01) and RV hypertrophy (RV/(LV+septum):24±1%vs.38±3%, P<0.05). Aldactone treatment had no effect on these parameters and did not improve LV or RV performance. CHF induced a restrictive respiratory syndrome characterized by a downward shift of the respiratory pressure-volume loop, important lung remodeling with nearly doubling of dry lung weight (P<0.01) and evidence of lung fibrosis demonstrated by histological lung collagen fractional area (P<0.05). The Aldactone therapy could not restore pulmonary function. Finally, isolated lung MYFs did not proliferate after 48hr exposure to aldosterone (10-7M and 10-6M). CONCLUSION: Aldosterone does not contribute to pulmonary remodeling and RV dysfunction associated with CHF. Other mechanisms of action must be responsible for the beneficial effects of Aldactone in CHF.

Insuffisance Cardiaque Congestive

Aldostérone

Maladies Pulmonaires Cardiovasculaires

Fonction pulmonaire

Récepteurs Minéralocorticoïdes

Aldactone

Spironolactone

Congestive Heart Failure

Aldosterone

Pulmonary Heart Disease

Pulmonary Function

Cardiovascular Therapeutics

Mineralocorticoid Receptors

Aldactone

Spironolactone

A N-acetilcisteína atenua a progressão da doença renal crônica / N-acetylcysteine attenuates the progression of chronic kidney disease

Shimizu, Maria Heloisa Massola

01 December 2005

Os biomarcadores do estresse oxidativo encontram-se elevados na urina e no plasma dos pacientes renais crônicos. A aldosterona (ALD) contribui para a lesão renal no modelo de rins remanescentes. Objetivos: 1- Determinar o efeito do antioxidante N-acetilcisteína (NAC) sobre a função renal e a aldosterona plasmática de animais com IRC. 2- Avaliar o efeito da NAC sobre a evolução da IRC, mesmo quando administrada tardiamente. 3- Avaliar os efeitos da NAC associada a Espironolactona (Spi). Material e Métodos: Ratos adultos Wistar machos foram submetidos a nefrectomia de 5/6 (Nx). No estudo 1: Animais foram tratados ou não com NAC na dose de (600mg/l na água de beber) iniciado 7dias após nefrectomia (Nx). Estudos de clearance foram realizados em todos os grupos, 21, 60 e 120 dias após Nx. No estudo 2: 6 animais foram tratados com NAC após 60 dias de Nx e estudados 120 dias após NX. No estudo 3: Os ratos foram tratados com Spi (1.5g/kg de dieta) associados ou não com NAC, ambos iniciados a partir do 7º dia da nefrectomia e estudados 60 dias após a Nx. Em todos os grupos foram avaliados: clearance de inulina (RFG, ml/min/100g peso); proteinúria (Uvpr., mg/24h); aldosterona plasmática (ng/dl); relação potássio/sódio urinário (UK/UNa), pressão arterial (mmHg), TBARS urinário (nmoles/24h) e o índice de glomeruloesclerose (%). Resultados: A ingestão média de NAC foi similar nos respectivos grupos tratados. Significante diminuição de TBARS (marcador de peroxidação lipídica), foi observada nos ratos Nx tratados com NAC (mesmo quando administrado tardiamente). O principal resultado deste estudo foi que a administração de NAC nos animais com nefrectomia de 5/6, protegeu a filtração glomerular (GFR) significativamente, com uma média de clearance de inulina de 0.45 ml/min (50% dos valores normais), mantendose estável 120 dias após a nefrectomia (0,51 ± 0,03). Ao contrário, GFR diminuiu progressivamente nos animais não tratados (0,16 ± 0,03). Nos animais Nx+NAC, a proteinúria, o índice de glomeruloesclerose e a pressão arterial, apresentaram diminuição após 120 dias de Nx e hipertrofia dos corações e das adrenais foram atenuadas. Estes efeitos benéficos estão associados com uma significante redução da aldosterona plasmática e da razão UK/UNa (marcador indireto da ação tubular da aldosterona) e foram observados mesmo com a administração tardia de NAC (60 dias após Nx). A mortalidade foi de 33% no grupo de Nx120, 25% no grupo Nx120+NAC e 10% nos animais Nx120+60NAC. No estudo 3: A espironolactona isoladamente diminuiu a proteinúria dos animais Nx, entretanto, quando associada a NAC promoveu maior proteção da filtração glomerular (Nx60 + NAC+Spi = 0,59±0,04 vs.Nx + 60 + NAC = 0,47 ± 0,05, p < 0,001) e menor pressão arterial (136±2mmHg) do que nos animais tratados apenas com NAC (154 ± 2 mmHg). Conclusões: 1. O antioxidante NAC exerceu efeito protetor sobre a filtração glomerular de ratos com insuficiência renal crônica, mesmo quando administrado tardiamente, além de diminuir as concentrações de aldosterona e TBARS, marcador de peroxidação lipídica. 2. A associação de NAC e espironolactona proporcionou efeito benéfico aditivo sobre a filtração glomerular, acompanhado de uma maior queda da pressão arterial. / Oxidative stress biomarkers are increased in urine and plasma from renal chronic patients. Aldosterone (ALD) contributes to the kidney lesion in the remnant kidney model. Objectives: This studies was carried out to: 1- Determine the effect of antioxidant N-acetylcysteine (NAC) on kidney function and plasma aldosterone on animals with chronic renal failure (CRF); 2- Evaluate the effect of NAC on the CRF evolution, even when administered at a later stage; 3- Evaluate the effects of NAC associated with spironolactone (SPI). Material and Methods: Adult male Wistar rats were submitted to 5/6 nephrectomy (Nx). In study 1: Animals were treated or not with NAC (600 mg/l in drinking water), started 7 days after Nx. Clearance studies were performed on all rats at 21, 60 and 120 days after Nx. In study 2: 6 rats were treated with NAC initiated 60 days after Nx and studied 120 days after Nx. In study 3: rats were treated with Spi (1.5 g/Kg diet) associated or not to NAC, both initiated 7 days after Nx-treated rats and studied 60 days after Nx. In all experiments the following were measured: inulin clearance (GRF, ml/min/100g body weight); proteinuria (Uvpr, mg/24h); plasma aldosterone (ng/dl); urinary potassium/sodium ratio (UK/UNa); blood pressure (mmHg); urinary TBARS (nmoles/24h) and glomerulosclerosis index (%). Results: Mean daily NAC ingestion was similar in respective treated groups. A significant decrease in urinary TBARS (an index of lipid peroxidation) was observed in the NAC treated rats even when administered at a later stage. The main new finding of this study is that NAC administration to 5/6-Nx rats protects the glomerular filtration rate (GFR) significantly, with a mean inulin clearance of 0.45 (50% of the normal values), remaining stable 120 days following nephrectomy (0.51±0.03). Conversely, GFR fell progressively in untreated rats (0.16±0.03). In Nx+NAC rats, proteinuria, glomerulosclerosis index and blood pressure all decreased by day 120, and heart and adrenal hypertrophy were attenuated. These beneficial effects were associated with a significant reduction in plasma aldosterone and urinary sodium/potassium (UK/UNa) ratio (indirect marker of aldosterone tubular action) and were observed even when NAC was administered later (60 days after Nx). Mortality was 33% in the Nx 120 group, 25% in the Nx120+NAC group and 14.3% in the Nx120 (Nx60+60NAC). In study 3: Spironolactone isolatedly decreased proteinuria in the Nx animals, however when associated with NAC it caused more protection of GFR (Nx60+NAC+Spi = 0.59±0.04 vs Nx60+NAC = 0.47 ± 0.05, p < 0.001) and lower blood pressure (136±2 mmHg) than in the animals treated only with NAC (154±2 mmHg). The combination of Spi and NAC lowered blood pressure and improve GFR protection. Conclusion: 1. In the remnant kidney model, NAC has a protective effect attributable to decreased plasma aldosterone and lower of lipid peroxidation indicative of thiobarbituric acid reactive substances (TBARS) lower levels, even in the later stages. 2. Combination of NAC and Spi showed an extra beneficial effect over glomerular filtration, and a higher decrease of blood pressure.

Acetilcisteína

Acetylcysteine

Aldosterona

Aldosterone

Chronic kidney failure

Espironolactona.

Insuficiência renal crônica

Inulin

Inulina

Kidney function renal

Lipid peroxidation

Peroxidação de lipídeos

Ratos Wistar

Spironolactone

Testes de função renal

Thiobarbituric acid reactive

Wistar rats

Chronische und akute Regelvorgänge im Salz-Wasser-Haushalt

Boemke, Willehad

29 January 2002

Diese kumulative Habilitation untersucht die Rolle des Renin-Angiotensin-Aldosteron-Systems (RAAS) bei chronischen und akuten Regelvorgänge im Salz-Wasser-Haushalt an wachen Hunden. Nach einer Einführung in die Methodik der Langzeitstudien werden zunächst die zirkardianen und ultradianen Veränderungen der Natriumausscheidung beschrieben, die wir bei den Hunden beobachten konnten. Es scheint, als sei das Natriumausscheidungsmuster bei Hunden das Resultat endogener Rhythmizität und exogen, reaktiver Prozesse. Beide Komponenten scheinen zur Aufrechterhaltung der Natriumhomöostase beizutragen. Bei der Infusion natriumretinierender Hormone wie Aldosteron und Angiotensin II verschob sich ein größerer Anteil der täglichen Natrium- und Wasserausscheidung in die Abend- und Nachtstunden. Wir haben dieses Phänomen als "Nachtverschiebung" bezeichnet. In Bilanzstudien über vier Tage wurde dann der Frage nachgegangen, ob das Ganz-Körper-(GK)-Natrium eine kontrollierte Variable ist. Wir konnten zeigen, dass zwei Faktoren bei der Kontrolle des GK-Natriums eine wesentliche Rolle spielen, die Aktivität des RAAS und der renale Perfusionsdruck. Ist nur eine dieser Komponenten gestört, kann sie durch die andere - was das Einstellen eines 24-Stunden Bilanzgleichgewichtes angeht - ausgeglichen werden, allerdings nur unter Inkaufnahme eines veränderten GK-Natriumbestands. Ebenfalls über vier Tage wurde die Bedeutung des NO (Stickoxid) für die langfristige Regelung des Natriumbestandes untersucht. Dabei wurde gefunden, dass die Plasma-Renin-Aktivität (PRA) während NO-Synthase-Inhibition durchweg niedriger als bei intaktem NO-System war. Der Aldosteron / PRA Quotient war unter NOS-Inhibition deutlich größer als in den jeweiligen Protokollen ohne NOS-Inhibition. In Kurzzeitstudien (3-4 Stunden) wurden wache Hunde während akuter Hypoxie, die akut mit einer Verminderung des Natrium- und Wasserbestandes einhergehen kann ("Höhendiurese"), sowie während kontrollierter maschineller Beatmung mit hohen positiv-end-exspiratorischen (PEEP) Drucken, die zur Natrium- und Wasserretention führen kann, untersucht. Unter Hypoxie zeigte sich, dass das in niedrigen Plasma-Konzentrationen als Adenosin-1-Rezeptorantagonist wirkende Theophyllin den Abfall der PRA und des Angiotensin II unter Hypoxie verhindern kann. Auf der anderen Seite fiel die Plasma-Aldosteron-Konzentration während Hypoxie unabhängig davon, ob Theophyllin infundiert wurde, wahrscheinlich wegen einer verminderten Aktivität der 18-Hydroxylase während Hypoxie. Die Untersuchungen unter PEEP-Beatmung ergaben u.a., dass bei bilateral denervierten, wachen Hunden, deren Natriumzufuhr normal ist, den Nierennerven keine wesentliche Rolle für die zu beobachtende Wasser- und Natriumretention während maschineller Beatmung zukommt. / This cumulative thesis investigates on conscious dogs the role of the renin-angiotensin-aldosterone system (RAAS) during chronic and acute challenges of salt and water homeostasis. After introducing the methods of long term studies in dogs, circadian and ultradian oscillations of sodium excretion are being described. We demonstrated, that the sodium excretion pattern in dogs is the result of endogenous rhythms and exogenous reactive processes. Both components seem to contribute to sodium homeostasis. When infusing sodium retaining hormones, such as aldosterone and angiotensin II, a greater share of the daily sodium and water excretion was shifted towards the evening and the night. This phenomenon was termed "night shift". In balance studies over four days it was investigated whether the total body sodium is a controlled variable. Two factors were identified to play a pivotal role in controlling total body sodium: the activity of the RAAS and renal perfusion pressure. If only one of these components is disturbed, the respective other component is able to equilibrate the 24 h sodium balance, but only on a different level of total body sodium. Also over a period of four days the significance of NO (nitric oxide) for the long-term regulation of sodium balance was investigated. Among others, it was found that compared to an intact NO system, the plasma-renin activity (PRA) was always lower during NO synthase (NOS) inhibition, and the aldosterone / PRA ratio was greater during NOS inhibition. In short-term studies (lasting 3-4 hours) awake dogs were studied during hypoxia - which is usually combined with a reduced total body sodium and water ("high altitude diuresis") - as well as during controlled mechanical ventilation with positive-end-expiratory pressure (PEEP) - which often leads to sodium and water retention. It was demonstrated that the decline in PRA and angiotensin II during hypoxia - which is a typical finding in conscious dogs - can be prevented by theophyllin, which acts as an adenosin-1-receptor antagonist in lower concentrations. On the other hand, plasma aldosterone concentration declined during hypoxia independent of whether theophyllin was infused or not, probably due to a reduced 18-hydroxylase activity during hypoxia. The PEEP studies demonstrated among others, that in bilaterally denervated conscious dogs - whose sodium intake was normal - the renal nerves play no substantial role for the water and sodium retention observed during PEEP ventilation.

Renin

Angiotensin

Aldosteron

Langzeit

renaler Perfusionsdruck

Natrium

Wasser

Homeostase

Hypoxie

PEEP

Renin

angiotensin

aldosterone

long term

renal perfusion pressure

sodium

water

homeostasis

hypoxia

PEEP

610 Medizin

33 Medizin

YI 4800

ddc:610

Effect of Tulbaghia violacea on the blood pressure and heart rate in male spontaneously hypertensive wistar rats

Raji, Ismaila

January 2011

<p>Tulbaghia violacea Harv. (Alliaceae) is a small bulbous herb which belongs to the family, Alliaceae, most commonly associated with onions and garlic. In South Africa (SA), this&nbsp / herb has been traditionally used in the treatment of various ailments, including fever, colds, asthma, paralysis, hypertension (HTN) and stomach problems. The aim of this study&nbsp / was to evaluate the effect of methanol leaf extracts (MLE) of T. violacea on the blood pressure (BP) and heart rate (HR) in anaesthetized male spontaneously hypertensive rats / &nbsp / and to find out the mechanism(s) by which it acts. The MLE of T. violacea (5 - 150 mg/kg), angiotensin I (ang I, 3.1 - 100 &mu / g/kg), captopril (10 mg/kg), angiotensin II (ang II, 3.1 - 50&nbsp / g/kg), losartan (30 mg/kg), phenylephrine (0.01 &ndash / 0.16 mg/kg), prazosin (1 mg/kg), dobutamine (0.2 &ndash / 10.0 &mu / g/kg), propranolol (0.1 - 12.8 mg/kg), muscarine (0.16 -10 &mu / g/kg),&nbsp / and atropine (0.02 - 20.48 mg/kg) were administered intravenously into male spontaneously hypertensive rats (SHR) weighing between 300 g and 350 g and aged less than 5&nbsp / months. The MLE of T. violacea and/or the standard drugs were infused alone, simultaneously, or separately into each animal. The BP and HR were measured via a pressure&nbsp / transducer connecting the femoral artery and the Powerlab. The vehicle (0.2 mls of a mixture of dimethylsulfoxide and normal saline), T. violacea (60 mg/kg) and captopril (10&nbsp / mg/kg) were injected intraperitoneally into some SHR for 21 days to investigate the chronic effect of these agents on plasma levels of aldosterone. The mean change, the mean&nbsp / of the individual percentage changes and the percentage difference (in mean) observed with each intervention was calculated and statistically analyzed using the Student&rsquo / s t test&nbsp / for significant difference (p &lt / 0.05). The Microsoft Excel software was used for statistical analysis. T. violacea significantly (p &lt / 0.05) reduced the systolic, diastolic, and mean&nbsp / arterial BP / and HR dose-dependently. In a dose-dependent manner, ang I, ang II, phenylephrine significantly (p &lt / 0.05) increased the BP, while propranolol, muscarine and&nbsp / atropine reduced the BP. The increases in BP due to dobutamine were not dose-dependent. In a dose dependent manner, phenylephrine and propranolol reduced the HR, while dobutamine increased the HR. The effect of ang I, ang II, muscarine and atropine on HR were not dose-dependent / with both increases as well as decreases observed with ang&nbsp / I, and II and atropine, while decreases were seen with muscarine. Captopril produced&nbsp / significant (p &lt / 0.05) reduction in BP which were not associated with any change in HR. The co-infusion of ang I with the MLE produced significant (p &lt / 0.05) reduction in BP, which were not associated with significant changes in HR. The co-infusion of ang II with the&nbsp / MLE did not produce any significant changes in BP or HR when compared to the infusion of the standard drug alone. The co-infusion of phenylephrine with the MLE did not&nbsp / produce any significant change in BP or HR when compared to the values obtained with the infusion of the standard drug alone, in both the absence and presence of prazosin.&nbsp / The co-infusion of dobutamine with T. violacea produced siginificant (p &lt / 0.05) increases in DBP which were associated with significant (p &lt / 0.05) reductions in HR, when&nbsp / compared to the values obtained with the infusion of the standard drug alone. Theco-infusion of atropine with the MLE did not produce any significant change in BP or HR when&nbsp / compared to the values obtained with the infusion of atropine alone. However, the infusion of T. violacea, 20 minutes after pre-treating animals with atropine (5.12 mg/kg) lead to&nbsp / dose dependent significant (p &lt / 0.05) increases in BP, which were associated with dose-dependent increases in HR. The chronic treatment of animals with T. violacea or&nbsp / captropril produced (a) signicant (p &lt / 0.05) reductions in the plasma levels of aldosterone when compared to the values obtained in the vehicle-treated group, (b) produced&nbsp / signifiant (p &lt / 0.05) reduction in BP in the captopril treated group when compared to the vehicle-treated, (c) did not produce any signficant change in BP in the T. violacea-treated&nbsp / group when compared to the vehicle-treated group and (d) did not produce any signifiant change in HR or body weight in any of the groups. The result obtained in this study&nbsp / suggests that T. violacea reduced BP and HR in the SHR. Secondly, the BP and HR reducing effect of the MLE may involve a) the inhibition of the ACE, b) the inhibition of the &beta / 1&nbsp / adrenoceptors, c) the stimulation of the muscarinic receptors and d) the reduction of the levels of aldosternone in plasma. The results also&nbsp / suggest that the MLE may not act&nbsp / through the angiotensin II receptors or the &alpha / 1 adrenergic receptors.&nbsp / </p>