Your search keyword '"Daniela Corna"' showing total 54 results

1. Addition of cyclic angiotensin-(1-7) to angiotensin-converting enzyme inhibitor therapy has a positive add-on effect in experimental diabetic nephropathy

Author

Domenico Cerullo, Paola Cassis, Mauro Abbate, Daniela Rottoli, Giuseppe Remuzzi, Sebastian Villa, Carlamaria Zoja, Ariela Benigni, Monica Locatelli, and Daniela Corna

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Kidney Glomerulus, 030232 urology & nephrology, Angiotensin-Converting Enzyme Inhibitors, Mice, Transgenic, Sulfides, Peptides, Cyclic, Podocyte, Diabetic nephropathy, Mice, 03 medical and health sciences, 0302 clinical medicine, Microscopy, Electron, Transmission, Lisinopril, Fibrosis, Internal medicine, medicine, Animals, Humans, Diabetic Nephropathies, Alanine, biology, business.industry, Angiotensin-converting enzyme, medicine.disease, Angiotensin II, Peptide Fragments, Disease Models, Animal, Proteinuria, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Diabetes Mellitus, Type 2, Nephrology, ACE inhibitor, Albuminuria, biology.protein, Drug Therapy, Combination, Angiotensin I, medicine.symptom, business, Half-Life, medicine.drug

Abstract

The Renin-Angiotensin System (RAS) possesses a counter-regulatory axis composed of angiotensin converting enzyme (ACE)2, angiotensin-(1-7) [Ang-(1-7)] and the Mas receptor, which opposes many AT1-receptor-mediated effects of ligand angiotensin II. Ang-(1-7), as a ligand of the Mas receptor, has inhibitory effects on renal inflammation and fibrosis in experimental diabetes. However, Ang-(1-7) has a short half-life in plasma, which may render it unsuitable for use in clinics. Here, we investigated the effects of the lanthionine-stabilized Ang-(1-7), cyclic (c)Ang-(1-7), a lanthipeptide that is more peptidase-resistant than the linear peptide, in BTBR ob/ob mice with type 2 diabetic nephropathy. BTBR ob/ob mice received vehicle, cAng-(1-7), or the ACE inhibitor lisinopril. The treatment started at ten weeks of age, when the animals had already developed albuminuria, and ended at 19-20 weeks of age. cAng-(1-7) limited albuminuria progression, and limited podocyte dysfunction similarly to lisinopril. cAng-(1-7), unlike lisinopril, reduced glomerular fibrosis and inflammation, and counteracted glomerular capillary rarefaction. Furthermore, when cAng-(1-7) was combined with lisinopril, a superior antiproteinuric effect than with lisinopril alone was found, in association with better preservation of podocyte proteins and amelioration of capillary density. Thus, adding cAng-(1-7) to ACE-inhibitor therapy could benefit those diabetic patients who do not respond completely to ACE-inhibitor therapy.

Published

2019

2. Protective Effects of Human Nonrenal and Renal Stromal Cells and Their Conditioned Media in a Rat Model of Chronic Kidney Disease

Author

Marina Morigi, Claudia Elisa Carminati, Chiara Capelli, Cinzia Rota, Ariela Benigni, Carlamaria Zoja, Daniëlle G. Leuning, Domenico Cerullo, Martino Introna, Ton J. Rabelink, Giuseppe Remuzzi, Barbara Imberti, Valerie A. Luyckx, Monica Locatelli, Daniela Corna, and Anna Pezzotta

Subjects

0301 basic medicine, medicine.medical_specialty, Stromal cell, 030232 urology & nephrology, Biomedical Engineering, renal repair, lcsh:Medicine, Podocyte, Cell therapy, Nephrin, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, Internal medicine, medicine, Animals, Humans, Renal Insufficiency, Chronic, stromal cells, Transplantation, biology, business.industry, Mesenchymal stem cell, lcsh:R, Cell Biology, medicine.disease, Rats, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, conditioned medium, biology.protein, renal perivascular cells, Original Article, business, Myofibroblast, chronic kidney disease, Kidney disease

Abstract

Mesenchymal stromal cells (MSCs) are emerging as a novel therapeutic option for limiting chronic kidney disease progression. Conditioned medium (CM) containing bioactive compounds could convey similar benefits, avoiding the potential risks of cell therapy. This study compared the efficacy of nonrenal and renal cell-based therapy with the corresponding CM in rats with renal mass reduction (RMR). Infusions of human kidney stromal cells (kPSCs) and CM-kPSCs, but not umbilical cord (uc) MSCs or CM-ucMSCs, reduced proteinuria and preserved podocyte number and nephrin expression in RMR rats. Glomerular fibrosis, microvascular rarefaction, and apoptosis were reduced by all treatments, while the peritubular microvascular loss was reduced by kPSCs and CM-kPSCs treatment only. Importantly, kPSCs and CM-kPSCs reduced NG2-positive pericytes, and all therapies reduced α-smooth muscle actin expression, indicating reduced myofibroblast expansion. Treatment with kPSCs also significantly inhibited the accumulation of ED1-positive macrophages in the renal interstitium of RMR rats. These findings demonstrate that the CM of ucMSCs and kPSCs confers similar renoprotection as the cells. kPSCs and CM-kPSCs may be superior in attenuating chronic renal injury as a cell source.

Published

2020

3. C3a receptor blockade protects podocytes from injury in diabetic nephropathy

Author

Ariela Benigni, Giuseppe Remuzzi, Silvia Bolognini, Daniela Corna, Monica Locatelli, Carlamaria Zoja, Simona Buelli, Paola Cassis, Claudia Elisa Carminati, Luca Perico, and Marina Morigi

Subjects

0301 basic medicine, medicine.medical_specialty, Kidney Glomerulus, SOD2, chemical and pharmacologic phenomena, Mitochondrion, urologic and male genital diseases, Protein oxidation, Podocyte, Diabetic nephropathy, Nephrin, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Cyclic AMP, medicine, Animals, Diabetic Nephropathies, Complement Activation, biology, Podocytes, Superoxide Dismutase, Chemistry, General Medicine, medicine.disease, Mitochondria, Receptors, Complement, Disease Models, Animal, Oxidative Stress, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Diabetes Mellitus, Type 2, 030220 oncology & carcinogenesis, Complement C3a, biology.protein, Albuminuria, C3a receptor, medicine.symptom, Research Article

Abstract

Renal activation of the complement system has been described in patients with diabetic nephropathy (DN), although its pathological relevance is still ill-defined. Here, we studied whether glomerular C3a, generated by uncontrolled complement activation, promotes podocyte damage, leading to proteinuria and renal injury in mice with type 2 diabetes. BTBR ob/ob mice exhibited podocyte loss, albuminuria, and glomerular injury accompanied by C3 deposits and increased C3a and C3a receptor (C3aR) levels. Decreased glomerular nephrin and α-actinin4 expression, coupled with integrin-linked kinase induction, were also observed. Treatment of DN mice with a C3aR antagonist enhanced podocyte density and preserved their phenotype, limiting proteinuria and glomerular injury. Mechanistically, ultrastructural and functional mitochondrial alterations, accompanied by downregulation of antioxidant superoxide dismutase 2 (SOD2) and increased protein oxidation, occurred in podocytes and were normalized by C3aR blockade. In cultured podocytes, C3a induced cAMP-dependent mitochondrial fragmentation. Alterations of mitochondrial membrane potential, SOD2 expression, and energetic metabolism were also found in response to C3a. Notably, C3a-induced podocyte motility was inhibited by SS-31, a peptide with mitochondrial protective effects. These data indicate that C3a blockade represents a potentially novel therapeutic strategy in DN for preserving podocyte integrity through the maintenance of mitochondrial functions.

Published

2020

4. Alteration of thyroid hormone signaling triggers the diabetes-induced pathological growth, remodeling, and dedifferentiation of podocytes

Author

Daniela Corna, Giuseppe Remuzzi, Valentina Benedetti, Rubina Novelli, Carlamaria Zoja, Christodoulos Xinaris, Monica Locatelli, Valerio Brizi, Ariela Benigni, Marta Todeschini, and Angelo Michele Lavecchia

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Deiodinase, Down-Regulation, Iodide Peroxidase, Streptozocin, Fetal Kidney, Cell Line, Diabetes Mellitus, Experimental, Muscle hypertrophy, Podocyte, Pathogenesis, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Internal medicine, medicine, Animals, Humans, Protein Isoforms, Diabetic Nephropathies, Receptor, biology, Podocytes, business.industry, Gene Expression Regulation, Developmental, Cell Cycle Checkpoints, General Medicine, Rats, Rats, Zucker, Up-Regulation, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Triiodothyronine, business, Signal Transduction, Thyroid Hormone Receptors alpha, Research Article, Hormone

Abstract

Thyroid hormone (TH) signaling is a universal regulator of metabolism, growth, and development. Here, we show that TH-TH receptor (TH-TR) axis alterations are critically involved in diabetic nephropathy–associated (DN-associated) podocyte pathology, and we identify TRα1 as a key regulator of the pathogenesis of DN. In ZSF1 diabetic rats, T(3) levels progressively decreased during DN, and this was inversely correlated with metabolic and renal disease worsening. These phenomena were associated with the reexpression of the fetal isoform TRα1 in podocytes and parietal cells of both rats and patients with DN and with the increased glomerular expression of the TH-inactivating enzyme deiodinase 3 (DIO3). In diabetic rats, TRα1-positive cells also reexpressed several fetal mesenchymal and damage-related podocyte markers, while glomerular and podocyte hypertrophy was evident. In vitro, exposing human podocytes to diabetes milieu typical components markedly increased TRα1 and DIO3 expression and induced cytoskeleton rearrangements, adult podocyte marker downregulation and fetal kidney marker upregulation, the maladaptive cell cycle induction/arrest, and TRα1-ERK1/2–mediated hypertrophy. Strikingly, T(3) treatment reduced TRα1 and DIO3 expression and completely reversed all these alterations. Our data show that diabetic stress induces the TH-TRα1 axis to adopt a fetal ligand/receptor relationship pattern that triggers the recapitulation of the fetal podocyte phenotype and subsequent pathological alterations.

Published

2019

5. ADAMTS13 Deficiency Shortens the Life Span of Mice With Experimental Diabetes

Author

Daniela Corna, Valentina Casieri, Giuseppe Remuzzi, Vincenzo Lionetti, Paola Cassis, Sara Conti, Rubina Novelli, Giulia Taraboletti, Sebastian Villa, Domenico Cerullo, Monica Locatelli, Carlamaria Zoja, Fabrizio Giordano, Marco Matteucci, Ariela Benigni, Sara Gastoldi, and Cristina Zanchi

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Connexin, ADAMTS13 Protein, 030204 cardiovascular system & hematology, Diabetes Mellitus, Experimental, Thrombospondin 1, 03 medical and health sciences, Mice, 0302 clinical medicine, hemic and lymphatic diseases, Diabetes mellitus, Ca2+/calmodulin-dependent protein kinase, Internal medicine, Dobutamine, Internal Medicine, medicine, Animals, Phosphorylation, Mice, Knockout, Thrombospondin, business.industry, Reverse Transcriptase Polymerase Chain Reaction, Streptozotocin, medicine.disease, Immunohistochemistry, ADAMTS13, 030104 developmental biology, Endocrinology, Connexin 43, cardiovascular system, business, Calcium-Calmodulin-Dependent Protein Kinase Type 2, Shear Strength, medicine.drug

Abstract

In patients with diabetes, impaired activity of ADAMTS13 (a disintegrin and metalloprotease with thrombospondin type 1 repeats, member 13), the plasma metalloprotease that cleaves highly thrombogenic von Willebrand factor multimers, is a major risk factor of cardiovascular events. Here, using Adamts13−/− mice made diabetic by streptozotocin, we investigated the impact of the lack of ADAMTS13 on the development of diabetes-associated end-organ complications. Adamts13−/− mice experienced a shorter life span than their diabetic wild-type littermates. It was surprising that animal death was not related to the occurrence of detectable thrombotic events. The lack of ADAMTS13 drastically increased the propensity for ventricular arrhythmias during dobutamine-induced stress in diabetic mice. Cardiomyocytes of diabetic Adamts13−/− mice exhibited an aberrant distribution of the ventricular gap junction connexin 43 and increased phosphorylation of Ca2+/calmodulin-dependent kinase II (CaMKII), and with the consequent CaMKII-induced disturbance in Ca2+ handling, which underlie propensity for arrhythmia. In vitro, thrombospondin 1 (TSP1) promoted, in a paracrine manner, CaMKII phosphorylation in murine HL-1 cardiomyocytes, and ADAMTS13 acted to inhibit TSP1-induced CaMKII activation. In conclusion, the deficiency of ADAMTS13 may underlie the onset of lethal arrhythmias in diabetes through increased CaMKII phosphorylation in cardiomyocytes. Our findings disclose a novel function for ADAMTS13 beyond its antithrombotic activity.

Published

2017

6. SGLT2 inhibitor dapagliflozin limits podocyte damage in proteinuric nondiabetic nephropathy

Author

Marina Morigi, Domenico Cerullo, Sebastian Villa, Paola Cassis, Carlamaria Zoja, Daniela Corna, Simona Buelli, Monica Locatelli, Cristina Zanchi, Giuseppe Remuzzi, and Ariela Benigni

Subjects

0301 basic medicine, Nephrology, Male, medicine.medical_specialty, 030232 urology & nephrology, Pharmacology, Nephropathy, Podocyte, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Glucosides, Sodium-Glucose Transporter 2, Internal medicine, medicine, Animals, Humans, Dapagliflozin, Benzhydryl Compounds, RNA, Small Interfering, Renal Insufficiency, Chronic, Sodium-Glucose Transporter 2 Inhibitors, Proteinuria, business.industry, Podocytes, Serum Albumin, Bovine, General Medicine, medicine.disease, Actin cytoskeleton, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, chemistry, ACE inhibitor, medicine.symptom, business, Injections, Intraperitoneal, medicine.drug, Kidney disease, Research Article

Abstract

Sodium-glucose cotransporter 2 (SGLT2) inhibitors have pleiotropic properties beyond blood glucose-lowering effects and modify important nonglycemic pathways, leading to end-organ protection. SGLT2 inhibitors display renoprotective effects in diabetic kidney disease, which creates a rationale for testing the therapeutic potential of this drug class in nondiabetic chronic kidney disease. Here, we have shown that dapagliflozin provided glomerular protection in mice with protein-overload proteinuria induced by bovine serum albumin (BSA), to a similar extent as an ACE inhibitor used as standard therapy for comparison. Dapagliflozin limited proteinuria, glomerular lesions, and podocyte dysfunction and loss. We provide the observation that SGLT2 was expressed in podocytes and upregulated after BSA injections. Through in vitro studies with cultured podocytes loaded with albumin we have identified what we believe to be a novel mechanism of action for SGLT2 inhibitor that directly targets podocytes and relies on the maintenance of actin cytoskeleton architecture. Whether SGLT2 inhibitors represent a possible future therapeutic option for some patients with proteinuric glomerular disease who do not have as yet an effective treatment will require ad hoc clinical studies.

Published

2017

7. Chronic administration of Norwegian Ascophyllum nodosum phytocomplex inhibits high-fat-diet-induced obesity in male rats

Author

Stefania Murzilli, Andreina Poggi, Donata Di Tommaso, Vincenzo Di Matteo, Daniela Corna, Luisa Sciulli, and Lorena Salvatore

Subjects

medicine.medical_specialty, Antioxidant, biology, medicine.medical_treatment, digestive, oral, and skin physiology, food and beverages, nutritional and metabolic diseases, Biological activity, Clinical nutrition, White adipose tissue, biology.organism_classification, Body weight, High fat diet induced obesity, Endocrinology, Internal medicine, Male rats, medicine, Ascophyllum, hormones, hormone substitutes, and hormone antagonists

Abstract

Several biologically active compounds are present in seaweeds that show a wide range of biological properties, such as antibiotic, anti-inflammatory, antioxidant, cytotoxic, antitumour and anti-obesity activities. The aim was to evaluate the anti-obesity effects of chronic treatment with Norwegian Ascophyllum nodosum phytocomplex in rats. We also investigated the effects of this phytocomplex on blood glucose and serum lipid levels, and α-amylase, lipase, alanine aminotransferase and aspartate aminotransferase activities. Five groups of male Sprague-Dawley rats were fed for 8 weeks with standard diet, highfat diet (HFD) or HFD plus three different doses of Norwegian A. nodosum phytocomplex (HFD Low, HFD Medium, HFD High). Feeding with HFD resulted in increased body weight and deposition of visceral and abdominal white adipose tissue. These effects were significantly reduced by supplementation with high doses of A. nodosum phytocomplex in the feed, which suggests a potent anti-obesity activity of this phytocomplex. Increased serum levels of triglycerides and α-amylase activity were observed in rats fed with HFD at sacrifice. These were inhibited in a dose-dependent manner by feeding with the added A. nodosum phytocomplex in HFD Medium and HFD High. Increased liver and kidney weights were also inhibited in a dose-dependent manner by added A. nodosum phytocomplex, with significant effects at the highest phytocomplex dose. Rats fed with HFD showed a changed, irregular, liver morphology, increased infiltration of inflammatory cells and increased intravascular spaces compared to controls. These effects were partially corrected by HFD High, which suggests potent anti-inflammatory activity of the A. nodosum phytocomplex.

Published

2014

8. β-Arrestin-1 Drives Endothelin-1–Mediated Podocyte Activation and Sustains Renal Injury

Author

Giuseppe Remuzzi, Luca Perico, Laura Rosanò, Lorena Longaretti, Carlamaria Zoja, Simona Buelli, Marina Morigi, Rubina Novelli, Anna Pezzotta, Daniela Corna, Anna Bagnato, Elena Gagliardini, Sara Conti, Ariela Benigni, and Paola Rizzo

Subjects

medicine.medical_specialty, Beta-catenin, biology, Beta-Arrestins, Glomerulonephritis, General Medicine, medicine.disease, Podocyte, Transactivation, Endocrinology, medicine.anatomical_structure, Growth factor receptor, Nephrology, Internal medicine, biology.protein, medicine, Cancer research, Gene silencing, Synaptopodin

Abstract

Activation of endothelin-A receptor (ETAR) by endothelin-1 (ET-1) drives epithelial-to-mesenchymal transition in ovarian tumor cells through β-arrestin signaling. Here, we investigated whether this pathogenetic pathway could affect podocyte phenotype in proliferative glomerular disorders. In cultured mouse podocytes, ET-1 caused loss of the podocyte differentiation marker synaptopodin and acquisition of the mesenchymal marker α-smooth muscle actin. ET-1 promoted podocyte migration via ETAR activation and increased β-arrestin-1 expression. Activated ETAR recruited β-arrestin-1 to form a trimeric complex with Src leading to epithelial growth factor receptor (EGFR) transactivation and β-catenin phosphorylation, which promoted gene transcription of Snail. Increased Snail expression fostered ET-1–induced migration as confirmed by Snail knockdown experiments. Silencing of β-arrestin-1 prevented podocyte phenotypic changes and motility and inhibited ETAR-driven signaling. In vitro findings were confirmed in doxorubicin (Adriamycin)-induced nephropathy. Mice receiving Adriamycin developed renal injury with loss of podocytes and hyperplastic lesion formation; β-arrestin-1 expression increased in visceral podocytes and in podocytes entrapped in pseudo-crescents. Administration of the selective ETAR antagonist sitaxsentan prevented podocyte loss, formation of the hyperplastic lesions, and normalized expression of glomerular β-arrestin-1 and Snail. Increased β-arrestin-1 levels in podocytes retrieved from crescents of patients with proliferative glomerulopathies confirmed the translational relevance of these findings and suggest the therapeutic potential of ETAR antagonism for a group of diseases still needing a specific treatment.

Published

2014

9. Analogs of bardoxolone methyl worsen diabetic nephropathy in rats with additional adverse effects

Author

Fabio Sangalli, Ariela Benigni, Giuseppe Remuzzi, Daniela Corna, Monica Locatelli, Mauro Abbate, Carla Zoja, Flavio Gaspari, Valeria Nava, and Fabiola Carrara

Subjects

Ramipril, medicine.medical_specialty, Proteinuria, Physiology, business.industry, Glomerulosclerosis, medicine.disease, Diabetic nephropathy, Endocrinology, Internal medicine, medicine, Albuminuria, Bardoxolone methyl, medicine.symptom, Bardoxolone, business, Kidney disease, medicine.drug

Abstract

Bardoxolone methyl is an antioxidant inflammation modulator acting through induction of Keap1-Nrf2 pathway. Results from a recent phase IIb clinical trial reported that bardoxolone methyl was associated with improvement in the estimated glomerular filtration rate in patients with advanced chronic kidney disease and Type 2 diabetes. However, increases in albuminuria, serum transaminase, and frequency of adverse events were noted. We studied the effect of 3-mo treatment with RTA 405, a synthetic triterpenoid analog of bardoxolone methyl in Zucker diabetic fatty rats with overt Type 2 diabetes. Rats were treated from 3 mo of age with vehicle, RTA 405, ramipril, or RTA 405 plus ramipril. RTA 405 caused severe changes in food intake and diuresis with decline in body weight, worsening of dyslipidemia, and increase in blood pressure. Early elevation in serum transaminase was followed by liver injury. RTA 405 worsened proteinuria, glomerulosclerosis, and tubular damage. Ramipril was renoprotective, but when given with RTA 405 it was not able to limit its worsening effects. These data could be due to degradation products in the drug substance used, as disclosed by the company once the study was concluded. To overcome such a drawback, the company offered to test dh404, a variant of RTA 405, in Zucker diabetic fatty rats. The dh404 did not display beneficial effects on proteinuria, glomerulosclerosis, and interstitial inflammation. Rather, kidneys from three rats receiving dh404 showed the presence of a granulomatous and inflammatory process reminiscent of a pseudotumor. Altogether these data raise serious concerns on the use of bardoxolone analogs in Type 2 diabetic nephropathy.

Published

2013

10. A previously unrecognized role of C3a in proteinuric progressive nephropathy

Author

Ariela Benigni, Monica Locatelli, Paola Rizzo, Lorena Longaretti, Daniela Corna, Carlamaria Zoja, Marina Morigi, Simona Buelli, Debora Conti, Cinzia Rota, Giuseppe Remuzzi, Mauro Abbate, and Luca Perico

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Bioinformatics, Kidney, Article, Podocyte, Nephropathy, 03 medical and health sciences, Mice, Young Adult, Downregulation and upregulation, Internal medicine, medicine, Glial cell line-derived neurotrophic factor, Animals, Humans, Cells, Cultured, Cell Proliferation, Mice, Knockout, Multidisciplinary, biology, business.industry, Glomerulosclerosis, Focal Segmental, Podocytes, Glomerulosclerosis, Epithelial Cells, Serum Albumin, Bovine, Middle Aged, medicine.disease, Epithelium, Complement system, Up-Regulation, Mice, Inbred C57BL, Disease Models, Animal, Proteinuria, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Complement Factor H, Alternative complement pathway, biology.protein, Complement C3a, Cattle, Female, business, Complement Factor B

Abstract

Podocyte loss is the initial event in the development of glomerulosclerosis, the structural hallmark of progressive proteinuric nephropathies. Understanding mechanisms underlying glomerular injury is the key challenge for identifying novel therapeutic targets. In mice with protein-overload induced by bovine serum albumin (BSA), we evaluated whether the alternative pathway (AP) of complement mediated podocyte depletion and podocyte-dependent parietal epithelial cell (PEC) activation causing glomerulosclerosis. Factor H (Cfh−/−) or factor B-deficient mice were studied in comparison with wild-type (WT) littermates. WT+BSA mice showed podocyte depletion accompanied by glomerular complement C3 and C3a deposits, PEC migration to capillary tuft, proliferation and glomerulosclerosis. These changes were more prominent in Cfh−/− +BSA mice. The pathogenic role of AP was documented by data that factor B deficiency preserved glomerular integrity. In protein-overload mice, PEC dysregulation was associated with upregulation of CXCR4 and GDNF/c-Ret axis. In vitro studies provided additional evidence of a direct action of C3a on proliferation and CXCR4-related migration of PECs. These effects were enhanced by podocyte-derived GDNF. In patients with proteinuric nephropathy, glomerular C3/C3a paralleled PEC activation, CXCR4 and GDNF upregulation. These results indicate that mechanistically uncontrolled AP complement activation is not dispensable for podocyte-dependent PEC activation resulting in glomerulosclerosis.

Published

2016

11. Lack of the Lectin-like Domain of Thrombomodulin Worsens Shiga Toxin-Associated Hemolytic Uremic Syndrome in Mice

Author

Daniela Corna, Giuseppe Remuzzi, Chiara Pagani, Edward M. Conway, Cristina Zanchi, Monica Locatelli, Carlamaria Zoja, Marina Noris, and Berend Isermann

Subjects

Male, medicine.medical_specialty, Chemokine, Mice, 129 Strain, Thrombomodulin, Immunology, Mice, Transgenic, Inflammation, urologic and male genital diseases, Severity of Illness Index, Shiga Toxin, Proinflammatory cytokine, Mice, Lectins, hemic and lymphatic diseases, Internal medicine, medicine, Animals, Immunology and Allergy, Kidney, biology, Shiga toxin, Microangiopathic hemolytic anemia, medicine.disease, Pathophysiology, Protein Structure, Tertiary, Endocrinology, medicine.anatomical_structure, Hemolytic-Uremic Syndrome, biology.protein, medicine.symptom

Abstract

Shiga toxin (Stx)-producing Escherichia coli is a primary cause of diarrhea-associated hemolytic uremic syndrome (HUS), a disorder of thrombocytopenia, microangiopathic hemolytic anemia, and acute renal failure. The pathophysiology of renal microvascular thrombosis in Stx-HUS is still ill-defined. Based on evidence that abnormalities in thrombomodulin (TM), an anticoagulant endothelial glycoprotein that modulates complement and inflammation, predispose to atypical HUS, we assessed whether impaired TM function may adversely affect evolution of Stx-HUS. Disease was induced by coinjection of Stx2/LPS in wild-type mice (TMwt/wt) and mice that lack the lectin-like domain of TM (TMLeD/LeD), which is critical for its anti-inflammatory and cytoprotective properties. After Stx2/LPS, TMLeD/LeD mice exhibited more severe thrombocytopenia and renal dysfunction than TMwt/wt mice. Lack of lectin-like domain of TM resulted in a stronger inflammatory reaction after Stx2/LPS with more neutrophils and monocytes/macrophages infiltrating the kidney, associated with PECAM-1 and chemokine upregulation. After Stx2/LPS, intraglomerular fibrin(ogen) deposits were detected earlier in TMLeD/LeD than in TMwt/wt mice. More abundant fibrin(ogen) deposits were also found in brain and lungs. Under basal conditions, TMLeD/LeD mice exhibited excess glomerular C3 deposits, indicating impaired complement regulation in the kidney that could lead to local accumulation of proinflammatory products. TMLeD/LeD mice with HUS had a higher mortality rate than TMwt/wt mice. If applicable to humans, these findings raise the possibility that genetic or acquired TM defects might have an impact on the severity of microangiopathic lesions after exposure to Stx-producing E. coli infections and raise the potential for using soluble TM in the treatment of Stx-HUS.

Published

2012

12. Distinct cardiac and renal effects of ETAreceptor antagonist and ACE inhibitor in experimental type 2 diabetes

Author

Monica Salio, Cinzia Bisighini, Sara Cattaneo, Ariela Benigni, Daniela Corna, Chiara Pagani, Vanessa Zambelli, Giuseppe Remuzzi, Carla Zoja, Daniela Rottoli, Vincenzo Lionetti, and Fabio Fiordaliso

Subjects

Blood Glucose, Male, Vascular Endothelial Growth Factor A, Ramipril, medicine.medical_specialty, Survival, Endothelin A Receptor Antagonists, Physiology, medicine.drug_class, Angiotensin-Converting Enzyme Inhibitors, Cell Count, Type 2 diabetes, Kidney, Kidney Function Tests, Real-Time Polymerase Chain Reaction, Diabetic nephropathy, Internal medicine, Diabetes mellitus, medicine, Animals, Muscle Cells, Endothelin-1, Chemistry, Myocardium, Body Weight, Hemodynamics, Glomerulosclerosis, Heart, medicine.disease, Receptor antagonist, Immunohistochemistry, Rats, Rats, Zucker, Collagen Type III, Receptors, Vascular Endothelial Growth Factor, Endocrinology, Diabetes Mellitus, Type 2, ACE inhibitor, Tyrosine, Endothelin receptor, medicine.drug

Abstract

Diabetic nephropathy is associated with cardiovascular morbidity. Angiotensin-converting enzyme (ACE) inhibitors provide imperfect renoprotection in advanced type 2 diabetes, and cardiovascular risk remains elevated. Endothelin (ET)-1 has a role in renal and cardiac dysfunction in diabetes. Here, we assessed whether combination therapy with an ACE inhibitor and ETAreceptor antagonist provided reno- and cardioprotection in rats with overt type 2 diabetes. Four groups of Zucker diabetic fatty (ZDF) rats were treated orally from 4 (when proteinuric) to 8 mo with vehicle, ramipril (1 mg/kg), sitaxsentan (60 mg/kg), and ramipril plus sitaxsentan. Lean rats served as controls. Combined therapy ameliorated proteinuria and glomerulosclerosis mostly as a result of the action of ramipril. Simultaneous blockade of ANG II and ET-1 pathways normalized renal monocyte chemoattractant protein-1 and interstitial inflammation. Cardiomyocyte loss, volume enlargement, and capillary rarefaction were prominent abnormalities of ZDF myocardium. Myocyte volume was reduced by ramipril and sitaxsentan, which also ameliorated heart capillary density. Drug combination restored myocardial structure and reestablished an adequate capillary network in the presence of increased cardiac expression of VEGF/VEGFR-1, and significant reduction of oxidative stress. In conclusion, in type 2 diabetes concomitant blockade of ANG II synthesis and ET-1 biological activity through an ETAreceptor antagonist led to substantial albeit not complete renoprotection, almost due to the ACE inhibitor. The drug combination also showed cardioprotective properties, which however, were mainly dependent on the contribution of the ETAreceptor antagonist through the action of VEGF.

Published

2011

13. Unlike each drug alone, lisinopril if combined with avosentan promotes regression of renal lesions in experimental diabetes

Author

Fabio Sangalli, Elena Gagliardini, Matteo Rossi, Carla Zoja, Lorena Longaretti, Daniela Rottoli, Sara Conti, Giuseppe Remuzzi, Andrea Remuzzi, Daniela Corna, Ariela Benigni, and Fabiola Carrara

Subjects

medicine.medical_specialty, Endothelin A Receptor Antagonists, Pyridines, Physiology, Kidney Glomerulus, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Cell Count, Pharmacology, Kidney, urologic and male genital diseases, Diabetes Mellitus, Experimental, Rats, Sprague-Dawley, Lisinopril, Diabetes mellitus, Internal medicine, medicine, Animals, Diabetic Nephropathies, RNA, Messenger, Podocytes, Reverse Transcriptase Polymerase Chain Reaction, Chemistry, Endothelin receptor antagonist, medicine.disease, Immunohistochemistry, Lipids, Angiotensin II, Capillaries, Rats, Pyrimidines, Endocrinology, Matrix Metalloproteinase 9, ACE inhibitor, Drug Therapy, Combination, Endothelin receptor, Kidney disease, medicine.drug

Abstract

In the present study, we evaluated the effect of simultaneously blocking angiotensin II synthesis and endothelin (ET)-1 activity as a multimodal intervention to implement renoprotection in overt diabetic nephropathy. Mechanisms underlying combined therapy effectiveness were addressed by investigating podocyte structure and function and glomerular barrier size-selective properties. Uninephrectomized rats made diabetic by streptozotocin received orally placebo, lisinopril (12.5 mg/l), the ETAreceptor antagonist avosentan (30 mg/kg), or their combination from 4 (when animals had proteinuria) to 8 mo. Proteinuria, renal damage, podocyte number, nephrin expression, and glomerular size selectivity by graded-size Ficoll molecule fractional clearance were assessed. Combined therapy normalized proteinuria, provided complete protection from tubulointerstitial damage, and induced regression of glomerular lesions, while only a partial renoprotection was achieved by each drug alone. Lisinopril plus avosentan restored to normal values the number of podocytes. Single therapies only limited podocyte depletion. Defective nephrin expression of diabetes was prevented by each drug. Altered glomerular size selectivity to large macromolecules of diabetic rats was remarkably improved by lisinopril and the combined treatment. Avosentan ameliorated peritubular capillary architecture and reduced interstitial inflammation and fibrosis. The ACE inhibitor and ETAreceptor antagonist induced regression of glomerular lesions in overt diabetic nephropathy. Regression of renal disease was conceivably the result of the synergistic effect of the ACE inhibitor of preserving glomerular permselective properties and the ETAantagonist in improving tubulointerstitial changes. These findings provide mechanistic insights to explain the antiproteinuric effect of this combined therapy in diabetes.

Published

2009

14. V1/V2 Vasopressin receptor antagonism potentiates the renoprotection of renin–angiotensin system inhibition in rats with renal mass reduction

Author

Daniela Corna, Lloyd Haskell, Carla Zoja, Giuseppe Remuzzi, Flavio Gaspari, Norberto Perico, and Daniela Rottoli

Subjects

Male, Vasopressin, Receptors, Vasopressin, Time Factors, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, urologic and male genital diseases, Nephrectomy, Rats, Sprague-Dawley, Renin-Angiotensin System, Eating, Enalapril, Medicine, angiotensin receptor blocker, Vasopressin receptor, renal mass reduction, Proteinuria, medicine.anatomical_structure, Losartan, Nephrology, Disease Progression, Drug Therapy, Combination, Kidney Diseases, Antidiuretic Hormone Receptor Antagonists, hormones, hormone substitutes, and hormone antagonists, medicine.drug, circulatory and respiratory physiology, medicine.medical_specialty, renal injury, Drinking, Article, Nephropathy, Hormone Antagonists, Internal medicine, ACE inhibitor, Animals, Spiro Compounds, business.industry, urogenital system, Body Weight, Benzazepines, medicine.disease, Angiotensin II, Diuresis, Rats, Disease Models, Animal, Endocrinology, Chronic Disease, proteinuric nephropathy, business, Angiotensin II Type 1 Receptor Blockers, Biomarkers, vasopressin receptor antagonist

Abstract

Blockade of the renin-angiotensin system (RAS), the standard treatment for chronic proteinuric nephropathy, slows but may not halt progression of the disease, particularly when therapy is started late. Because vasopressin may also play a role in the progression of renal disease, we measured the effect of a dual V(1a) and V(2) vasopressin receptor antagonist (RWJ-676070) alone or combined with angiotensin-converting enzyme inhibition or angiotensin II type 1 receptor blockade on proteinuria and renal disease progression during overt nephropathy. Twenty-one days after renal mass reduction, a time of established injury, rats were given vehicle, RWJ-676070, enalapril, losartan, RWJ-676070 plus enalapril, or losartan in drinking water for an additional 39 days. RWJ-676070 returned the blood pressure to pre-treatment levels, which were significantly lower than those in vehicle-treated rats. Enalapril, losartan, and the combined therapies reduced blood pressure to a greater extent. RWJ-676070 afforded a partial antiproteinuric effect, which was enhanced by the addition of enalapril or losartan. Renal functional impairment, and glomerular and tubular changes were partially ameliorated by RWJ-676070; parameters significantly improved with either enalapril or losartan alone and improved to a greater extent with the combined therapies. Our findings suggest that vasopressin receptor antagonists could be of additional therapeutic value in the treatment of chronic proteinuric nephropathy.

Published

2009

15. Complement-Mediated Dysfunction of Glomerular Filtration Barrier Accelerates Progressive Renal Injury

Author

Silvia Berlingeri, Daniela Corna, Daniela Rottoli, Mauro Abbate, Marina Morigi, Marina Noris, Cristina Zanchi, Carla Zoja, Susanna Tomasoni, Nadia Azzollini, and Giuseppe Remuzzi

Subjects

Male, Nephrology, medicine.medical_specialty, Pathology, Renal function, Podocyte, Mice, Internal medicine, medicine, Animals, Renal Insufficiency, Proteinuria, business.industry, Lisinopril, Complement C3, General Medicine, medicine.disease, Complement system, Basic Research, medicine.anatomical_structure, Endocrinology, Disease Progression, Glomerular Filtration Barrier, medicine.symptom, business, Glomerular Filtration Rate, medicine.drug, Kidney disease

Abstract

Intrarenal complement activation leads to chronic tubulointerstitial injury in animal models of proteinuric nephropathies, making this process a potential target for therapy. This study investigated whether a C3-mediated pathway promotes renal injury in the protein overload model and whether the abnormal exposure of proximal tubular cells to filtered complement could trigger the resulting inflammatory response. Mice with C3 deficiency were protected to a significant degree against the protein overload-induced interstitial inflammatory response and tissue damage, and they had less severe podocyte injury and less proteinuria. When the same injury was induced in wild-type (WT) mice, antiproteinuric treatment with the angiotensin-converting enzyme inhibitor lisinopril reduced the amount of plasma protein filtered, decreased the accumulation of C3 by proximal tubular cells, and protected against interstitial inflammation and damage. For determination of the injurious role of plasma-derived C3, as opposed to tubular cell-derived C3, C3-deficient kidneys were transplanted into WT mice. Protein overload led to the development of glomerular injury, accumulation of C3 in podocytes and proximal tubules, and tubulointerstitial changes. Conversely, when WT kidneys were transplanted into C3-deficient mice, protein overload led to a more mild disease and abnormal C3 deposition was not observed. These data suggest that the presence of C3 increases the glomerular filtration barrier's susceptibility to injury, ultrafiltered C3 contributes more to tubulointerstitial damage induced by protein overload than locally synthesized C3, and local C3 synthesis is irrelevant to the development of proteinuria. It is speculated that therapies targeting complement combined with interventions to minimize proteinuria would more effectively prevent the progression of renal disease.

Published

2008

16. Insulin-Like Growth Factor-1 Sustains Stem Cell–Mediated Renal Repair

Author

Mauro Abbate, Daniela Corna, Jun Wang, Lorena Longaretti, Federica Valsecchi, Ariela Benigni, Marina Morigi, Carla Zoja, Giuseppe Remuzzi, Daniela Rottoli, Barbara Imberti, Susanna Tomasoni, and Cinzia Rota

Subjects

Male, Nephrology, medicine.medical_specialty, Cell Survival, medicine.medical_treatment, Cell Culture Techniques, Mesenchymal Stem Cell Transplantation, Kidney Tubules, Proximal, Metabolism, transport and motion [NCMLS 2], Mice, Internal medicine, medicine, Animals, Insulin-Like Growth Factor I, Cell Proliferation, Kidney, business.industry, Cell growth, Growth factor, Mesenchymal stem cell, Acute kidney injury, Epithelial Cells, Mesenchymal Stem Cells, General Medicine, medicine.disease, Coculture Techniques, Mice, Inbred C57BL, medicine.anatomical_structure, Cell culture, Immunology, Cancer research, Female, Kidney Diseases, Cisplatin, Stem cell, Cellular energy metabolism [UMCN 5.3], business

Abstract

Item does not contain fulltext In mice with cisplatin-induced acute kidney injury, administration of bone marrow-derived mesenchymal stem cells (MSC) restores renal tubular structure and improves renal function, but the underlying mechanism is unclear. Here, we examined the process of kidney cell repair in co-culture experiments with MSC and cisplatin-injured proximal tubular epithelial cells (PTEC). Exposure of PTEC to cisplatin markedly reduced cell viability at 4 days, but co-culture with MSC provided a protective effect by promoting tubular cell proliferation. This effect was mediated by insulin-like growth factor-1 (IGF-1), highly expressed by MSC as mRNA and protein, since blocking the growth factor's function with a specific antibody attenuated cell proliferation of PTEC. Confirming this, knocking down IGF-1 expression in MSC by small interfering-RNA also resulted in a significant decrease in PTEC proliferation and increased apoptosis. Furthermore, in the murine model of cisplatin-induced kidney injury, administering IGF-1 gene-silenced MSC limited their protective effect on renal function and tubular structure. These findings indicate that MSC exert beneficial effects on tubular cell repair in acute kidney injury by producing the mitogenic and pro-survival factor IGF-1.

Published

2007

17. Therapy with a Selective Cannabinoid Receptor Type 2 Agonist Limits Albuminuria and Renal Injury in Mice with Type 2 Diabetic Nephropathy

Author

Jean-Michel Adam, Fabiana Piscitelli, Giorgio Ottaviani, Carlamaria Zoja, Giuseppe Remuzzi, Valeria Nava, Roberta Verde, Vincenzo Di Marzo, Juergen Fingerle, Monica Locatelli, Mauro Abbate, Agnes Bénardeau, Daniela Corna, Sebastian Villa, Benno Rothenhaeusler, Daniela Rottoli, and Ariela Benigni

Subjects

0301 basic medicine, Agonist, Blood Glucose, Male, medicine.medical_specialty, Cannabinoid receptor, Endocannabinoid system, medicine.drug_class, medicine.medical_treatment, Glomerular inflammation, Mice, Obese, Blood Pressure, Diabetic nephropathy, Kidney, Receptor, Cannabinoid, CB2, 03 medical and health sciences, Bridged Bicyclo Compounds, Mice, Diabetic Neuropathies, Internal medicine, Cannabinoid receptor type 2, medicine, Albuminuria, Animals, CB2 agonist, Cannabinoid Receptor Agonists, business.industry, Podocytes, musculoskeletal, neural, and ocular physiology, medicine.disease, 030104 developmental biology, Endocrinology, nervous system, Diabetes Mellitus, Type 2, BTBR ob/ob mice, lipids (amino acids, peptides, and proteins), Kidney Diseases, Cannabinoid, medicine.symptom, business, psychological phenomena and processes, Glomerular Filtration Rate

Abstract

Background/Aims: A critical involvement of the endocannabinoid/cannabinoid receptor system in diabetes and its complications has been recognized. Experimental evidence suggested that activation of the cannabinoid receptor type 2 (CB2), which is expressed in the kidney by podocytes and inflammatory cells, had a protective role in early streptozotocin-induced type 1 diabetes in mice. No experimental evidence is so far available on the effects of CB2 agonists in type 2 diabetes. In this study, we investigated the effects of a CB2 agonist given at a phase of overt disease on renal functional and structural changes in BTBR ob/ob mice, a model of type 2 diabetic nephropathy. Methods: BTBR ob/ob mice received, from 10 to 21 weeks of age, vehicle, the selective CB2 agonist HU910, or lisinopril used as standard therapy for comparison. BTBR wild-type mice served as controls. Results: Treatment with CB2 agonist reduced progressive albuminuria of BTBR ob/ob mice to a similar extent as ACE inhibitor. The antiproteinuric effect of CB2 agonist was associated with the amelioration of the defective nephrin expression in podocytes of diabetic mice. CB2 agonist limited mesangial matrix expansion, fibronectin accumulation and sclerosis. Glomerular infiltration of Mac-2-positive monocytes/machrophages was attenuated by CB2 agonist, at least in part due to the drug's ability to reduce MCP-1 chemotactic signals. Renoprotective effects of CB2 were similar to those achieved by ACE inhibitor. Conclusion: These results suggest that CB2 agonism is a potential option to be added to the available therapeutic armamentarium for type 2 diabetic nephropathy.

Published

2015

18. Targeted Deletion of Angiotensin II Type 1A Receptor Does not Protect Mice from Progressive Nephropathy of Overload Proteinuria

Author

Carla Zoja, Daniela Corna, Norberto Perico, Giuseppe Remuzzi, Ariela Benigni, Lorena Longaretti, Elena Gagliardini, and Thomas M. Coffman

Subjects

Photomicrography, Nephrology, Angiotensin receptor, medicine.medical_specialty, Molecular Sequence Data, Angiotensin-Converting Enzyme Inhibitors, urologic and male genital diseases, Glomerulonephritis, Membranous, Receptor, Angiotensin, Type 2, Sensitivity and Specificity, Nephropathy, Renin-Angiotensin System, Mice, Internal medicine, medicine, Animals, Probability, Proteinuria, Angiotensin II receptor type 1, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Glomerulonephritis, General Medicine, medicine.disease, Immunohistochemistry, Angiotensin II, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, Disease Progression, medicine.symptom, business, Kidney disease

Abstract

In experimental and human renal diseases, progression is limited by angiotensin-converting enzyme inhibitors. Whether renoprotection was due to their capacity of reducing proinflammatory and profibrotic effects of angiotensin II (Ang II) or limiting proteinuria and its long term toxicity is debated. For dissecting the relative contribution of Ang II and proteinuria to chronic renal damage, the protein-overload proteinuria model was used in genetically modified mice lacking the major isoform of murine AT1 receptor (AT1A). Uninephrectomized AT1A+/+ and -/- mice received a daily injection of BSA or saline for 4 or 11 wk. AT1A-/-BSA mice acquired a renal phenotype of proteinuria and renal glomerular and tubulointerstitial lesions, albeit attenuated with respect to AT1A+/+BSA. Administration of the calcium channel blocker lacidipine to reduce BP of AT1A+/+BSA mice to levels of AT1A-/-BSA translated into comparable values of protein excretion rate and glomerular and tubulointerstitial injury in both strains. These results confirm that the toxic effect of protein trafficking on renal disease progression is not necessarily dependent on Ang II to the extent that targeted deletion of AT1A does not prevent disease progression. A role of Ang II via AT1B or AT2 receptors is still a possibility that cannot be ruled out by the present experimental approach. These findings provide a clear rationale for specifically targeting proteinuria in pharmacologic interventions of chronic nephropathies.

Published

2004

19. Protein Overload Induces Fractalkine Upregulation in Proximal Tubular Cells through Nuclear Factor κB– and p38 Mitogen-Activated Protein Kinase–Dependent Pathways

Author

Marina Morigi, Ariela Benigni, Roberta Donadelli, Giuseppe Remuzzi, Daniela Rottoli, Carla Zoja, Simona Buelli, Susanna Tomasoni, Cristina Zanchi, Daniela Corna, Mauro Abbate, and Cristian Batani

Subjects

medicine.medical_specialty, MAP Kinase Signaling System, p38 mitogen-activated protein kinases, CX3C Chemokine Receptor 1, Inflammation, IκB kinase, p38 Mitogen-Activated Protein Kinases, Antibodies, Cell Line, Kidney Tubules, Proximal, Mice, Downregulation and upregulation, Albumins, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Bovine serum albumin, Protein kinase A, Messenger RNA, biology, Chemokine CX3CL1, NF-kappa B, Membrane Proteins, General Medicine, Molecular biology, Chemokines, CX3C, Up-Regulation, Mice, Inbred C57BL, Protein Transport, Proteinuria, Endocrinology, Solubility, Nephrology, Cell culture, biology.protein, Receptors, Chemokine, Mitogen-Activated Protein Kinases, medicine.symptom

Abstract

Investigated was the effect of high albumin concentrations on proximal tubular cell expression of fractalkine. Human proximal tubular cells (HK-2) were incubated with human serum albumin (HSA), which induced a dose-dependent increase in fractalkine mRNA associated with increased levels of both membrane-bound and soluble forms of the protein. To evaluate the role of nuclear factor κB (NF-κB) activation in HSA-induced fractalkine mRNA, HK-2 cells were infected with a recombinant adenovirus encoding the natural inhibitor of NF-κB, IkBα; a 43% reduction of fractalkine mRNA levels resulted. Similarly, when cells were infected with the recombinant adenovirus expressing dominant negative mutant of the IkB kinase 2, a 55% inhibition of fractalkine mRNA was achieved. p38 mitogen-activated protein kinase was activated by HSA and was involved in NF-κB–dependent transcription of fractalkine. In kidneys of mice with bovine serum albumin overload proteinuria, fractalkine mRNA levels were 2.3-fold greater than those of controls. Fractalkine expression was also induced in tubular epithelial cells in this model. Anti-CXCR1 antibody treatment limited interstitial accumulation of mononuclear cells. Protein overload is a promoter of fractalkine gene induction mediated by NF-κB and p38 activation in proximal tubular cells. Fractalkine might contribute to direct mononuclear cells into peritubular interstitium and enhance their adhesion property, which in turn would favor inflammation and disease progression. E-mail: gremuzzi@marionegri.it

Published

2003

20. Combining lisinopril and L-arginine slows disease progression and reduces endothelin-1 in passive Heymann nephritis

Author

Carla Zoja, Lorena Longaretti, Marta Todeschini, Giuseppe Remuzzi, Ariela Benigni, Daniela Corna, and Davide Camozzi

Subjects

Male, medicine.medical_specialty, Systole, Renal function, L-arginine, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Pharmacology, urologic and male genital diseases, Arginine, Kidney, Nephropathy, Rats, Sprague-Dawley, Heymann Nephritis, Glomerulonephritis, Membranous nephropathy, Lisinopril, Internal medicine, ACE inhibitor, medicine, Animals, Cyclic GMP, Proteinuria, Endothelin-1, business.industry, passive Heymann nephritis, medicine.disease, Rats, Drug Combinations, medicine.anatomical_structure, Endocrinology, Nephrology, Disease Progression, medicine.symptom, business, medicine.drug

Abstract

Combining lisinopril and L-arginine slows disease progression and reduces endothelin-1 in passive Heymann nephritis. Background Despite angiotensin-converting enzyme (ACE) inhibition is a very powerful therapy, it may not be uniformly renoprotective in patients with proteinuric nephropathies who might refer late in the course of the disease. In accelerated passive Heymann nephritis (PHN), a severe rat model of human membranous nephropathy, with proteinuria and increased urinary excretion of endothelin-1 (ET-1), early treatment with an ACE inhibition limited proteinuria as well as the exuberant formation of renal ET-1, while late treatment reduced urinary proteins not to a significant extent. Since biologic effects and production of ET-1 within the kidney are counteracted by nitric oxide, we studied the effect of combining lisinopril and L-arginine, the natural precursor of nitric oxide, starting late in the disease. Methods Uninephrectomized PHN rats were divided in four groups ( N = 10) and daily given orally: vehicle; 1.25 g/L L-arginine; 40mg/L lisinopril; and L-arginine + lisinopril. Treatments started at 2 months, when rats had massive proteinuria, until 9 months. Six normal rats served as control. Results Increase in systolic blood pressure was significantly limited by L-arginine. Lisinopril alone and the combination were more effective. Renal function impairment was not affected by L-arginine, partially ameliorated by ACE inhibitor and normalized by the combined therapy. In rats given L-arginine, proteinuria levels were similar to vehicle. ACE inhibitor kept proteinuria at values comparable to pretreatment and numerically lower than vehicle. Addition of L-arginine to lisinopril was more effective, with values significantly lower than vehicle. Glomerular and tubular changes were limited by the ACE inhibitor and further ameliorated by the combined therapy. Exaggerated urinary ET-1 of PHN was reduced by 23% and 40% after L-arginine and lisinopril, respectively, and by 62% with the combination. Defective urinary excretion of cyclic guanosine monophosphate (cGMP) was partially restored by lisinopril, while normalized by the combined therapy. Conclusion Combining L-arginine with ACE inhibitors would represent a novel strategy for patients with severe nephropathy not completely responsive to ACE inhibition. Restoring the nitric oxide/ET-1 balance could be of benefit in halting renal disease progression.

Published

2003

21. Effects of MCP-1 inhibition by Bindarit therapy in a rat model of polycystic kidney disease

Author

Anna Pezzotta, Carlamaria Zoja, Daniela Corna, Angelo Guglielmotti, Simona Buelli, Cristina Zanchi, Monica Locatelli, Norberto Perico, Giuseppe Remuzzi, Andrea Remuzzi, Marina Morigi, and Daniela Rottoli

Subjects

Male, medicine.medical_specialty, Indazoles, Podocyte, CCL2, In Vitro Techniques, Monocytes, Rats, Mutant Strains, Nephrin, Rats, Sprague-Dawley, chemistry.chemical_compound, Polycystic kidney disease, PCK rat, Interstitial inflammation, MCP-1, Bindarit, Proteinuria, Internal medicine, medicine, Animals, RNA, Messenger, Chemokine CCL2, Creatinine, Kidney, biology, business.industry, Podocytes, Macrophages, Settore ING-IND/34 - Bioingegneria Industriale, medicine.disease, Polycystic Kidney, Autosomal Dominant, Rats, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, chemistry, Slit diaphragm, biology.protein, medicine.symptom, Propionates, business

Abstract

Background/Aims: Experimental and clinical evidence suggested that monocyte chemoattractant protein-1 (MCP-1/CCL2) has a role in the development of interstitial inflammation and renal failure in polycystic kidney disease (PKD). We investigated whether bindarit, an inhibitor of MCP-1/CCL2 synthesis, could influence the evolution of PKD in PCK rats. Methods: PCK rats were treated from 5 to 15 weeks of age with vehicle or bindarit. Sprague-Dawley rats served as control. For in vitro studies, murine podocytes were exposed to albumin with or without bindarit. Results: MCP-1 mRNA was upregulated in the kidney of PCK rats and reduced by bindarit. Treatment limited overexpression of MCP-1 protein by epithelial cells of dilated tubules and cysts, and interstitial inflammatory cells. Excessive renal accumulation of monocytes/macrophages was lowered by bindarit by 41%. Serum creatinine slightly increased in PCK rats on vehicle and was similar to controls after bindarit. Kidney and liver cysts were not affected by treatment. Bindarit significantly reduced progressive proteinuria of PCK rats. The antiproteinuric effect was associated with the restoration of the defective nephrin expression in podocytes of PCK rats. Bindarit limited podocyte foot process effacement and ameliorated slit diaphragm frequency. In cultured podocytes, bindarit reduced MCP-1 production in response to albumin and inhibited albumin-induced cytoskeletal remodeling and cell migration. Conclusion: This study showed that although bindarit did not prevent renal cyst growth, it limited interstitial inflammation and renal dysfunction and reduced proteinuria in PKD. Thus, bindarit could be considered a therapeutic intervention complementary to therapies specifically acting to block renal cyst growth.

Published

2015

22. Effect of combining ACE inhibitor and statin in severe experimental nephropathy

Author

Susanna Tomasoni, Daniela Corna, Dario Cattaneo, Cristina Zanchi, Carla Zoja, Mauro Abbate, Daniela Rottoli, and Giuseppe Remuzzi

Subjects

CD4-Positive T-Lymphocytes, Male, Simvastatin, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, urologic and male genital diseases, Rats, Sprague-Dawley, Eating, Glomerulonephritis, Lisinopril, Chemokine CCL2, Proteinuria, Alanine Transaminase, progressive renal disease, passive Heymann nephritis, Cholesterol, Nephrology, Drug Therapy, Combination, angiotensin converting enzyme inhibitor, medicine.symptom, multidrug therapy, medicine.drug, medicine.medical_specialty, Statin, medicine.drug_class, Urology, Nephropathy, Membranous nephropathy, Internal medicine, medicine, Animals, Aspartate Aminotransferases, RNA, Messenger, Triglycerides, business.industry, Body Weight, nutritional and metabolic diseases, Glomerulosclerosis, medicine.disease, Rats, Disease Models, Animal, Endocrinology, ACE inhibitor, Hydroxymethylglutaryl-CoA Reductase Inhibitors, proteinuria, business, MCP-1

Abstract

Effect of combining ACE inhibitor and statin in severe experimental nephropathy. Background Angiotensin-converting enzyme (ACE) inhibitor therapy given soon after disease induction uniformly prevents proteinuria in virtually all models of disease progression. This does not necessarily apply to patients with proteinuric nephropathies, who might be referred late in the course of their disease. Here we used a severe rat model of passive Heymann nephritis (PHN), which may mimic advanced phases of human membranous nephropathy, to study the response to ACE inhibitor alone or in combination with a HMG CoA reductase inhibitor (statin) that independently of the cholesterol-lowering effect influences pathways involved in inflammatory and fibrogenic processes. Therapies started when animals had massive proteinuria and renal lesions. Methods PHN was accelerated by uninephrectomy seven days after IV injection of rabbit anti-FX1A antibody. Four months later, when massive proteinuria and renal lesions were present, the rats were divided into five groups and daily given orally: vehicle; lisinopril 40mg/L; lisinopril 400mg/L; simvastatin 2mg/kg b.i.d; or lisinopril 40mg/L plus simvastatin. Six normal rats served as controls. Animals were sacrificed at 10 months. Results By the end of the study three PHN rats died in the vehicle group, four in the group given lisinopril at 40mg/L and two in the group at 400mg/L, whereas all rats on simvastatin or combined therapy were alive. Blood pressure increased during time in PHN and was normalized by treatment with ACE inhibitor and combined therapy. Even at the high dose lisinopril failed to reduce proteinuria. Simvastatin only partially affected proteinuria. However, combining lisinopril with simvastatin had a remarkable antiproteinuric effect, such that at 10 months the urinary proteins were comparable to pre-treatment values and significantly lower than either the vehicle or lisinopril groups. Hypercholesterolemia of PHN rats was limited by combined therapy, and a positive correlation was found between serum cholesterol and proteinuria. Renal function was only partially ameliorated by simvastatin but significantly improved by combined therapy. Drug combination significantly limited glomerulosclerosis, tubular damage and interstitial inflammation, compared to vehicle or drugs alone. Up-regulation of monocyte chemoattractant protein-1 (MCP-1) mRNA in PHN kidneys was not affected by lisinopril, it was inhibited by 30% after simvastatin, and almost completely normalized by lisinopril plus simvastatin. Conclusions These data suggest that a combined ACE inhibitor and statin approach could represent a therapeutic option for patients with advanced renal disease in whom ACE inhibitors alone fail to lower proteinuria and injury to any substantial extent.

Published

2002

23. Renoprotection by nitric oxide donor and lisinopril in the remnant kidney model

Author

Ariela Benigni, Marina Noris, Marta Todeschini, Isabella Bruzzi, Daniela Corna, Giuditta Benedetti, Carla Zoja, and Giuseppe Remuzzi

Subjects

Male, medicine.medical_specialty, Reserpine, Molsidomine, Nitrous Oxide, Renal function, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, Nitric Oxide, Nephrectomy, Rats, Sprague-Dawley, Eating, chemistry.chemical_compound, Lisinopril, Internal medicine, medicine, Animals, Nitric Oxide Donors, Endothelin-1, business.industry, Body Weight, Hydralazine, medicine.disease, Uremia, Rats, Hydrochlorothiazide, Blood pressure, Endocrinology, medicine.anatomical_structure, chemistry, Nephrology, Creatinine, ACE inhibitor, Disease Progression, business, medicine.drug

Abstract

Previous studies showed a renoprotective effect of l-arginine in experimental uremia. Whether this was caused by an increased nitric oxide (NO) release or depended on l-arginine per se is not clear. Here, we evaluated whether chronic administration of an NO donor, molsidomine, controlled systemic blood pressure and renal disease progression and prolonged survival in rats with renal mass reduction (RMR). Rats with RMR received the following daily in the drinking water: group 1 (n = 21), no specific therapy (vehicle); group 2 (n = 12), molsidomine, 120 mg/L; group 3 (n = 9), lisinopril, 25 mg/L; and group 4 (n = 12), reserpine, 5 mg/L, hydralazine, 80 mg/L, and hydrochlorothiazide, 25 mg/L, from day 21 after surgery, when rats had hypertension and proteinuria, until the death of the vehicle-treated rats. Molsidomine normalized systemic hypertension, only partially reduced proteinuria and serum creatinine levels, but significantly prolonged animal survival, particularly in the early stage of the disease. Lisinopril at a similar systemic blood pressure was even better than molsidomine in limiting proteinuria, preserving renal function, and prolonging survival, but triple therapy, despite being effective on blood pressure, offered no renoprotection or prolonged survival. Endothelin-1 (ET-1) levels, formed in excessive amounts by the kidneys of these animals, were reduced by molsidomine and lisinopril, but not by triple therapy. The prolongation of survival by NO donor could be attributed to its effect of reducing ET levels, which in turn may limit the smooth muscle cell proliferation and matrix accumulation responsible for organ and, especially, myocardial fibrosis in uremia.

Published

1999

24. In progressive nephropathies, overload of tubular cells with filtered proteins translates glomerular permeability dysfunction into cellular signals of interstitial inflammation

Author

Carla Zoja, Tullio Bertani, Giuseppe Remuzzi, Mauro Abbate, Matteo Capitanio, and Daniela Corna

Subjects

Male, Pathology, medicine.medical_specialty, Cell Membrane Permeability, Sialoglycoproteins, Kidney Glomerulus, Inflammation, Biology, Kidney Tubules, Proximal, Rats, Sprague-Dawley, Heymann Nephritis, Reference Values, Albumins, Internal medicine, medicine, Animals, Osteopontin, Microscopy, Immunoelectron, Ultrasonography, Kidney, Reabsorption, Histocompatibility Antigens Class II, Glomerulonephritis, General Medicine, Phosphoproteins, medicine.disease, Immunohistochemistry, Rats, Cellular infiltration, Disease Models, Animal, Proteinuria, medicine.anatomical_structure, Endocrinology, Nephrology, Immunoglobulin G, Disease Progression, biology.protein, Nephritis, Interstitial, medicine.symptom, Infiltration (medical), Signal Transduction

Abstract

Progression to end-stage renal failure is the final common pathway of many forms of glomerular disease, independent of the type of initial insult. Progressive glomerulopathies have in common persistently high levels of urinary protein excretion and tubulointerstitial lesions at biopsy. Among the cellular mechanisms that may determine progression regardless of etiology, the traffic of excess proteins filtered from glomerulus in renal tubule may have functional importance by initiating interstitial inflammation in the early phase of parenchymal injury. This study analyzes the time course and sites of protein accumulation and interstitial cellular infiltration in two different models of proteinuric nephropathies. In remnant kidneys after 5/6 renal mass ablation, albumin and IgG accumulation by proximal tubular cells was visualized in the early stage, preceding interstitial infiltration of MHC-II-positive cells and macrophages. By double-staining, infiltrates developed at or near tubules containing intracellular IgG or luminal casts. This relationship persisted thereafter despite more irregular distribution of infiltrate. Similar patterns were found in an immune model (passive Heymann nephritis), indicating that the interstitial inflammatory reaction develops at the sites of protein overload, regardless of the type of glomerular injury. Osteopontin was detectable in cells of proximal tubules congested with protein in both models at sites of interstitial infiltration, and by virtue of its chemoattractive action this is likely mediator of a proximal tubule-dependent inflammatory pathway in response to protein load. Protein overload of tubules is a key candidate process translating glomerular protein leakage into cellular signals of interstitial inflammation. Mechanisms underlying the proinflammatory response of tubular cells to protein challenge in diseased kidney should be explored, as well as ways of limiting protein reabsorption/deposition to prevent consequent inflammation and progressive disease.

Published

1998

25. Bindarit retards renal disease and prolongs survival in murine lupus autoimmune disease

Author

Daniela Corna, Tullio Bertani, Marina Morigi, Roberta Donadelli, Giuseppe Remuzzi, Carla Zoja, Mario Pinza, Angelo Guglielmotti, and Giuditta Benedetti

Subjects

medicine.medical_specialty, Indazoles, medicine.medical_treatment, monocyte chemoattractant protein-1, Lupus nephritis, Kidney, Methylprednisolone, Gastroenterology, murine lupus autoimmune disease, Blood Urea Nitrogen, Nephropathy, Mice, Internal medicine, medicine, Animals, Humans, Blood urea nitrogen, Chemokine CCL2, Chemotherapy, immunosuppression, Systemic lupus erythematosus, Mice, Inbred NZB, business.industry, Immunosuppression, glomerular hypercellularity, medicine.disease, Lupus Nephritis, Rats, Proteinuria, Endocrinology, inflammation, Nephrology, Antibodies, Antinuclear, Female, Inflammation Mediators, Propionates, business, medicine.drug, Kidney disease

Abstract

Bindarit retards renal disease and prolongs survival in murine lupus autoimmune disease. As an alternative to classical immunosuppressants in experimental lupus nephritis, we looked at bindarit, 2-methyl-2-{[1-phenylmethyl)-1H-indazol-3-y1]methoxy}propanoic acid, a novel molecule devoid of immunosuppressive effects, which selectively reduces chronic inflammation in rat adjuvant arthritis. Two groups of NZB/W mice (N = 55 for each group) were given bindarit, (50 mg/kg/day p.o.) or vehicle starting at 2 months of age. Mice were sacrificed at 2, 6, 8 and 10 months or used for survival studies. Bindarit delayed the onset of proteinuria (% proteinuric mice, bindarit vs. vehicle, 6 months: 0 vs. 33% and 8 months: 7% vs. 60%, P < 0.005; 10 months: 53% vs. 80%) and significantly (P < 0.05) protected from renal function impairment (serum BUN, bindarit vs. vehicle: 8 months, 30 ± 3 vs. 127 ± 42; 10 months, 53 ± 5 vs. 140 ± 37 mg/dl). Appearance of anti-DNA antibodies was retarded and survival significantly (P < 0.0001) prolonged by bindarit (% survival, bindarit vs. vehicle: 8 months, 100% vs. 80%; 10 months, 87% vs. 40%; 12 months, 27% vs. 20%). Bindarit significantly limited glomerular hypercellularity, interstitial inflammation and tubular damage. Renal expression of monocyte chemoattractant protein (MCP-1) mRNA (Northern blot) markedly increased (7- 12-fold in 8- 10-month-old mice vs. 2-month-old) during the progression of nephritis in association with mononuclear cell infiltration. Bindarit completely prevented MCP-1 up-regulation. In another series of experiments, bindarit (0.25% and 0.5% medicated diet, N = 16 for each group) when started at 4.5 months of age in NZB/W mice improved survival in respect to untreated mice (N = 17) in a dose-dependent manner (% survival: 8 months, 94% and 100%, respectively, vs. 47%; 10 months, 75% and 100% vs. 35%; 12 months, 31% and 75% vs. 12%). Survival was even more prolonged when bindarit (0.5% medicated diet) was combined with a low dose of methylprednisolone (1.5 mg/kg i.p.), which that only partially modifies proteinuria and survival of lupus mice, in an additional group of animals (N = 16). Thus, at 14.5 months when all mice given bindarit alone died, 50% of mice on combined therapy were still alive (P < 0.023). Studies are needed to establish whether bindarit may function as a steroid sparing drug in human lupus.

Published

1998

26. Shiga Toxin Promotes Podocyte Injury in Experimental Hemolytic Uremic Syndrome via Activation of the Alternative Pathway of Complement

Author

Anna Pezzotta, Joshua M. Thurman, Susanna Tomasoni, Simona Buelli, Luca Perico, Giuseppe Remuzzi, Daniela Corna, Monica Locatelli, Marina Morigi, Daniela Rottoli, Debora Conti, Paola Rizzo, and Carlamaria Zoja

Subjects

Lipopolysaccharides, Male, medicine.medical_specialty, Complement Pathway, Alternative, Kidney Glomerulus, Cell Culture Techniques, Protein Serine-Threonine Kinases, urologic and male genital diseases, Complement factor B, Shiga Toxin 2, Podocyte, Nephrin, Mice, Downregulation and upregulation, Internal medicine, hemic and lymphatic diseases, medicine, Animals, Humans, biology, Podocytes, Glomerular basement membrane, General Medicine, Complement system, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, Basic Research, Nephrology, Hemolytic-Uremic Syndrome, biology.protein, Cancer research, Alternative complement pathway, Complement C3a, C3a receptor, Signal Transduction

Abstract

Shiga toxin (Stx)-producing Escherichia coli is the offending agent of postdiarrhea-associated hemolytic uremic syndrome (HUS), a disorder of glomerular ischemic damage and widespread microvascular thrombosis. We previously documented that Stx induces glomerular complement activation, generating C3a responsible for microvascular thrombosis in experimental HUS. Here, we show that the presence of C3 deposits on podocytes is associated with podocyte damage and loss in HUS mice generated by the coinjection of Stx2 and LPS. Because podocyte adhesion to the glomerular basement membrane is mediated by integrins, the relevance of integrin-linked kinase (ILK) signals in podocyte dysfunction was evaluated. Podocyte expression of ILK increased after the injection of Stx2/LPS and preceded the upregulation of Snail and downregulation of nephrin and α-actinin-4. Factor B deficiency or pretreatment with an inhibitory antibody to factor B protected mice against Stx2/LPS-induced podocyte dysregulation. Similarly, pretreatment with a C3a receptor antagonist limited podocyte loss and changes in ILK, Snail, and α-actinin-4 expression. In cultured podocytes, treatment with C3a reduced α-actinin-4 expression and promoted ILK-dependent nuclear expression of Snail and cell motility. These results suggest that Stx-induced activation of the alternative pathway of complement and generation of C3a promotes ILK signaling, leading to podocyte dysfunction and loss in Stx-HUS.

Published

2014

27. The renoprotective properties of angiotensin-converting enzyme inhibitors in a chronic model of membranous nephropathy are solely due to the inhibition of angiotensin II: Evidence based on comparative studies with a receptor antagonist

Author

Carla Zoja, Roberta Donadelli, Daniela Corna, Tullio Bertani, Elena Luzzana, Raffaello Maffi, Vittoria Colosio, Daniela Facchinetti, Davide Testa, and Giuseppe Remuzzi

Subjects

Male, medicine.medical_specialty, Renal Plasma Flow, Tetrazoles, Bradykinin, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, urologic and male genital diseases, Glomerulonephritis, Membranous, Rats, Sprague-Dawley, Angiotensin Receptor Antagonists, chemistry.chemical_compound, Membranous nephropathy, Lisinopril, Transforming Growth Factor beta, Internal medicine, medicine, Animals, Extracellular Matrix Proteins, biology, business.industry, Angiotensin II, Imidazoles, Glomerulosclerosis, Angiotensin-converting enzyme, medicine.disease, Rats, Proteinuria, medicine.anatomical_structure, Endocrinology, chemistry, Nephrology, Chronic Disease, ACE inhibitor, biology.protein, business, Glomerular Filtration Rate, medicine.drug

Abstract

In several models of renal disease progression, angiotensin-converting enzyme (ACE) inhibitors reduced proteinuria and limited glomerulosclerosis, which suggested that reduction of renal angiotensin II (Ang II) activity is crucial for the preservation of glomerular structure and function. However, it cannot be ruled out that other hormonal systems, including inhibition of the bradykinin breakdown, also play a role. We compared the effects of chronic treatment with the ACE inhibitor lisinopril with those of a specific Ang II receptor antagonist, L-158,809, on proteinuria and renal injury in passive Heymann nephritis (PHN), a model of immune renal disease that closely resembles human membranous nephropathy, with long-lasting proteinuria followed by tubulointerstitial damage and glomerulosclerosis. Passive Heymann nephritis was induced with 0.5 mL/100 g of rabbit anti-Fx1A antibody in 24 male Sprague-Dawley rats. The animals were divided into three groups of eight rats each, and were given the following in the drinking water on a daily basis: lisinopril (40 mg/L), L-158,809 (50 mg/L), or no therapy. Treatment started at day 7 (proteinuria was already present) and lasted 12 months. Eight normal rats were used as controls. Untreated PHN rats developed hypertension, while rats with PHN given lisinopril or L-158,809 all had systolic blood pressure values even lower than those of normal rats. Urinary protein excretion progressively increased with time in untreated PHN rats, who developed tubulointerstitial damage and glomerulosclerosis. Both lisinopril and L-158,809 exhibited a potent antiproteinuric effect and preserved glomerular and tubular structural integrity at a similar extent. Renal gene expression of transforming growth factor-β and extracellular matrix proteins was also effectively reduced by the two treatments. These results indicate that ACE inhibitors and Ang II receptor antagonists are equally effective in preventing renal injury in PHN and suggest that the renoprotective effects of ACE inhibitors in this model are solely due to inhibition of Ang II.

Published

1997

28. Renal Expression of FGF23 in Progressive Renal Disease of Diabetes and the Effect of Ace Inhibitor

Author

Flavio Gaspari, Ariela Benigni, Cristina Zanchi, Daniela Rottoli, Susanna Tomasoni, Giuseppe Remuzzi, Carlamaria Zoja, Monica Locatelli, and Daniela Corna

Subjects

Fibroblast growth factor 23, Male, Anatomy and Physiology, 030232 urology & nephrology, lcsh:Medicine, Gene Expression, Veterinary Anatomy and Physiology, Angiotensin-Converting Enzyme Inhibitors, urologic and male genital diseases, Kidney, Biochemistry, Diabetic nephropathy, 0302 clinical medicine, Endocrinology, Molecular Cell Biology, lcsh:Science, Klotho, Glucuronidase, 0303 health sciences, Multidisciplinary, Animal Renal Anatomy, biology, Animal Models, medicine.anatomical_structure, Disease Progression, Medicine, medicine.drug, Research Article, Ramipril, medicine.medical_specialty, Endocrine System, Peptidyl-Dipeptidase A, Phosphates, Molecular Genetics, 03 medical and health sciences, Model Organisms, Internal medicine, medicine, Genetics, Animals, Biology, Klotho Proteins, 030304 developmental biology, Diabetic Endocrinology, Endocrine Physiology, business.industry, lcsh:R, Kidney metabolism, Computational Biology, Angiotensin-converting enzyme, Sodium-Phosphate Cotransporter Proteins, Renal System, Diabetes Mellitus Type 2, medicine.disease, Hormones, Rats, Fibroblast Growth Factors, stomatognathic diseases, Diabetes Mellitus, Type 2, Gene Expression Regulation, Cytoprotection, ACE inhibitor, biology.protein, Rat, lcsh:Q, Veterinary Science, business

Abstract

Fibroblast growth factor 23 (FGF23) is a phosphaturic hormone mainly produced by bone that acts in the kidney through FGF receptors and Klotho. Here we investigated whether the kidney was an additional source of FGF23 during renal disease using a model of type 2 diabetic nephropathy. Renal expression of FGF23 and Klotho was assessed in Zucker diabetic fatty (ZDF) and control lean rats at 2, 4, 6, 8 months of age. To evaluate whether the renoprotective effect of angiotensin converting enzyme (ACE) inhibitor in this model was associated with changes in FGF23 and Klotho, ZDF rats received ramipril from 4, when proteinuric, to 8 months of age. FGF23 mRNA was not detectable in the kidney of lean rats, nor of ZDF rats at 2 months of age. FGF23 became measurable in the kidney of diabetic rats at 4 months and significantly increased thereafter. FGF23 protein localized in proximal and distal tubules. Renal Klotho mRNA and protein decreased during time in ZDF rats. As renal disease progressed, serum phosphate levels increased in parallel with decline of fractional phosphorus excretion. Ramipril limited proteinuria and renal injury, attenuated renal FGF23 upregulation and ameliorated Klotho expression. Ramipril normalized serum phosphate levels and tended to increase fractional phosphorus excretion. These data indicate that during progressive renal disease the kidney is a site of FGF23 production which is limited by ACE inhibition. Interfering pharmacologically with the delicate balance of FGF23 and phosphorus in diabetes may have implications in clinics.

Published

2013

29. A Study of Low-Nutrient Diets Used for Aging Studies in the Rat

Author

Daniela Corna, F. Norido, M. E. Coates, C. Zoja, C. Fiorito, and Tullio Bertani

Subjects

Male, Aging, medicine.medical_specialty, Low protein, Rodent, media_common.quotation_subject, Biology, Kidney, Nephropathy, Rats, Sprague-Dawley, Eating, Nutrient, Animal science, biology.animal, Internal medicine, Abdomen, Diet, Protein-Restricted, medicine, Animals, media_common, Proteinuria, Glomerulosclerosis, Focal Segmental, Body Weight, Glomerulosclerosis, medicine.disease, Obesity, Diet, Rats, Kidney Tubules, Endocrinology, Adipose Tissue, Kidney Diseases, Dietary Proteins, Geriatrics and Gerontology, Reproduction, medicine.symptom, Energy Intake, Energy Metabolism

Abstract

The effects of diets of low caloric value on rats used in aging studies were investigated. Groups of 85 Sprague-Dawley rats were fed ad libitum from 3 months of age on three different diets containing 8 or 10 Megajoule (MJ) of metabolizable energy and 80 or 100 g of crude protein/kg. Body weights, food consumption, and morphological and biochemical parameters were monitored throughout life. Kidneys were examined histologically. Rats given the diet with highest energy and protein ate less food, attained greater weights, and had larger abdominal fat deposits than those on the lower energy diets. They had a raised proteinuria, and nearly half developed glomerulosclerosis and tubulo-interstitial damage by 26 months. There was no significant difference in mortality between the groups, and no other serious abnormalities were observed. It is concluded that rats can be maintained into old age with no signs of nutritional inadequacy on diets with lower energy and protein contents than those in general use. T HE nutrient content of laboratory animal diets currently in use, though generally well able to sustain good growth and reproduction, is much more than adequate for maintenance. In the sheltered conditions of the laboratory, with a constant supply of food, laboratory rodents overeat, become obese, and are prone to nephropathies and neoplastic diseases that influence mortality and interfere with the objectives of long-term experiments. It is well known that restricting food intake has a life-prolonging effect (see review by Cohen, 1979), and several groups have shown that mortality and incidence of disease in laboratory rodents can be reduced by limiting food intake (Tucker, 1979; Conybeare et al., 1986; Masoro, 1988). Restriction can be imposed by rationing the animals to a given weight of food daily or, more simply, by allowing them free access to food for a limited time each day. Both systems are demanding of time and labor and may impose stress on animals whose natural habit is to eat small quantities of food over a long period. A more practical solution would be to compound a nutritionally adequate diet of reduced caloric value that could be fed ad libitum without inducing obesity and the attendant deleterious effects (Cohen, 1979; Coates, 1991). The work reported here was undertaken to explore this suggestion, with a view to the production of rats for studies of aging. Three diets of low protein and energy content were formulated from natural materials commonly used in commercial rodent diets. They were fed to rats from the age of 3 months, and growth, food intake, and morphological and biochemical parameters were monitored until the animals were more than 2 years old. Because aging in rats is commonly associated with development of chronic nephropathy, the kidneys of a representative sample of rats from each treatment were examined histologically at 12

Published

1996

30. Adenoviral-mediated gene transfer restores plasma ADAMTS13 antigen and activity in ADAMTS13 knockout mice

Author

Lorena Longaretti, G. Remuzzi, Daniela Corna, D Motto, Miriam Galbusera, Ariela Benigni, Susanna Tomasoni, and Piera Trionfini

Subjects

medicine.medical_specialty, Genetic Vectors, Thrombotic thrombocytopenic purpura, ADAMTS13 Protein, Spleen, Adenoviridae, Mice, Von Willebrand factor, Transduction, Genetic, hemic and lymphatic diseases, Internal medicine, Genetics, medicine, Animals, Secretion, Molecular Biology, Mice, Knockout, Metalloproteinase, Kidney, biology, Purpura, Thrombotic Thrombocytopenic, business.industry, Metalloendopeptidases, Genetic Therapy, medicine.disease, ADAMTS13, medicine.anatomical_structure, Endocrinology, Immunology, Knockout mouse, biology.protein, Molecular Medicine, business

Abstract

ADAMTS13 is a plasma metalloprotease that regulates the size of the von Willebrand factor (VWF) multimers. Genetic or acquired deficiency of ADAMTS13 causes thrombotic thrombocytopenic purpura (TTP) in humans. Plasma infusion is the treatment of choice for patients with congenital ADAMTS13 deficiency. However, this practice exposes patients to the risk of infections, allergies and fluid volume overload. The search for alternative treatments is required. Here, we tested the ability of systemically administered adenovirus encoding human ADAMTS13 to restore the deficient protein in the circulation of Adamts13(-/-) mice. Injection of the adenovirus efficiently transduced the liver, kidney, lung, heart and spleen, resulting in the secretion of ADAMTS13 into plasma. A reduced area of thrombi was observed when blood from Ad-ADAMTS13-treated mice was perfused over a collagen-coated surface in a parallel plate flow chamber compared with blood of Ad-betaGal-treated controls. The secreted ADAMTS13 protein was functionally active even after 2 months from injection. The data provide the proof of principle for developing a novel therapy for the correction of ADAMTS13 deficiency in patients with hereditary TTP.

Published

2009

31. Proteasomal Processing of Albumin by Renal Dendritic Cells Generates Antigenic Peptides

Author

Giuseppe Remuzzi, Elena Gagliardini, Chiara Chiabrando, Caterina Mele, Simona Buelli, Silvia Schiarea, Daniela Macconi, Carla Zoja, Ariela Benigni, Marina Noris, Sistiana Aiello, Daniela Corna, Linda Cassis, and Roberto Fanelli

Subjects

medicine.medical_specialty, Proteasome Endopeptidase Complex, Antigen presentation, CD8-Positive T-Lymphocytes, Kidney, Immune tolerance, Kidney Tubules, Proximal, Rats, Sprague-Dawley, Antigen, Internal medicine, Albumins, MHC class I, medicine, Immune Tolerance, Animals, Antigen Presentation, biology, Histocompatibility Antigens Class I, General Medicine, Dendritic Cells, Cell biology, CD11c Antigen, Rats, Proteinuria, Endocrinology, medicine.anatomical_structure, Basic Research, Proteasome, Nephrology, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, Lymph, Proteasome Inhibitors, CD8

Abstract

The role of dendritic cells (DC) that accumulate in the renal parenchyma of non-immune-mediated proteinuric nephropathies is not well understood. Under certain circumstances, DC capture immunologically ignored antigens, including self-antigens, and present them within MHC class I, initiating an autoimmune response. We studied whether DC could generate antigenic peptides from the self-protein albumin. Exposure of rat proximal tubular cells to autologous albumin resulted in its proteolytic cleavage to form an N-terminal 24-amino acid peptide (ALB1-24). This peptide was further processed by the DC proteasome into antigenic peptides that had binding motifs for MHC class I and were capable of activating syngeneic CD8+ T cells. In vivo, the rat five-sixths nephrectomy model allowed the localization and activation of renal DC. Accumulation of DC in the renal parenchyma peaked 1 wk after surgery and decreased at 4 wk, concomitant with their appearance in the renal draining lymph nodes. DC from renal lymph nodes, loaded with ALB1-24, activated syngeneic CD8+ T cells in primary culture. The response of CD8+ T cells of five-sixths nephrectomized rats was amplified with secondary stimulation. In contrast, DC from renal lymph nodes of five-sixths nephrectomized rats treated with the proteasomal inhibitor bortezomib lost their capacity to stimulate CD8+ T cells in primary and secondary cultures. These data suggest that albumin can be a source of potentially antigenic peptides upon renal injury and that renal DC play a role in processing self-proteins through a proteasome-dependent pathway.

Published

2009

32. Disruption of the Ang II type 1 receptor promotes longevity in mice

Author

Daniela Corna, Marina Morigi, Ariela Benigni, Sara Conti, Thomas M. Coffman, Carla Zoja, Paola Cassis, Daniela Rottoli, Monica Salio, Lorena Longaretti, Roberto Latini, Giuseppe Remuzzi, and Aurelio Sonzogni

Subjects

Blood Glucose, medicine.medical_specialty, SIRT3, Heart Diseases, Longevity, Nicotinamide phosphoribosyltransferase, Down-Regulation, Inflammation, Biology, medicine.disease_cause, Mitochondrial Proteins, chemistry.chemical_compound, Mice, Downregulation and upregulation, Internal medicine, Sirtuin 3, medicine, Animals, Sirtuins, Vascular Diseases, Receptor, Nicotinamide Phosphoribosyltransferase, Adaptor Proteins, Signal Transducing, Mice, Knockout, Angiotensin II receptor type 1, Body Weight, General Medicine, Up-Regulation, Oxidative Stress, Endocrinology, Phenotype, chemistry, Rotarod Performance Test, Sirtuin, biology.protein, cardiovascular system, Cytokines, medicine.symptom, Energy Intake, Oxidative stress, hormones, hormone substitutes, and hormone antagonists, Research Article

Abstract

The renin-angiotensin system plays a role in the etiology of hypertension and the pathophysiology of cardiac and renal diseases in humans. Ang II is the central product of this system and is involved in regulating immune responses, inflammation, cell growth, and proliferation by acting through Ang II type 1 receptors (AT1 and AT2). Here, we show that targeted disruption of the Agtr1a gene that encodes AT1A results in marked prolongation of life span in mice. Agtr1a-/- mice developed less cardiac and vascular injury, and multiple organs from these mice displayed less oxidative damage than wild-type mice. The longevity phenotype was associated with an increased number of mitochondria and upregulation of the prosurvival genes nicotinamide phosphoribosyltransferase (Nampt) and sirtuin 3 (Sirt3) in the kidney. In cultured tubular epithelial cells, Ang II downregulated Sirt3 mRNA, and this effect was inhibited by an AT1 antagonist. These results demonstrate that disruption of AT1 promotes longevity in mice, possibly through the attenuation of oxidative stress and overexpression of prosurvival genes, and suggests that the Ang II/AT1 pathway may be targeted to influence life span in mammals.

Published

2008

33. Oral zeranol shortens the prolonged bleeding time of uremic rats

Author

Giuseppe Remuzzi, Carla Zoja, Silvio Garattini, Gianluigi Viganò, Daniela Corna, and Mario Salmona

Subjects

Male, medicine.medical_specialty, Bleeding Time, medicine.drug_class, Administration, Oral, Estrogen receptor, chemistry.chemical_compound, Prolonged bleeding time, Oral administration, Bleeding time, Internal medicine, medicine, Zeranol, Animals, Uremia, Hemostasis, medicine.diagnostic_test, business.industry, Rats, Inbred Strains, Resorcinols, medicine.disease, Rats, Endocrinology, Receptors, Estrogen, chemistry, Estrogen, Nephrology, business, hormones, hormone substitutes, and hormone antagonists

Abstract

Oral zeranol shortens the prolonged bleeding time of uremic rats.Intravenous conjugated estrogens reduce the prolonged bleeding time in uremic patients and in a rat model of uremia. However, estrogens have major side effects related to their hormonal activity. We investigated whether a β-resorcylic acid lactone, zeranol (a compound with close spatial similarity to estrogens but with a weak estrogenic activity), improves primary hemostasis in uremic rats and whether the effect is mediated by estrogen receptors. The results showed that single oral administration of zeranol significantly (P < 0.01) shortened the bleeding time of uremic rats, 20 mg/kg being the minimum effective dose. This effect was long-lasting (72 hours). The dose of 30 mg/kg zeranol reproduced the pattern observed after 20 mg/kg but bleeding time values were still significantly (P < 0.01) shortened 96 hours after the administration. No changes in hematocrit, platelet and leukocyte count, and serum creatinine were detected after zeranol administration. When uremic rats were pre-treated orally with two estrogen receptor antagonists, tamoxifen and clomiphene (3 mg/kg), zeranol did not shorten the bleeding time, thus suggesting that the hemostatic effect of zeranol was due to an estrogen receptor-mediated mechanism. These results might have important future implications for the management of uremic bleeding in humans.

Published

1990

34. Cyclin-dependent kinase inhibition limits glomerulonephritis and extends lifespan of mice with systemic lupus

Author

Regiane Aparecida Cavinato, Federica Casiraghi, Daniela Corna, Ariela Benigni, Giuseppe Remuzzi, Sara Conti, Daniela Rottoli, and Carla Zoja

Subjects

medicine.medical_specialty, medicine.medical_treatment, T cell, T-Lymphocytes, Immunology, Longevity, Anti-Inflammatory Agents, Autoimmunity, Mice, Inbred Strains, Methylprednisolone, chemistry.chemical_compound, Mice, Glomerulonephritis, Rheumatology, Cyclin-dependent kinase, Internal medicine, medicine, Roscovitine, Immunology and Allergy, Animals, Lupus Erythematosus, Systemic, Pharmacology (medical), Protein Kinase Inhibitors, B cell, Seliciclib, Cell Proliferation, B-Lymphocytes, Systemic lupus erythematosus, biology, Mice, Inbred NZB, business.industry, medicine.disease, Cyclin-Dependent Kinases, Disease Models, Animal, Proteinuria, Endocrinology, medicine.anatomical_structure, Cytokine, chemistry, Purines, biology.protein, Drug Therapy, Combination, Female, business, medicine.drug

Abstract

Objective To examine whether the cyclin-dependent kinase (CDK) inhibitor seliciclib ameliorates autoimmune nephritis in (NZB × NZW)F1 mice. Methods In experiment 1, NZB × NZW mice received seliciclib (100 mg/kg or 200 mg/kg) or vehicle by gavage, beginning at age 2 months and ending at 8 months of age. In experiment 2, seliciclib (200 mg/kg) was administered alone or combined with low-dose methylprednisolone, starting at age 5 months, when immune complex deposition in the kidney had already occurred. Animals were followed up until all vehicle-treated mice died. In 2 additional groups of NZB × NZW mice treated with seliciclib or vehicle from 2 months of age until 5 months of age, splenocytes were isolated and tested ex vivo for T cell and B cell activity. Results Seliciclib, given at an early phase of disease, prolonged survival, delayed the onset of proteinuria and renal function impairment, and protected the kidney against glomerular hypercellularity, tubulointerstitial damage, and inflammation. Combining seliciclib with low-dose methylprednisolone in mice with established disease extended the lifespan and limited proteinuria and renal damage more than treatment with either agent alone. Seliciclib limited immunologic signs of disease, reducing glomerular IgG and C3 deposits and levels of serum anti-DNA antibodies. Moreover, it inhibited ex vivo T cell and B cell proliferative responses to polyclonal stimuli. T cell production of interferon-γ and interleukin-10 and B cell release of IgG2a were reduced by treatment with seliciclib. Conclusion These findings suggest that CDK activity may be a useful target in the treatment of systemic lupus erythematosus. A direct immunomodulatory action of seliciclib on T cells and B cells may be one of the mechanisms underlying the beneficial effects.

Published

2007

35. Imatinib ameliorates renal disease and survival in murine lupus autoimmune disease

Author

Mauro Abbate, Daniela Corna, Daniela Rottoli, G. Remuzzi, Carlamaria Zoja, and Cristina Zanchi

Subjects

NZB/W mice, medicine.medical_specialty, transforming growth factor, medicine.drug_class, Lupus nephritis, Kidney, Tyrosine-kinase inhibitor, Piperazines, Nephropathy, platelet-derived growth factor, Mice, Internal medicine, medicine, Animals, Lupus Erythematosus, Systemic, Receptors, Platelet-Derived Growth Factor, Protein Kinase Inhibitors, Autoimmune disease, Systemic lupus erythematosus, biology, business.industry, Imatinib, Muscle, Smooth, Fibroblasts, medicine.disease, Antigens, Differentiation, Lupus Nephritis, Actins, Proteinuria, Endocrinology, Pyrimidines, imatinib, Nephrology, Immunology, Benzamides, biology.protein, Imatinib Mesylate, Leukocytes, Mononuclear, Female, business, Platelet-derived growth factor receptor, Kidney disease, medicine.drug

Abstract

Platelet-derived growth factor (PDGF) has been proved to play an important role in progressive glomerular disease of systemic lupus. The present study investigated the tyrosine kinase inhibitor of PDGF receptor, imatinib, as a novel therapeutic approach for the cure of lupus nephritis in New Zealand Black/White (NZB/W)F1 hybrid mice with established disease. Two groups of NZB/W mice (N=30 each group), starting at 5 months of age, were given by gavage vehicle or imatinib (50 mg/kg b.i.d). Fifteen mice for each group were used for the survival study. The remaining were killed at 8 months. Imatinib significantly (P=0.0022) ameliorated animal survival with respect to vehicle. The drug significantly delayed the onset of proteinuria (% proteinuric mice, 7 and 8 months: 33 and 47 vs vehicle, 80 and 87, P0.05) and limited the impairment of renal function. Imatinib protected the kidney against glomerular hypercellularity and deposits, tubulointerstitial damage, and accumulation of F4/80-positive mononuclear cells and alpha-smooth actin-positive myofibroblasts. The abnormal transforming growth factor-beta mRNA expression in kidneys of lupus mice was reduced by imatinib. In conclusion, findings of amelioration of animal survival and renal manifestations in NZB/W lupus mice with established disease by imatinib suggests the possibility to explore whether imatinib may function as steroid-sparing drug in human lupus nephritis.

Published

2006

36. Beneficial effect of TGFbeta antagonism in treating diabetic nephropathy depends on when treatment is started

Author

Daniela Corna, Giuseppe Remuzzi, Ariela Benigni, Elena Gagliardini, Marco Campana, Fabio Sangalli, Daniela Rottoli, Sara Conti, Steve Ledbetter, and Carla Zoja

Subjects

Nephrology, Male, medicine.medical_specialty, Time Factors, Physiology, Renal glomerulus, Kidney Glomerulus, Angiotensin-Converting Enzyme Inhibitors, Antibodies, Podocyte, Diabetes Mellitus, Experimental, Diabetic nephropathy, Rats, Sprague-Dawley, Enalapril, Transforming Growth Factor beta, Internal medicine, Diabetes mellitus, Genetics, medicine, Albuminuria, Animals, Diabetic Nephropathies, Proteinuria, business.industry, Podocytes, Glomerulosclerosis, General Medicine, medicine.disease, Rats, Endocrinology, medicine.anatomical_structure, medicine.symptom, business, Kidney disease

Abstract

Background: In diabetic rats with maximal activation of RAS induced by uninephrectomy, late treatment with anti-TGFβ antibody limited renal injury only when combined with ACE inhibitor. We investigated whether in a two-kidney diabetic model the time at which treatment started predicted the response to TGFβ antagonist. Methods: 27 weeks after streptozotocin injection, animals had mild proteinuria and were randomized to receive irrelevant antibody, anti-TGFβ antibody (1D11) or enalapril till 52 weeks (early treatment). The effect of agents alone or combined was also evaluated at the time of overt proteinuria (late treatment, 52–61 weeks). Results: When given early, 1D11 displayed marked antihypertensive and antiproteinuric effects. Glomerulosclerosis was reduced to the extent that a remarkable percentage of glomeruli without sclerosis appeared after treatment. Podocyte number was normalized. Renoprotection of 1D11 was comparable to enalapril. Despite control of blood pressure, in late treatment single agents did not reduce proteinuria significantly. Glomerulosclerosis and podocyte loss were partially limited by 1D11 or enalapril, but full protection was achieved by combination. Conclusions: Renoprotective effect of TGFβ antagonism crucially depends on the time at which treatment started. Effectiveness of early treatment with 1D11 would indicate that TGFβ is a major mediator of damage in early diabetes. To tackle the renal damage in the phase of advanced disease, a combined treatment with ACE inhibitor is needed.

Published

2006

37. Add-on anti-TGF-beta antibody to ACE inhibitor arrests progressive diabetic nephropathy in the rat

Author

Sara Conti, Daniela Corna, Carla Zoja, Giuseppe Remuzzi, Marco Campana, Ariela Benigni, Mauro Abbate, Daniela Rottoli, Steve Ledbetter, Cristina Zanchi, Cristina Zatelli, and Elena Gagliardini

Subjects

Male, medicine.medical_specialty, DNA, Complementary, Time Factors, Angiotensin-Converting Enzyme Inhibitors, Kidney, Nephropathy, Diabetic nephropathy, Rats, Sprague-Dawley, Mice, Lisinopril, Transforming Growth Factor beta, Internal medicine, medicine, Animals, Humans, Protein Isoforms, Diabetic Nephropathies, RNA, Messenger, Chemokine CCL2, Proteinuria, business.industry, Body Weight, Glomerulosclerosis, General Medicine, medicine.disease, Blotting, Northern, Angiotensin II, Immunohistochemistry, Rats, Up-Regulation, Endocrinology, Collagen Type III, Nephrology, ACE inhibitor, Leukocytes, Mononuclear, medicine.symptom, business, Kidney disease, medicine.drug, Densitometry

Abstract

Renin-angiotensin system (RAS) inhibitors are effective in reducing renal disease progression in early diabetic nephropathy, but they provide imperfect protection at a later stage. Due to the pivotal role of transforming growth factor–β (TGF-β) in the pathogenesis of diabetic kidney disease, this study tested the effect of simultaneously interrupting TGF-β and angiotensin II on disease progression in diabetic rats with overt nephropathy. Diabetes was induced by streptozotocin injection in uninephrectomized rats. Diabetic rats received murine (1D11) or human (CAT-192) anti-TGF-β monoclonal antibodies alone or in combination with lisinopril, 13C4 irrelevant murine antibody, saline or lisinopril from month 4 (when animals had proteinuria) to month 8. Normal animals served as controls. Systolic BP increase was controlled by single treatments and even more by the combined therapies. 1D11 and lisinopril kept proteinuria at levels numerically lower than irrelevant antibody and saline, while CAT-192 was ineffective. The addition of either TGF-β antibody to lisinopril normalized proteinuria. Consistent results were obtained for glomerulosclerosis and tubular damage, which were abrogated by the combined therapy. Interstitial volume expansion and infiltration of lymphocytes/macrophages were limited by 1D11 and lisinopril and further reduced by their combination. The increase of type III collagen in the renal interstitium was partially attenuated by 1D11 and lisinopril while normalized by their combination. It is concluded that anti–TGF-β antibody when added to a background of chronic angiotensin-converting enzyme (ACE) inhibition fully arrests proteinuria and renal injury of overt diabetic nephropathy, providing a novel route to therapy and remission of disease for diabetic patients who do not respond to RAS inhibition. E-mail: zoja@marionegri.it

Published

2003

38. How to fully protect the kidney in a severe model of progressive nephropathy: a multidrug approach

Author

Giuseppe Remuzzi, Davide Camozzi, Daniela Corna, Mauro Abbate, Cristian Batani, Cristina Zanchi, Dario Cattaneo, Carla Zoja, and Daniela Rottoli

Subjects

Male, medicine.medical_specialty, Angiotensin II receptor antagonist, Angiotensin-Converting Enzyme Inhibitors, Pharmacology, Peptidyl-Dipeptidase A, urologic and male genital diseases, Kidney, Receptor, Angiotensin, Type 1, Nephropathy, Rats, Sprague-Dawley, Angiotensin Receptor Antagonists, Glomerulonephritis, Transforming Growth Factor beta, Internal medicine, medicine, Animals, cardiovascular diseases, RNA, Messenger, Triglycerides, business.industry, Lisinopril, Glomerulosclerosis, Cerivastatin, General Medicine, medicine.disease, Rats, medicine.anatomical_structure, Endocrinology, Cholesterol, Nephrology, ACE inhibitor, Drug Therapy, Combination, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, medicine.drug, Kidney disease

Abstract

The current therapy for chronic proteinuric nephropathies is angiotensin-converting enzyme inhibitors (ACEi), which slow, but may not halt, the progression of disease, and which may be not effective to the same degree in all patients. In accelerated passive Heymann nephritis (PHN), this study assessed the effect of combining ACEi with angiotensin II receptor antagonist (AIIRA) and with statin that, besides lowering cholesterol, influences inflammatory and fibrogenic processes. Uninephrectomized PHN rats were divided into four groups ( n = 10 each) and daily given oral doses of the following: vehicle; 40 mg/L lisinopril; 100 mg/L lisinopril plus L-158,809; 0.3 mg/kg lisinopril plus L-158,809 plus cerivastatin. Treatments started at 2 mo when rats had massive proteinuria and signs of renal injury and lasted until 10 mo. Increases in BP were equally lowered by treatments. ACEi kept proteinuria at levels comparable to pretreatment and numerically lower than vehicle. The addition of AIIRA to lisinopril was more effective, being proteinuria reduced below pretreatment values and significantly lower than vehicle. When cerivastatin was added on top of ACE inhibition and AIIR blockade, urinary protein regressed to normal values and renal failure was prevented. Renal ACE activity was increased threefold in PHN, it was inhibited by more than 60% after ACEi, and decreased below control values with triple therapy. Cerivastatin inhibited ACE activity by 30%. Glomerulosclerosis, tubular damage and interstitial inflammation were ameliorated by ACEi alone or combined with AIIRA, and prevented by addition of statin. TGF-β 1 mRNA upregulation in PHN kidney was partially reduced after ACEi or combined with AIIRA and almost normalized after adding statin. Cerivastatin inhibited TGF-β 1 gene upregulation by 25%. These data suggest a possible future strategy to induce remission of proteinuria, lessen renal injury, and protect from loss of function in those patients who do not fully respond to ACEi therapy.

Published

2002

39. Protein traffic activates NF-kB gene signaling and promotes MCP-1-dependent interstitial inflammation

Author

Cristina Zanchi, Daniela Corna, Ariela Benigni, Giuseppe Remuzzi, Roberta Donadelli, Mauro Abbate, Susanna Tomasoni, and Carla Zoja

Subjects

medicine.medical_specialty, Inflammation, Angiotensin-Converting Enzyme Inhibitors, urologic and male genital diseases, Proinflammatory cytokine, Nephropathy, Downregulation and upregulation, Internal medicine, medicine, RNA, Messenger, Chemokine CCL2, business.industry, Monocyte, Lisinopril, NF-kappa B, medicine.disease, NFKB1, Protein Transport, Proteinuria, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, Nephrology, ACE inhibitor, Cancer research, Kidney Diseases, medicine.symptom, business, medicine.drug

Abstract

Mononuclear cells accumulate in the renal interstitium and contribute to renal injury in proteinuric nephropathies. Angiotensin-converting enzyme (ACE) inhibitors reduce protein trafficking and also lessen renal structural and functional damage. Many proinflammatory genes, including monocyte chemoattractant protein-1 (MCP-1), a chemoattractant for monocytes and T lymphocytes, are transcriptionally regulated by nuclear factor-kappa B (NF-kB). We aimed to study NF-kB activation and MCP-1 expression over time in two models of progressive proteinuric nephropathies (5/6 nephrectomy and passive Heymann nephritis [PHN]) and evaluate the effect of antiproteinuric therapy with an ACE inhibitor on these factors. In both models, increased urinary protein excretion over time was associated with a remarkable increase in NF-kB activity, which was almost completely suppressed by reducing proteinuria with lisinopril. NF-kB activation was paralleled by upregulation of MCP-1 messenger RNA and interstitial accumulation of ED-1-positive monocytes/macrophages and CD8-positive T cells. Lisinopril inhibited MCP-1 upregulation and limited interstitial inflammation. In a group of PHN rats with advanced disease and severe proteinuria, a dose of lisinopril high enough to inhibit renal ACE activity failed to reduce proteinuria and also did not limit NF-kB activation, which was sustained over time, along with MCP-1 gene overexpression and interstitial inflammation. These data suggest that NF-kB is activated in the presence of increased protein traffic, enhancing the nuclear transcription of the MCP-1 gene with potent chemotactic and inflammatory properties. This mechanism may help explain the long-term renal toxicity of filtered proteins.

Published

2000

40. Consultants for the American Journal of Nephrology 2007

Author

Robert J. Schotzinger, Shou-Shang Chiang, Yingjie Liang, Tun-Jun Tsai, Janet B. McGill, Masayo Aizawa, Hsueh-Fang Chuang, Areti Makedou, L. Ferder, Jun Miyoshi, F. Inserra, Colin E. Murdoch, Katsunori Sawada, Shigeo Yamamoto, Kimihiko Yanase, Chih-Ching Yang, Mark E. Williams, Eiji Kawasaki, Ariela Benigni, Rajiv Agarwal, Niansheng Yang, Carla Zoja, Fabio Sangalli, Kuan-Yu Hung, Rintarou Moriguchi, Flavio Gaspari, Katsumi Eguchi, Raja G. Khalifah, M. Ferder, Pavlos Malindretos, Masaaki Izumi, Fabiola Carrara, Min Zhang, Daniela Corna, Mingqian Luo, Tsuyoshi Tanimoto, Chwei-Shiun Yang, Yu-Sen Peng, Yukiko Hasuike, Alex Sirker, W. Kline Bolton, Takeshi Nakanishi, Ajay M. Shah, Yoshimi Takai, Kouji Miyagawa, Kali Makedou, Kei Maki, Dario Cattaneo, Thorsten P. Degenhardt, Chun-Fu Lai, Yuefang Huang, Diego Brancaccio, Vasilios Raptis, Mario Cozzolino, Toshiji Iwasaka, Maurizio Gallieni, Pantelis Sarafidis, Giuseppe Remuzzi, Gian Vico Melzi d’Eril, Reiko Hata, Andrea Remuzzi, Maria Luisa Biondi, Yih-Ron Lien, Kunihiro Ichinose, Ming-Shiou Wu, Chung-Hsin Chang, Xueqing Yu, Takahiro Kuragano, Andrea Galassi, Dimirios M. Grekas, Rong Li, Igor Rudenco, Satoshi Morimoto, Ching-Jyh Shiah, Norberto Perico, Kwan-Dun Wu, Rui Zhang, Chia-Sheng Lu, Yu-Ting Wang, E.M.V. de Cavanagh, Fang Wang, Lili Zhang, Wang-Yu Chen, and Yutaka Yano

Subjects

Nephrology, medicine.medical_specialty, business.industry, Internal medicine, Family medicine, medicine, business

Published

2007

41. Renoprotective effect of contemporary blocking of angiotensin II and endothelin-1 in rats with membranous nephropathy

Author

Daniela Corna, Raffaello Maffi, Giuditta Benedetti, Giuseppe Remuzzi, Ariela Benigni, and Carla Zoja

Subjects

Trandolapril, Male, medicine.medical_specialty, Indoles, Blood Pressure, urologic and male genital diseases, Kidney, Rats, Sprague-Dawley, chemistry.chemical_compound, Glomerulonephritis, Membranous nephropathy, Internal medicine, medicine, Animals, Creatinine, biology, Endothelin-1, Phenylpropionates, business.industry, Endothelin receptor antagonist, Angiotensin II, Glomerulosclerosis, Angiotensin-converting enzyme, medicine.disease, Rats, Proteinuria, Endocrinology, Pyrimidines, chemistry, Nephrology, ACE inhibitor, biology.protein, business, medicine.drug

Abstract

Background. We previously showed that chronic administration of an angiotensin converting enzyme (ACE) inhibitor to rats with passive Heymann nephritis (PHN), a model of membranous nephropathy with proteinuria and increased renal synthesis of endothelin-1 (ET-1), reduces urinary proteins and partially limits the exaggerated ET-1 renal synthesis. Here we compared the effect of an ETA receptor antagonist and an ACE-inhibitor given as single therapies with a combination of the two drugs in uninephrectomized PHN rats. Methods. PHN was induced with a single i.v. injection of rabbit anti-Fx1A antibody in 40 male Sprague Dawley rats. To accelerate the onset of renal damage rats underwent uninephrectomy seven days later and were subsequently treated until eight months with the ETA receptor antagonist LU-135252 (50 mg/kg b.i.d. p.o.) or the ACE-inhibitor trandolapril (1 mg/kg in the drinking water) or the combination of the two drugs. Results. Either LU-135252 or trandolapril given alone prevented the increase in systolic blood pressure (SBP). Combined therapy was even more effective than single drugs. While LU135252 and trandolapril reduced proteinuria by 23 to 25%, the drug combination resulted in 45% lowering of urinary proteins. Serum creatinine was significantly decreased by the combination, but not by the single drugs. Glomerulosclerosis and tubulointerstitial damage were more reduced by combined therapy than by LU-135252 or trandolapril alone. Conclusions. These data suggest that contemporary blocking angiotensin II (Ang II) and ET-1 in an accelerated model of PHN had an additive renoprotective effect than single blocking Ang II or ET-1 and would represent a therapeutic advantage for renal disease patients who do not completely respond to ACE inhibitors.

Published

1998

42. Pharmacologic control of angiotensin II ameliorates renal disease while reducing renal TGF-beta in experimental mesangioproliferative glomerulonephritis

Author

Simon Oldroyd, Giuseppe Remuzzi, Isabella Bruzzi, Matteo Capitanio, Ariela Benigni, Daniela Corna, Mauro Abbate, Carla Zoja, and Roberta Donadelli

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Glomerulonephritis, Membranoproliferative, Kidney Glomerulus, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, Monocytes, Rats, Sprague-Dawley, Lisinopril, Transforming Growth Factor beta, Internal medicine, medicine, Animals, Antilymphocyte Serum, Proteinuria, biology, business.industry, Angiotensin II, Macrophages, Glomerulonephritis, medicine.disease, Receptor antagonist, Rats, Endocrinology, Nephrology, Enzyme inhibitor, Creatinine, Immunoglobulin G, ACE inhibitor, biology.protein, medicine.symptom, business, Cell Division, medicine.drug, Kidney disease

Abstract

We evaluated the effect of blocking angiotensin II (AngII) on the development of proteinuria and glomerular injury in antithymocyte serum (ATS) glomerulonephritis. Disease was induced in Sprague-Dawley rats by a single intravenous injection of rabbit ATS. Three groups of rats were considered: group 1 (n = 13), ATS rats with no therapy; group 2 (n = 13), ATS rats treated with angiotensin-converting enzyme inhibitor (40 mg/L lisinopril in the drinking water); and group 3 (n = 13), ATS rats treated with AngII receptor antagonist (50 mg/L L-158,809 in the drinking water). Treatment started 3 hours after ATS injection and lasted 4 days. An additional group of control rats (group 4, n = 13) received preimmune serum. At day 4, ATS rats developed proteinuria (46+/-5 mg/d v control 12+/-1 mg/d; P0.01), which was prevented by both lisinopril and L-158,809 (14+/-0.2 mg/d and 15+/-1.6 mg/d, respectively, P0.01 v ATS). Systolic blood pressure was comparable in ATS rats and in controls (119+/-4 mm Hg v 120+/-2 mm Hg). Systolic blood pressure values were significantly decreased after either lisinopril or L-158,809 (104+/-3 mm Hg and 101+/-5 mm Hg, respectively; P0.01 v ATS). Serum creatinine levels were similar in all groups. Quantitation of proliferating cells and macrophages by analysis of proliferating cell nuclear antigen-positive and ED1-positive cells/glomerular cross-section showed a marked increase in proliferating cell nuclear antigen-positive cells in glomeruli of ATS rats over controls (12.6+/-0.5 cells/glomerular cross-section v 1.9+/-0.2 cells/glomerular cross-section; P0.01), which was significantly (P0.01) prevented by both treatments (lisinopril, 5.7+/-1.0 cells/glomerular cross-section; L-158,809, 4.8+/-1.5 cells/glomerular cross-section). The increase in ED1-positive cells (10+/-0.7 cells/glomerular cross-section v controls, 1.8+/-0.2 cells/glomerular cross-section; P0.01) was also significantly (P0.01) reduced by lisinopril and L-158,809 (4.1+/-0.7 cells/glomerular cross-sections and 2.6+/-0.6 cells/glomerular cross-section, respectively). Blocking of AngII activity prevented almost completely the formation of microaneurysms in ATS rats (percent of glomeruli with microaneurysms: ATS, 11.5%+/-3.5%; ATS + lisinopril, 0.4%+/-0.2%; ATS + L-158,809, 0.8%+/-0.8%; controls, 0%). Because AngII is a potent inducer of renal transforming growth factor-beta (TGF-beta), a cytokine involved in the regulation of cell proliferation, matrix deposition, and monocyte migration (which is overexpressed in the kidney of ATS rats), we then evaluated the effect of AngII inhibitors on renal gene expression of TGF-beta1 and on urinary TGF-beta1. TGF-beta1 mRNA levels in kidneys of ATS rats were 3.6-fold higher than those of controls and were reduced by 46% and 32% after treatment with lisinopril and L-158,809, respectively. Urinary TGF-beta1 excretion increased in ATS (37.3+/-6.0 ng/d v controls, 13.8+/-3.4 ng/d; P0.01) but was normalized by lisinopril and L-158,809 (7.6+/-1.9 ng/d and 6.4+/-0.4 ng/d, respectively; P0.01). Thus, in ATS, blocking AngII synthesis prevents proteinuria and reduces glomerular cell proliferation and inflammatory cell infiltration, possibly by reducing excessive renal TGF-beta synthesis. These findings may be relevant for future strategies in the treatment of human mesangioproliferative glomerulonephritis.

Published

1998

43. Renal and systemic nitric oxide synthesis in rats with renal mass reduction

Author

Daniela Corna, Sergio Zappella, Marina Noris, Giuseppe Remuzzi, Carla Zoja, Marta Todeschini, Daniela Cavallotti, Sistiana Aiello, Ariela Benigni, and Chiara Foglieni

Subjects

Male, medicine.medical_specialty, hypertension, Time Factors, Renal glomerulus, injury, Renal function, In Vitro Techniques, Kidney, Nitric Oxide, Nitroarginine, Nitric oxide, Rats, Sprague-Dawley, chemistry.chemical_compound, chronic renal failure, Internal medicine, medicine, Animals, Enzyme Inhibitors, Uremia, business.industry, medicine.disease, Immunohistochemistry, Pathophysiology, Rats, medicine.anatomical_structure, Endocrinology, chemistry, Nephrology, Nitric Oxide Synthase, business, Kidney disease, Blood vessel

Abstract

Renal and systemic nitric oxide synthesis in rats with renal mass reduction. In rats undergoing renal mass reduction (RMR) oral supplementation with the nitric oxide (NO) precursor L-arginine increases glomerular filtration rate and ameliorates signs of glomerular injury, suggesting that chronic renal failure in the rats is a condition of low NO formation in the kidney. On the contrary, data are available that in the systemic circulation of uremics, both rats and human beings, NO is formed in excessive amounts and may contribute to platelet dysfunction and bleeding tendency, well-known complications of uremia. The present study was designed to clarify the pathophysiology of renal and systemic NO synthesis in uremia. We showed that renal ex vivo NO generation, measured as the conversion of [ 3 H] L-arginine to [ 3 H] L-citrulline, was lower than normal in RMR rats, seven days after surgery, and progressively worsened with time in close correlation with signs of renal injury. Consistent with these results, urinary excretion of the stable NO metabolites, NO 2 − / NO 3 − , significantly decreased in rats with RMR. To go deeper into the cellular origin and biochemical nature of this abnormality we used two histochemical approaches that could locate either NO synthase (NOS) catalytic activity (NADPH-diaphorase) or NOS isoenzyme expression (immunoperoxidase). NADPH-diaphorase documented a progressive loss of renal NOS activity in RMR rats that co-localized with a strong progressive decrease of inducible NOS isoenzyme (iNOS) immunostaining. At variance with iNOS, endothelial cell NOS (ecNOS) staining was rather comparable in RMR and control kidneys. At variance to the kidney, in the systemic circulation of RMR rats the synthesis of NO increased as reflected by higher than normal plasma NO 2 − / NO 3 − concentrations. High systemic NO likely derives from vessels as documented by the increased NOS activity and higher expression of both iNOS and ecNOS in the aorta of RMR rats. Up-regulation of systemic NO synthesis might be an early defense mechanism against hypertension of uremia. On the other hand, more NO available to circulating cells may sustain the bleeding tendency, a well-known complication of uremia.

Published

1997

44. Renal protective effect of angiotensin-converting enzyme inhibition in aging rats

Author

Tullio Bertani, Norberto Perico, Carla Zoja, Giuseppe Remuzzi, Andrea Remuzzi, and Daniela Corna

Subjects

Male, medicine.medical_specialty, Aging, Kidney Glomerulus, Angiotensin-Converting Enzyme Inhibitors, urologic and male genital diseases, Permeability, Excretion, Internal medicine, Perindopril, medicine, Animals, chemistry.chemical_classification, Analysis of Variance, Proteinuria, biology, urogenital system, business.industry, Glomerulosclerosis, Focal Segmental, Glomerulosclerosis, Settore ING-IND/34 - Bioingegneria Industriale, Angiotensin-converting enzyme, Rats, Inbred Strains, General Medicine, medicine.disease, female genital diseases and pregnancy complications, Rats, Endocrinology, Blood pressure, Enzyme, chemistry, ACE inhibitor, biology.protein, medicine.symptom, business, medicine.drug

Abstract

Aging in rats with intact kidneys is associated with changes in selective glomerular permeability to macromolecules resulting in proteinuria and progressive glomerular sclerosis. We have previously reported that angiotensin-converting enzyme (ACE) inhibition in Munich Wistar Fromter/Ztm (MWF/Ztm) rats resulted in a significant reduction of proteinuria, in respect to untreated animals, and that treated animals were protected against the development of glomerular sclerotic lesions. The present study was designed to establish whether ACE inhibition protects against glomerular injury in male Sprague-Dawley rats, which develop spontaneous proteinuria and glomerulosclerosis with age. The effect of ACE inhibition was tested when proteinuria was already present. Four-month treatment with the ACE inhibitor perindopril prevented the increase in systolic blood pressure, compared with vehicle-treated animals, and significantly decreased urinary protein excretion of aging rats. Partial protection of the development of glomerular sclerosis was also observed.

Published

1992

45. 131. Studies on the renal protective effect of angiotensin converting enzyme inhibition in ageing rats

Author

Daniela Corna, Carlamaria Zoja, Giuseppe Remuzzi, and Andrea Remuzzi

Subjects

biology, Physiology, Ageing, business.industry, Internal Medicine, biology.protein, Medicine, Angiotensin-converting enzyme, Pharmacology, Cardiology and Cardiovascular Medicine, business

Published

1991

46. Mycophenolate mofetil combined with a cyclooxygenase-2 inhibitor ameliorates murine lupus nephritis

Author

Daniela Corna, Ariela Benigni, Federica Casiraghi, Mauro Abbate, Marina Noris, Giuseppe Remuzzi, Daniela Rottoli, Marcella Pagnoncelli, and Carla Zoja

Subjects

Lupus nephritis, Pharmacology, Kidney, DFU, Blood Urea Nitrogen, Mice, anti-inflammatory, Systemic lupus erythematosus, immunosuppression, Mice, Inbred NZB, nephrotoxicity, Lupus Nephritis, Isoenzymes, Survival Rate, Proteinuria, progressive nephritis, Nephrology, Antibodies, Antinuclear, Drug Therapy, Combination, Female, Nephritis, Immunosuppressive Agents, medicine.medical_specialty, autoimmune disease, 6-Ketoprostaglandin F1 alpha, Gene Expression Regulation, Enzymologic, Nephrotoxicity, Nephropathy, Internal medicine, medicine, Animals, Cyclooxygenase Inhibitors, Lymphocyte Count, Furans, Lupus erythematosus, Cyclooxygenase 2 Inhibitors, business.industry, Therapeutic effect, Membrane Proteins, Mycophenolic Acid, medicine.disease, Lymphocyte Subsets, Thromboxane B2, Disease Models, Animal, Endocrinology, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, inflammation, Cyclooxygenase 1, business, Spleen, Kidney disease

Abstract

Mycophenolate mofetil combined with a cyclooxygenase-2 inhibitor ameliorates murine lupus nephritis.BackgroundApproaches to the treatment of lupus nephritis include immunosuppressants associated with anti-inflammatory drugs, mainly steroids, which, however, cause major side effects. Mycophenolate mofetil (MMF) has been described as being less toxic than conventional immunosuppressants, and it was effective in preventing progressive nephritis in lupus mice. Our study evaluated the therapeutic effect of MMF in NZB/W F1 hybrid mice with established disease. We also examined the combination of MMF with a selective cyclooxygenase-2 (COX-2) inhibitor, DFU, based on previous findings of excessive renal production of COX-2-derived thromboxane A2 (TXA2) in lupus nephritis.MethodsFour groups of NZB/W mice (N = 30 each group), starting at five months of age, were given daily by gavage the following: vehicle, MMF 60 mg/kg, DFU 3 mg/kg, or MMF + DFU. Fifteen mice for each group were used for the survival studies, and the remaining mice were sacrificed at nine months.ResultsMMF or DFU alone partially delayed the onset of proteinuria compared with vehicle. Combined therapy was significantly (P < 0.05) more effective than single drugs. Animal survival was partially ameliorated by MMF and significantly improved by the drug combination in comparison with the vehicle (P = 0.005) and DFU alone (P < 0.03). At nine months, serum blood urea nitrogen (BUN) levels were lower in all of the treated groups than in the vehicle group. Renal damage was also limited, but to a greater extent in mice given the combined therapy. In untreated mice, renal COX-2 mRNA expression was up-regulated, and generation of TXB2, the stable breakdown product of TXA2, increased. DFU prevented the abnormal renal TXB2 production, confirming the COX-2 origin of this eicosanoid, whereas renal 6-keto-PGF1α and prostaglandin E2 (PGE2) were not affected substantially.ConclusionsThese results offer a strong case for exploring the possibility that in humans MMF combined with COX-2 inhibitors has a role in the treatment options for lupus nephritis. This combined drug therapy may be at least as effective as steroids but without the obvious nephrotoxicity of the latter.

47. Vasopeptidase inhibitor restores the balance of vasoactive hormones in progressive nephropathy

Author

Carla Zoja, Paola Maggioni, Lorena Longaretti, Marta Todeschini, Ariela Benigni, Daniela Rottoli, Cristina Zatelli, Giuseppe Remuzzi, Marina Noris, and Daniela Corna

Subjects

Nephrology, Male, medicine.medical_specialty, Urinary system, Angiotensin-Converting Enzyme Inhibitors, Blood Pressure, Kidney, urologic and male genital diseases, Nephrectomy, Nephropathy, Rats, Sprague-Dawley, Atrial natriuretic peptide, Enalapril, vasopeptidase inhibitor, nitric oxide, Internal medicine, ACE inhibitor, medicine, Animals, remnant kidney, Cyclic GMP, Antihypertensive Agents, Nitrites, Nitrates, Endothelin-1, business.industry, medicine.disease, ET-1, Rats, Proteinuria, Endocrinology, medicine.anatomical_structure, Kidney Diseases, Neprilysin, business, Heterocyclic Compounds, 3-Ring, ANP, medicine.drug, Kidney disease

Abstract

Vasopeptidase inhibitor restores the balance of vasoactive hormones in progressive nephropathy.BackgroundThe mechanism(s) underlying greater renoprotection of combined blockade of angiotensin-converting enzyme (ACE) and neutral endopeptidase (NEP) by vasopeptidase over ACE inhibitors are ill defined. We previously found that progressive renal disease is associated with increased renal synthesis of endothelin-1 (ET-1) in the face of reduced generation of renal nitric oxide (NO) in the remnant kidney model. Here we compared changes in urinary excretion of ET-1 and nitrite/nitrate, markers of renal ET-1, and NO synthesis, respectively, and urinary cGMP, an indirect index of renal atrial natriuretic peptide (ANP) synthesis, after administration of vasopeptidase or ACE inhibitor in rats with renal mass reduction (RMR).MethodsTwenty-one days after 5/6 nephrectomy, after the onset of hypertension and overt proteinuria, rats were divided in 3 groups (N = 7–8) and given daily by gavage: vehicle, the vasopeptidase inhibitor AVE7688 (3 mg/kg bid), or enalapril (5 mg/kg bid) until day 90. Normal rats (N = 5) served as control rats.ResultsSystolic blood pressure in RMR rats was equally controlled by AVE7688 and enalapril. AVE7688 resulted in a significant antiproteinuric effect, with urinary protein levels being reduced on average by 83% in respect to vehicle (88 ± 28 vs. 518 ± 27 mg/day, P < 0.0001). Enalapril achieved a 47% reduction in proteinuria (277 ± 81 mg/day, P < 0.01 vs. vehicle) to levels that remained higher (P < 0.01), however, than those after AVE7688. Renal function impairment and glomerular and tubular changes were significantly (P < 0.05 vs. vehicle) ameliorated by AVE7688, and partially affected by enalapril. AVE7688 reduced the abnormal urinary excretion of ET-1 of RMR animals (98 ± 8 vs. vehicle: 302 ± 50 pg/24h, P < 0.001) more than enalapril (159 ± 14 pg/24h, P < 0.05 vs. AVE7688). Consistently, AVE7688 was more effective than enalapril in augmenting renal synthesis of NO (2487 ± 267 and 1519 ± 217 vs. vehicle: 678 ± 71 nmol/15 h; P < 0.001, AVE7688 vs. vehicle, P < 0.01 AVE7688 vs. enalapril). AVE7688 significantly increased urinary cGMP (78 ± 6 vs. vehicle 45 ± 9 nmol/24h; P < 0.01).ConclusionThe superior renoprotection achieved by AVE7688 over enalapril in progressive renal injury is due to the correction of the altered balance of vasoconstrictor/vasodilator mediators in the kidney.

48. Renal endothelin gene expression is increased in remnant kidney and correlates with disease progression

Author

Daniela Corna, Giuseppe Remuzzi, Silvia Orisio, Norberto Perico, Carla Zoja, Isabella Bruzzi, Luca Benatti, and Ariela Benigni

Subjects

Male, medicine.medical_specialty, Urinary system, medicine.medical_treatment, Molecular Sequence Data, Gene Expression, Peptide hormone, Biology, Kidney, urologic and male genital diseases, Nephrectomy, Excretion, Rats, Sprague-Dawley, Internal medicine, Gene expression, medicine, Animals, Base Sequence, Glomerulosclerosis, Focal Segmental, Endothelins, Glomerulosclerosis, Glomerulonephritis, DNA, medicine.disease, Rats, Disease Models, Animal, Proteinuria, Endocrinology, Nephrology, Endothelin receptor

Abstract

Renal endothelin gene expression is increased in remnant kidney and correlates with disease progression. We previously demonstrated that urinary endothelin excretion is increased in rats with extensive renal mass reduction, a model of progressive renal disease. Here we explored whether the increased urinary endothelin in this model were due to induction of renal pre-pro-endothelin-1 gene and whether changes in endothelin synthetic pathway correlated with the development of glomerulosclerosis. Four groups of rats with renal mass reduction and four groups of sham-operated control rats were studied 7, 30, 60 and 120 days after the surgical procedure. Urinary protein excretion in renal mass ablation animals did not differ from controls at seven days, but was already significantly elevated (P < 0.01) 30 days after surgery. Then proteinuria progressively increased in rats with remnant kidney at values above 400 mg/day at day 120. Serum creatinine concentration also progressively increased with time in renal mass ablation rats, unlike sham-operated animals, and values were significantly different (P < 0.01) at each of the points considered. Rats with renal mass reduction, unlike sham-operated animals, developed focal glomerulosclerosis that affected 8% of glomeruli at day 30, and 24% of glomeruli at day 120. Seven days after renal mass reduction renal pre-proendothelin-1 (pre-pro ET) mRNA was comparable to that of sham-operated rats, while a 2.5-, 5- and fourfold increase in 2.3 Kb pre-proET-1 transcript was observed at 30, 60 and 120 days, respectively. Urinary excretion of endothelin was significantly elevated (P < 0.01) in rats with renal mass reduction with respect to sham-operated rats, starting from 30 days after surgery and increased further thereafter. A significant correlation (P < 0.01) was found between urinary endothelin-1 excretion values and the percent of glomeruli affected by glomerulosclerosis. We conclude that the progression of renal disease after surgical ablation of renal mass is associated with an increased renal endothelin-1 gene expression together with an excessive urinary excretion of the corresponding protein. It is speculated that endothelin may mediate glomerular structural abnormalities associated with the progression of renal disease in this model.

49. Proximal tubular cells promote fibrogenesis by TGF-β1–mediated induction of peritubular myofibroblasts

Author

Susanna Tomasoni, Daniela Rottoli, Giuseppe Remuzzi, Daniela Corna, Mauro Abbate, and Carla Zoja

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Cell, Angiotensin-Converting Enzyme Inhibitors, macrophage, Biology, Kidney Tubules, Proximal, Rats, Sprague-Dawley, Transforming Growth Factor beta1, Fibrosis, Lisinopril, Transforming Growth Factor beta, Internal medicine, medicine, Macrophage, Animals, Tissue Distribution, RNA, Messenger, Kidney, Staining and Labeling, urogenital system, Growth factor, Macrophages, fibrosis, Proteins, Muscle, Smooth, progressive renal disease, Fibroblasts, medicine.disease, Actins, Cell biology, Rats, Cytokine, medicine.anatomical_structure, Endocrinology, Kidney Tubules, Nephrology, Immunoglobulin G, α-smooth muscle actin, proteinuria, angiotensin converting enzyme inhibitor, Myofibroblast, Cell Division, Transforming growth factor, tubulointerstitial injury

Abstract

Proximal tubular cells promote fibrogenesis by TGF - β1–mediated induction of peritubular myofibroblasts . Background In proteinuric nephropathies with increasingly severe defects of the glomerular filtering barrier, interstitial fibrogenesis is a major effector of scarring. An early event in this process is the peritubular accumulation of myofibroblasts that express α-smooth muscle actin (α-SMA) and contribute to abnormal matrix production. Common trigger factors are poorly understood. Enhanced protein trafficking may play a role by up-regulating inflammatory and fibrogenic genes in proximal tubular cells. Methods The remnant kidney model in rats was used to ( 1 ) analyze interactions between activated proximal tubular cells, peritubular cells expressing the myofibroblast marker, and inflammatory cells at time intervals (days 7, 14, and 30) after surgery, and ( 2 ) evaluate the effects of angiotensin-converting enzyme inhibitor (ACEi) on protein trafficking, fibrogenic signaling, and α-SMA expression. Results Abnormal uptake of ultrafiltered proteins by proximal tubular cells (IgG staining) occurred at an early stage (day 7) and was subsequently associated with macrophage and α-SMA+ cell accumulation into the peritubular interstitium. α-SMA+ cells clustered with macrophages into the interstitium. These changes were associated with appearance of transforming growth factor-β1 (TGF-β1) mRNA in proximal tubular cells and in the infiltrating cells with time. At day 30, focal α-SMA staining also was found in the tubular cells and in peritubular endothelial cells on semithin ultracryosections. ACEi prevented both proteinuria and abnormal protein accumulation in tubular cells, as well as the inflammatory and fibrogenic reaction with peritubular α-SMA expression. Conclusions Profibrogenic signaling from both proximal tubular cells on challenge with filtered protein and inflammatory cells is implicated as a key candidate trigger of progressive tubulointerstitial injury.

50. Experimental Goodpasture's syndrome in Wistar-Kyoto rats immunized with α3 chain of type IV collagen

Author

Daniela Corna, Mauro Abbate, Raghuram Kalluri, Naoto Yamaguchi, Billy G. Hudson, Giuseppe A. Andres, Giuseppe Remuzzi, Robert T. McCluskey, and Carla Zoja

Subjects

Male, medicine.medical_specialty, GBM α3(IV) NC1 peptide, Anti-Glomerular Basement Membrane Disease, dendritic cell, extracellular matrix, macromolecular substances, urologic and male genital diseases, Rats, Inbred WKY, Antibodies, Epitope, 03 medical and health sciences, Type IV collagen, 0302 clinical medicine, Antigen, Antibody Specificity, Internal medicine, medicine, Goodpasture's syndrome, Animals, Goodpasture syndrome, Lung, anti-GBM disease, 030304 developmental biology, 030203 arthritis & rheumatology, Autoimmune disease, 0303 health sciences, biology, urogenital system, business.industry, thymocyte, Glomerulonephritis, medicine.disease, Rats, 3. Good health, lung hemorrhage, Proteinuria, Endocrinology, Nephrology, biology.protein, Cattle, Immunization, Collagen, Antibody, business, glomerulonephritis

Abstract

Experimental Goodpasture's syndrome in Wistar-Kyoto rats immunized with α3 chain of type IV collagen.BackgroundGlomerulonephritis and lung hemorrhage of autoimmune Goodpasture syndrome develop due to immune reactions against epitope(s) of the non-collagenous (NC1) domain of α3-chain of type IV collagen [α3(IV) NC1]. Whether thymic mechanisms have a role in the loss of tolerance to the Goodpasture epitope has not been established. We studied the renal and pulmonary effects of immunization with different forms (monomer, dimer, or hexamer) of α3(IV) NC1 collagen in Wistar-Kyoto (WKY) rats, and assessed whether the intrathymic inoculation of the antigen may protect against anti-GBM disease.MethodsWKY rats were immunized with bovine α3(IV) monomer, dimer, or hexamer, or with α3(IV) NC1 synthetic peptide. Renal function, kidney and lung immunohistology, and circulating and tissue bound antibodies to type IV collagen chains were analyzed. Effects of intrathymic inoculation of antigen on subsequent disease induction were analyzed in WKY rats given α3(IV) NC1 dimer or GBM preparation intrathymically 48hours before immunization.ResultsProteinuria, linear IgG deposition in GBM, and crescentic glomerulonephritis developed in WKY rats immunized with α3(IV) NC1 dimer or hexamer. Lesions were dose-dependent upon injections of 10 to 100 μg dimer. The α3(IV) NC1 monomer induced less severe proteinuria and no crescents. Pulmonary hemorrhage was detectable in 35% of rats immunized with 25 to 100 μg α3(IV) NC1 dimer; α3(IV) synthetic peptide (36 carboxyl terminal) did not induce disease. Rats injected intrathymically with up to 100 μg α3(IV) NC1 dimer or with GBM 48hours before immunization were not protected against subsequent development of proteinuria and glomerulonephritis.ConclusionsThese findings document that glomerulonephritis and lung hemorrhage can be elicited in WKY rats by immunization with α3(IV) NC1. Failure of the intrathymic inoculation of antigen to prevent disease suggests that immunological tolerance cannot be achieved by this intervention, in contrast to other autoimmune conditions, and may imply independent roles for cellular and humoral nephritogenic pathways in anti-GBM nephritis.