Your search keyword '"Mara Ferrandi"' showing total 82 results

1. Selective SERCA2a activator as a candidate for chronic heart failure therapy

Author

Martina Arici, Shih-Che Hsu, Mara Ferrandi, Paolo Barassi, Carlotta Ronchi, Eleonora Torre, Andrea Luraghi, Gwo-Jyh Chang, Patrizia Ferrari, Giuseppe Bianchi, Francesco Peri, Antonio Zaza, and Marcella Rocchetti

Subjects

SERCA2a, Istaroxime, PST3093, Heart failure, Diastolic dysfunction, STZ, Medicine

Abstract

Abstract Background The sarcoplasmic reticulum (SR) Ca2+ ATPase (SERCA2a) depression substantially contributes to diastolic dysfunction in heart failure (HF), suggesting that SERCA2a stimulation may be a mechanism-based HF therapy. Istaroxime is a drug endowed with both a SERCA2a stimulatory activity and a Na+/K+ pump inhibitory activity for acute HF treatment. Its main metabolite PST3093 shows a more favorable therapeutic profile as compared to the parent drug, but it is still unsuitable for chronic usage. Novel PST3093 derivatives have been recently developed for oral (chronic) HF treatment; compound 8 was selected among them and here characterized. Methods Effects of compound 8 were evaluated in a context of SERCA2a depression, by using streptozotocin-treated rats, a well-known model of diastolic dysfunction. The impact of SERCA2a stimulation by compound 8 was assessed at the cellular level ad in vivo, following i.v. infusion (acute effects) or oral administration (chronic effects). Results As expected from SERCA2a stimulation, compound 8 induced SR Ca2+ compartmentalization in STZ myocytes. In-vivo echocardiographic analysis during i.v. infusion and after repeated oral administration of compound 8, detected a significant improvement of diastolic function. Moreover, compound 8 did not affect electrical activity of healthy guinea-pig myocytes, in line with the absence of off-target effects. Finally, compound 8 was well tolerated in mice with no evidence of acute toxicity. Conclusions The pharmacological evaluation of compound 8 indicates that it may be a safe and selective drug for a mechanism-based treatment of chronic HF by restoring SERCA2a activity. Graphical Abstract

Published

2024

2. Structural and Electrophysiological Changes in a Model of Cardiotoxicity Induced by Anthracycline Combined With Trastuzumab

Author

Claudia Altomare, Alessandra Maria Lodrini, Giuseppina Milano, Vanessa Biemmi, Edoardo Lazzarini, Sara Bolis, Nicolò Pernigoni, Eleonora Torre, Martina Arici, Mara Ferrandi, Lucio Barile, Marcella Rocchetti, and Giuseppe Vassalli

Subjects

doxorubicin, trastuzumab, cardiotoxicity, T-tubules, electrophysiology, calcium handling, Physiology, QP1-981

Abstract

BackgroundCombined treatment with anthracyclines (e.g., doxorubicin; Dox) and trastuzumab (Trz), a humanized anti-human epidermal growth factor receptor 2 (HER2; ErbB2) antibody, in patients with HER2-positive cancer is limited by cardiotoxicity, as manifested by contractile dysfunction and arrhythmia. The respective roles of the two agents in the cardiotoxicity of the combined therapy are incompletely understood.ObjectiveTo assess cardiac performance, T-tubule organization, electrophysiological changes and intracellular Ca2+ handling in cardiac myocytes (CMs) using an in vivo rat model of Dox/Trz-related cardiotoxicity.Methods and ResultsAdult rats received 6 doses of either Dox or Trz, or the two agents sequentially. Dox-mediated left ventricular (LV) dysfunction was aggravated by Trz administration. Dox treatment, but not Trz, induced T-tubule disarray. Moreover, Dox, but not Trz monotherapy, induced prolonged action potential duration (APD), increased incidence of delayed afterdepolarizations (DADs) and beat-to-beat variability of repolarization (BVR), and slower Ca2+ transient decay. Although APD, DADs, BVR and Ca2+ transient decay recovered over time after the cessation of Dox treatment, subsequent Trz administration exacerbated these abnormalities. Trz, but not Dox, reduced Ca2+ transient amplitude and SR Ca2+ content, although only Dox treatment was associated with SERCA downregulation. Finally, Dox treatment increased Ca2+ spark frequency, resting Ca2+ waves, sarcoplasmic reticulum (SR) Ca2+ leak, and long-lasting Ca2+ release events (so-called Ca2+ “embers”), partially reproduced by Trz treatment.ConclusionThese results suggest that in vivo Dox but not Trz administration causes T-tubule disarray and pronounced changes in electrical activity of CMs. While adaptive changes may account for normal AP shape and reduced DADs late after Dox administration, subsequent Trz administration interferes with such adaptive changes. Intracellular Ca2+ handling was differently affected by Dox and Trz treatment, leading to SR instability in both cases. These findings illustrate the specific roles of Dox and Trz, and their interactions in cardiotoxicity and arrhythmogenicity.

Published

2021

3. Lack of salt-inducible kinase 2 (SIK2) prevents the development of cardiac hypertrophy in response to chronic high-salt intake.

Author

Sergej Popov, Hiroshi Takemori, Takeshi Tokudome, Yuanjie Mao, Kentaro Otani, Naoki Mochizuki, Nuno Pires, Maria João Pinho, Anders Franco-Cereceda, Lucia Torielli, Mara Ferrandi, Anders Hamsten, Patricio Soares-da-Silva, Per Eriksson, Alejandro M Bertorello, and Laura Brion

Subjects

Medicine, Science

Abstract

Cardiac left ventricle hypertrophy (LVH) constitutes a major risk factor for heart failure. Although LVH is most commonly caused by chronic elevation in arterial blood pressure, reduction of blood pressure to normal levels does not always result in regression of LVH, suggesting that additional factors contribute to the development of this pathology. We tested whether genetic preconditions associated with the imbalance in sodium homeostasis could trigger the development of LVH without concomitant increases in blood pressure. The results showed that the presence of a hypertensive variant of α-adducin gene in Milan rats (before they become hypertensive) resulted in elevated expression of genes associated with LVH, and of salt-inducible kinase 2 (SIK2) in the left ventricle (LV). Moreover, the mRNA expression levels of SIK2, α-adducin, and several markers of cardiac hypertrophy were positively correlated in tissue biopsies obtained from human hearts. In addition, we found in cardiac myocytes that α-adducin regulates the expression of SIK2, which in turn mediates the effects of adducin on hypertrophy markers gene activation. Furthermore, evidence that SIK2 is critical for the development of LVH in response to chronic high salt diet (HS) was obtained in mice with ablation of the sik2 gene. Increases in the expression of genes associated with LVH, as well as increases in LV wall thickness upon HS, occurred only in sik2+/+ but not in sik2-/- mice. Thus LVH triggered by HS or the presence of a genetic variant of α-adducin requires SIK2 and is independent of elevated blood pressure. Inhibitors of SIK2 may constitute part of a novel therapeutic regimen aimed at prevention/regression of LVH.

Published

2014

4. Early consequences of the phospholamban mutation PLN-R14del+/-in a transgenic mouse model

Author

Claudia Maniezzi, Marem Eskandr, Chiara Florindi, Mara Ferrandi, Paolo Barassi, Elena Sacco, Valentina Pasquale, Angela S. Maione, Giulio Pompilio, Vivian Oliveira Nunes Teixeira, Rudolf A de Boer, Herman H W Silljé, Francesco Lodola, and Antonio Zaza

Abstract

AimsThe heterozygous phospholamban (PLN) mutation R14del (PLN R14del+/-) is associated with a severe arrhythmogenic cardiomyopathy (ACM) developing in the adult. “Superinhibition” of SERCA2a by PLN R14del is widely assumed to underlie the pathogenesis, but alternative mechanisms such abnormal energy metabolism have also been reported. This work aims to 1) to evaluate Ca2+dynamics and energy metabolism in a transgenic (TG) mouse model of the mutation prior to cardiomyopathy development; 2) to test whether they are causally connected.Methods and ResultsCa2+dynamics, energy metabolism parameters, reporters of mitochondrial integrity, energy and redox homeostasis were measured in ventricular myocytes of 8-12 weeks-old, phenotypically silent, TG mice. Mutation effects were compared to pharmacological PLN antagonism and analysed during modulation of sarcoplasmic reticulum (SR) and cytosolic Ca2+compartments. Transcripts and proteins of relevant signalling pathways were evaluated. The mutation was characterized by hyperdynamic Ca2+handling, similar to that induced by PLN antagonism. Albeit all components of energy metabolism were depressed at rest, functional signs of mitochondrial damage or energy starvation were absent and cell energy charge was preserved. The response of mitochondrial O2consumption to SERCA2a blockade was lost in mutant myocytes (SR-mitochondrial uncoupling) and ER-stress signalling was activated.Conclusions1) PLN R14del+/-loses its ability to inhibit SERCA2a, which argues against SERCA2a superinhibition as a mechanism of ACM; 2) depression of resting energy metabolism may at least partly reflect impairment of SR-mitochondrial coupling; 3) ER-stress may be an early factor in the pathogenesis.

Published

2023

5. SERCA2a stimulation by istaroxime improves intracellular Ca2+ handling and diastolic dysfunction in a model of diabetic cardiomyopathy

Author

Gaspare Mostacciuolo, Claudio Bussadori, Shih-Che Hsu, E. Boz, Claudia Altomare, Martina Arici, Gwo-Jyh Chang, Marcella Rocchetti, Giuseppe Bianchi, Alessandra Maria Lodrini, Emanuela Sala, Paolo Barassi, Mara Ferrandi, Sara Vagni, Patrizia Ferrari, Eleonora Torre, Torre, E, Arici, M, Lodrini, A, Ferrandi, M, Barassi, P, Hsu, S, Chang, G, Boz, E, Sala, E, Vagni, S, Altomare, C, Mostacciuolo, G, Bussadori, C, Ferrari, P, Bianchi, G, and Rocchetti, M

Subjects

medicine.medical_specialty, Diabetic Cardiomyopathies, Physiology, Cardiac fibrosis, Diastole, Stimulation, Context (language use), Istaroxime, Diabetes Mellitus, Experimental, Sarcoplasmic Reticulum Calcium-Transporting ATPases, BIO/09 - FISIOLOGIA, SERCA, Physiology (medical), Diabetic cardiomyopathy, Internal medicine, Etiocholanolone, Animals, Medicine, Calcium handling, Streptozotocin, business.industry, medicine.disease, Rats, Phospholamban, Sarcoplasmic Reticulum, Endocrinology, cardiovascular system, Diastolic dysfunction, Calcium, Sodium-Potassium-Exchanging ATPase, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Aims Diabetic cardiomyopathy is a multifactorial disease characterized by an early onset of diastolic dysfunction (DD) that precedes the development of systolic impairment. Mechanisms that can restore cardiac relaxation improving intracellular Ca2+ dynamics represent a promising therapeutic approach for cardiovascular diseases associated to DD. Istaroxime has the dual properties to accelerate Ca2+ uptake into sarcoplasmic reticulum (SR) through the SR Ca2+ pump (SERCA2a) stimulation and to inhibit Na+/K+ ATPase (NKA). This project aims to characterize istaroxime effects at a concentration (100 nmol/L) marginally affecting NKA, in order to highlight its effects dependent on the stimulation of SERCA2a in an animal model of mild diabetes. Methods and results Streptozotocin (STZ) treated diabetic rats were studied at 9 weeks after STZ injection in comparison to controls (CTR). Istaroxime effects were evaluated in vivo and in left ventricular (LV) preparations. STZ animals showed 1) marked DD not associated to cardiac fibrosis, 2) LV mass reduction associated to reduced LV cell dimension and T-tubules loss, 3) reduced LV SERCA2 protein level and activity and 4) slower SR Ca2+ uptake rate, 5) LV action potential (AP) prolongation and increased short-term variability (STV) of AP duration, 6) increased diastolic Ca2+, and 7) unaltered SR Ca2+ content and stability in intact cells. Acute istaroxime infusion (0.11 mg/kg/min for 15 min) reduced DD in STZ rats. Accordingly, in STZ myocytes istaroxime (100 nmol/L) stimulated SERCA2a activity and blunted STZ-induced abnormalities in LV Ca2+ dynamics. In CTR myocytes, istaroxime increased diastolic Ca2+ level due to NKA blockade albeit minimal, while its effects on SERCA2a were almost absent. Conclusions SERCA2a stimulation by istaroxime improved STZ-induced DD and intracellular Ca2+ handling anomalies. Thus, SERCA2a stimulation can be considered a promising therapeutic approach for DD treatment. Translational perspective Deficient sarcoplasmic reticulum (SR) Ca2+ uptake has been identified in cardiomyocytes from failing human hearts with impaired diastolic relaxation (e.g. diabetic hearts) and has been associated with a decreased SERCA2a expression and activity and/or with a higher SERCA2a inhibition by phospholamban. Thus, SERCA2a may represent a pharmacological target for interventions aimed at improving cytosolic Ca2+ compartmentalization into the SR to limit diastolic dysfunction pathologies. In this context, istaroxime is the first-in-class luso-inotropic agent targeting SERCA2a that has already demonstrated its efficacy in clinical trials and may be useful to clarify the relevance of SERCA2a stimulation in controlling cytosolic Ca2+ level.

Published

2021

6. Istaroxime Metabolite PST3093 Selectively Stimulates SERCA2a and Reverses Disease-Induced Changes in Cardiac Function

Author

Paolo Barassi, SC Hsu, Mara Ferrandi, Marcella Rocchetti, Giuseppe Bianchi, Antonio Zaza, Gwo-Jyh Chang, Francesco Peri, Martina Arici, Carlotta Ronchi, Luraghi A, Patrizia Ferrari, Eleonora Torre, Arici, M, Ferrandi, M, Barassi, P, Hsu, S, Torre, E, Luraghi, A, Ronchi, C, Chang, G, Peri, F, Ferrari, P, Bianchi, G, Rocchetti, M, and Zaza, A

Subjects

Cardiac function curve, Digoxin, Physiology, Metabolite, Cardiomyopathy, SERCA2, istaroxime, heart failure, diastolic dysfunction, metabolite, Pharmacology, Sarcoplasmic Reticulum Calcium-Transporting ATPases, chemistry.chemical_compound, Pharmacokinetics, BIO/09 - FISIOLOGIA, Etiocholanolone, Medicine, Humans, Animals, Myocytes, Cardiac, Heart Failure, Adenosine Triphosphatases, business.industry, Heart, medicine.disease, Rats, Istaroxime, chemistry, Pharmacodynamics, Heart failure, Molecular Medicine, business, medicine.drug

Abstract

BackgroundHeart failure (HF) therapeutic toolkit would strongly benefit from the availability of ino-lusitropic agents with a favorable pharmacodynamics and safety profile. Istaroxime is a promising agent, which combines Na+/K+ pump inhibition with SERCA2a stimulation; however, it has a very short half-life and extensive metabolism to a molecule, named PST3093. The present work aims to investigate whether PST3093, still retains the pharmacodynamic and pharmacokinetic properties of its parent compound.MethodsWe studied PST3093 for its effects on SERCA2a and Na+/K+ ATPase activities, Ca2+ dynamics in isolated myocytes and hemodynamic effects in an in-vivo rat model of diabetic (streptozotocin (STZ)-induced) cardiomyopathy.ResultsIstaroxime infusion in HF patients led to accumulation of PST3093 in the plasma; clearance was substantially slower for PST3093 than for istaroxime. In cardiac rat preparations PST3093 did not inhibit the Na+/K+ ATPase activity, but retained SERCA2a stimulatory activity. In in-vivo echocardiographic assessment, PST3093 improved overall cardiac performance and reversed most STZ-induced abnormalities. PST3093 i.v. toxicity was considerably lower than that of istaroxime and it failed to significantly interact with 50 off-targets.ConclusionsOverall, PST3093 is a “selective” SERCA2a activator, the prototype of a novel pharmacodynamic category with a potential in the ino-lusitropic approach to HF with prevailing diastolic dysfunction. Its pharmacodynamics are peculiar and its pharmacokinetics are suitable to prolong the cardiac beneficial effect of istaroxime infusion.Graphical abstract

Published

2022

7. Highly Selective SERCA2a Activators: Preclinical Development of a Congeneric Group of First-in-Class Drug Leads against Heart Failure

Author

Andrea Luraghi, Mara Ferrandi, Paolo Barassi, Martina Arici, Shih-Che Hsu, Eleonora Torre, Carlotta Ronchi, Alessio Romerio, Gwo-Jyh Chang, Patrizia Ferrari, Giuseppe Bianchi, Antonio Zaza, Marcella Rocchetti, Francesco Peri, Luraghi, A, Ferrandi, M, Barassi, P, Arici, M, Hsu, S, Torre, E, Ronchi, C, Romerio, A, Chang, G, Ferrari, P, Bianchi, G, Zaza, A, Rocchetti, M, and Peri, F

Subjects

Heart Failure, Drug Discovery, Guinea Pigs, Molecular Medicine, Animals, Arrhythmias, Cardiac, Calcium, Myocytes, Cardiac, Medicinal chemistry, drug development, hearth failure, Serca 2a, steroids, istaroxime, Rats, Sarcoplasmic Reticulum Calcium-Transporting ATPases

Abstract

The stimulation of sarcoplasmic reticulum calcium ATPase SERCA2a emerged as a novel therapeutic strategy to efficiently improve overall cardiac function in heart failure (HF) with reduced arrhythmogenic risk. Istaroxime is a clinical-phase IIb compound with a double mechanism of action, Na+/K+ ATPase inhibition and SERCA2a stimulation. Starting from the observation that istaroxime metabolite PST3093 does not inhibit Na+/K+ ATPase while stimulates SERCA2a, we synthesized a series of bioisosteric PST3093 analogues devoid of Na+/K+ ATPase inhibitory activity. Most of them retained SERCA2a stimulatory action with nanomolar potency in cardiac preparations from healthy guinea pigs and streptozotocin (STZ)-treated rats. One compound was further characterized in isolated cardiomyocytes, confirming SERCA2a stimulation and in vivo showing a safety profile and improvement of cardiac performance following acute infusion in STZ rats. We identified a new class of selective SERCA2a activators as first-in-class drug candidates for HF treatment.

Published

2022

8. Highly Selective SERCA2a Activators: Preclinical Development of a Congeneric Group of First-in-Class Drug Leads against Heart Failure

Author

Luraghi, A, Ferrandi, M, Barassi, P, Arici, M, Hsu, S, Torre, E, Ronchi, C, Romerio, A, Chang, G, Ferrari, P, Bianchi, G, Zaza, A, Rocchetti, M, Peri, F, Andrea Luraghi, Mara Ferrandi, Paolo Barassi, Martina Arici, Shih-Che Hsu, Eleonora Torre, Carlotta Ronchi, Alessio Romerio, Gwo-Jyh Chang, Patrizia Ferrari, Giuseppe Bianchi, Antonio Zaza, Marcella Rocchetti, Francesco Peri, Luraghi, A, Ferrandi, M, Barassi, P, Arici, M, Hsu, S, Torre, E, Ronchi, C, Romerio, A, Chang, G, Ferrari, P, Bianchi, G, Zaza, A, Rocchetti, M, Peri, F, Andrea Luraghi, Mara Ferrandi, Paolo Barassi, Martina Arici, Shih-Che Hsu, Eleonora Torre, Carlotta Ronchi, Alessio Romerio, Gwo-Jyh Chang, Patrizia Ferrari, Giuseppe Bianchi, Antonio Zaza, Marcella Rocchetti, and Francesco Peri

Abstract

The stimulation of sarcoplasmic reticulum calcium ATPase SERCA2a emerged as a novel therapeutic strategy to efficiently improve overall cardiac function in heart failure (HF) with reduced arrhythmogenic risk. Istaroxime is a clinical-phase IIb compound with a double mechanism of action, Na+/K+ ATPase inhibition and SERCA2a stimulation. Starting from the observation that istaroxime metabolite PST3093 does not inhibit Na+/K+ ATPase while stimulates SERCA2a, we synthesized a series of bioisosteric PST3093 analogues devoid of Na+/K+ ATPase inhibitory activity. Most of them retained SERCA2a stimulatory action with nanomolar potency in cardiac preparations from healthy guinea pigs and streptozotocin (STZ)-treated rats. One compound was further characterized in isolated cardiomyocytes, confirming SERCA2a stimulation and in vivo showing a safety profile and improvement of cardiac performance following acute infusion in STZ rats. We identified a new class of selective SERCA2a activators as first-in-class drug candidates for HF treatment.

Published

2022

9. Antihypertensive treatment guided by genetics: PEARL-HT, the randomized proof-of-concept trial comparing rostafuroxin with losartan

Author

Mara Ferrandi, Daniele Cusi, Tzung-Dau Wang, Patrizia Ferrari, Roberto Bigazzi, Jan A. Staessen, Lit Fui Lau, Kang Ling Wang, Chern En Chiang, Giuseppe A. Scioli, Giuseppe Bianchi, Nicola Glorioso, Li Xiaoyi, Chiara Lanzani, Silvio Cavuto, Paolo Manunta, Lorena Citterio, Citterio, L., Bianchi, G., Scioli, G. A., Glorioso, N., Bigazzi, R., Cusi, D., Staessen, J. A., Cavuto, S., Ferrandi, M., Lanzani, C., Li, X., Lau, L. -F., Chiang, C. -E., Wang, T. -D., Wang, K. -L., Ferrari, P., and Manunta, P.

Subjects

0301 basic medicine, Male, Blood Pressure, 030204 cardiovascular system & hematology, 0302 clinical medicine, Clinical endpoint, Pharmacology & Pharmacy, Ouabain, Genetics & Heredity, Genetics, Disease genetics, Middle Aged, Asians, Losartan, ADD1, Cardiovascular diseases, Treatment Outcome, Italy, ADD3, Hypertension, Molecular Medicine, Female, Life Sciences & Biomedicine, medicine.drug, Adult, Taiwan, Predictive markers, White People, Article, 03 medical and health sciences, Asian People, Double-Blind Method, medicine, Humans, Androstanols, Genetic Testing, OSBP, Antihypertensive Agents, Genetic association study, Pharmacology, Science & Technology, Genetic heterogeneity, business.industry, Whites, Gene Expression Profiling, 030104 developmental biology, Blood pressure, Pharmacogenetics, Pharmacogenomics, business

Abstract

We compared a standard antihypertensive losartan treatment with a pharmacogenomics-guided rostafuroxin treatment in never-treated Caucasian and Chinese patients with primary hypertension. Rostafuroxin is a digitoxigenin derivative that selectively disrupts the binding to the cSrc-SH2 domain of mutant α-adducin and of the ouabain-activated Na-K pump at 10–11 M. Of 902 patients screened, 172 were enrolled in Italy and 107 in Taiwan. After stratification for country and genetic background, patients were randomized to rostafuroxin or losartan, being the difference in the fall in office systolic blood pressure (OSBP) after 2-month treatment the primary endpoint. Three pharmacogenomic profiles (P) were examined, considering: P1, adding to the gene variants included in the subsequent P2, the variants detected by post-hoc analysis of a previous trial; P2, variants of genes encoding enzymes for endogenous ouabain (EO) synthesis (LSS and HSD3B1), EO transport (MDR1/ABCB1), adducin (ADD1 and ADD3); P3, variants of the LSS gene only. In Caucasians, the group differences (rostafuroxin 50 μg minus losartan 50 mg in OSBP mmHg) were significant both in P2 adjusted for genetic heterogeneity (P2a) and P3 LSS rs2254524 AA [9.8 (0.6–19.0), P = 0.038 and 13.4 (25.4–2.5), P = 0.031, respectively]. In human H295R cells transfected with LSS A and LSS C variants, the EO production was greater in the former (P = 0.038); this difference was abolished by rostafuroxin at 10–11 M. Chinese patients had a similar drop in OSBP to Caucasians with losartan but no change in OSBP with rostafuroxin. These results show that genetics may guide drug treatment for primary hypertension in Caucasians.

Published

2021

10. Abstract P118: Antihypertensive Treatment Guided By Genetics: Pearl-ht, The Randomized Proof-of-concept Trial Comparing Rostafuroxin With Losartan

Author

Daniele Cusi, Patrizia Ferrari, Paolo Manunta, Lorena Citterio, Mara Ferrandi, Kang-Ling Wang, Chern-En Chiang, Chiara Lanzani, and Giuseppe Bianchi

Subjects

Losartan, business.industry, Rostafuroxin, Pharmacogenomics, Internal Medicine, engineering, Medicine, engineering.material, Pharmacology, business, Pearl, Angiotensin II, medicine.drug

Abstract

Primary hypertension contributes to more than 50% of all the worldwide cardiovascular deaths. Current antihypertensive therapy is still targeting the physiological mechanisms regulating blood pressure, but not the “causal” ones. So far, genetic studies have been unable to prove gene causation in human primary hypertension. In this study we compared a standard antihypertensive losartan treatment with a pharmacogenomics-guided rostafuroxin treatment in never-treated Caucasian and Chinese patients with primary hypertension (PEARL-HT trial registration: EudraCT: 2010-022073-34, ClinicalTrials.gov: NCT01320397). Rostafuroxin is a digitoxigenin derivative that selectively disrupts the binding to the cSrc-SH2 domain of mutant α-adducin and of the ouabain-activated Na-K pump at 10 -11 M. Of 902 patients screened, 172 were enrolled in Italy and 107 in Taiwan. After stratification for country and genetic background, patients were randomized to rostafuroxin or losartan, being the difference in the fall in Office Systolic Blood Pressure (OSBP) after two-month treatment the primary endpoint. Three pharmacogenomic profiles (P) were examined, considering: P1, adding to the gene variants included in the subsequent P2, the variants detected by post-hoc analysis of a previous trial; P2, variants of genes encoding enzymes for endogenous ouabain (EO) synthesis ( LSS and HSD3B1 ), EO transport ( MDR1/ABCB1 ), adducin ( ADD1 and ADD3 ); P3, variants of the LSS gene only. In Caucasians, the group differences (rostafuroxin 50 μg minus losartan 50 mg in OSBP mmHg) were significant both in P2 adjusted for genetic heterogeneity (P2a) and P3 LSS rs2254524 AA [9.8 (0.6-19.0), P =0.038 and 13.4 (25.4-2.5), P =0.031, respectively]. In human H295R cells transfected with LSS A and LSS C variants, the EO production was greater in the former ( P =0.038); this difference was abolished by rostafuroxin at 10 -11 M. Chinese patients had a similar drop in OSBP to Caucasians with losartan but no change in OSBP with rostafuroxin. These results show that the selective blockade of mutant adducin and endogenous ouabain pressor mechanisms by rostafuroxin improves the therapy of primary hypertension in in Caucasians carriers of the related gene variants.

Published

2020

11. Istaroxime stimulates SERCA2a and accelerates calcium cycling in heart failure by relieving phospholamban inhibition

Author

Giuseppe Bianchi, Maria Rosa Moncelli, Isabella Molinari, Cristina Reina, Francesco Tadini-Buoninsegni, Paolo Barassi, Gianluca Bartolommei, Mara Ferrandi, Maria Grazia Tripodi, and Patrizia Ferrari

Subjects

Pharmacology, Inotrope, medicine.medical_specialty, Lusitropy, SERCA, business.industry, chemistry.chemical_element, Calcium, medicine.disease, Phospholamban, Contractility, Istaroxime, Endocrinology, chemistry, Heart failure, Internal medicine, medicine, business

Abstract

Background and Purpose Calcium handling is known to be deranged in heart failure. Interventions aimed at improving cell Ca2+ cycling may represent a promising approach to heart failure therapy. Istaroxime is a new luso-inotropic compound that stimulates cardiac contractility and relaxation in healthy and failing animal models and in patients with acute heart failure (AHF) syndrome. Istaroxime is a Na-K ATPase inhibitor with the unique property of increasing sarcoplasmic reticulum (SR) SERCA2a activity as shown in heart microsomes from humans and guinea pigs. The present study addressed the molecular mechanism by which istaroxime increases SERCA2a activity.

Published

2013

12. Ouabain Contributes to Kidney Damage in a Rat Model of Renal Ischemia-Reperfusion Injury

Author

Isabella Molinari, Roberta Buono, Paolo Manunta, Mara Ferrandi, Fabio Benigni, Luca Villa, Francesco Montorsi, Arianna Bettiga, Giorgia Colciago, Masami Ikehata, Maria Pia Rastaldi, Andrea Salonia, Elisabetta Messaggio, Villa, Luca, Buono, Roberta, Ferrandi, Mara, Molinari, Isabella, Benigni, Fabio, Bettiga, Arianna, Colciago, Giorgia, Ikehata, Masami, Messaggio, Elisabetta, Rastaldi, Maria Pia, Montorsi, Francesco, Salonia, Andrea, and Manunta, Paolo

Subjects

Kidney Disease, medicine.medical_treatment, Rostafuroxin, renal damage, 030204 cardiovascular system & hematology, urologic and male genital diseases, Kidney, Nephrectomy, Ouabain, Catalysi, lcsh:Chemistry, Rats, Sprague-Dawley, 0302 clinical medicine, lcsh:QH301-705.5, Saline, Spectroscopy, warm ischemia, Warm ischemia, biology, Chemistry, Communication, ouabain, Computer Science Applications1707 Computer Vision and Pattern Recognition, General Medicine, nephrin, Na-K ATPase, Computer Science Applications, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Reperfusion Injury, Kidney Diseases, medicine.drug, medicine.medical_specialty, Catalysis, Androstanol, Nephrin, Inorganic Chemistry, 03 medical and health sciences, Internal medicine, medicine, Renal damage, Animals, Androstanols, Na+/K+-ATPase, Physical and Theoretical Chemistry, Molecular Biology, Renal ischemia, Animal, urogenital system, Organic Chemistry, medicine.disease, Rats, rostafuroxin, Endocrinology, lcsh:Biology (General), lcsh:QD1-999, biology.protein, Rat, Kidney disease

Abstract

Warm renal ischemia performed during partial nephrectomy has been found to be associated with kidney disease. Since endogenous ouabain (EO) is a neuro-endocrine hormone involved in renal damage, we evaluated the role of EO in renal ischemia-reperfusion injury (IRI). We measured plasma and renal EO variations and markers of glomerular and tubular damage (nephrin, KIM-1, Kidney-Injury-Molecule-1, α1 Na-K ATPase) and the protective effect of the ouabain inhibitor, rostafuroxin. We studied five groups of rats: (1) normal; (2) infused for eight weeks with ouabain (30 µg/kg/day, OHR) or (3) saline; (4) ouabain; or (5) saline-infused rats orally treated with 100 µg/kg/day rostafuroxin for four weeks. In group 1, 2–3 h after IRI, EO increased in ischemic kidneys while decreased in plasma. Nephrin progressively decreased and KIM-1 mRNA increased starting from 24 h. Ouabain infusion (group 2) increased blood pressure (from 111.7 to 153.4 mmHg) and ouabain levels in plasma and kidneys. In OHR ischemic kidneys at 120 h from IRI, nephrin, and KIM-1 changes were greater than those detected in the controls infused with saline (group 3). All these changes were blunted by rostafuroxin treatment (groups 4 and 5). These findings support the role of EO in IRI and suggest that rostafuroxin pre-treatment of patients before partial nephrectomy with warm ischemia may reduce IRI, particularly in those with high EO.

Published

2016

13. Mutation in the beta adducin subunit causes tissue-specific damage to myogenic tone

Author

Kazuhiko Sonoyama, Antonio Schiavone, Mara Ferrandi, Patrizia Ferrari, Rosella Micheletti, Anthony M. Heagerty, Grazia Tripodi, Adam Greenstein, Reza Aghamohammadzadeh, and Sarah B Withers

Subjects

medicine.medical_specialty, Physiology, Protein subunit, Cerebral arteries, Blood Pressure, Phenylephrine, Renal Artery, Internal medicine, medicine.artery, Internal Medicine, medicine, Animals, Renal artery, Kidney, Proteinuria, Electrical impedance myography, business.industry, Age Factors, Endothelial Cells, Rats, medicine.anatomical_structure, Endocrinology, Blood pressure, Organ Specificity, Vasoconstriction, Mutation, Calmodulin-Binding Proteins, medicine.symptom, Cardiology and Cardiovascular Medicine, business

Abstract

Damage to renal artery myogenic tone is universally associated with progressive kidney damage. Recently, we have observed that mutations in the beta adducin subunit are associated with proteinuria in the Milan rat. Because of the role of adducin as a component of the cytoskeleton we hypothesized that this mutation may be associated with changes in myogenic tone.Congenic rats were generated with beta adducin subunit mutation (NB rats) and compared with a previously studied rat model with alpha adducin subunit mutation (NAs rats). Blood pressure and urinary protein excretion were studied at two time points: 6 weeks and 4 months of age, and at these time points, small renal, middle cerebral and skeletal (cremaster) arteries were isolated and studied using pressure myography. Agonist-induced vasoconstriction was not different between the two groups at any age. However, myogenic tone in renal arteries was significantly damaged in the NB rat compared to its NAs counterpart and this was associated with a decrease in vascular distensibility. There was a smaller reduction in myogenic tone in the middle cerebral arteries from the NB rat, whereas in the skeletal arteries there was no difference between the two strains. In the NB rat, this tissue-specific damage to myogenic tone was associated with progressive proteinuria despite lower blood pressure than the NAs rat.Mutations in the beta subunit of the adducin protein result in damage to renal artery myogenic tone and this is associated with renal damage as manifest by proteinuria.

Published

2011

14. Personalized Therapy of Hypertension: the Past and the Future

Author

Mara Ferrandi, Daniele Cusi, Paolo Manunta, Patrizia Ferrari, Jan A. Staessen, Giuseppe Bianchi, Manunta, Paolo, Ferrandi, Mara, Cusi, Daniele, Ferrari, Patrizia, Staessen, Jan, and Bianchi, Giuseppe

Subjects

0301 basic medicine, Candidate gene, Rostafuroxin, Mutant, Genome-wide association study, Personalized therapy, Bioinformatics, Essential hypertension, Pharmacogenomic, 03 medical and health sciences, Genetic, Internal Medicine, Genetics, Animals, Humans, Medicine, GWAS, Genetic Testing, Precision Medicine, Gene, Antihypertensive Agents, Endogenous ouabain, Animal, business.industry, Sodium, Adducin, medicine.disease, Clinical trial, Antihypertensive Agent, 030104 developmental biology, Pharmacogenomics, Hypertension, Personalized medicine, Kidney cross-transplantation, business, Human

Abstract

During the past 20 years, the studies on genetics or pharmacogenomics of primary hypertension provided interesting results supporting the role of genetics, but no actionable finding ready to be translated into personalized medicine. Two types of approaches have been applied: a "hypothesis-driven" approach on the candidate genes, coding for proteins involved in the biochemical machinery underlying the regulation of BP, and an "unbiased hypothesis-free" approach with GWAS, based on the randomness principles of frequentist statistics. During the past 10-15 years, the application of the latter has overtaken the application of the former leading to an enlargement of the number of previously unknown candidate loci or genes but without any actionable result for the therapy of hypertension. In the present review, we summarize the results of our hypothesis-driven approach based on studies carried out in rats with genetic hypertension and in humans with essential hypertension at the pre-hypertensive and early hypertensive stages. These studies led to the identification of mutant adducin and endogenous ouabain as candidate genetic-molecular mechanisms in both species. Rostafuroxin has been developed for its ability to selectively correct Na(+) pump abnormalities sustained by the two abovementioned mechanisms and to selectively reduce BP in rats and in humans carrying the gene variants underlying the mutant adducin and endogenous ouabain (EO) effects. A clinical trial is ongoing to substantiate these findings. Future studies should apply both the candidate gene and GWAS approaches to fully exploit the potential of genetics in optimizing the personalized therapy.

Published

2016

15. Istaroxime, a Stimulator of Sarcoplasmic Reticulum Calcium Adenosine Triphosphatase Isoform 2a Activity, as a Novel Therapeutic Approach to Heart Failure

Author

Fiorentina Palazzo, Giuseppe Bianchi, Mara Ferrandi, Paolo Barassi, Oberdan Parodi, Giuseppe Giacalone, Patrizia Ferrari, Antonio Schiavone, Barbara Moro, and R. Micheletti

Subjects

Cardiac function curve, medicine.medical_specialty, Cardiotonic Agents, SERCA, Guinea Pigs, chemistry.chemical_element, Calcium, Muscle, Smooth, Vascular, Sarcoplasmic Reticulum Calcium-Transporting ATPases, Internal medicine, Etiocholanolone, Animals, Humans, Medicine, Heart Failure, business.industry, medicine.disease, Adenosine, Enzyme Activation, Transplantation, Endocrinology, Istaroxime, chemistry, Heart failure, cardiovascular system, Cardiology, Sodium-Potassium-Exchanging ATPase, Cardiology and Cardiovascular Medicine, business, Isovolumic relaxation time, medicine.drug

Abstract

Interventions involving calcium cycling may represent a promising approach to heart failure (HF) therapy because calcium handling is known to be deranged in human and experimental HF. Istaroxime is a sodium-potassium adenosine triphosphatase (ATPase) inhibitor with the unique property of increasing sarcoplasmic reticulum calcium ATPase (SERCA) isoform 2a (SERCA2a) activity. Because this was demonstrated in normal experimental models, we investigated whether istaroxime is able to improve global cardiac function and stimulate SERCA in failing hearts. In guinea pigs with 3-month aortic banding (AoB), echocardiographic results showed that istaroxime intravenous infusion (0.11 mg/kg per min) significantly increased both indices of contraction and relaxation (fractional shortening, +18+/-3.7%; aortic flow rate, +19+/-2.9%; peak myocardial systolic velocity, +36+/-7%; circumferential fiber shortening, +24+/-4.1%; peak atrial flow velocity, +69+/-8.6%; isovolumic relaxation time, +19+/-6.9%; and peak myocardial early diastolic velocity, +42+/-12%). In left ventricular sarcoplasmic reticulum microsomes from AoB animals, 100 nmol/L istaroxime normalized the depressed (-32%) SERCA2a maximum velocity and increased SERCA activity (+17%). In muscle strips from hearts from patients undergoing cardiac transplantation, istaroxime (0.1-1.0 micromol/L) increased (in a concentration-dependent manner) developed tension, the maximum and minimum first derivative of tension, and absolute velocity of contraction, while stimulating SERCA activity in sarcoplasmic reticulum microsomes at physiologic free calcium concentrations. In conclusion, istaroxime is presently the only available compound that stimulates SERCA2a activity and produces a luso-inotropic effect in HF.

Published

2007

16. A Primary Kidney Abnormality in Essential Hypertension1

Author

Giuseppe Bianchi, Mara Ferrandi, Daniele Cusi, E. Niutta, Grazia Tripodi, Giuseppe Vezzoli, Cristina Barlassina, Ettore Guidi, Patrizia Ferrari, and Sergio Salardi

Subjects

Kidney, medicine.medical_specialty, medicine.anatomical_structure, Primary (chemistry), business.industry, Internal medicine, medicine, Abnormality, Essential hypertension, medicine.disease, business

Published

2015

17. Ouabain Antagonists as Antihypertensive Agents

Author

P. Barassi, Mara Ferrandi, Isabella Molinari, E. Minotti, Patrizia Ferrari, Lucia Torielli, G. Tripodi, and Bianchi Giuseppe

Subjects

medicine.medical_specialty, Pharmacology, Essential hypertension, Ouabain, Muscle hypertrophy, Rats, Inbred SHR, Internal medicine, Drug Discovery, medicine, Animals, Humans, Androstanols, Na+/K+-ATPase, Receptor, Antihypertensive Agents, Renal sodium reabsorption, business.industry, medicine.disease, Rats, Endocrinology, Blood pressure, Mechanism of action, Hypertension, Sodium-Potassium-Exchanging ATPase, medicine.symptom, business, medicine.drug

Abstract

The evidence that high levels of endogenous ouabain (EO), a closely related isomer of ouabain, are implicated in human hypertension and cardiac hypertrophy and failure stimulated the pharmacological research for developing novel anti-hypertensive agents active as ouabain antagonists. The pathogenetic mechanisms through which increased EO levels affect cardiovascular system involve the modulation of Na-K ATPase, the key enzyme responsible for renal tubular sodium reabsorption and the activation of signalling transduction pathways implicated in growth-related gene transcription. By studying both genetic and experimental rat models of hypertension and comparing them with humans, our group has demonstrated that elevated levels of circulating EO and the genetic polymorphism of the cytoskeletal protein adducin associate with hypertension and high renal Na-K pump activity. Ouabain itself induces hypertension and up-regulates renal Na-K pump when chronically infused at low doses into rats (OS). In renal cultured cells, either incubated for several days with nanomolar concentrations of ouabain or transfected with the hypertensive adducin genetic variant, the Na-K pump results enhanced. Moreover, both EO and adducin polymorphism affect cardiac complications associated to hypertension, the former through the activation of a signalling transduction pathway. As a consequence, a compound able to interact with the cellular and molecular alterations, sustained by EO or mutated adducin, may represent the suitable treatment for those patients in whom these mechanisms are at work. A new antihypertensive compound, PST 2238, that selectively antagonises the pressor effect and the alteration of renal Na-K pump, sustained both by ouabain and adducin polymorphism, is described. A selective ability of PST 2238 to antagonise the ouabain-induced organ hypertrophy is also documented. The specificity of PST 2238 mechanism of action is supported by the absence of interactions with receptors or hormones involved in blood pressure regulation and by the lack of diuretic activity and diuretic-associated side effects. It is concluded that this compound could be useful for the treatment of those forms of essential hypertension in which renal Na handling alterations and cardiac complications are associated with either increased EO levels and/or adducin polymorphism.

Published

2005

18. Effect of Add1 gene transfer on blood pressure in reciprocal congenic strains of Milan rats

Author

Heike Zimdahl, Monica Florio, Patrizia Ferrari, Mara Ferrandi, Rossana Modica, Giuseppe Bianchi, Norbert Hubner, and Grazia Tripodi

Subjects

Male, medicine.medical_specialty, Genetic Linkage, Biophysics, Congenic, Blood Pressure, Biology, Quantitative trait locus, Biochemistry, Chromosomes, Animals, Congenic, Genetic linkage, Internal medicine, medicine, Animals, Humans, Molecular Biology, Gene, Crosses, Genetic, Genetics, Models, Genetic, Gene Transfer Techniques, Chromosome Mapping, DNA, Cell Biology, Rats, DNA-Binding Proteins, Blood pressure, Endocrinology, ADD1, ADD3, ADD2, Hypertension, CCAAT-Enhancer-Binding Proteins, Calmodulin-Binding Proteins, Female, Sterol Regulatory Element Binding Protein 1, Transcription Factors

Abstract

Genetic variants of alpha adducin (ADD1) taken alone or in interaction with those of beta (ADD2) and gamma (ADD3) subunits have been associated with primary hypertension in humans and in Milan hypertensive (MHS) rats. In this study, we report the dissection of the individual contribution of each rat Add gene to blood pressure, by congenic substitution mapping. Congenic strains were developed by introgressing Add1, Add2, and Add3 genes (and chr14, chr4, and chr1 associated segments) of MHS in the Milan normotensive rat (MNS) genetic background (MNS.H-Add1, MNS.H-Add2, and MNS.H-Add3) and vice versa (MHS.N-Add1, MHS.N-Add2, and MHS.N-Add3). Systolic blood pressure (SBP) of MNS.H-Add1 rats was significantly higher (+10 mmHg) than that of MNS, whereas SBP of MHS.N-Add1 was significantly lower (-10 mmHg) than that of MHS. The differences account for 43% of the blood pressure differences between MHS and MNS. In contrast, SBPs of Add2 and Add3 congenic strains were not different from those of the correspondent recipient parental strain. The fine mapping of chr14 congenic segment supports the identity of blood pressure QTL with Add1 gene.

Published

2004

19. Organ Hypertrophic Signaling within Caveolae Membrane Subdomains Triggered by Ouabain and Antagonized by PST 2238

Author

Isabella Molinari, Mara Ferrandi, Patrizia Ferrari, Paolo Barassi, E. Minotti, and Giuseppe Bianchi

Subjects

Male, medicine.medical_specialty, Heart Ventricles, ATPase, Blood Pressure, Caveolae, Kidney, Biochemistry, Ouabain, Rats, Sprague-Dawley, chemistry.chemical_compound, In vivo, Internal medicine, medicine, Animals, Androstanols, Enzyme Inhibitors, Phosphorylation, Molecular Biology, Immunosorbent Techniques, Mitogen-Activated Protein Kinase 1, Mitogen-Activated Protein Kinase 3, biology, Tyrosine phosphorylation, Hypertrophy, Organ Size, Cell Biology, Rats, Enzyme Activation, src-Family Kinases, Endocrinology, chemistry, biology.protein, Tyrosine, Amlodipine, Mitogen-Activated Protein Kinases, Sodium-Potassium-Exchanging ATPase, Signal transduction, Signal Transduction, Proto-oncogene tyrosine-protein kinase Src, medicine.drug

Abstract

In addition to inhibition of the Na-K ATPase, ouabain activates a signal transduction function, triggering growth and proliferation of cultured cells even at nanomolar concentrations. An isomer of ouabain (EO) circulates in mammalians at subnanomolar concentrations, and increased levels are associated with cardiac hypertrophy and hypertension. We present here a study of cardiac and renal hypertrophy induced by ouabain infused into rats for prolonged periods and relate this effect to the recently described ouabain-induced activation of the Src-EGFr-ERK signaling pathway. Ouabain infusion into rats (15 microg/kg/day for 18 weeks) doubled plasma ouabain levels from 0.3 to 0.7 nm and increased blood pressure by 20 mm Hg (p < 0.001), cardiac left ventricle (+11%, p < 0.05), and kidney weight (+9%, p < 0.01). These effects in vivo are associated with a significant enrichment of alpha1, beta1, gammaa Na-K ATPase subunits together with Src and EGFr in isolated renal caveolae membranes and activation of ERK1/2. In caveolae, direct Na-K ATPase/Src interactions can be demonstrated by co-immunoprecipitation. The interaction is amplified by ouabain, at a high affinity binding site, detectable in caveolae but not in total rat renal membranes. The high affinity site for ouabain is associated with Src-dependent tyrosine phosphorylation of rat alpha1 Na-K ATPase. The antihypertensive compound, PST 2238, antagonized all ouabain-induced effects at 10 microg/kg/day in vivo or 10(-10)-10(-8) m in vitro. These findings provide a molecular mechanism for the in vivo pro-hypertrophic and hypertensinogenic activity of ouabain, or by analogy those of EO in humans. They also explain the pharmacological basis for PST 2238 treatment.

Published

2004

20. PST 2238: A New Antihypertensive Compound That Modulates Renal Na-K Pump Function Without Diuretic Activity in Milan Hypertensive Rats

Author

E. Minotti, Mara Ferrandi, Paolo Barassi, Isabella Molinari, Liliana Duzzi, Patrizia Ferrari, and Giuseppe Bianchi

Subjects

medicine.medical_specialty, medicine.medical_treatment, Blood Pressure, Kidney, Oral administration, Internal medicine, Renin–angiotensin system, medicine, Animals, Androstanols, Na+/K+-ATPase, Pharmacology, Reabsorption, business.industry, Lipid metabolism, Diuresis, Rats, Hydrochlorothiazide, Endocrinology, Blood pressure, Renal physiology, Hypertension, Sodium-Potassium-Exchanging ATPase, Diuretic, Cardiology and Cardiovascular Medicine, business

Abstract

PST 2238 is a new antihypertensive compound that is able to correct the molecular and functional alterations of the renal Na-K pump and the pressor effect associated with either alpha-adducin mutations or high circulating levels of endogenous ouabain (EO) in genetic and experimental rat models. Due to the close relationship between renal Na-K pump function and tubular Na reabsorption, PST 2238 was investigated to determine whether it is endowed with diuretic activity and consequently might trigger alterations of the renin-aldosterone system and the carbohydrate and lipid metabolism often associated with chronic diuretic therapy. In Milan hypertensive (MHS) rats, in which hypertension is genetically associated with alpha-adducin mutation, increased tubular Na reabsorption, and hyperactivation of the renal Na-K pump. PST 2238 reduced blood pressure and normalized the renal Na-K pump activity at oral doses of micro g/kg, but did not induce, either acutely or chronically, any diuretic activity or hormonal or metabolic alterations. In contrast, HCTZ, given to MHS rats orally at 40 mg/kg, although it displayed diuretic activity and reduced the renal Na-K pump activity, did not lower blood pressure and caused hyperactivation of the renin-aldosterone system, hypokaliemia, and hyperglycemia. The findings lead to the conclusion that PST 2238 is a new antihypertensive compound that normalizes the altered function of the renal Na-K pump associated with hypertension in rat models, but that it is devoid of diuretic activity and does not induce the diuretic-associated side effects.

Published

2002

21. SIK1 localizes with nephrin in glomerular podocytes and its polymorphism predicts kidney injury

Author

Isabella Molinari, G. Zerbini, Paolo Ferrari, Mara Ferrandi, M. Simonini, Laura Giardino, V. Matafora, Paolo Manunta, Maria Pia Rastaldi, F. Trevisani, Ferrandi, M., Molinari, I., Matafora, V., Zerbini, G., Trevisani, F., Rastaldi, M. P., Simonini, M., Giardino, L., Ferrari, P., and Manunta, P.

Subjects

medicine.medical_specialty, Kidney, biology, urogenital system, Kinase, ATPase, Mutant, Congenic, General Medicine, urologic and male genital diseases, female genital diseases and pregnancy complications, Ouabain, Podocyte, Nephrin, Endocrinology, medicine.anatomical_structure, Internal medicine, Genetics, medicine, biology.protein, Molecular Biology, Genetics (clinical), medicine.drug

Abstract

Mutant α-adducin and endogenous ouabain levels exert a causal role in hypertension by affecting renal Na-K ATPase. In addition, mutant β-adducin is involved in glomerular damage through nephrin down-regulation. Recently, the salt-inducible kinase 1 (SIK1) has been shown to exert a permissive role on mutant α-adducin effects on renal Na-K ATPase activity involved in blood pressure (BP) regulation and a SIK1 rs3746951 polymorphism has been associated with changes in vascular Na-K ATPase activity and BP. Here, we addressed the role of SIK1 on nephrin and glomerular functional modifications induced by mutant β-adducin and ouabain, by using congenic substrains of the Milan rats expressing either mutant α- or β-adducin, alone or in combination, ouabain hypertensive rats (OHR) and hypertensive patients. SIK1 co-localized and co-immunoprecipitated with nephrin from glomerular podocytes and associated with caveolar nephrin signaling. In cultured podocytes, nephrin-gene silencing decreased SIK1 expression. In mutant β-adducin congenic rats and in OHR, the podocyte damage was associated with decreased nephrin and SIK1 expression. Conversely, when the effects of β-adducin on podocytes were blocked by the presence of mutant α-adducin, nephrin and SIK1 expressions were restored. Ouabain effects were also reproduced in cultured podocytes. In hypertensive patients, nephrinuria, but not albuminuria, was higher in carriers of mutant SIK1 rs3746951 than in wild-type, implying a more direct effect of SIK1 on glomerular damage. These results demonstrate that, through nephrin, SIK1 is involved in the glomerular effects of mutant adducin and ouabain and a direct effect of SIK1 is also likely to occur in humans.

Published

2014

22. Late sodium current (INaL) in pancreatic β-cells

Author

Luca Sala, Federico Bertuzzi, Isabella Molinari, Alice Villa, Marcella Rocchetti, Riccardo Rizzetto, Mara Ferrandi, Carlotta Ronchi, Antonio Zaza, Rizzetto, R, Rocchetti, M, Sala, L, Ronchi, C, Villa, A, Ferrandi, M, Molinari, I, Bertuzzi, F, and Zaza, A

Subjects

medicine.medical_specialty, Potassium Channels, Time Factors, Physiology, medicine.medical_treatment, Clinical Biochemistry, Nerve Tissue Proteins, Voltage-Gated Sodium Channels, Potassium Channels, Sodium-Activated, Cell Line, Membrane Potentials, chemistry.chemical_compound, Tolbutamide, Ranolazine, BIO/09 - FISIOLOGIA, Internal medicine, Late sodium current, Physiology (medical), Insulin-Secreting Cells, Insulin Secretion, medicine, Potassium Channel Blockers, Animals, Humans, Hypoglycemic Agents, Insulin, Secretion, RNA, Messenger, Pancreatic β-cell, Membrane potential, Voltage-Gated Sodium Channel Blockers, geography, geography.geographical_feature_category, Sodium-activated potassium current, Sodium, Depolarization, Islet, Rats, Endocrinology, Glucose, chemistry, Tetrodotoxin, Veratridine, medicine.drug

Abstract

Recent evidence of beneficial effects of ranolazine (RAN) in type II diabetes motivates interest in the role of the late sodium current (INaL) in glucose-stimulated insulin secretion. In the present work, we characterize INaL and its function in rat INS-1E cells and human islets cells. INaL was identified as steady-state current blocked by 10 μM RAN (IRAN) or 0.5 μM tetrodotoxin (TTX) (ITTX). Veratridine (VERA, 40 μM) was used as INaL enhancer. Baseline INaL was similar between INS-1E and human islet cells. In INS-1E cells, activated by glucose or tolbutamide, TTX or RAN hyperpolarized membrane potential (V m). VERA-induced depolarization was countered by TTX or RAN. ITTX and IRAN reversal potentials were negative to Na+ equilibrium one, but they approached it after Na+ substitution with Li+ or when K+ channels were blocked. This revealed INaL coupling with Na+-activated K+ current (IKNa); expression of IKNa channels (Slick/Slack) was confirmed by transcript analysis and Western blot. RAN or TTX blunted cytosolic Ca2+ response to depolarization. Long-term incubation in high (33 mM) glucose (CHG) constitutively enhanced INaL. VERA immediately increased glucose-stimulated insulin secretion. CHG increased glucose-independent secretion instead and abolished the secretory response to glucose. RAN or TTX countered VERA- and CHG-induced changes in insulin secretion. Our study demonstrated that (1) INaL was expressed in insulin-secreting cells and coupled to IKNa; INaL affected cytosolic Ca2+ but, unless enhanced, barely contributed to glucose-stimulated insulin secretion (GSIS); and (2) sustained hyperglycemic stress enhanced INaL, which contributed to the attending increase of glucose-independent insulin “leak” and GSIS impairment.

Published

2014

23. Involvement of the Na+,K+-ATPase and its inhibitors in cardiovascular diseases

Author

Luisa Quadri and Mara Ferrandi

Subjects

Pharmacology, Inotrope, medicine.medical_specialty, Digoxin, biology, business.industry, Endogeny, Digitalis, General Medicine, medicine.disease, biology.organism_classification, Ouabain, Endocrinology, Dig, Heart failure, Internal medicine, Drug Discovery, medicine, Na+/K+-ATPase, business, medicine.drug

Abstract

+,K+-ATPase inhibitors have been shown to be effective in the treatment of congestive heart failure and cardiac arrhythmias. The Digitalis Investigation Group (DIG) trial has demonstrated that long-term digoxin treatment improves symptoms of congestive heart failure and the quality of life in patients and, unlike cyclic adenosine monophosphatase (cAMP) dependent positive inotropes, does not have a negative effect on survival. Recently, evidence has been provided that the Na+,K+-ATPase may also be functionally modulated by endogenous inhibitors, such as ouabain-like factor (OLF). Elevated OLF levels have been documented in pathological conditions, such as cardiovascular disorders and particular genetic or essential forms of human hypertension. Na+,K+-ATPase and OLF could represent a novel pharmacological target for the treatment of those forms of hypertension sustained by this mechanism. This review will cover patenting activity in this field of research and will focus on the more significant patents publi...

Published

1998

24. Role of The Ouabain-Like Factor and Na-K Pump in Rat and Human Genetic Hypertension

Author

Paolo Manunta, Mara Ferrandi, Patrizia Ferrari, Rodolfo Rivera, Giuseppe Bianchi, Ferrandi, M, Manunta, Paolo, Rivera, R, Bianchi, G, and Ferrari, P.

Subjects

Digoxin, medicine.medical_specialty, Physiology, Hypothalamus, Radioimmunoassay, Endogeny, Biology, Ouabain, Pathogenesis, Biological Factors, Rats, Inbred SHR, Internal medicine, Adrenal Glands, Internal Medicine, medicine, Animals, Humans, Enzyme Inhibitors, Na+/K+-ATPase, Chromatography, High Pressure Liquid, Ion transporter, Kidney, Biological activity, General Medicine, Saponins, Pathophysiology, Rats, Cardenolides, medicine.anatomical_structure, Endocrinology, Pituitary Gland, Hypertension, Sodium-Potassium-Exchanging ATPase, medicine.drug

Abstract

Endogenous ouabain-like factor (OLF) is present in mammal tissues and after standardized extraction procedure can be similarly quantified by two independent assays: RIA and Na-KATPase inhibition. OLF was quantified both from plasma and tissues obtained from MHS hypertensive and MNS normotensive rats, maintained under the same environmental and dietary conditions, and from plasma of healthy volunteers and essential hypertensive patients. OLF biochemical characterization shows that it behaves like ouabain except for a 1000-fold higher affinity for the ouabain low-affinity Na-KATPase isoforms than ouabain. Tissue and plasma levels of OLF are higher in MHS than in MNS rats and are not influenced by exogenous OLF sources. Plasma OLF is also increased in a subgroup of hypertensive patients. Both in rats and humans a primary cell membrane alteration affecting ion transports seems to be linked to the increased levels of OLF. An antihypertensive compound which selectively antagonizes the pressor effect of OLF and corrects the ion transport defect is under development and can represent a new pharmacological approach to the treatment of hypertension.

Published

1998

25. Quantitative proteomics reveals novel therapeutic and diagnostic markers in hypertension

Author

Laura Zagato, Gianpaolo Zerbini, Angela Bachi, Isabella Molinari, Mara Ferrandi, Paolo Manunta, Giovambattista Capasso, Simona Delli Carpini, Nunzia Casamassima, Chiara Lanzani, Francesco Trepiccione, Vittoria Matafora, Matafora, V, Zagato, L, Ferrandi, M, Molinari, I, Zerbini, G, Casamassima, N, Lanzani, C, DELLI CARPINI, S, Trepiccione, F, Manunta, Paolo, Bachi, A, Capasso, G., Matafora, Vittoria, Zagato, Laura, Ferrandi, Mara, Molinari, Isabella, Zerbini, Gianpaolo, Casamassima, Nunzia, Lanzani, Chiara, Delli Carpini, Simona, Trepiccione, Francesco, Bachi, Angela, and Capasso, Giovambattista

Subjects

BP, blood pressure, medicine.medical_specialty, Tamm–Horsfall protein, Urinary system, BMI, body mass index, Quantitative proteomics, Glomerular injury, Salt homeostasis, Bioinformatics, SBP, systolic BP, Pathology and Forensic Medicine, Nephrin, Pathogenesis, Physiology (medical), Internal medicine, GO, Gene Ontology, Quantitative proteomic, Uromodulin, medicine, MBP, mean BP, Stroke, Salt homeostasi, biology, Chemistry, SR, salt resistant, Regular Article, medicine.disease, DBP, diastolic BP, Endocrinology, MQ, MaxQuant, Urinary biomarker, Nephrinuria, biology.protein, Slit diaphragm, Albuminuria, SS, salt sensitive, Molecular Medicine, LC–MS/MS, liquid chromatography coupled to tandem mass spectrometry, Salt sensitive hypertension, medicine.symptom

Abstract

Hypertension is a prevalent disorder in the world representing one of the major risk factors for heart attack and stroke. These risks are increased in salt sensitive individuals. Hypertension and salt sensitivity are complex phenotypes whose pathophysiology remains poorly understood and, remarkably, salt sensitivity is still laborious to diagnose. Here we present a urinary proteomic study specifically designed to identify urinary proteins relevant for the pathogenesis of hypertension and salt sensitivity. Despite previous studies that underlined the association of UMOD gene variants with hypertension, this work provides novel evidence showing different uromodulin protein level in the urine of hypertensive patients compared to healthy individuals. Notably, we also show that patients with higher level of uromodulin are homozygous for UMOD risk variant and display a decreased level of salt excretion, highlighting the essential role of UMOD in the regulation of salt reabsorption in hypertension. Additionally, we found that urinary nephrin 1, a marker of glomerular slit diaphragm, may predict a salt sensitive phenotype and positively correlate with increased albuminuria associated with this type of hypertension., Highlights • We identified urinary proteins differently excreted in hypertensive patients. • Nephrin 1 might predict salt sensitive phenotype and glomerular complications. • Uromodulin impacts salt homeostasis in hypertension. • We provide new insights into the pathogenesis of hypertension and salt sensitivity.

Published

2014

26. Inal in the Pathophysiology of Insulin-Secretion: A 'Cardiac' Paradigm in a New Cell Type

Author

Alice Villa, Riccardo Rizzetto, Marcella Rocchetti, Mara Ferrandi, Luca Sala, Antonio Zaza, Carlotta Ronchi, and Isabella Molinari

Subjects

Membrane potential, medicine.medical_specialty, Chemistry, Biophysics, Ranolazine, Depolarization, Blockade, Cytosol, chemistry.chemical_compound, Endocrinology, Internal medicine, medicine, Patch clamp, Veratridine, Intracellular, medicine.drug

Abstract

BACKGROUND: enhancement of the sustained component of the sodium current (INaL) is a major factor contributing to myocardial damage. A beneficial effect of the INaL blocker Ranolazine (RAN) on glycemic control was recently described in the MERLIN-TIMI 36 trial in diabetic patients. However, the mechanism underlying this finding hasn't been elucidated yet.AIM: To characterize INaL in insulin-secreting cells (INS-1E) and evaluate its role in glucose-stimulated insulin secretion (GSIS).METHODS: INaL, identified as the steady-state current blocked by 10 μM RAN (IRAN) or 0.5 μM TTX (ITTX), and its impact on membrane potential (Vm) were assessed by patch clamp. Veratridine (VERA) was used as INaL enhancer. INaL-dependent intracellular Ca2+ changes were detected by Fluo-4AM. To simulate hyperglycemic stress (CHG), INS-1E cells were exposed to 33 mM glucose for 24 hrs. GSIS was measured by HTRF assay.RESULTS: Glucose- and tolbutamide-triggered action potentials were suppressed by TTX, but not by RAN. VERA caused depolarization, countered by INaL blockade. The reversal potentials of ITTX and IRAN were negative to Na+ equilibrium potential, but they approached it when K+-channels were blocked. This revealed INaL coupling to Na+-activated K+ current (IKNa); expression of IKNa channels (Slo2.1/2.2) was confirmed by transcript analysis. INaL blockade blunted cytosolic Ca2+ response to depolarization. CHG enhanced INaL. Whereas acute INaL enhancement (VERA) increased GSIS, chronic one (CHG or VERA) depressed GSIS, which was partially restored by RAN.CONCLUSIONS: INaL is expressed in insulin-secreting cells, is coupled to IKNa , affects Ca2+ signalling and, when enhanced acutely, increases GSIS. However, constitutive INaL enhancement, induced by chronic hyperglycemic stress, and leads to GSIS depression instead. Overall, chronic INaL enhancement may represent a mechanism of damage progression common to myocardial and insulin-secreting cells.

Published

2014

27. Ouabain-like Factor Quantification in Mammalian Tissues and Plasma

Author

Paolo Manunta, Mara Ferrandi, John M. Hamlyn, Patrizia Ferrari, Silvana Balzan, Giuseppe Bianchi, Ferrandi, M, Manunta, Paolo, Balzan, S, Hamlyn, Jm, Bianchi, G, and Ferrari, P.

Subjects

Male, Digoxin, medicine.medical_specialty, ATPase, Hypothalamus, Radioimmunoassay, High-performance liquid chromatography, Ouabain, Biological Factors, Dogs, Internal medicine, Adrenal Glands, Blood plasma, Methods, Internal Medicine, medicine, Animals, Humans, Enzyme Inhibitors, Na+/K+-ATPase, Chromatography, High Pressure Liquid, Antiserum, Chromatography, biology, Tissue Extracts, Chemistry, Immune Sera, Osmolar Concentration, Rats, Inbred Strains, Saponins, Rats, Cardenolides, Endocrinology, Polyclonal antibodies, Pituitary Gland, biology.protein, Sodium-Potassium-Exchanging ATPase, medicine.drug

Abstract

Abstract The resolution of controversies that concern the detectability of an endogenous ouabain-like factor (OLF) in mammalian tissues and plasma was approached by the application of a standardized method for its extraction and quantification. Two independent assays were used to quantify the OLF: (1) a radioimmunoassay, which used a polyclonal antiouabain antiserum, and (2) a radioenzymatic assay based on the inhibition of dog kidney Na + ,K + -ATPase. Plasma and tissues were obtained from the Milan hypertensive strain (MHS) and the Milan normotensive strain (MNS) of rats and from healthy human volunteers. Results indicate that (1) a single high-performance liquid chromatography (HPLC) fraction identical to that of ouabain was identified by both assay methods in the rat hypothalamus and hypophysis and in both rat and human plasma; (2) dilution curves of OLF and standard ouabain were parallel and with a similar K d , both in radioimmunoassay (3 nmol/L) and ATPase assay (14 nmol/L); (3) after HPLC, OLF was similarly quantified by the two methods in the hypothalamus, hypophysis, adrenals, and plasma of rats and in human plasma; (4) OLF was present in larger amounts in the hypothalamus, hypophysis, and plasma of MHS rats than that of MNS rats; (5) the HPLC fraction of human plasma was quantified similarly by both assays (range, 60 to 150 pmol/L); (6) recovery of standard ouabain in pre-HPLC plasma extracts was approximately 90%; and (7) pre-HPLC OLF concentrations in human plasma ranged between 0.05 and 0.75 nmol/L. Rat cerebral tissues and both rat and human plasma contained measurable amounts of OLF, which were quantified similarly by radioimmunoassay and ATPase assay, both before and after HPLC fractionation. The increased MHS tissue and plasma levels of OLF are in keeping with the pathogenetic role of this factor in MHS hypertension.

Published

1997

28. Istaroxime stimulates SERCA2a and accelerates calcium cycling in heart failure by relieving phospholamban inhibition

Author

Mara, Ferrandi, Paolo, Barassi, Francesco, Tadini-Buoninsegni, Gianluca, Bartolommei, Isabella, Molinari, Maria Grazia, Tripodi, Cristina, Reina, Maria Rosa, Moncelli, Giuseppe, Bianchi, and Patrizia, Ferrari

Subjects

Heart Failure, Male, Guinea Pigs, Calcium-Binding Proteins, In Vitro Techniques, Spodoptera, Research Papers, Sarcoplasmic Reticulum Calcium-Transporting ATPases, Sarcoplasmic Reticulum, Dogs, Microsomes, Etiocholanolone, cardiovascular system, Commentary, Animals, Humans, Calcium, Rabbits

Abstract

Calcium handling is known to be deranged in heart failure. Interventions aimed at improving cell Ca(2) (+) cycling may represent a promising approach to heart failure therapy. Istaroxime is a new luso-inotropic compound that stimulates cardiac contractility and relaxation in healthy and failing animal models and in patients with acute heart failure (AHF) syndrome. Istaroxime is a Na-K ATPase inhibitor with the unique property of increasing sarcoplasmic reticulum (SR) SERCA2a activity as shown in heart microsomes from humans and guinea pigs. The present study addressed the molecular mechanism by which istaroxime increases SERCA2a activity.To study the effect of istaroxime on SERCA2a-phospholamban (PLB) complex, we applied different methodologies in native dog healthy and failing heart preparations and heterologous canine SERCA2a/PLB co-expressed in Spodoptera frugiperda (Sf21) insect cells.We showed that istaroxime enhances SERCA2a activity, Ca(2) (+) uptake and the Ca(2) (+) -dependent charge movements into dog healthy and failing cardiac SR vesicles. Although not directly demonstrated, the most probable explanation of these activities is the displacement of PLB from SERCA2a.E2 conformation, independently from cAMP/PKA. We propose that this displacement may favour the SERCA2a conformational transition from E2 to E1, thus resulting in the acceleration of Ca(2) (+) cycling.Istaroxime represents the first example of a small molecule that exerts a luso-inotropic effect in the failing human heart through the stimulation of SERCA2a ATPase activity and the enhancement of Ca(2) (+) uptake into the SR by relieving the PLB inhibitory effect on SERCA2a in a cAMP/PKA independent way.

Published

2013

29. Renal Na,K-ATPase in Genetic Hypertension

Author

Mara Ferrandi, Monica Florio, Paolo Barassi, Sergio Salardi, Paolo Parenti, Steven J.D. Karlish, Patrizia Ferrari, Rossana Modica, Alla Shainskaya, Grazia Tripodi, Giuseppe Bianchi, Ferrandi, M, Tripodi, G, Salardi, S, Florio, M, Modica, R, Barassi, P, Parenti, P, Shainskaya, A, Karlish, S, Bianchi, G, and Ferrari, P

Subjects

Aging, medicine.medical_specialty, Sodium, Protein subunit, chemistry.chemical_element, Pathogenesis, Downregulation and upregulation, In vivo, Culture Techniques, Microsomes, Internal medicine, Internal Medicine, medicine, Animals, RNA, Messenger, Na+/K+-ATPase, Kidney Medulla, Kidney, Animal, Culture Technique, Microsome, BIO/10 - BIOCHIMICA, Rats, Endocrinology, medicine.anatomical_structure, chemistry, Hypertension, Rat, Sodium-Potassium-Exchanging ATPase

Abstract

Milan hypertensive rats (MHS) develop hypertension because of a primary renal alteration. Both apical and basolateral sodium transport are faster in membrane vesicles derived from renal tubules of MHS than in those of Milan normotensive control rats (MNS). These findings suggest that the increased renal sodium retention and concomitant development of hypertension in MHS may be linked to an altered transepithelial sodium transport. Since this transport is mainly under the control of the Na-K pump, we investigated whether an alteration of the enzymatic activity and/or protein expression of the renal Na,K-ATPase is detectable in prehypertensive MHS. We measured the Na,K-ATPase activity, Rb + occlusion, turnover number, α 1 - and β 1 -subunit protein abundance, and α 1 and β 1 mRNA levels in microsomes from renal outer medulla of young (prehypertensive) and adult (hypertensive) MHS and in age-matched MNS. In both young and adult MHS, the Na,K-ATPase activity was significantly higher because of an enhanced number of active pump sites, as determined by Rb + occlusion maximal binding. The higher number of pump sites was associated with a significant pretranslational increase of α 1 and β 1 mRNA levels that preceded the development of hypertension in MHS. Since a molecular alteration of the cytoskeletal protein adducin is genetically associated with hypertension in MHS and is able to affect the actin-cytoskeleton and Na-K pump activity in transfected renal cells, we propose that the in vivo upregulation of Na-K pump in MHS is primary and linked to a genetic alteration of adducin.

Published

1996

30. Preoperative Endogenous Ouabain Predicts Acute Kidney Injury in Cardiac Surgery Patients

Author

Chiara Lanzani, Elena Frati, Mara Ferrandi, John M. Hamlyn, Marco Simonini, Patrizia Ferrari, Ottavio Alfieri, Nunzia Casamassima, Elisabetta Messaggio, Alberto Zangrillo, Laura Corno, Keyur B. Shah, Giuseppe Bianchi, Elena Bignami, Paolo Manunta, Anna Mizzi, Stephen S. Gottlieb, Bignami, E, Casamassima, N, Frati, E, Lanzani, C, Corno, L, Alfieri, Ottavio, Gottlieb, S, Simonini, M, Shah, Kb, Mizzi, A, Messaggio, E, Zangrillo, Alberto, Ferrandi, M, Ferrari, P, Bianchi, G, Hamlyn, Jm, and Manunta, Paolo

Subjects

Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Urinary system, Urology, Renal function, Critical Care and Intensive Care Medicine, Essential hypertension, Article, Rats, Sprague-Dawley, chemistry.chemical_compound, Postoperative Complications, Predictive Value of Tests, medicine, Animals, Humans, Prospective Studies, Coronary Artery Bypass, Ouabain, Dialysis, Aged, Kidney, Creatinine, business.industry, Acute kidney injury, Acute Kidney Injury, Middle Aged, medicine.disease, Heart Valves, Surgery, Rats, medicine.anatomical_structure, chemistry, Models, Animal, Preoperative Period, Female, business, Biomarkers, Kidney disease

Abstract

Approximately 2 million cardiac surgeries are performed around the world each year. Acute kidney injury (AKI) is a frequent complication of cardiac surgery (1). Patients who double their serum creatinine or need acute dialysis have a two- to five-fold higher risk of death (2, 3), and patients who recover their kidney function remain at increased risk of chronic kidney disease (CKD) and premature death (4, 5). A number of novel plasma and urinary early postoperative biomarkers have recently been proposed to assess the risk of postoperative AKI on the assumption that early detection of renal damage may limit its progression to overt renal failure with appropriate therapeutic interventions (6). However, there are neither preoperative biomarkers nor robust validated risk models that predict AKI not requiring dialysis. Preoperative biomarkers offer the potential to target and develop therapeutic intervention aimed at blocking the initial sequence of events that lead to AKI (7). Certainly AKI is multifaceted in nature with derangements at various intrarenal sites (glomerular and tubular) and is triggered by a variety of factors including reduced cardiac output, systemic hypotension, and activation of neuroendocrine reflexes (8, 9). Endogenous ouabain (EO) is a neuroendocrine hormone that may contribute to the development of AKI in critically ill patients. Numerous human and intact animal studies, as well as adrenocortical cell culture studies, indicate that EO is synthesized in the adrenal cortex (10–13). EO may be considered a stress hormone secreted by the adrenal gland since a) normal rats after exposure to acute swim stress have significant increases of EO in plasma and adrenal glands (14); b) marked and rapid increases of plasma EO in humans during physical exercise have been reported (15); c) about 50% of humans with untreated essential hypertension have significantly elevated plasma EO that correlates directly with blood pressure (BP [16–18]); d) increased circulating EO has been related to cardiomyopathy (19) and decreased renal function (20, 21); and e) different types of endogenous glycosides, including EO, are elevated in a large proportion of critically ill patients. The occurrence of these substances is associated with increased morbidity and hospital mortality rates (22). EO modulates the activity of the Na,K-ATPase and induces signal transduction via sodium-calcium exchange and the Src-dependent pathway (23). EO exerts a biphasic effect on Na,K-ATPase, either stimulating or inhibiting its activity at low (subnanomolar) or high (nanomolar) concentrations, respectively (24, 25). The accumulating clinical and experimental data show that prolonged exposure to elevated levels of EO in vivo induces underlying kidney damage that is not clinically obvious. We propose that when individuals with elevated preoperative EO and with or without underlying kidney damage are exposed to the acute stress of surgery, further elevations of circulating EO occur and contribute directly to AKI. This hypothesis was tested in three settings: By measuring EO levels in patients before cardiac surgery and correlating these levels to the outcome after surgery including AKI; By infusing ouabain in rats and measuring BP, renal function, and podocyte proteins; By measuring podocyte proteins in primary culture incubated with and without ouabain. Therefore, the rationale underlying this approach was that high levels of EO may favor the development of AKI and do so by direct actions that lead to damage of podocytes.

Published

2013

31. Combining SERCA2a activation and Na-K ATPase inhibition: a promising new approach to managing acute heart failure syndromes with low cardiac output

Author

Mihai, Gheorghiade, Andrew P, Ambrosy, Mara, Ferrandi, and Patrizia, Ferrari

Subjects

Heart Failure, Etiocholanolone, Cardiac Output, Low, Animals, Humans, Sodium-Potassium-Exchanging ATPase, Models, Biological, Sarcoplasmic Reticulum Calcium-Transporting ATPases

Abstract

Heart failure (HF) patients are a medically complex and heterogeneous population with multiple cardiac and non-cardiac comorbidities. Although there are a multitude of etiologic substrates and initiating and amplifying mechanisms contributing to disease progression, these pathophysiologic processes ultimately all lead to impaired myocardial function. The myocardium must both pump oxygenated, nutrient-rich blood throughout the body (systolic function) and receive deoxygenated, nutrient-poor blood returning from the periphery (diastolic function). At the molecular level, it is well-established that Ca2+ plays a central role in excitation-contracting coupling with action potentials stimulating the opening of L-type Ca2+ in the plasma membrane and ryanodine receptor 2 (RyR2) in the sarcoplasmic reticulum (SR) membrane during systole and the Na-Ca2+ exchanger and SERCA2a returning Ca2+ to the extracellular space and SR, respectively, during diastole. However, there is increasing recognition that impaired Ca2+ cycling may contribute to myocardial dysfunction. Preclinical studies and clinical trials indicate that combining SERCA2a activation and Na-K ATPase inhibition may increase contractility (inotropy) and facilitate active relaxation (lusitropy), improving both systolic and diastolic functions. Istaroxime, a novel luso-inotrope that activates SERCA2a and inhibits the Na-K ATPase, is currently in phase II clinical development and has been shown to improve systolic and diastolic functions and central hemodynamics, increase systolic but not diastolic blood pressure, and decrease substantially heart rate. Irrespective of its clinical utility, the development of istaroxime has evolved our understanding of the clinical importance of inhibiting the Na-K ATPase in order to obtain a clinically significant effect from SERCA2a activation in the setting of myocardial failure.

Published

2011

32. NKCC2 is activated in Milan hypertensive rats contributing to the maintenance of salt-sensitive hypertension

Author

Federica Rizzo, Giovanna Valenti, Monica Carmosino, Patrizia Ferrari, Giuseppe Bianchi, Mara Ferrandi, Lucia Torielli, and Maria Svelto

Subjects

Male, medicine.medical_specialty, Physiology, Sodium-Potassium-Chloride Symporters, Clinical Biochemistry, Blood Pressure, Protein Serine-Threonine Kinases, Sodium Chloride, Urine, Kidney, Natriuresis, chemistry.chemical_compound, Furosemide, Physiology (medical), Internal medicine, medicine, Animals, Humans, Diuretics, Aldosterone, Solute Carrier Family 12, Member 1, urogenital system, Reabsorption, Chemistry, Kidney metabolism, Rats, Inbred Strains, Sodium, Dietary, Rats, Blood pressure, Endocrinology, medicine.anatomical_structure, Hypertension, Phosphorylation, medicine.drug

Abstract

The Milan hypertensive strain of rats (MHS) develops hypertension as a consequence of the increased tubular Na(+) reabsorption sustained by enhanced expression and activity of the renal tubular Na-K-ATPase. To verify whether the Na-K-2Cl cotransporter (NKCC2) is involved in the maintenance of hypertension in MHS rats, we have analysed the phosphorylation state and the activation of NKCC2 in Milan rats. Western blotting and immunofluorescence experiments were performed using specific antibodies against the regulatory phospho-threonines in the NKCC2 N terminus (R5 antibody). The phosphorylation levels of NKCC2 were significantly increased in the kidney of MHS rats. Moreover, the administration of furosemide in vivo decreased the blood pressure and increased the urine output and natriuresis in MHS rats demonstrating the actual involvement of NKCC2 activity in the pathogenesis of hypertension in this strain of rats. The up-regulation of NKCC2 activity is most probably mediated by a STE20/SPS1-related proline/alanine-rich kinase (SPAK) phosphorylation at serine-325 since it was significantly increased in MHS rats. Interestingly, aldosterone treatment caused an increase in NKCC2 phosphorylation in NKCC2-expressing MDCK cells. In conclusion, we demonstrated an increase in the activity of NKCC2 along the TAL that significantly contributes to the increase in systemic blood pressure in MHS rats. The elevated plasma levels of aldosterone, found in MHS rats, may influence Na(+) balance through a SPAK-dependent regulation of NKCC2 accounting for the maintenance of the hypertensive state in MHS rats.

Published

2010

33. A Correction to the Research Article Titled: 'Adducin- and Ouabain-Related Gene Variants Predict the Antihypertensive Activity of Rostafuroxin. Part 1: Experimental Studies' by Mara Ferrandi, Isabella Molinari, Lucia Torielli, Gloria Padoani, Sergio Salardi, Maria Pia Rastaldi, Patrizia Ferrari, Giuseppe Bianchi

Author

Lucia Torielli, Sergio Salardi, Patrizia Ferrari, Giuseppe Bianchi, Mara Ferrandi, Isabella Molinari, Gloria Padoani, and Maria Pia Rastaldi

Subjects

Rostafuroxin, business.industry, Translational medicine, Medicine, General Medicine, Pharmacology, Related gene, business, Ouabain, medicine.drug

Published

2010

34. Adducin- and ouabain-related gene variants predict the antihypertensive activity of rostafuroxin, part 1: experimental studies

Author

Mara Ferrandi, Isabella Molinari, Lucia Torielli, Gloria Padoani, Sergio Salardi, Maria Pia Rastaldi, Patrizia Ferrari, and Giuseppe Bianchi

Subjects

Male, Cell-Free System, Fluorescent Antibody Technique, Blood Pressure, General Medicine, Kidney, Transfection, Cell Line, Rats, Enzyme Activation, Rats, Sprague-Dawley, src Homology Domains, Protein Transport, src-Family Kinases, Animals, Humans, Calmodulin-Binding Proteins, Mutant Proteins, Androstanols, Sodium-Potassium-Exchanging ATPase, Ouabain, Antihypertensive Agents, Protein Binding, Signal Transduction

Abstract

Essential hypertension is a complex, multifactorial disease associated with a high cardiovascular risk and whose genetic-molecular basis is heterogeneous and largely unknown. Although multiple antihypertensive therapies are available, the large individual variability in drug response results in only a modest reduction of the cardiovascular risk and unsatisfactory control of blood pressure in the hypertensive population as a whole. Two mechanisms, among others, are associated with essential hypertension and related organ damage: mutant α-adducin variants and high concentrations of endogenous ouabain. An antihypertensive agent, rostafuroxin, selectively inhibits these mechanisms in rodents. We investigated the molecular and functional effects of mutant α-adducin, ouabain, and rostafuroxin in hypertensive rats, human cells, and cell-free systems and demonstrated that both mutant α-adducin variants and the ouabain-Na,K-ATPase (Na(+)- and K(+)-dependent adenosine triphosphatase) complex can interact with the Src-SH2 (Src homology 2) domain, increasing Src activity and the Src-dependent Na,K-ATPase phosphorylation and activity. Wild-type α-adducin or Na,K-ATPase in the absence of ouabain showed no interaction with the Src-SH2 domain. Rostafuroxin disrupted the interactions between the Src-SH2 domain and mutant α-adducin or the ouabain-Na,K-ATPase complex and blunted Src activation and Na,K-ATPase phosphorylation, resulting in blood pressure normalization in the hypertensive rats. We have also shown the translatability of these data to humans in a pharmacogenomic clinical trial, as described in the companion paper.

Published

2010

35. Adducin- and ouabain-related gene variants predict the antihypertensive activity of rostafuroxin, part 2: clinical studies

Author

Chiara Lanzani, Grazia Tripodi, Fabio Macciardi, Bianchi Giuseppe, Simona Delli Carpini, Erika Salvi, Paolo Manunta, Daniele Cusi, Mara Ferrandi, Elisabetta Messaggio, Giuseppe Argiolas, Giovanni Valentini, Lorena Citterio, Jan A. Staessen, Patrizia Ferrari, Nicola Glorioso, Lanzani, C, Citterio, L, Glorioso, N, Manunta, Paolo, Tripodi, G, Salvi, E, DELLI CARPINI, S, Ferrandi, M, Messaggio, E, Staessen, Ja, Cusi, D, Macciardi, F, Argiolas, G, Valentini, G, Ferrari, P, BIANCHI G., also on behalf of OASIS HT Investigators, Epidemiologie, and RS: CARIM School for Cardiovascular Diseases

Subjects

Male, medicine.medical_specialty, Time Factors, Systole, Population, Mutant, Blood Pressure, 030204 cardiovascular system & hematology, Pharmacology, Essential hypertension, Kidney, Transfection, Polymorphism, Single Nucleotide, Ouabain, Losartan, Placebos, 03 medical and health sciences, Enzyme activator, 0302 clinical medicine, Internal medicine, medicine, Humans, Androstanols, education, Intramolecular Transferases, Antihypertensive Agents, 030304 developmental biology, 0303 health sciences, education.field_of_study, business.industry, General Medicine, Middle Aged, medicine.disease, 3. Good health, Endocrinology, Hydrochlorothiazide, Genetic Loci, Hypertension, Phosphorylation, Calmodulin-Binding Proteins, Female, Mutant Proteins, Signal transduction, business, Proto-oncogene tyrosine-protein kinase Src, medicine.drug

Abstract

Twenty years of genetic studies have not contributed to improvement in the clinical management of primary arterial hypertension. Genetic heterogeneity, epistatic-environmental-biological interactions, and the pathophysiological complexity of hypertension have hampered the clinical application of genetic findings. In the companion article, we furnished data from rodents and human cells demonstrating two hypertension-triggering mechanisms-variants of adducin and elevated concentrations of endogenous ouabain (within a particular range)-and their selective inhibition by the drug rostafuroxin. Here, we have investigated the relationship between variants of genes encoding enzymes for ouabain synthesis [LSS (lanosterol synthase) and HSD3B1 (hydroxy-δ-5-steroid dehydrogenase, 3β- and steroid δ-isomerase 1)], ouabain transport {MDR1/ABCB1 [ATP-binding cassette, sub-family B (MDR/TAP), member 1]}, and adducin activity [ADD1 (adducin 1) and ADD3], and the responses to antihypertensive medications. We determined the presence of these variants in newly recruited, never-treated patients. The genetic profile defined by these variants predicted the antihypertensive effect of rostafuroxin (a mean placebo-corrected systolic blood pressure fall of 14 millimeters of mercury) but not that of losartan or hydrochlorothiazide. The magnitude of the rostafuroxin antihypertensive effect was twice that of antihypertensive drugs recently tested in phase 2 clinical trials. One-quarter of patients with primary hypertension display these variants of adducin or concentrations of endogenous ouabain and would be expected to respond to therapy with rostafuroxin. Because the mechanisms that are inhibited by rostafuroxin also underlie hypertension-related organ damage, this drug may also reduce the cardiovascular risk in these patients beyond that expected by the reduction in systolic blood pressure alone. ispartof: Science Translational Medicine vol:2 issue:59 ispartof: location:United States status: published

Published

2010

36. α- and β-Adducin polymorphisms affect podocyte proteins and proteinuria in rodents and decline of renal function in human IgA nephropathy

Author

Francesco Paolo Schena, Claudio Camisasca, Laura Giardino, Luanne L. Peters, Patrizia Ferrari, Maria Pia Rastaldi, Daniele Cusi, Paolo Manunta, Isabella Molinari, Cristina Barlassina, Silvia Armelloni, Li Min, Fiorentina Palazzo, Giuseppe Bianchi, Deborah Mattinzoli, Mara Ferrandi, Lucia Del Vecchio, Dario Roccatello, Carmelita Marcantoni, and Fabio Macciardi

Subjects

medicine.medical_specialty, Rodentia, 030204 cardiovascular system & hematology, Kidney, Kidney Function Tests, Nephropathy, Podocyte, Nephrin, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Drug Discovery, medicine, Animals, Humans, Genetics(clinical), Genetics (clinical), 030304 developmental biology, Glomerular disease, Medicine(all), 0303 health sciences, Polymorphism, Genetic, biology, Podocytes, Adducin, Genetic renal disease, Glomerulonephritis, IGA, Glomerulonephritis, IgA nephropathy, medicine.disease, Rats, 3. Good health, Proteinuria, medicine.anatomical_structure, Endocrinology, ADD2, Podocin, biology.protein, Molecular Medicine, Original Article, Calmodulin-Binding Proteins, Synaptopodin

Abstract

Adducins are cytoskeletal actin-binding proteins (α, β, γ) that function as heterodimers and heterotetramers and are encoded by distinct genes. Experimental and clinical evidence implicates α- and β-adducin variants in hypertension and renal dysfunction. Here, we have addressed the role of α- and β-adducin on glomerular function and disease using β-adducin null mice, congenic substrains for α- and β-adducin from the Milan hypertensive (MHS) and Milan normotensive (MNS) rats and patients with IgA nephropathy. Targeted deletion of β-adducin in mice reduced urinary protein excretion, preceded by an increase of podocyte protein expression (phospho-nephrin, synaptopodin, α-actinin, ZO-1, Fyn). The introgression of polymorphic MHS β-adducin locus into MNS (Add2, 529R) rats was associated with an early reduction of podocyte protein expression (nephrin, synaptopodin, α-actinin, ZO-1, podocin, Fyn), followed by severe glomerular and interstitial lesions and increased urinary protein excretion. These alterations were markedly attenuated when the polymorphic MHS α-adducin locus was also present (Add1, 316Y). In patients with IgA nephropathy, the rate of decline of renal function over time was associated to polymorphic β-adducin (ADD2, 1797T, rs4984) with a significant interaction with α-adducin (ADD1, 460W, rs4961). These findings suggest that adducin genetic variants participate in the development of glomerular lesions by modulating the expression of specific podocyte proteins. Electronic supplementary material The online version of this article (doi:10.1007/s00109-009-0549-x) contains supplementary material, which is available to authorized users.

Published

2010

37. Ouabainlike factor in Milan hypertensive rats

Author

Bianchi Giuseppe, Patrizia Ferrari, Sergio Salardi, Monica Florio, Mara Ferrandi, and E. Minotti

Subjects

Male, Digoxin, medicine.medical_specialty, Erythrocytes, Physiology, ATPase, Hypothalamus, Kidney, Ouabain, Reference Values, Internal medicine, Adrenal Glands, medicine, Animals, Na+/K+-ATPase, biology, Chemistry, Brain, Kidney metabolism, Rats, Inbred Strains, Biological activity, Saponins, Rubidium, Ligand (biochemistry), Rats, Calcium ATPase, Cardenolides, Endocrinology, medicine.anatomical_structure, Hypertension, Potassium, biology.protein, Cattle, Sodium-Potassium-Exchanging ATPase, medicine.drug

Abstract

Ouabainlike factor (OLF) has been extracted from the hypothalamus and adrenals of the ox and rats of the Milan hypertensive strain (MHS) and their normotensive controls (MNS). OLF was identified by its ability to 1) inhibit ouabain-sensitive 86Rb uptake into human erythrocytes, 2) displace [3H]ouabain binding, and 3) inhibit purified dog kidney Na-K-adenosinetriphosphatase (ATPase). Rat and bovine OLF have similar characteristics. Those that are close to ouabain are 1) ligand conditions for maximal inhibitory activity, 2) high-performance liquid chromatography retention time, 3) reversibility of inhibitory activity on Na-K-ATPase, 4) reduced Na-K pump inhibitory activity by K, 5) high affinity for Na-K-ATPase, and 6) no activity on calcium ATPase. OLF does not resemble ouabain in the following characteristics: 1) the capacity of OLF to inhibit ouabain low-affinity Na-K-ATPase isoform is greater than that of ouabain and 2) the capacity of OLF to inhibit renal Na-K-ATPase isoforms is greater when the enzyme is obtained from adult rather than young rats. The yield of OLF is greater from MHS than MNS. These findings represent the first direct evidence that a higher amount of OLF is present in tissues from genetically hypertensive rats than from their inbred normotensive controls, maintained under the same dietary and environmental conditions. This further supports previous observations on the role of OLF in the pathogenesis of MHS hypertension.

Published

1992

38. Endogenous ouabain in cardiovascular function and disease

Author

Paolo Manunta, Mara Ferrandi, John M. Hamlyn, Giuseppe Bianchi, Manunta, Paolo, Ferrandi, M, Bianchi, G, and Hamlyn, Jm

Subjects

medicine.medical_specialty, Physiology, Radioimmunoassay, Endogeny, Disease, Ouabain, Natriuresis, Pathogenesis, Cardiovascular Physiological Phenomena, Internal medicine, Internal Medicine, Medicine, Animals, Humans, Secretion, Chromatography, High Pressure Liquid, business.industry, Saponins, Body Fluids, Diet, Cardenolides, Endocrinology, Cardiovascular Diseases, Adrenal Cortex, Cardiology and Cardiovascular Medicine, business, Function (biology), medicine.drug

Abstract

An endogenous ouabain has been isolated and conclusively identified from several mammalian tissues, including human plasma, by a number of independent laboratories. Substantial evidence from independent laboratories in several continents is consistent with an adrenal source for most if not all of the circulating endogenous ouabain. Accumulating evidence suggests that circulating levels of endogenous ouabain in humans are modulated by dietary salt and chronic volume status. Endogenous ouabain is linked significantly with vascular function in hypertension and likely impacts the pathogenesis of heart and renal failure. Moreover, the molecular mechanism of endogenous ouabain-linked hypertension involves the sodium pump/sodium-calcium exchange duet. The outstanding analytical issues include the elucidation of distal events in the biosynthetic pathway for endogenous ouabain and identification of molecular mechanisms that regulate its secretion and clearance.

Published

2008

39. Na+/K+/Cl−-cotransporter mediated Rb+ fluxes in membrane vesicles from kidneys of normotensive and hypertensive rats

Author

Giuseppe Bianchi, Sergio Salardi, Paolo Parenti, Mara Ferrandi, R. Braw, Paolo Ferrari, Steven J.D. Karlish, Ferrandi, M, Salardi, S, Parenti, P, Ferrari, P, Bianchi, G, Braw, R, and Karlish, S

Subjects

Male, medicine.medical_specialty, Rats, Inbred Strain, Biophysics, Diaphragm pump, In Vitro Techniques, Kidney, Chloride, Rats, Inbred WKY, Biochemistry, Chlorides, Furosemide, Microsomes, Rats, Inbred SHR, Internal medicine, medicine, Renal medulla, Na-K-Cl cotransporter, Animals, Na+/K+-ATPase, Ion transporter, biology, Animal, Chemistry, Sodium, Microsome, Rats, Inbred Strains, Biological Transport, Cell Biology, Rubidium, BIO/10 - BIOCHIMICA, Rats, Endocrinology, medicine.anatomical_structure, Hypertension, Potassium, biology.protein, Rat, Cotransporter, Bumetanide, medicine.drug

Abstract

This paper describes experiments to examine Rb + fluxes via the Na + /K + /Cl − cotransporter in membrane vesicles from renal outer medulla of three strains of rat: (A) Wistar (B) Milan hypertensive (MHS) and normotensive (MNS), and (C) Sabra salt-sensitive hypertensive (SBH) and salt-resistant (SBN). Initially, Na + -dependent furosemide- or bumetanide-inhibited 86 Rb + fluxes were characterised using Wistar rat microsomes. The latter were partially purified on a metrizamide cushion, and assay conditions were optimized for use with microsomes from the other rats. The major result is that in microsomes from adult Milan hypetensive (MHS) rats the rate of the Na + /K + /Cl − -cotransporter mediated 86 Rb flux at sub-saturating concentrations of Rb, appears to be significantly greater than in the normotensive (MNS) controls. The effect reflects an increased apparent Rb affinity of the cotransporter in MHS microsomes. There is no difference in maximal rate or in the apparent Na + activation affinity of the 86 Rb + flux. In addition bumetanide appears to be a somewhat more effective inhibitor in MHS compared to MNS microsomes. The 86 Rb + flux result is compatible with a previous finding that in red cells, Na + /K + -cotransporter mediated fluxes are increased in MHS compared to MNS. It supports the notion that the Na + /K + /Cl − -cotransporter in both red cells and kidney is a genetic marker for hypertension. It is of interest that apparetly more than one Na + transport system is affected in MHS hypertensive kidneys (a) the Na + /K + /Cl − cotransporter i nthe thick ascending limb of Henle and (b) the Na + /H + exchanger and/or a conductive Na + -pathway in brush-border membranes from proximal tubule. It is conceivable that in the hypertensive animals a common regulatory pathway (e.g., phosphorylation) or protein (e.g., cytoskeleton) is affected along the length of the nephron. In Sabra SBH and SBN rat microsomes, no difference was found for the 86 Rb + flux via the Na + /K + /Cl − cotransporter (or via a K + channel).

Published

1990

40. Glomerular barrier dysfunction in glomerulosclerosis-resistant Milan rats with experimental diabetes: the role of renal haemodyamics

Author

M.P. Rastaldi, P Fioretto, Deborah Mattinzoli, Silvia Armelloni, Mara Ferrandi, Giuseppe Pugliese, Laura Giardino, Carlo Ricci, Stefano Menini, Francesco Pugliese, and Carla Iacobini

Subjects

Blood Glucose, Male, medicine.medical_specialty, Aging, Kidney Glomerulus, Weight Gain, Rats, Mutant Strains, Pathology and Forensic Medicine, Podocyte, Diabetes Mellitus, Experimental, Nephrin, Diabetic nephropathy, chemistry.chemical_compound, Renal Artery, Species Specificity, Internal medicine, medicine, Animals, Diabetic Nephropathies, Genetic Predisposition to Disease, Glycated Hemoglobin, Creatinine, Proteinuria, biology, business.industry, Podocytes, Glomerulosclerosis, Serum Albumin, Bovine, medicine.disease, Rats, Endocrinology, medicine.anatomical_structure, chemistry, biology.protein, Glomerular Filtration Barrier, Disease Progression, Synaptopodin, medicine.symptom, business

Abstract

Rats of the Milan hypertensive strain (MHS) are resistant to both hypertensive and diabetic renal disease. Genetically determined hypertrophy of intrarenal arteries has been suggested as the putative mechanism preventing transmission of systemic hypertension to the glomerular microcirculation or diabetes-induced loss of autoregulation, which lead to glomerular hypertension and consequent podocyte injury and proteinuria. This study aimed to investigate glomerular barrier function and structure in ageing and diabetic MHS rats under basal conditions and after injection of 2.5 g of bovine serum albumin (BSA) causing increased workload and possibly removing haemodynamic protection by inducing renal cortical vasodilatation. Genetically related rats of the Milan normotensive strain (MNS) served as a proteinuric counterpart. No change in renal function or structure was detected in diabetic MHS rats, whereas MNS rats developed diabetic nephropathy superimposed on that occurring spontaneously in this strain. Diabetic, but not non-diabetic, MHS rats showed significantly reduced synaptopodin and nephrin expression, though to a lesser extent than non-diabetic and diabetic MNS rats, together with unchanged podocyte number, density and structure and no proteinuria. Agrin expression was significantly altered in diabetic versus non-diabetic MHS animals, whereas collagen I was expressed only in diabetic MHS rats and collagen IV content did not change significantly between the two groups. Upon BSA injection, proteinuria increased markedly and abundant BSA was detected only in kidneys from diabetic MHS rats. BSA injection was associated with changes in intrarenal arteries suggesting vasodilatation, without any influx of inflammatory cells. These data indicate that while MNS rats show marked changes in the glomerular filtration barrier with either age or diabetes, glomerulosclerosis-resistant MHS rats develop only minor diabetes-induced podocyte (and extracellular matrix) alterations, which are not associated with proteinuria unless they are unmasked by an increased workload or removal of the haemodynamic protection.

Published

2007

41. Adducin polymorphisms and the treatment of hypertension

Author

Paolo Manunta, Chiara Lanzani, Mara Ferrandi, Lorena Citterio, Manunta, Paolo, Citterio, L, Lanzani, C, and Ferrandi, M.

Subjects

medicine.medical_specialty, Candidate gene, Bioinformatics, Essential hypertension, Internal medicine, Genetics, medicine, Genetic predisposition, Animals, Humans, Diuretics, Ouabain, Pharmacology, Polymorphism, Genetic, business.industry, medicine.disease, ADD1, Blood pressure, Endocrinology, ADD3, Pharmacogenomics, Multigene Family, Hypertension, Molecular Medicine, Calmodulin-Binding Proteins, business, Pharmacogenetics

Abstract

Hypertension is an important public health problem affecting more than 50 million individuals in the USA alone. The most common form, essential hypertension, results from the complex interplay between genetic predisposition and environmental influences. Epidemiological, migration, intervention and genetic studies in humans and animals provide very strong evidence of a causal link between high salt intake and high blood pressure. One of the candidate genes for salt-sensitive hypertension is adducin. Adducin is a heterodimeric cytoskeleton protein, the three subunits of which are encoded by genes (ADD1, ADD2 and ADD3) that map to three different chromosomes. A long series of parallel studies in the Milan hypertensive rat strain model of hypertension and humans indicated that an altered adducin function might cause hypertension through enhanced constitutive tubular sodium reabsorption. An example of a prospective efficacy of pharmacogenetics and pharmacogenomics is the detection and impact of adducin polymorphisms on hypertension. In particular, the selective advantages of diuretics in preventing myocardial infarction and stroke over other antihypertensive therapies that produce a similar blood pressure reduction in carriers of the mutated adducin may support new strategies aimed at optimizing the use of new antihypertensive agents for the prevention of hypertension-associated organ damage.

Published

2007

42. Targeting Ouabain- and Adducin-dependent mechanisms of hypertension and cardiovascular remodeling as a novel pharmacological approach

Author

Patrizia Ferrari, Paolo Manunta, Giovanni Valentini, Mara Ferrandi, Giuseppe Bianchi, Ferrari, P, Ferrandi, M, Valentini, G, Manunta, Paolo, and Bianchi, G.

Subjects

MAPK/ERK pathway, medicine.medical_specialty, Pharmacology, Essential hypertension, Cardiovascular System, Ouabain, Muscle hypertrophy, Internal medicine, medicine, Animals, Humans, Androstanols, Antihypertensive Agents, Kidney, Reabsorption, business.industry, Models, Cardiovascular, General Medicine, medicine.disease, Blood pressure, medicine.anatomical_structure, Endocrinology, Hypertension, Calmodulin-Binding Proteins, Signal transduction, Sodium-Potassium-Exchanging ATPase, business, medicine.drug

Abstract

Essential hypertension is a heterogeneous multifactorial syndrome associated with a high cardiovascular risk. A multiple choice of antihypertensive drugs is available; however, a high individual variability to the antihypertensive therapy is still responsible for a modest reduction of the CV risk and not satisfactory control of blood pressure levels. The success of future hypertension treatment will depend upon the understanding of the genetic molecular mechanisms operating in subsets of patients, and the ability of new drugs to specifically correct such alterations. Two mechanisms, among others, are involved in determining the abnormalities of tubular Na(+) reabsorption observed in essential hypertension: the polymorphism of the cytoskeletal protein alpha-adducin and the increased circulating levels of endogenous ouabain (EO). Both lead to increased activity and expression of the renal Na-K pump, the driving force for tubular Na transport. Morphological and functional cardiovascular alterations have also been associated with adducin and EO. Rostafuroxin is a new oral antihypertensive agent able to selectively antagonize adducin and EO hypertensive and molecular effects. It is endowed with high potency and efficacy in reducing blood pressure and preventing organ hypertrophy in animal models representative of both adducin and EO mechanisms. At molecular level, in the kidney, Rostafuroxin normalizes the enhanced activity of the Na-K pump induced by adducin mutation and antagonizes the EO triggering of the Src-EGFr-dependent signaling pathway leading to renal Na-K pump, and ERK Tyrosin phosphorylation and activation. In the vasculature, it normalizes the increased myogenic tone caused by ouabain. A very high safety ratio and an absence of interaction with other mechanisms involved in blood pressure regulation, together with initial evidence of high tolerability and efficacy in hypertensive patients, indicate Rostafuroxin as the first example of a new class of antihypertensive agents designed to antagonize adducin and EO-hypertensive mechanisms. Currently, a phase II multicenter European clinical trial is ongoing for providing the proof of concept that such a compound is effective in the subset of patients where these two mechanisms are at work.

Published

2006

43. A new antihypertensive agent that antagonizes the prohypertensive effect of endogenous ouabain and adducin

Author

Patrizia Ferrari, Mara Ferrandi, Paolo Manunta, and Elisabetta Messaggio

Subjects

medicine.medical_specialty, Sodium, Population, chemistry.chemical_element, Blood Pressure, Sodium Chloride, Ouabain, Muscle hypertrophy, chemistry.chemical_compound, Risk Factors, Internal medicine, medicine, Humans, Androstanols, Salt intake, education, Antihypertensive Agents, Pharmacology, education.field_of_study, Hematology, Digitoxigenin, Blood pressure, Endocrinology, chemistry, Hypertension, Calmodulin-Binding Proteins, Sodium-Potassium-Exchanging ATPase, Cardiology and Cardiovascular Medicine, Homeostasis, medicine.drug

Abstract

Endogenous Ouabain (EO) and Adducin enhance the Na-K pump function and play an important role in sodium homeostasis and blood pressure (BP) regulation. In the general population, plasma EO modulates BP either by inhibiting the prohypertensive effect of an excessive salt intake or counteracting the depressor action of normal-moderate salt intake. Almost 50% of hypertensive patients have increased circulating plasma levels of EO. EO has been associated both to left ventricular dysfunction and hypertrophy. A new antihypertensive agent, PST2238, (17beta-(3-furyl)-5beta-androstan-3beta, 14beta, 17alpha-triol a digitoxigenin derivative) able to selectively antagonize both the EO and adducin prohypertensive and molecular effects, has been developed. In hypertensive rats (MHS strain) carrying both adducin mutations and increased plasma EO and in ouabain-infused rats (OS), PST2238 lowers BP by normalizing the renal Na-K pump function. In OS rats, PST antagonized the cardiac and renal pro-hypertrophic ouabain effect associated to the activation of the Src-EGFr-ERK(1/2) signaling cascade. Phase 1 clinical studies demonstrated a high tolerability of PST2238. In a preliminary phase 2 study on 42 mild never-treated hypertensive patients, PST2238 given for 3 months at 0.5 mg/day, significantly reduced BP in subjects with moderate salt intake, implying that it may be selectively effective in conditions where EO plays a prohypertensive role. In conclusion, PST2238, because of its peculiar action mechanism, represents a new tool to disentangle the complex relationship between salt intake, genetic control of renal sodium handling and EO effect.

Published

2006

44. Rostafuroxin: an ouabain antagonist that corrects renal and vascular Na+-K+- ATPase alterations in ouabain and adducin-dependent hypertension

Author

Giovanni Valentini, Mara Ferrandi, Patrizia Ferrari, and Giuseppe Bianchi

Subjects

medicine.medical_specialty, Physiology, Sodium-Potassium-Exchanging ATPase, Treatment outcome, Pharmacology, Biology, Essential hypertension, Kidney, Ouabain, Physiology (medical), Internal medicine, medicine, Animals, Humans, Androstanols, Na+/K+-ATPase, Antihypertensive Agents, Rostafuroxin, Antagonist, Kidney metabolism, medicine.disease, Endocrinology, Treatment Outcome, Hypertension, Blood Vessels, Calmodulin-Binding Proteins, medicine.drug

Abstract

The genetic and environmental heterogeneity of essential hypertension is responsible for the individual variability of antihypertensive therapy. An understanding of the molecular mechanisms underlying hypertension and related organ complications is a key aspect for developing new, effective, and safe antihypertensive agents able to cure the cause of the disease. Two mechanisms, among others, are involved in determining the abnormalities of tubular Na+reabsorption observed in essential hypertension: the polymorphism of the cytoskeletal protein α-adducin and the increased circulating levels of endogenous ouabain (EO). Both lead to increased activity and expression of the renal Na+-K+pump, the driving force for tubular Na transport. Morphological and functional vascular alterations have also been associated with EO. Rostafuroxin (PST 2238) is a new oral antihypertensive agent able to selectively antagonize EO, adducin pressor, and molecular effects. It is endowed with high potency and efficacy in reducing blood pressure and preventing organ hypertrophy in animal models representative of both adducin and EO mechanisms. At molecular level, in the kidney, Rostafuroxin antagonizes EO triggering of the Src-epidermal growth factor receptor (EGFr)-dependent signaling pathway leading to renal Na+-K+pump, and ERK tyrosine phosphorylation and activation. In the vasculature, it normalizes the increased myogenic tone caused by nanomolar ouabain. A very high safety ratio and an absence of interaction with other mechanisms involved in blood pressure regulation, together with initial evidence of high tolerability and efficacy in hypertensive patients, indicate Rostafuroxin as the first example of a new class of antihypertensive agents designed to antagonize adducin and EO-hypertensive mechanisms.

Published

2006

45. Cardiac glycosides and cardiomyopathy

Author

Mara Ferrandi, Paolo Manunta, Manunta, Paolo, and Ferrandi, M.

Subjects

Inotrope, medicine.medical_specialty, Cardiac output, Cardiac cycle, business.industry, Cardiac muscle, Cardiomyopathy, medicine.disease, Myocardial Contraction, Bufanolides, Cardiac Glycosides, medicine.anatomical_structure, Heart failure, Internal medicine, Internal Medicine, medicine, Cardiology, Intravascular volume status, Animals, Humans, Exertion, business, Cardiomyopathies, Uremia

Abstract

Digitalis-like steroids and related agents have been a mainstay in the treatment of congestive heart failure ever since the publication, in 1785, of Withering’s seminal monograph on foxglove. Heart failure refers to the clinical syndrome that results when the heart is unable to pump sufficient blood to keep up with the metabolic demands of the body. Congestive heart failure is characterized by excessive neuronal and hormonal-mediated fluid retention, expanded intravascular volume, high pulmonary and systemic venous pressures with consequent dyspnea (shortness of breath) on exertion, reduced exercise tolerance, and fatigue. Most heart failure patients also have impaired ventricular systolic function and depressed cardiac output; these are the patients most often treated with digitalis glycosides. These drugs are positive inotropic agents and enhance cardiac contraction. The “cardiotonic steroids” cause cardiac muscle to lose K+ and gain Na+ because they inhibit the Na+ pump (Na+,K+–ATPase), a plasma membrane protein, present in all cells. The Na+ pump uses the energy from ATP to extrude Na+ and …

Published

2006

46. The endogenous ouabain: molecular basis of its role in hypertension and cardiovascular complications

Author

Paolo Manunta, Mara Ferrandi, Patrizia Ferrari, Giuseppe Bianchi, Ferrandi, M, Manunta, Paolo, Ferrari, P, and Bianchi, G.

Subjects

medicine.medical_specialty, Blood Pressure, Pharmacology, Sodium Chloride, Ouabain, Muscle hypertrophy, chemistry.chemical_compound, In vivo, Risk Factors, Internal medicine, Rats, Inbred SHR, medicine, Animals, Humans, Na+/K+-ATPase, Renal sodium reabsorption, business.industry, Rats, Digitoxigenin, Endocrinology, Blood pressure, chemistry, Hypertension, Signal transduction, business, medicine.drug

Abstract

Elevated levels of the endogenous ouabain (EO), a closely related isomer of ouabain, are implicated in rat and human hypertension and in related cardiovascular complications. The pathogenetic mechanisms through which EO affects the cardiovascular system involve the modulation of the renal Na/K-ATPase, implicated in renal tubular sodium reabsorption, and the activation of signal transduction pathways, promoting the transcription of growth-related genes. Experimental and clinical evidence on rats and humans stimulated the pharmacological research for developing novel anti-hypertensive agents able to antagonize the cellular and molecular alterations mediated by EO. Among them, the digitoxigenin derivate, PST 2238, has been selected for its ability to antagonize the ouabain-induced effects on blood pressure and organ hypertrophy at oral doses of microgram/kg/day in vivo. The pharmacological selectivity and safety of PST 2238 suggests that the compound may be effective for the treatment of those forms of hypertension in which renal sodium handling alterations and cardiovascular complications are associated with increased production of EO.

Published

2005

47. Different effects of marinobufagenin and endogenous ouabain

Author

Mara Ferrandi, Paolo Manunta, Manunta, Paolo, and Ferrandi, M.

Subjects

Heart Failure, Marinobufagenin, Physiology, Endogenous ouabain, business.industry, Myocardium, Pharmacology, Bufanolides, chemistry.chemical_compound, chemistry, Internal Medicine, Medicine, Animals, Humans, Enzyme Inhibitors, Sodium-Potassium-Exchanging ATPase, Cardiology and Cardiovascular Medicine, business, Ouabain

Published

2004

48. Ouabain

Author

Paolo Manunta, Mara Ferrandi, and Giuseppe Bianchi

Published

2004

49. Antihypertensive compounds that modulate the Na-K pump

Author

Paolo Barassi, Piero Melloni, Lucia Torielli, Mara Ferrandi, Giuseppe Bianchi, E. Minotti, Patrizia Ferrari, Grazia Tripodi, and Isabella Molinari

Subjects

medicine.medical_specialty, Renal Hypertrophy, Blood Pressure, Kidney, Transfection, General Biochemistry, Genetics and Molecular Biology, Ouabain, History and Philosophy of Science, In vivo, Internal medicine, Microsomes, medicine, Animals, Humans, Androstanols, Na+/K+-ATPase, Antihypertensive Agents, Cells, Cultured, Chemistry, General Neuroscience, Recombinant Proteins, Rats, Blood pressure, medicine.anatomical_structure, Endocrinology, Ventricle, Sodium-Potassium-Exchanging ATPase, medicine.drug

Abstract

A primary impairment of the kidney sodium excretion has been documented both in hypertensive patients (EH) and genetic animal models (Milan hypertensive rat [MHS]) carrying mutations of the cytoskeletal protein adducin and/or increased plasma levels of endogenous ouabain (EO). Ouabain (OU) itself induces hypertension in rats and both OU and mutated adducin activate the renal Na/K-ATPase function both in vivo and in cultured renal cells (NRK). A new antihypertensive agent, PST 2238, able to selectively interact with these alterations has been developed. PST lowers blood pressure (BP) by normalizing the expression and activity of the renal Na-K pump selectively in those rat models carrying the adducin mutation (MHS) and/or increased EO levels (OS) at oral doses of 0.1-10 micro g/kg. In NRK cells either transfected with mutated adducin or incubated with 10(-9) M OU, PST normalizes the Na-K pump activity. Recently, an association between EO and cardiac complications has been observed in both EH and rat models consistent with a prohypertrophic activity of OU. OS rats showed a 10% increase of left ventricle and kidney weights as compared with controls, and PST 2238 (1 micro g/kg OS) prevented both ventricle and renal hypertrophy. This effect was associated with the ability of PST to antagonize the OU-dependent activation of growth-related genes, in the membrane subdomains of caveolae. In conclusion, PST is a new antihypertensive agent that may prevent cardiovascular complications associated with hypertension through the selective modulation of the Na-K pump function.

Published

2003

50. Endogenous ouabain and hemodynamic and left ventricular geometric patterns in essential hypertension

Author

A. Bucci, John M. Hamlyn, Sante D. Pierdomenico, Paolo Manunta, Mara Ferrandi, Franco Cuccurullo, Rodolfo Rivera, Andrea Mezzetti, Domenico Lapenna, Pierdomenico, Sd, Bucci, A, Manunta, Paolo, Rivera, R, Ferrandi, M, Hamlyn, Jm, Lapenna, D, Cuccurullo, F, and Mezzetti, A.

Subjects

Adult, Male, medicine.medical_specialty, Cardiac output, Digoxin, Cardiac index, Concentric hypertrophy, Cardiomegaly, Essential hypertension, Ventricular Function, Left, Biological Factors, Internal medicine, Internal Medicine, medicine, Humans, Systole, Ventricular remodeling, Body surface area, Ventricular Remodeling, business.industry, Hemodynamics, Stroke volume, Middle Aged, Saponins, medicine.disease, Cardenolides, Echocardiography, Hypertension, Cardiology, Female, business

Abstract

We sought to evaluate the relationships among circulating levels of an endogenous ouabain-like factor (EO) and systemic hemodynamics and left ventricular (LV) geometry in patients with recently diagnosed essential hypertension. We selected 92 never-treated patients with essential hypertension. Blood samples were drawn for estimation of plasma EO (radioimmunoassay) and subjects underwent echocardiographic examination to evaluate LV end-systolic and end-diastolic wall thickness and internal dimensions. LV volumes, stroke volume, cardiac output, total peripheral resistance, LV mass, and relative wall thickness were calculated, and all except the last parameter were indexed by body surface area. LV mass also was indexed by height. On the basis of the values of LV mass index (body surface area or height) and relative wall thickness, subjects were divided into groups with either normal geometry, concentric remodeling, concentric hypertrophy, or eccentric nondilated hypertrophy. In the study population as a whole, circulating EO levels were significantly and directly correlated with mean blood pressure (r = 0.21, P = .048), relative wall thickness (r = 0.34, P = .001), and total peripheral resistance index (r = 0.37, P = .0003). Plasma EO also was significantly and inversely correlated with LV end-diastolic volume index (r = -0.32, P = .002), stroke index (r = -0.34, P = .0009), and cardiac index (r = -0.35, P = .0007). In multiple regression analysis, plasma EO was an independent correlate of total peripheral resistance index, cardiac index, and relative wall thickness. Regardless of the indexation method used for LV mass, plasma EO was higher in patients with concentric remodeling than in those with either normal geometry or concentric hypertrophy. Plasma EO tended to be higher (indexation by body surface area) or was significantly higher (indexation by height) in subjects with concentric remodeling than in those with eccentric nondilated hypertrophy. Patients with concentric remodeling showed the highest total peripheral resistance index and the lowest cardiac index. Our data suggest that EO plays a role in regulating systemic hemodynamics and LV geometry in patients with essential hypertension.

Published

2001