Your search keyword '"Robert N. Willette"' showing total 61 results

1. CXA-10, a Nitrated Fatty Acid, Is Renoprotective in Deoxycorticosterone Acetate-Salt Nephropathy

Author

Cynthia Arbeeny, Francisco J. Schopfer, Hong Ling, Stephen J. O'Brien, Robert N. Willette, Mandy M. Smith, Diane K. Jorkasky, Stefan Wawersik, Allen McAlexander, and Steven R. Ledbetter

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Oleic Acids, Kidney, Nephropathy, 03 medical and health sciences, Desoxycorticosterone Acetate, Mice, 0302 clinical medicine, Fibrosis, Internal medicine, medicine, Animals, Tissue Distribution, Pharmacology, chemistry.chemical_classification, Fatty acid, Kidney metabolism, Glomerulosclerosis, medicine.disease, Nitro Compounds, Oxidative Stress, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, chemistry, Cytoprotection, Albuminuria, Molecular Medicine, Kidney Diseases, Salts, medicine.symptom, 030217 neurology & neurosurgery, Kidney disease

Abstract

Underlying pathogenic mechanisms in chronic kidney disease (CKD) include chronic inflammation, oxidant stress, and matrix remodeling associated with dysregulated nuclear factor-κ B, nuclear factor-κ B, and SMAD signaling pathways, respectively. Important cytoprotective mechanisms activated by oxidative inflammatory conditions are mediated by nitrated fatty acids that covalently modify proteins to limit inflammation and oxidant stress. In the present study, we evaluated the effects of chronic treatment with CXA-10 (10-nitro-9(E)-octadec-9-enoic acid) in the uninephrectomized deoxycorticosterone acetate-high-salt mouse model of CKD. After 4 weeks of treatment, CXA-10 [2.5 millligrams per kilogram (mpk), p.o.] significantly attenuated increases in plasma cholesterol, heart weight, and kidney weight observed in the model without impacting systemic arterial blood pressure. CXA-10 also reduced albuminuria, nephrinuria, glomerular hypertrophy, and glomerulosclerosis in the model. Inflammatory MCP-1 and fibrosis (collagen, fibronectin, plasminogen activator inhibitor-1, and osteopontin) renal biomarkers were significantly reduced in the CXA-10 (2.5 mpk) group. The anti-inflammatory and antifibrotic effects, as well as glomerular protection, were not observed in the enalapril-treated group. Also, CXA-10 appears to exhibit hormesis as all protective effects observed in the low-dose group were absent in the high-dose group (12.5 mpk). Taken together, these findings demonstrate that, at the appropriate dose, the nitrated fatty acid CXA-10 exhibits anti-inflammatory and antifibrotic effects in the kidney and limits renal injury in a model of CKD.

Published

2018

2. Activation of the Amino Acid Response Pathway Blunts the Effects of Cardiac Stress

Author

Deepak K. Rajpal, Pelin Arabacilar, Julius del Rosario, Ganesh M. Sathe, Erding Hu, Yuanjun Guo, Stephen H. Eisennagel, Quinn Lu, Maria Faelth Savitski, Gatto Gregory J, Roberta E. Bernard, Ashley M. Hughes, Mohamad Nayal, Wensheng Xie, Robert N. Willette, Pu Qin, Theresa J. Roethke, George P. Livi, Xiaoyan Qu, Michael P. Quaile, Gerard Joberty, Weike Bao, Robert B. Kirkpatrick, Alan R. Olzinski, Marcus Bantscheff, Christine G. Schnackenberg, Wendy S. Halsey, Thomas Force, Hind Lal, Fe Wright, Michael Platchek, and Giovanna Bergamini

Subjects

0301 basic medicine, Male, Time Factors, Ventricular Function, Left, Muscle hypertrophy, Piperidines, Fibrosis, Myocytes, Cardiac, Amino Acids, Enzyme Inhibitors, Cells, Cultured, Original Research, chemistry.chemical_classification, Protein Synthesis Inhibitors, Ventricular Remodeling, Kinase, amino acid response, Cell biology, Amino acid, Hypertrophy, Left Ventricular, Cardiology and Cardiovascular Medicine, hypertrophy, medicine.medical_specialty, Induced Pluripotent Stem Cells, Protein Serine-Threonine Kinases, Amino Acyl-tRNA Synthetases, 03 medical and health sciences, halofuginone, Stress, Physiological, Internal medicine, medicine, Autophagy, Animals, Humans, Quinazolinones, Heart Failure, Protein-Serine-Threonine Kinases, Dose-Response Relationship, Drug, business.industry, fibrosis, Fibroblasts, medicine.disease, Mice, Inbred C57BL, GENERAL CONTROL NONDEREPRESSIBLE 2, Disease Models, Animal, 030104 developmental biology, Endocrinology, chemistry, business

Abstract

Background The amino acid response ( AAR ) is an evolutionarily conserved protective mechanism activated by amino acid deficiency through a key kinase, general control nonderepressible 2. In addition to mobilizing amino acids, the AAR broadly affects gene and protein expression in a variety of pathways and elicits antifibrotic, autophagic, and anti‐inflammatory activities. However, little is known regarding its role in cardiac stress. Our aim was to investigate the effects of halofuginone, a prolyl‐ tRNA synthetase inhibitor, on the AAR pathway in cardiac fibroblasts, cardiomyocytes, and in mouse models of cardiac stress and failure. Methods and Results Consistent with its ability to inhibit prolyl‐ tRNA synthetase, halofuginone elicited a general control nonderepressible 2–dependent activation of the AAR pathway in cardiac fibroblasts as evidenced by activation of known AAR target genes, broad regulation of the transcriptome and proteome, and reversal by l ‐proline supplementation. Halofuginone was examined in 3 mouse models of cardiac stress: angiotensin II /phenylephrine, transverse aortic constriction, and acute ischemia reperfusion injury. It activated the AAR pathway in the heart, improved survival, pulmonary congestion, left ventricle remodeling/fibrosis, and left ventricular function, and rescued ischemic myocardium. In human cardiac fibroblasts, halofuginone profoundly reduced collagen deposition in a general control nonderepressible 2–dependent manner and suppressed the extracellular matrix proteome. In human induced pluripotent stem cell–derived cardiomyocytes, halofuginone blocked gene expression associated with endothelin‐1‐mediated activation of pathologic hypertrophy and restored autophagy in a general control nonderepressible 2/ eIF 2α‐dependent manner. Conclusions Halofuginone activated the AAR pathway in the heart and attenuated the structural and functional effects of cardiac stress.

Published

2017

3. Combined TRPC3 and TRPC6 blockade by selective small-molecule or genetic deletion inhibits pathological cardiac hypertrophy

Author

Joseph P. Marino, Peter P. Rainer, Kinya Seo, Su Hyun Jo, David A. Kass, Ting Liu, Christine G. Schnackenberg, Asger Andersen, John J. Lepore, Robert N. Willette, Xiaoping Xu, Lutz Birnbaumer, Virginia S. Hahn, and Dong Ik Lee

Subjects

medicine.medical_specialty, Heart disease, Cardiomegaly, Biology, Pharmacology, CALCIUM, TRPC6, Muscle hypertrophy, purl.org/becyt/ford/1 [https], NUCLEAR FACTOR OF ACTIVATED, Ciencias Biológicas, Mice, Transient receptor potential channel, TRPC3, Internal medicine, TRPC6 Cation Channel, ION CHANNELS, medicine, Animals, Humans, Phosphorylation, purl.org/becyt/ford/1.6 [https], TRPC Cation Channels, Mice, Knockout, Pressure overload, Multidisciplinary, Biological Sciences, Bioquímica y Biología Molecular, medicine.disease, Angiotensin II, humanities, Rats, Blockade, Mice, Inbred C57BL, HEK293 Cells, Endocrinology, T CELLS, CIENCIAS NATURALES Y EXACTAS

Abstract

Chronic neurohormonal and mechanical stresses are central fea-tures of heart disease. Increasing evidence supports a role forthe transient receptor potential canonical channels TRPC3 andTRPC6 in this pathophysiology. Channel expression for both is nor-mally very low but is increased by cardiac disease, and geneticgain- or loss-of-function studies support contributions to hypertro-phy and dysfunction. Selective small-molecule inhibitors remainscarce, and none target both channels, which may be useful giventhe high homology among them and evidence of redundant sig-naling. Here we tested selective TRPC3/6 antagonists (GSK2332255Band GSK2833503A; IC50,3–21 nM against TRPC3 and TRPC6) andfound dose-dependent blockade of cell hypertrophy signaling trig-gered by angiotensin II or endothelin-1 in HEK293T cells as well as inneonatal and adult cardiac myocytes. In vivo efficacy in mice andrats was greatly limited by rapid metabolism and high protein bind-ing, although antifibrotic effects with pressure overload were ob-served. Intriguingly, although gene deletion of TRPC3 or TRPC6alone did not protect against hypertrophy or dysfunction frompressure overload, combined deletion was protective, support-ing the value of dual inhibition. Further development of thispharmaceutical class may yield a useful therapeutic agent forheart disease management. Fil: Seo, Kinya. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos Fil: Rainer, Peter P.. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos. Medical University of Graz. Department of Medicine; Austria Fil: Shalkey Hahn, Virginia. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos Fil: Lee, Dong-ik. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos Fil: Jo, Su-Hyun. Kangwon National University School of Medicine; Corea del Sur. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos Fil: Andersen, Asger. Aarhus University Hospital. Department of Cardiology; Dinamarca Fil: Liu, Ting. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos Fil: Xu, Xiaoping. GlaxoSmithKline Heart Failure Discovery Performance Unit; Estados Unidos Fil: Willette, Robert N.. GlaxoSmithKline Heart Failure Discovery Performance Unit; Estados Unidos Fil: Lepore, John J.. GlaxoSmithKline Heart Failure Discovery Performance Unit; Estados Unidos Fil: Marino, Joseph P.. GlaxoSmithKline Heart Failure Discovery Performance Unit; Estados Unidos Fil: Birnbaumer, Lutz. ational Institute of Environmental Health Sciences; Estados Unidos. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto de Investigaciones Biomédicas. Universidad de Buenos Aires. Facultad de Medicina. Instituto de Investigaciones Biomédicas; Argentina Fil: Schnackenberg, Christine G.. GlaxoSmithKline Heart Failure Discovery Performance Unit; Estados Unidos Fil: Kass, David A.. Johns Hopkins Medical Institutions. Department of Medicine; Estados Unidos

Published

2014

4. Soluble Epoxide Hydrolase Inhibition Does Not Prevent Cardiac Remodeling and Dysfunction After Aortic Constriction in Rats and Mice

Author

Bao Hoang, Stephen H. Eisennagel, James Tunstead, Shufang Zhao, Alan R. Olzinski, Beat M. Jucker, David J. Behm, Tao Wang, John J. Upson, Joseph P. Marino, Lisa A. Morgan, and Robert N. Willette

Subjects

Male, Epoxide hydrolase 2, medicine.medical_specialty, Cardiomegaly, Vasodilation, Constriction, Pathologic, Muscle hypertrophy, Rats, Sprague-Dawley, Mice, Piperidines, Species Specificity, Fibrosis, Internal medicine, medicine.artery, medicine, Animals, Enzyme Inhibitors, Aorta, Epoxide Hydrolases, Pharmacology, Pressure overload, Cyclohexylamines, Ventricular Remodeling, Triazines, business.industry, Anatomy, medicine.disease, Rats, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, Ventricle, Heart failure, cardiovascular system, Cardiology and Cardiovascular Medicine, business

Abstract

Epoxyeicosatrienoic acids, substrates for soluble epoxide hydrolase (sEH), exhibit vasodilatory and antihypertrophic activities. Inhibitors of sEH might therefore hold promise as heart failure therapeutics. We examined the ability of sEH inhibitors GSK2188931 and GSK2256294 to modulate cardiac hypertrophy, fibrosis, and function after transverse aortic constriction (TAC) in rats and mice. GSK2188931 administration was initiated in rats 1 day before TAC, whereas GSK2256294 treatment was initiated in mice 2 weeks after TAC. Four weeks later, cardiovascular function was assessed, plasma was collected for drug and sEH biomarker concentrations, and left ventricle was isolated for messenger RNA and histological analyses. In rats, although GSK2188931 prevented TAC-mediated increases in certain genes associated with hypertrophy and fibrosis (α-skeletal actin and connective tissue growth factor), the compound failed to attenuate TAC-induced increases in left ventricle mass, posterior wall thickness, end-diastolic volume and pressure, and perivascular fibrosis. Similarly, in mice, GSK2256294 did not reverse cardiac remodeling or systolic dysfunction induced by TAC. Both compounds increased the sEH substrate/product (leukotoxin/leukotoxin diol) ratio, indicating sEH inhibition. In summary, sEH inhibition does not prevent cardiac remodeling or dysfunction after TAC. Thus, targeting sEH seems to be insufficient for reducing pressure overload hypertrophy.

Published

2013

5. GSK1562590, a slowly dissociating urotensin-II receptor antagonist, exhibits prolonged pharmacodynamic activity ex vivo

Author

Krista B. Goodman, Mark A. Hilfiker, David J. Behm, Gren Z. Wang, John J. McAtee, Sarah E. Dowdell, CA Leach, Alan R. Olzinski, Jason W. Dodson, Robert N. Willette, Nambi Aiyar, Clark A. Sehon, Harpel, Stephen A. Douglas, and Michael J. Neeb

Subjects

Pharmacology, medicine.medical_specialty, Neurotransmitter uptake, Intrinsic activity, Antagonist, Biological activity, Urotensin-II receptor, Biology, Endocrinology, In vivo, Competitive antagonist, Internal medicine, medicine, Ex vivo

Abstract

BACKGROUND AND PURPOSE Recently identified antagonists of the urotensin–II (U-II) receptor (UT) are of limited utility for investigating the (patho)physiological role of U-II due to poor potency and limited selectivity and/or intrinsic activity. EXPERIMENTAL APPROACH The pharmacological properties of two novel UT antagonists, GSK1440115 and GSK1562590, were compared using multiple bioassays. KEY RESULTS GSK1440115 (pKi= 7.34–8.64 across species) and GSK1562590 (pKi= 9.14–9.66 across species) are high affinity ligands of mammalian recombinant (mouse, rat, cat, monkey, human) and native (SJRH30 cells) UT. Both compounds exhibited >100-fold selectivity for UT versus 87 distinct mammalian GPCR, enzyme, ion channel and neurotransmitter uptake targets. GSK1440115 showed competitive antagonism at UT in arteries from all species tested (pA2= 5.59–7.71). In contrast, GSK1562590 was an insurmountable UT antagonist in rat, cat and hUT transgenic mouse arteries (pKb= 8.93–10.12 across species), but a competitive antagonist in monkey arteries (pKb= 8.87–8.93). Likewise, GSK1562590 inhibited the hU-II-induced systemic pressor response in anaesthetized cats at a dose 10-fold lower than that of GSK1440115. The antagonistic effects of GSK1440115, but not GSK1562590, could be reversed by washout in rat isolated aorta. In ex vivo studies, GSK1562590 inhibited hU-II-induced contraction of rat aorta for at least 24 h following dosing. Dissociation of GSK1562590 binding was considerably slower at rat than monkey UT. CONCLUSIONS AND IMPLICATIONS Whereas both GSK1440115 and GSK1562590 represent high-affinity/selective UT antagonists suitable for assessing the (patho)physiological role of U-II, only GSK1562590 exhibited sustained UT residence time and improved preclinical efficacy in vivo.

Published

2010

6. Chronic Inhibition of Hypoxia-inducible Factor Prolyl 4-hydroxylase Improves Ventricular Performance, Remodeling, and Vascularity After Myocardial Infarction in the Rat

Author

Beat M. Jucker, Connie L. Erickson-Miller, Weike Bao, Saul Needle, G. C. Teg Pipes, Jennifer L. Ariazi, Robert N. Willette, Alan R. Olzinski, Erding Hu, John J. Lepore, David J. Behm, Shufang Zhao, Kevin J. Duffy, and Pu Qin

Subjects

Male, medicine.medical_specialty, Angiogenesis, Glycine, Myocardial Infarction, Procollagen-Proline Dioxygenase, Inflammation, Quinolones, Cell Line, Rats, Sprague-Dawley, Vascularity, Internal medicine, medicine, Animals, Transcription factor, Pharmacology, Ventricular Remodeling, business.industry, Hemodynamics, Hypoxia-Inducible Factor 1, alpha Subunit, Coronary Vessels, Rats, Oxygen tension, Endocrinology, Hypoxia-inducible factors, Rats, Inbred Lew, Erythropoietin, Erythropoiesis, Hypoxia-Inducible Factor 1, medicine.symptom, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Hypoxia inducible factors (HIFs) are transcription factors that are regulated by HIF-prolyl 4-hydroxylases (PHDs) in response to changes in oxygen tension. Once activated, HIFs play an important role in angiogenesis, erythropoiesis, proliferation, cell survival, inflammation, and energy metabolism. We hypothesized that GSK360A, a novel orally active HIF-PHD inhibitor, could facilitate local and systemic HIF-1 alpha signaling and protect the failing heart after myocardial infarction (MI).GSK360A is a potent (nanomolar) inhibitor of HIF-PHDs (PHD1PHD2 = PHD3) capable of activating the HIF-1 alpha pathway in a variety of cell types including neonatal rat ventricular myocytes and H9C2 cells. Male rats treated orally with GSK360A (30 mg x kg x d) had a sustained elevation in circulating levels of erythropoietin and hemoglobin and increased hemoxygenase-1 expression in the heart and skeletal muscle. In a rat model of established heart failure with systolic dysfunction induced by ligation of left anterior descending coronary artery, chronic treatment with GSK360A for 28 days prevented the progressive reduction in ejection fraction, ventricular dilation, and increased lung weight, which were observed in the vehicle-treated animals, for up to 3 months. In addition, the microvascular density in the periinfarct region was increased (2-fold) in GSK360A-treated animals. Treatment was well tolerated (survival was 89% in the GSK360A group vs. 82% in the placebo group).Chronic post-myocardial infarction treatment with a selective HIF PHD inhibitor (GSK360A) exerts systemic and local effects by stabilizing HIF-1 alpha signaling and improves long-term ventricular function, remodeling, and vascularity in a model of established ventricular dysfunction. These results suggest that HIF-PHD inhibitors may be suitable for the treatment of post-MI remodeling and heart failure.

Published

2010

7. Differential Effects of p38 Mitogen-Activated Protein Kinase and Cyclooxygenase 2 Inhibitors in a Model of Cardiovascular Disease

Author

Timothy D. Westfall, Chris P. Doe, Shufang Zhao, Ross G. Bentley, Alan R. Olzinski, Robert W. Coatney, Marianne E. Eybye, Kristeen Maniscalco, Robert N. Willette, Nambi Aiyar, and David J. Behm

Subjects

Cyclopropanes, Male, MAPK/ERK pathway, medicine.medical_specialty, Pyridines, Interleukin-1beta, Renal function, Blood Pressure, Inflammation, Kidney Function Tests, p38 Mitogen-Activated Protein Kinases, Plasma renin activity, Electrocardiography, Lactones, chemistry.chemical_compound, Rats, Inbred SHR, Internal medicine, Renin, medicine, Animals, Sulfones, Enzyme Inhibitors, Aldosterone, Rofecoxib, Pharmacology, Cyclooxygenase 2 Inhibitors, Ventricular Remodeling, biology, business.industry, Lipid Metabolism, medicine.disease, Rats, Vasodilation, Endocrinology, chemistry, Cardiovascular Diseases, Cyclooxygenase 2, Cyclooxygenase 1, biology.protein, Cytokines, Molecular Medicine, Endothelium, Vascular, Cyclooxygenase, medicine.symptom, business, Dyslipidemia, medicine.drug

Abstract

The evidence is compelling for a role of inflammation in cardiovascular diseases; however, the chronic use of anti-inflammatory drugs for these indications has been disappointing. The recent study compares the effects of two anti-inflammatory agents [cyclooxygenase 2 (COX2) and p38 inhibitors] in a model of cardiovascular disease. The vascular, renal, and cardiac effects of 4-(4-methylsulfonylphenyl)-3-phenyl-5H-furan-2-one (rofecoxib; a COX2 inhibitor) and 6-{5-[(cyclopropylamino)carbonyl]-3-fluoro-2-methylphenyl}-N-(2,2-dimethylpropyl)-3-pyridinecarboxamide [GSK-AHAB, a selective p38 mitogen-activated protein kinase (MAPK) inhibitor], were examined in the spontaneously hypertensive stroke-prone rat (SHR-SP). In SHR-SPs receiving a salt-fat diet (SFD), chronic treatment with GSK-AHAB significantly and dose-dependently improved survival, endothelial-dependent and -independent vascular relaxation, and indices of renal function, and it attenuated dyslipidemia, hypertension, cardiac remodeling, plasma renin activity (PRA), aldosterone, and interleukin-1beta (IL-1beta). In contrast, chronic treatment with a COX2-selective dose of rofecoxib exaggerated the harmful effects of the SFD, i.e., increasing vascular and renal dysfunction, dyslipidemia, hypertension, cardiac hypertrophy, PRA, aldosterone, and IL-1beta. The protective effects of a p38 MAPK inhibitor are clearly distinct from the deleterious effects of a selective COX2 inhibitor in the SHR-SP and suggest that anti-inflammatory agents can have differential effects in cardiovascular disease. The results also suggest a method for evaluating long-term cardiovascular efficacy and safety.

Published

2009

8. p38 MAPK inhibitors suppress biomarkers of hypertension end-organ damage, osteopontin and plasminogen activator inhibitor-1

Author

Tian-Li Yue, Sandhya S. Nerurkar, Rosanna C. Mirabile, Alan R. Olzinski, Kendall S. Frazier, D. Rajagopalan, Robert N. Willette, S. P. O'Brien, and J. Jing

Subjects

Male, medicine.medical_specialty, End organ damage, Health, Toxicology and Mutagenesis, p38 mitogen-activated protein kinases, Clinical Biochemistry, Enzyme-Linked Immunosorbent Assay, p38 Mitogen-Activated Protein Kinases, Biochemistry, Lesion, chemistry.chemical_compound, stomatognathic system, Rats, Inbred SHR, Internal medicine, Plasminogen Activator Inhibitor 1, Gene expression, medicine, Animals, Osteopontin, Protein Kinase Inhibitors, Oligonucleotide Array Sequence Analysis, biology, medicine.disease, Immunohistochemistry, Rats, Endocrinology, chemistry, Plasminogen activator inhibitor-1, Hypertension, biology.protein, medicine.symptom, Plasminogen activator, Biomarkers

Abstract

The assessment of target organ damage is important in defining the optimal treatment of hypertension and blood pressure-related cardiovascular disease. The aims of the present study were (1) to investigate candidate biomarkers of target organ damage, osteopontin (OPN) and plasminogen activator inhibitor-1 (PAI-1), in models of malignant hypertension with well characterized end-organ pathology; and (2) to evaluate the effects of chronic treatment with a p38 MAPK inhibitor. Gene expression, plasma concentrations, and renal immunohistochemical localization of OPN and PAI-1 were measured in stroke-prone spontaneously hypertensive rats on a salt-fat diet (SFD SHR-SP) and in spontaneously hypertensive rats receiving N(omega)-nitro-L-arginine methyl ester (L-NAME SHR). Plasma concentrations of OPN and PAI-1 increased significantly in SFD SHR-SP and L-NAME SHR as compared with controls, (2.5-4.5-fold for OPN and 2.0-9.0-fold for PAI-1). The plasma levels of OPN and PAI-1 were significantly correlated with the urinary excretion of albumin (p0.0001). Elevations in urinary albumin, plasma OPN and PAI-1 were abolished by chronic treatment (4-8 weeks) with a specific p38 MAPK inhibitor, SB-239063AN. OPN immunoreactivity was localized predominantly in the apical portion of tubule epithelium, while PAI-1 immunoreactivity was robust in glomeruli, tubules and renal artery endothelium. Treatment with the p38 MAPK inhibitor significantly reduced OPN and PAI-1 protein expression in target organs. Kidney gene expression was increased for OPN (4.9- and 7.9-fold) and PAI-1 (2.8- and 11.5-fold) in SFD SHR-SP and L-NAME SHR, respectively. In-silico pathway analysis revealed that activation of p38 MAPK was linked to OPN and PAI-1 via SPI, c-fos and c-jun; suggesting that these pathways may play an important role in p38 MAPK-dependent hypertensive renal dysfunction. The results suggest that enhanced OPN and PAI-1 expression reflects end-organ damage in hypertension and that suppression correlates with end-organ protection regardless of overt antihypertensive action.

Published

2007

9. Lysophosphatidylcholine induces inflammatory activation of human coronary artery smooth muscle cells

Author

Douglas G. Johns, Nambi Aiyar, Stephen A. Douglas, Haisong Ju, Sandhya S. Nerurkar, Jyoti Disa, Colin H. Macphee, Zhaohui Ao, and Robert N. Willette

Subjects

medicine.medical_specialty, Vascular smooth muscle, medicine.medical_treatment, Myocytes, Smooth Muscle, Clinical Biochemistry, Basic fibroblast growth factor, 6-Ketoprostaglandin F1 alpha, Arachidonic Acids, Tritium, Leukotriene B4, Proinflammatory cytokine, chemistry.chemical_compound, Phospholipase A2, Internal medicine, medicine, Humans, Myocyte, Molecular Biology, Cells, Cultured, Inflammation, Arachidonic Acid, biology, Growth factor, Lysophosphatidylcholines, Cell Biology, General Medicine, Coronary Vessels, Lipids, Endocrinology, Lysophosphatidylcholine, chemistry, Phospholipases, biology.protein, Cytokines, Fibroblast Growth Factor 2, lipids (amino acids, peptides, and proteins), Arachidonic acid

Abstract

Lysophosphatidylcholine (LPC) is the major bioactive lipid component of oxidized LDL, thought to be responsible for many of the inflammatory effects of oxidized LDL described in both inflammatory and endothelial cells. Inflammation-induced transformation of vascular smooth muscle cells from a contractile phenotype to a proliferative/secretory phenotype is a hallmark of the vascular remodeling that is characteristic of atherogenesis; however, the role of LPC in this process has not been fully described. The present study tested the hypothesis that LPC is an inflammatory stimulus in coronary artery smooth muscle cells (CASMCs). In cultured human CASMCs, LPC stimulated time- and concentration-dependent release of arachidonic acid that was sensitive to phospholipase A2 and C inhibition. LPC stimulated the release of arachidonic acid metabolites leukotriene-B4 and 6-keto-prostaglandin F1alpha, within the same time course. LPC was also found to stimulate basic fibroblast growth factor release as well as stimulating the release of the cytokines GM-CSF, IL-6, and IL-8. Optimal stimulation of these signals was obtained via palmitic acid-substituted LPC species. Stimulation of arachidonic acid, inflammatory cytokines and growth factor release, implies that LPC might play a multifactorial role in the progression of atherosclerosis, by affecting inflammatory processes.

Published

2006

10. The peptidic urotensin-II receptor ligand GSK248451 possesses less intrinsic activity than the low-efficacy partial agonists SB-710411 and urantide in native mammalian tissues and recombinant cell systems

Author

Henry M. Sarau, Valeria Camarda, Stephen A. Douglas, Girolamo Calo, David G. Lambert, Nambi Aiyar, Robert N. Willette, Dulcie B. Schmidt, Parvathi Nuthulaganti, Gerald Stankus, Christopher P. Doe, David J. Behm, James J. Foley, James A. Fornwald, and Robert S. Ames

Subjects

Pharmacology, Agonist, medicine.medical_specialty, Intrinsic activity, medicine.drug_class, HEK 293 cells, Urotensin-II receptor, Biology, Partial agonist, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, medicine, Urotensin-II, Receptor, G protein-coupled receptor

Abstract

Several peptidic urotensin-II (UT) receptor antagonists exert 'paradoxical' agonist activity in recombinant cell- and tissue-based bioassay systems, likely the result of differential urotensin-II receptor (UT receptor) signal transduction/coupling efficiency between assays. The present study has examined this phenomenon in mammalian arteries and recombinant UT-HEK (human embryonic kidney) cells.BacMam-mediated recombinant UT receptor upregulation in HEK cells augmented agonist activity for all four peptidic UT ligands studied. The nominal rank order of relative intrinsic efficacy was U-II>urantide ([Pen(5)-DTrp(7)-Orn(8)]hU-II(4-11))>SB-710411 (Cpa-c[DCys-Pal-DTrp-Lys-Val-Cys]-Cpa-amide)>>GSK248451 (Cin-c[DCys-Pal-DTrp-Orn-Val-Cys]-His-amide) (the relative coupling efficiency of recombinant HEK cells was cat>human>>rat UT receptor). The present study further demonstrated that the use of high signal transduction/coupling efficiency isolated blood vessel assays (primate>cat arteries) is required in order to characterize UT receptor antagonism thoroughly. This cannot be attained simply by using the rat isolated aorta, an artery with low signal transduction/coupling efficiency in which low-efficacy agonists appear to function as antagonists. In contrast to the 'low-efficacy agonists' urantide and SB-710411, GSK248451 functioned as a potent UT receptor antagonist in all native isolated tissues studied (UT receptor selectivity was confirmed in the rat aorta). Further, GSK248451 exhibited an extremely low level of relative intrinsic activity in recombinant HEK cells (4-5-fold less than seen with urantide). Since GSK248451 (1 mg kg(-1), i.v.) blocked the systemic pressor actions of exogenous U-II in the anaesthetized cat, it represents a suitable peptidic tool antagonist for delineating the role of U-II in the aetiology of mammalian cardiometabolic diseases.

Published

2006

11. Hypertensive target organ damage is attenuated by a p38 MAPK inhibitor: role of systemic blood pressure and endothelial protection

Author

Chavon M Milliner, Alan R. Olzinski, David J. Behm, Marianne E. Eybye, Rosanna C. Mirabile, Ross Bentley, Shufang Q. Zhao, Kristeen Maniscalco, Tara A McCafferty, Robert W. Coatney, Robert N. Willette, and Kendall S. Frazier

Subjects

Male, medicine.medical_specialty, Endothelium, Physiology, End organ damage, Concentric hypertrophy, In Vitro Techniques, Kidney, p38 Mitogen-Activated Protein Kinases, Spontaneously hypertensive rat, Rats, Inbred SHR, Physiology (medical), Internal medicine, Animals, Medicine, Endothelial dysfunction, business.industry, Myocardium, Imidazoles, Kidney metabolism, medicine.disease, Rats, NG-Nitroarginine Methyl Ester, Pyrimidines, medicine.anatomical_structure, Blood pressure, Endocrinology, Echocardiography, Hypertension, Models, Animal, Vascular Resistance, Nitric Oxide Synthase, Cardiology and Cardiovascular Medicine, business

Abstract

Objective : Evidence suggests important relationships among chronic inflammatory processes, endothelial dysfunction, hypertension and target organ damage. The present study examined the effects of chronic treatment with an anti-inflammatory p38 mitogen-activated protein kinase (MAPK) inhibitor (SB-239063AN) in the N ω-nitro-l-arginine methyl ester-treated spontaneously hypertensive rat (SHR+l-NAME) model of severe hypertension and accelerated target organ damage. Methods: SHRs were divided into control ( n =16), l-NAME ( n =26) and l-NAME+SB-239063AN ( n =24) groups. l-NAME was delivered by the drinking water ad lib (50 mg/L) and SB-239063AN was administered by the diet (1200 ppm) for 4 weeks. Arterial blood pressure (telemetry) and target organ damage (kidney, heart, and vasculature) were examined. Results: The introduction of l-NAME to the drinking water elicited a severe/sustained increase in blood pressure and significant morbidity and mortality. Chronic treatment with SB-239063AN had no effect on the initial blood pressure response (7 days) to l-NAME but attenuated subsequent increases in diastolic blood pressure and significantly reduced morbidity/mortality (42% vs. 5%, p

Published

2005

12. Anti-apoptotic effects of rosiglitazone in hypercholesterolemic rabbits subjected to myocardial ischemia and reperfusion

Author

Tian-Li Yue, Eliot H. Ohlstein, Erhe Gao, Xin-Liang Ma, Robert N. Willette, Bernard L. Lopez, Huirong Liu, Theodore A. Christopher, and Ling Tao

Subjects

Male, medicine.medical_specialty, Normal diet, MAP Kinase Signaling System, Physiology, Hypercholesterolemia, Myocardial Ischemia, Ischemia, Receptors, Cytoplasmic and Nuclear, Apoptosis, Myocardial Reperfusion Injury, Nitric Oxide, High cholesterol, Rosiglitazone, chemistry.chemical_compound, Reperfusion therapy, Physiology (medical), Internal medicine, In Situ Nick-End Labeling, medicine, Animals, business.industry, Nitrotyrosine, medicine.disease, Diet, Endocrinology, chemistry, Enzyme Induction, Thiazolidinediones, Rabbits, Cardiology and Cardiovascular Medicine, business, Reperfusion injury, Transcription Factors, medicine.drug

Abstract

Objectives: This study examined the effects of diet-induced hypercholesterolemia on the extent of postischemic myocyte apoptosis and elucidated the potential mechanisms involved. Furthermore, the effects of rosiglitazone (RSG) on postischemic myocardial apoptosis in HC rabbits were investigated. Methods: Male New Zealand rabbits were fed normal or high cholesterol diets for 8 weeks. Three weeks after being fed a high cholesterol diet, HC rabbits were randomized to receive vehicle or RSG during the remaining 5 weeks. Rabbits were then subjected to 60 min of coronary occlusion followed by 4 h of reperfusion. Results: Compared with rabbits fed with a normal diet, HC rabbits had increased caspase-3 activity, apoptotic cell death and retarded contractile function recovery after reperfusion. HC increased iNOS expression, total NOx and nitrotyrosine contents, indicating that an increased nitrative stress occurred in HC myocardial tissue. Activity of a hypertrophic/anti-apoptotic mitogen-activated protein kinase (MAPK), ERK1/2, was significantly decreased while activation of a pro-apoptotic MAPK, p38, was increased. Treatment with RSG in HC rabbits attenuated postischemic myocardial nitrative stress, restored a beneficial balance between pro- and anti-apoptotic MAPK signaling, reduced postischemic myocardial apoptosis, and improved cardiac functional recovery. Conclusions: Our results demonstrated that HC increased postischemic myocardial apoptosis likely by increasing the production of pro-apoptotic molecules, activating pro-apoptotic signaling pathways and inhibiting anti-apoptotic signaling. In addition, our results suggest that peroxisome proliferator-activated receptor (PPAR) γ agonists may not only attenuate the formation of atherosclerosis associated with hypercholesterolemia as previously reported, but may also protect the heart from subsequent ischemic/reperfusion-induced myocardial apoptosis.

Published

2004

13. p38 MAPK Inhibitors Ameliorate Target Organ Damage in Hypertension: Part 2. Improved Renal Function as Assessed by Dynamic Contrast-Enhanced Magnetic Resonance Imaging

Author

Rogely W. Boyce, Thomas R. Schaeffer, Rosanna C. Mirabile, Robert N. Willette, Beat M. Jucker, David F. Adams, Stephen C. Lenhard, and Sandhya S. Nerurkar

Subjects

Gadolinium DTPA, MAPK/ERK pathway, medicine.medical_specialty, p38 mitogen-activated protein kinases, Contrast Media, Renal function, In Vitro Techniques, Kidney, Kidney Function Tests, p38 Mitogen-Activated Protein Kinases, Pathogenesis, In vivo, Rats, Inbred SHR, Internal medicine, medicine, Albuminuria, Animals, Enzyme Inhibitors, Pharmacology, medicine.diagnostic_test, business.industry, Imidazoles, Sodium, Dietary, Magnetic resonance imaging, Dietary Fats, Magnetic Resonance Imaging, Rats, Stroke, Pyrimidines, Blood pressure, Endocrinology, Creatinine, Hypertension, Molecular Medicine, Endothelium, Vascular, Mitogen-Activated Protein Kinases, medicine.symptom, business, Glomerular Filtration Rate

Abstract

Recent evidence suggests p38 mitogen-activated protein kinase (MAPK) signal transduction plays an important role in the pathogenesis of progressive renal disease. Using dynamic contrast enhanced magnetic resonance imaging (MRI), we evaluated chronic treatment with a p38 MAPK inhibitor, trans-1-(4-hydroxycyclohexyl)-4-(4-fluorophenyl-methoxypyridimidin-4-yl)imidazole (SB-239063), on renal function in a hypertension model of progressing renal dysfunction. Spontaneously hypertensive-stroke prone rats were placed on a high salt/fat diet (SFD) or maintained on normal chow diet (ND). SFD animals with albuminuria at 4 to 8 weeks (or =10 mg/day inclusion criteria), were randomized into p38 MAPK inhibitor treatment (SB-239063, 1200 ppm in diet) or vehicle groups. The progression of blood pressure and albuminuria during the treatment period (approximately 6 weeks) was decreased by 12 and 60%, respectively, in the SFD + SB-239063 versus SFD control group. Renal perfusion and filtration were assessed by in vivo MRI at the end of the study. Relative cortical perfusion was increased in the SFD + SB-239063 group compared with the SFD control group as reflected by a 29% decrease in time to peak of contrast agent in the cortex. Additionally, the regional renal glomerular filtration rate index (Kcl) was increased by 39% in the SFD + SB-239063 versus SFD control group and was normalized to the ND control group. Greater functional heterogeneity was observed in the SFD control versus SFD + SB-239063 or ND control group. All alterations of renal function were supported by histopathological findings. In conclusion, chronic treatment with a p38 MAPK inhibitor, SB-239063, attenuates functional and structural renal degeneration in a hypertensive model of established renal dysfunction.

Published

2003

14. p38 MAPK Inhibitors Ameliorate Target Organ Damage in Hypertension: Part 1. p38 MAPK-Dependent Endothelial Dysfunction and Hypertension

Author

Robin E. Haimbach, Haisong Ju, Alan R. Olzinski, Marianne E. Eybye, Stephen A. Douglas, Sandyha Nerurkar, David J. Behm, and Robert N. Willette

Subjects

Male, MAPK/ERK pathway, medicine.medical_specialty, Survival, Endothelium, p38 mitogen-activated protein kinases, Blotting, Western, Blood Pressure, Muscarinic Agonists, p38 Mitogen-Activated Protein Kinases, Umbilical vein, Rats, Inbred SHR, Internal medicine, Adventitia, medicine, Albuminuria, Animals, Humans, Telemetry, Enzyme Inhibitors, Endothelial dysfunction, Pharmacology, business.industry, Imidazoles, Hypoxia (medical), medicine.disease, Immunohistochemistry, Rats, Stroke, Pyrimidines, Endocrinology, medicine.anatomical_structure, Hypertension, cardiovascular system, Molecular Medicine, Carbachol, Tumor necrosis factor alpha, Endothelium, Vascular, Mitogen-Activated Protein Kinases, medicine.symptom, business, Cell Adhesion Molecules

Abstract

Numerous mediators, believed to play a role in endothelial dysfunction (e.g., neurohormones, cytokines, hypoxia, and stretch), have been shown to activate p38 mitogen-activated protein kinase (MAPK) in a variety of cell types. The purpose of the present study was to examine the regulation of p38 MAPK in endothelium and its role in endothelial dysfunction and salt sensitivity. In cultured human umbilical vein endothelial cells (HUVECs), tumor necrosis factor-alpha and lipopolysaccharide increased phosphorylation of p38 MAPK (P-p38 MAPK) and increased ICAM-1 expression. Preincubation with highly selective p38 MAPK inhibitors, 1-(1,3-dihydroxyprop-2-yl)-4-(4-fluorophenyl)-5-[2-phenoxypyrimidin-4-yl] imidazole (SB-239063AN) or SB-239063, dose dependently reduced intercellular adhesion molecule-1 expression in HUVECs. In spontaneously hypertensive-stroke prone rats (SHR-SP), P-p38 MAPK was localized by immunohistochemistry to the aortic endothelium and adventitia but was undetectable in aortae from normotensive rats. Introduction of a salt/fat diet (SFD) to the SHR-SP strain induced endothelial dysfunction (ex vivo vascular reactivity analysis), albuminuria, and an increase in blood pressure within 4 weeks. Chronic dietary dosing (approx. 100 mg/kg/day) with SB-239063AN inhibited the SFD diet-induced hypertension. In addition, delayed treatment also significantly improved survival and restored nitric oxide-mediated endothelium-dependent relaxation in SFD-SHR-SPs with established endothelial dysfunction. These results suggest an important role for p38 MAPK in endothelial inflammation and dysfunction as well as providing the first evidence for p38 MAPK-dependent hypertension.

Published

2003

15. Deletion of the UT receptor gene results in the selective loss of urotensin-II contractile activity in aortae isolated from UT receptor knockout mice

Author

Stephen M. Harrison, Kristeen Maniscalco, David J. Behm, Zhaohui Ao, Robert N. Willette, Susan J. Pickering, Stephen A. Douglas, Evelyn Grau, Robert W. Coatney, Douglas G. Johns, Christopher P. Doe, and Tina N Woods

Subjects

Pharmacology, medicine.medical_specialty, Carbachol, Anatomy, Biology, Endothelin 1, chemistry.chemical_compound, medicine.anatomical_structure, Endocrinology, chemistry, Internal medicine, Knockout mouse, medicine, medicine.symptom, Receptor, Urotensin-II, Mesenteric arteries, Phenylephrine, Vasoconstriction, medicine.drug

Abstract

1 Urotensin-II (U-II) is among the most potent mammalian vasoconstrictors identified and may play a role in the aetiology of essential hypertension. Currently, only one mouse U-II receptor (UT) gene has been cloned. It is postulated that this protein is solely responsible for mediating U-II-induced vasoconstriction. 2 This hypothesis has been investigated in the present study, which assessed basal haemodynamics and vascular reactivity to hU-II in wild-type (UT((+/+))) and UT receptor knockout (UT((-/-))) mice. 3 Basal left ventricular end-diastolic and end-systolic volumes/pressures, stroke volumes, mean arterial blood pressures, heart rates, cardiac outputs and ejection fractions in UT((+/+)) mice and in UT((-/-)) mice were similar. 4 Relative to UT((+/+)) mouse isolated thoracic aorta, where hU-II was a potent spasmogen (pEC(50)=8.26+/-0.08) that evoked relatively little vasoconstriction (17+/-2% 60 mM KCl), vessels isolated from UT((-/-)) mice did not respond to hU-II. However, in contrast, the superior mesenteric artery isolated from both the genotypes did not contract in the presence of hU-II. Reactivity to unrelated vasoconstrictors (phenylephrine, endothelin-1, KCl) and endothelium-dependent/independent vasodilator agents (carbachol, sodium nitroprusside) was similar in the aorta and superior mesenteric arteries isolated from both the genotypes. 5 The present study is the first to directly link hU-II-induced vasoconstriction with the UT receptor. Deletion of the UT receptor gene results in loss of hU-II contractile action with no 'nonspecific' alterations in vascular reactivity. However, as might be predicted based on the limited contractile efficacy recorded in vitro, the contribution that hU-II and its receptor make to basal systemic haemodynamics appears to be negligible in this species.

Published

2003

16. Activation of Caspase-3/Caspase-3-Like Activity in Rat Cardiomyocytes by an RGD Peptide, but not the GPIIb/IIIa Antagonist Lotrafiban

Author

Melanie A. Gabriel, Eliot H. Ohlstein, Frank C. Barone, Andrew A. Parsons, Robert N. Willette, John R. Toomey, Joseph A. Erhardt, and Tian-Li Yue

Subjects

medicine.medical_specialty, Platelet Aggregation, Caspase 3, Platelet Glycoprotein GPIIb-IIIa Complex, Biology, Rats, Sprague-Dawley, Benzodiazepines, Fibrinolytic Agents, Piperidines, Coumarins, Internal medicine, medicine, Animals, Myocyte, Cells, Cultured, chemistry.chemical_classification, Gpiib iiia antagonist, Myocardium, Antagonist, Heart, Biological activity, Hematology, Molecular biology, Rats, Enzyme Activation, Lotrafiban, Endocrinology, Enzyme, chemistry, Caspases, Oligopeptides, Platelet Aggregation Inhibitors, Cysteine

Published

2001

17. Differential vasoconstrictor activity of human urotensin-II in vascular tissue isolated from the rat, mouse, dog, pig, marmoset and cynomolgus monkey

Author

Henry M. Sarau, Nambi Aiyar, Eliot H. Ohlstein, Valerie Piercy, Anthony C Sulpizio, Robert N. Willette, Robert S. Ames, and Stephen A. Douglas

Subjects

Pharmacology, medicine.medical_specialty, Biology, Urotensin-II receptor, Endothelin 1, chemistry.chemical_compound, Endocrinology, medicine.anatomical_structure, chemistry, Internal medicine, Circulatory system, medicine, Vasoconstrictor Agents, medicine.symptom, Urotensin-II, Phenylephrine, Vasoconstriction, medicine.drug, Blood vessel

Abstract

1. Urotensin-II (U-II) and its G-protein-coupled receptor, GPR14, are expressed within mammalian cardiac and peripheral vascular tissue and, as such, may regulate mammalian cardiovascular function. The present study details the vasoconstrictor profile of this cyclic undecapeptide in different vascular tissues isolated from a diverse range of mammalian species (rats, mice, dogs, pigs, marmosets and cynomolgus monkeys). 2. The vasoconstrictor activity of human U-II was dependent upon the anatomical origin of the vessel studied and the species from which it was isolated. In the rat, constrictor responses were most pronounced in thoracic aortae and carotid arteries: -log[EC(50)]s 9.09+/-0.19 and 8.84+/-0.21, R(max)s 143+/-21 and 67+/-26% 60 mM KCl, respectively (compared, for example, to -log[EC(50)] 7.90+/-0.11 and R(max) 142+/-12% 60 mM KCl for endothelin-1 [ET-1] in thoracic aortae). Responses were, however, absent in mice aortae (-log[EC(50)]

Published

2000

18. Application of real-time polymerase chain reaction to quantitate induced expression of interleukin-1? mRNA in ischemic brain tolerance

Author

Frank C. Barone, Xinkang Wang, R. William Currie, Robert N. Willette, Xiang Li, and Giora Z. Feuerstein

Subjects

medicine.medical_specialty, Messenger RNA, Ischemia, Interleukin, Biology, medicine.disease, Molecular biology, Neuroprotection, Cellular and Molecular Neuroscience, Real-time polymerase chain reaction, Endocrinology, Internal medicine, medicine.artery, Middle cerebral artery, medicine, Immunohistochemistry, Ischemic preconditioning

Abstract

A short duration of ischemia (i.e., ischemic preconditioning) was shown to result in significant tolerance to subsequent ischemic injury. Since previous reports suggest that interleukin-1beta (IL-1beta) may be involved in both ischemic damage and neuroprotection, the present work examined the expression of IL-1beta mRNA in cortical brain tissue after an established preconditioning (PC) stimulus known to produce significant brain tolerance to focal stroke after 1-7 days. Significant induction of IL-1beta mRNA was observed in the ipsilateral cortex at 6 hr (87+/-9 copies of the mRNA per microgram of brain tissue compared to 16+/-5 copies in sham-operated samples, P < 0.001, n = 4) and 8 hr (46+/-4 copies, P < 0.01, n = 4) after PC by means of real-time Taqman polymerase chain reaction (PCR). The peak expression of IL-1beta mRNA after PC was significantly (P < 0.01) lower than that after permanent occlusion of the middle cerebral artery (MCAO), i.e., 87+/-9 and 546+/-92 copies of RNA per microgram tissue at peak levels for PC and focal stroke, respectively. Immunohistochemistry studies revealed a parallel induction of IL-1beta in the ipsilateral cortex after PC. The maximal expression of IL-1beta was observed during the first week post-PC, showing marked parallelism with the duration of ischemic tolerance. These data suggest that the significant but low levels of IL-1beta induction after PC may contribute to ischemic brain tolerance.

Published

2000

19. Human Urotensin-II is a Potent Vasoactive Peptide

Author

Derek H. Ohlstein, Robert W. Coatney, Daryl J. Ashton, Nambi Aiyar, Stephen A. Douglas, Charles F. Sauermelch, Robert N. Willette, Michael R. Ruffolo, and Eliot H. Ohlstein

Subjects

Male, medicine.medical_specialty, Vascular smooth muscle, Urotensins, In Vitro Techniques, Biology, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Dogs, Species Specificity, In vivo, Internal medicine, medicine, Animals, Humans, Receptor, Pharmacology, Dose-Response Relationship, Drug, Hemodynamics, Endothelin 1, Rats, Cardiovascular physiology, Mice, Inbred C57BL, Macaca fascicularis, medicine.anatomical_structure, Endocrinology, chemistry, Vasoconstriction, Endothelin receptor, Urotensin-II, Cardiology and Cardiovascular Medicine, Blood vessel

Abstract

The observation that the novel G-protein-coupled receptor (GPCR) GPR14 and its cognate ligand, urotensin-II (U-II), are expressed within the mammalian vasculature raises the possibility that they may influence cardiohemodynamic homeostasis. To this end, this study examined the vasoactive properties of U-II in rodents, dogs and primates. In vitro, human U-II was a sustained vasoconstrictor with a potency (pD2sor = 9) approximately an order of magnitude greater than that seen with endothelin-1 (ET-1), making it one of the most, if not the most, potent mammalian vasoconstrictor identified to date. However, in vitro responses exhibited significant anatomical and/or species-dependency, that is, human U-II was a selective 'aorto-coronary' vasoconstrictor in rats and dogs, inactive in mice and contracted all primate arteries studied. In vivo, this peptide evoked a complex, dose-dependent hemodynamic response in the anesthetized primate, culminating in severe myocardial depression and fatal circulatory collapse. As such, U-II may represent a novel neurohumoral regulator of mammalian cardiovascular physiology and pathology in particular disorders characterized by aberrant vascular smooth muscle and/or myocardial function.

Published

2000

20. Human urotensin-II is a potent vasoconstrictor and agonist for the orphan receptor GPR14

Author

Anne M. Romanic, Douglas W. P. Hay, Shelagh Wilson, Eliot H. Ohlstein, Nambi Aiyar, Calvert Louden, Wu-Schyong Liu, Henry M. Sarau, George I. Glover, Stephen A. Douglas, Stephen Dudley Holmes, Charles F. Sauermelch, Nabil Elshourbagy, Usman Shabon, John D. Martin, Robert W. Coatney, James J. Foley, Johathan K. Chambers, Derk J. Bergsma, Catherine E. Ellis, Dean E. McNulty, Robert S. Ames, John J. Trill, Zhaohui Ao, Robert N. Willette, Jeffrey M. Stadel, and Jyoti Disa

Subjects

Male, Agonist, medicine.medical_specialty, DNA, Complementary, medicine.drug_class, Urotensins, Molecular Sequence Data, Central nervous system, Receptors, Cell Surface, Biology, Urotensin-II receptor, Cell Line, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, chemistry.chemical_compound, GTP-Binding Proteins, Internal medicine, medicine, Animals, Humans, Vasoconstrictor Agents, Tissue Distribution, Amino Acid Sequence, Cloning, Molecular, Receptor, Orphan receptor, Multidisciplinary, Base Sequence, Sequence Homology, Amino Acid, Rats, Macaca fascicularis, medicine.anatomical_structure, Endocrinology, chemistry, Calcium, medicine.symptom, Urotensin-II, Vasoconstriction

Abstract

Urotensin-II (U-II) is a vasoactive ‘somatostatin-like’ cyclic peptide which was originally isolated from fish spinal cords1,2, and which has recently been cloned from man3. Here we describe the identification of an orphan human G-protein-coupled receptor homologous to rat GPR14 (refs 4, 5) and expressed predominantly in cardiovascular tissue, which functions as a U-II receptor. Goby and human U-II bind to recombinant human GPR14 with high affinity, and the binding is functionally coupled to calcium mobilization. Human U-II is found within both vascular and cardiac tissue (including coronary atheroma) and effectively constricts isolated arteries from non-human primates. The potency of vasoconstriction of U-II is an order of magnitude greater than that of endothelin-1, making human U-II the most potent mammalian vasoconstrictor identified so far. In vivo, human U-II markedly increases total peripheral resistance in anaesthetized non-human primates, a response associated with profound cardiac contractile dysfunction. Furthermore, as U-II immunoreactivity is also found within central nervous system and endocrine tissues, it may have additional activities.

Published

1999

21. Correction

Author

Robert N. Willette, Jop H. van Berlo, Orlando F. Bueno, Federica Accornero, John N. Lorenz, Sanjeewa A. Goonasekera, Mannix Auger-Messier, and Jeffery D. Molkentin

Subjects

Null mice, medicine.medical_specialty, Endocrinology, Physiology, business.industry, p38 mitogen-activated protein kinases, Internal medicine, medicine, Cardiomyopathy, Cardiology and Cardiovascular Medicine, medicine.disease, business

Published

2013

22. Chronic inhibition of 11 β -hydroxysteroid dehydrogenase type 1 activity decreases hypertension, insulin resistance, and hypertriglyceridemia in metabolic syndrome

Author

Mark R. Harpel, Robert N. Willette, Daniel J. Krosky, Jianqi Cui, Christine G. Schnackenberg, Charlene W. Wu, Tian-Li Yue, Melissa H. Costell, and Victor S. Hong

Subjects

medicine.medical_specialty, Article Subject, Adipose tissue, lcsh:Medicine, Biology, Weight Gain, Plasma renin activity, General Biochemistry, Genetics and Molecular Biology, Insulin resistance, 11β-hydroxysteroid dehydrogenase type 1, Internal medicine, 11-beta-Hydroxysteroid Dehydrogenase Type 1, medicine, Animals, Humans, Obesity, Glucocorticoids, Hypertriglyceridemia, Metabolic Syndrome, General Immunology and Microbiology, lcsh:R, General Medicine, medicine.disease, Rats, Endocrinology, Liver, Hypertension, biology.protein, Receptors, Leptin, Metabolic syndrome, Insulin Resistance, Dyslipidemia, Glucocorticoid, hormones, hormone substitutes, and hormone antagonists, medicine.drug, Research Article

Abstract

Metabolic syndrome is a constellation of risk factors including hypertension, dyslipidemia, insulin resistance, and obesity that promote the development of cardiovascular disease. Metabolic syndrome has been associated with changes in the secretion or metabolism of glucocorticoids, which have important functions in adipose, liver, kidney, and vasculature. Tissue concentrations of the active glucocorticoid cortisol are controlled by the conversion of cortisone to cortisol by 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1). Because of the various cardiovascular and metabolic activities of glucocorticoids, we tested the hypothesis that 11β-HSD1 is a common mechanism in the hypertension, dyslipidemia, and insulin resistance in metabolic syndrome. In obese and lean SHR/NDmcr-cp (SHR-cp), cardiovascular, metabolic, and renal functions were measured before and during four weeks of administration of vehicle or compound 11 (10 mg/kg/d), a selective inhibitor of 11β-HSD1. Compound 11 significantly decreased 11β-HSD1 activity in adipose tissue and liver of SHR-cp. In obese SHR-cp, compound 11 significantly decreased mean arterial pressure, glucose intolerance, insulin resistance, hypertriglyceridemia, and plasma renin activity with no effect on heart rate, body weight gain, or microalbuminuria. These results suggest that 11β-HSD1 activity in liver and adipose tissue is a common mediator of hypertension, hypertriglyceridemia, glucose intolerance, and insulin resistance in metabolic syndrome.

Published

2012

23. Unrestrained p38 MAPK activation in Dusp1/4 double-null mice induces cardiomyopathy

Author

Orlando F. Bueno, John N. Lorenz, Federica Accornero, Robert N. Willette, Mannix Auger-Messier, Sanjeewa A. Goonasekera, Jeffery D. Molkentin, and Jop H. van Berlo

Subjects

MAPK/ERK pathway, medicine.medical_specialty, Mice, 129 Strain, Time Factors, Physiology, p38 mitogen-activated protein kinases, Phosphatase, Cardiomyopathy, Protein tyrosine phosphatase, Biology, p38 Mitogen-Activated Protein Kinases, Article, Mice, Internal medicine, medicine, Animals, Myocytes, Cardiac, Phosphorylation, Protein Kinase Inhibitors, Cells, Cultured, Mice, Knockout, Kinase, Calcium-Binding Proteins, Hemodynamics, Dual Specificity Phosphatase 1, Fibroblasts, medicine.disease, Myocardial Contraction, Cell biology, Enzyme Activation, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, Gene Expression Regulation, Calcium, Signal transduction, Protein Tyrosine Phosphatases, Cardiology and Cardiovascular Medicine, Cardiomyopathies, Signal Transduction

Abstract

Rationale: Mitogen-activated protein kinases (MAPKs) are activated in the heart by disease-inducing and stress-inducing stimuli, where they participate in hypertrophy, remodeling, contractility, and heart failure. A family of dual-specificity phosphatases (DUSPs) directly inactivates each of the MAPK terminal effectors, potentially serving a cardioprotective role. Objective: To determine the role of DUSP1 and DUSP4 in regulating p38 MAPK function in the heart and the effect on disease. Methods and Results: Here, we generated mice and mouse embryonic fibroblasts lacking both Dusp1 and Dusp4 genes. Although single nulls showed no molecular effects, combined disruption of Dusp1/4 promoted unrestrained p38 MAPK activity in both mouse embryonic fibroblasts and the heart, with no change in the phosphorylation of c-Jun N-terminal kinases or extracellular signal-regulated kinases at baseline or with stress stimulation. Single disruption of either Dusp1 or Dusp4 did not result in cardiac pathology, although Dusp1/4 double-null mice exhibited cardiomyopathy and increased mortality with aging. Pharmacological inhibition of p38 MAPK with SB731445 ameliorated cardiomyopathy in Dusp1/4 double-null mice, indicating that DUSP1/4 function primarily through p38 MAPK in affecting disease. At the cellular level, unrestrained p38 MAPK activity diminished cardiac contractility and Ca 2+ handling, which was acutely reversed with a p38 inhibitory compound. Poor function in Dusp1/4 double-null mice also was partially rescued by phospholamban deletion. Conclusions: Our data demonstrate that Dusp1 and Dusp4 are cardioprotective genes that play a critical role in the heart by dampening p38 MAPK signaling that would otherwise reduce contractility and induce cardiomyopathy.

Published

2012

24. Comparison of Soluble Guanylate Cyclase Stimulators and Activators in Models of Cardiovascular Disease Associated with Oxidative Stress

Author

John J. Lepore, Anne Marie Jeanne Bouillot, Kristeen Maniscalco, Olivier Mirguet, Alan R. Olzinski, Christine G. Schnackenberg, Larry J. Jolivette, John J. Upson, Nerina Dodic, Françoise Gellibert, Lisa A. Morgan, Shu Fang Zhao, Pascal Grondin, Robert W. Coatney, Beat M. Jucker, David J. Behm, Victoria L. T. Ballard, Robert N. Willette, Roberta E. Bernard, Nicolas Ancellin, Kenny Herry, and Melissa H. Costell

Subjects

soluble guanylate cyclase, SHR-SP, medicine.medical_specialty, Mean arterial pressure, End organ damage, Vasodilation, Left ventricular hypertrophy, medicine.disease_cause, Nitric oxide, BAY 60-4552, chemistry.chemical_compound, Internal medicine, Medicine, Pharmacology (medical), Original Research, GSK2181236A, Pharmacology, business.industry, lcsh:RM1-950, VASP, medicine.disease, cGMP, Endocrinology, lcsh:Therapeutics. Pharmacology, chemistry, cardiovascular system, Microalbuminuria, Sodium nitroprusside, business, Oxidative stress, medicine.drug

Abstract

Soluble guanylate cyclase (sGC), the primary mediator of nitric oxide (NO) bioactivity, exists as reduced (NO-sensitive) and oxidized (NO-insensitive) forms. We tested the hypothesis that the cardiovascular protective effects of NO-insensitive sGC activation would be potentiated under conditions of oxidative stress compared to those of NO-sensitive sGC stimulation. The cardiovascular effects of the NO-insensitive sGC activator GSK2181236A [a low, non-depressor dose, and a high dose which lowered mean arterial pressure (MAP) by 5-10 mmHg] and those of equi-efficacious doses of the NO-sensitive sGC stimulator BAY 60-4552 were assessed in (1) Sprague Dawley rats during coronary artery ischemia/reperfusion (I/R) and (2) spontaneously hypertensive stroke prone rats (SHR-SP) on a high salt/fat diet (HSFD). In I/R, neither compound reduced infarct size 24 h after reperfusion. In SHR-SP, HSFD increased MAP, urine output, microalbuminuria, and mortality, caused left ventricular hypertrophy with preserved ejection fraction, and impaired endothelium-dependent vasorelaxation. The low dose of BAY 60-4552, but not that of GSK2181236A, decreased urine output, and improved survival. Conversely, the low dose of GSK2181236A, but not that of BAY 60-4552, attenuated the development of cardiac hypertrophy. The high doses of both compounds similarly attenuated cardiac hypertrophy and improved survival. In addition to these effects, the high dose of BAY 60-4552 reduced urine output and microalbuminuria and attenuated the increase in MAP to a greater extent than did GSK2181236A. Neither compound improved endothelium-dependent vasorelaxation. In SHR-SP isolated aorta, the vasodilatory responses to the NO-dependent compounds carbachol and sodium nitroprusside were attenuated by HSFD. In contrast, the vasodilatory responses to both GSK2181236A and BAY 60-4552 were unaltered by HSFD, indicating that reduced NO-bioavailability and not changes in the oxidative state of sGC is responsible for the vascular dysfunction. In summary, GSK2181236A and BAY 60-4552 provide partial benefit against hypertension-induced end-organ damage. The differential beneficial effects observed between these compounds could reflect tissue-specific changes in the oxidative state of sGC and might help direct the clinical development of these novel classes of therapeutic agents.

Published

2012

25. Nonpeptide endothelin antagonist. Cerebrovascular characterization and effects on delayed cerebral vasospasm

Author

Eliot H. Ohlstein, M P Mitchell, Robert N. Willette, H Zhang, C F Sauermelch, and A C Sulpizio

Subjects

Endothelin Receptor Antagonists, Male, medicine.medical_specialty, Vascular smooth muscle, Subarachnoid hemorrhage, medicine.drug_class, Cerebral arteries, Viper Venoms, Muscle, Smooth, Vascular, Dogs, Cerebral vasospasm, Internal medicine, medicine.artery, Basilar artery, Animals, Vasoconstrictor Agents, Medicine, Cells, Cultured, Advanced and Specialized Nursing, Dose-Response Relationship, Drug, business.industry, Endothelins, Vasospasm, Arteries, Cerebral Arteries, Subarachnoid Hemorrhage, medicine.disease, Receptor antagonist, Disease Models, Animal, Endocrinology, Spinal Cord, Ischemic Attack, Transient, Vasoconstriction, Basilar Artery, Cerebrovascular Circulation, Indans, cardiovascular system, Neurology (clinical), Mitogens, Cardiology and Cardiovascular Medicine, business, Endothelin receptor

Abstract

(+/-)-SB 209670, a potent nonpeptide endothelin (ET) receptor antagonist, was used to investigate the potential role of ET in cerebral vasospasm associated with subarachnoid hemorrhage. The effects of (+/-)-SB 209670 were evaluated in isolated segments of canine posterior cerebral arteries in vitro, vascular smooth muscle cells in culture, and in the canine two-hemorrhage model of delayed cerebral vasospasm in vivo. In the canine basilar and anterior spinal arteries, (+/-)-SB 209670 caused a dose-related inhibition of contractile responses mediated by ET (KB = 4.6 nmol/L and apparent KB = 2.7 nmol/L, respectively). The effects of (+/-)-SB 209670 were mediated by inhibition of ETA receptors since the ETB selective agonist sarafotoxin 6c did not contract these posterior cerebral vessels. (+/-)-SB 209670 also produced a concentration-dependent inhibition (IC50 = 1 nmol/L) of the mitogenic response induced by ET-1 in vascular smooth muscle cell culture. In the canine model of delayed cerebral vasospasm, animals received intracisternal vehicle (saline) or (+/-)-SB 209670 (360 +/- 10 micrograms/d) via osmotic minipump for 7 days. On day 7, the cross-sectional areas in the (+/-)-SB 209670 group were significantly greater than those in the vehicle group in both the basilar artery (68% versus 27%) and anterior spinal artery (78% versus 38%). No differences in blood pressure or heart rate were noted in the two groups, and the vasospasm in the vehicle group did not differ from that of historic controls in this model. The results suggest that ET plays a significant role in the development of delayed cerebral vasospasm via an interaction with ETA receptors. Furthermore, ETA receptor antagonists may represent a novel therapeutic approach to the treatment of subarachnoid hemorrhage.

Published

1994

26. A comparison of (+) SK & F 10047 and MK-801 on cortical spreading depression

Author

Robert N. Willette, Charles F. Sauermelch, and Paul G. Lysko

Subjects

Male, medicine.medical_specialty, N-Methylaspartate, Microinjections, Hyperemia, Potassium Chloride, Rats, Sprague-Dawley, Stereotaxic Techniques, Phenazocine, Internal medicine, medicine, Animals, Molecular Biology, ED50, Dose-Response Relationship, Drug, Chemistry, General Neuroscience, Cortical Spreading Depression, Glutamate receptor, Antagonist, Electroencephalography, Rats, Dizocilpine, Dose–response relationship, Endocrinology, Cerebrovascular Circulation, Cortical spreading depression, Injections, Intravenous, Stereotaxic technique, NMDA receptor, Neurology (clinical), Dizocilpine Maleate, Developmental Biology, medicine.drug

Abstract

MK-801 and (+)SKF 10047 produced a dose-related inhibition of the EEG suppression and cortical hyperemia associated with cortical spreading depression (CSD) and reduced the CSD propagation rate; ED50 = 1 mg/kg, i.v. and 15 mg/kg, i.v., respectively. MK-801 had a delayed onset of action (inversely related to dose) and a prolonged duration of action at all doses (2 h). In contrast, (+)SKF 10047 had a rapid onset of action (30 min) and a predictable dose-related duration of action. These results suggests that an efficacious compound acting with moderate affinity as a non-competitive antagonist at the NMDA-receptor channel may possess a preferable time-course and toxicity profile when compared to agents acting similarly, but with high affinity.

Published

1994

27. Albiglutide, a long lasting glucagon-like peptide-1 analog, protects the rat heart against ischemia/reperfusion injury: evidence for improving cardiac metabolic efficiency

Author

John J. Lepore, Weike Bao, David Richard Citerone, Beat M. Jucker, Mark R. Harpel, Matthew Szapacs, Thimmaiah P Chendrimada, Hasan Alsaid, Karpagam Aravindhan, and Robert N. Willette

Subjects

Blood Glucose, Male, Anatomy and Physiology, Transcription, Genetic, medicine.medical_treatment, Myocardial Infarction, lcsh:Medicine, Cardiotonic Agents, Cardiovascular, Biochemistry, Rats, Sprague-Dawley, Endocrinology, Glucagon-Like Peptide 1, Cyclic AMP, Insulin, Myocardial infarction, lcsh:Science, Principal Component Analysis, Multidisciplinary, digestive, oral, and skin physiology, Heart, Animal Models, Glucagon-like peptide-1, Albiglutide, Cardiovascular physiology, Heart Function Tests, Carbohydrate Metabolism, Medicine, hormones, hormone substitutes, and hormone antagonists, Metabolic Networks and Pathways, Research Article, endocrine system, medicine.medical_specialty, Drugs and Devices, Drug Research and Development, Ischemia, Myocardial Reperfusion Injury, Endocrine System, Biology, In Vitro Techniques, Cardiovascular Pharmacology, Model Organisms, Internal medicine, medicine, Animals, Lactic Acid, Diabetic Endocrinology, Endocrine Physiology, Myocardium, Acute Cardiovascular Problems, lcsh:R, Body Weight, Hemodynamics, Feeding Behavior, medicine.disease, Rats, Metabolism, Rat, lcsh:Q, Energy Metabolism, Reperfusion injury

Abstract

BACKGROUND: The cardioprotective effects of glucagon-like peptide-1 (GLP-1) and analogs have been previously reported. We tested the hypothesis that albiglutide, a novel long half-life analog of GLP-1, may protect the heart against I/R injury by increasing carbohydrate utilization and improving cardiac energetic efficiency. METHODS/PRINCIPAL FINDINGS: Sprague-Dawley rats were treated with albiglutide and subjected to 30 min myocardial ischemia followed by 24 h reperfusion. Left ventricle infarct size, hemodynamics, function and energetics were determined. In addition, cardiac glucose disposal, carbohydrate metabolism and metabolic gene expression were assessed. Albiglutide significantly reduced infarct size and concomitantly improved post-ischemic hemodynamics, cardiac function and energetic parameters. Albiglutide markedly increased both in vivo and ex vivo cardiac glucose uptake while reducing lactate efflux. Analysis of metabolic substrate utilization directly in the heart showed that albiglutide increased the relative carbohydrate versus fat oxidation which in part was due to an increase in both glucose and lactate oxidation. Metabolic gene expression analysis indicated upregulation of key glucose metabolism genes in the non-ischemic myocardium by albiglutide. CONCLUSION/SIGNIFICANCE: Albiglutide reduced myocardial infarct size and improved cardiac function and energetics following myocardial I/R injury. The observed benefits were associated with enhanced myocardial glucose uptake and a shift toward a more energetically favorable substrate metabolism by increasing both glucose and lactate oxidation. These findings suggest that albiglutide may have direct therapeutic potential for improving cardiac energetics and function.

Published

2011

28. Sodium and water homeostasis is maintained in rats with chronic TRPV4 blockade

Author

Roberta E. Bernard, Mui Cheung, Theresa J. Roethke, Melissa H. Costell, Kevin S. Thorneloe, Robert N. Willette, Gerald P. McCafferty, Christine G. Schnackenberg, and Larry J. Jolivette

Subjects

TRPV4, medicine.medical_specialty, Chemistry, Sodium, chemistry.chemical_element, Biochemistry, Blockade, Endocrinology, Internal medicine, Genetics, medicine, Molecular Biology, Homeostasis, Biotechnology

Published

2011

29. Inhibition of p38 mitogen-activated protein kinase improves nitric oxide-mediated vasodilatation and reduces inflammation in hypercholesterolemia

Author

Sharon M.L. Wallace, Zixing Fang, John J. Lepore, John R. Cockcroft, Joseph Cheriyan, Dennis L. Sprecher, Robert N. Willette, Andrew J. Webb, Lea Sarov-Blat, Ian B. Wilkinson, David Collier, Maysoon Elkhawad, John M. Morgan, and Kaisa M. Mäki-Petäjä

Subjects

Nitroprusside, MAPK/ERK pathway, medicine.medical_specialty, RM, Vasodilator Agents, Hypercholesterolemia, Inflammation, Vasodilation, Nitric Oxide, p38 Mitogen-Activated Protein Kinases, Nitric oxide, chemistry.chemical_compound, Physiology (medical), Internal medicine, medicine, Humans, Infusions, Intra-Arterial, Protein kinase A, Protein Kinase Inhibitors, omega-N-Methylarginine, Losmapimod, business.industry, Acetylcholine, Plethysmography, Forearm, Endocrinology, chemistry, Sodium nitroprusside, medicine.symptom, Cardiology and Cardiovascular Medicine, business, medicine.drug, Lipoprotein, RC

Abstract

Background— Oxidized low-density lipoprotein reduces endothelial nitric oxide production (an important mediator of vasoregulation) and activates p38 mitogen-activated protein kinase (MAPK), a mediator of vascular inflammation. Animal models of vascular stress have previously predicted improvements in vascular function after p38 MAPK inhibition. We hypothesized that a selective p38α/β MAPK inhibitor (losmapimod; GW856553) would improve compromised nitric oxide–mediated vasoregulation in patients with hypercholesterolemia. Methods and Results— Untreated hypercholesterolemic patients (low-density lipoprotein cholesterol >4.1 mmol/L) were randomized to receive losmapimod 7.5 mg (n=27) or placebo (n=29) twice daily for 28 days. Patients with known vascular disorders (eg, diabetes mellitus, coronary heart disease) were excluded. Forearm blood flow was measured by venous occlusion plethysmography in response to serial intra-arterial infusion of acetylcholine, sodium nitroprusside, and N G -monomethyl- l -arginine (L-NMMA). Acetylcholine and L-NMMA responses were significantly impaired ( P =0.01 and P =0.03) compared with responses in control subjects (n=12). In hypercholesterolemic patients treated with losmapimod, responses to acetylcholine were improved by 25% (95% confidence interval, 5 to 48; P =0.01), to sodium nitroprusside by 20% (95% confidence interval, 3 to 40; P =0.02), and to L-NMMA by 10% (95% confidence interval, −1 to 23; P =0.07) compared with placebo. C-reactive protein was reduced by 57% (95% confidence interval, −81 to −6%; P Conclusions— Losmapimod improves nitric oxide–mediated vasodilatation in hypercholesterolemic patients, which is consistent with findings in previous translational animal models. These data support the hypothesis that attenuating the inflammatory milieu by inhibiting p38 MAPK activity improves NO activity. This suggests p38 MAPK as a novel target for patients with cardiovascular disease. Clinical Trial Registration— URL: http://clinicaltrials.gov . Unique identifier: NCT00474864.

Published

2011

30. The Novel Soluble Guanylate Cyclase Activator PPCA Reverses Acute Hypoxia‐induced Pulmonary Hypertension in Dogs

Author

Christine G. Schnackenberg, Tao Wang, Gerald P. McCefferty, Beat M. Jucker, Robert N. Willette, and David J. Behm

Subjects

medicine.medical_specialty, business.industry, Activator (genetics), GUCY1A3, Guanylate cyclase 2C, medicine.disease, Biochemistry, Pulmonary hypertension, Acute hypoxia, Endocrinology, Internal medicine, Genetics, Medicine, business, Molecular Biology, Biotechnology, Guanylate cyclase

Published

2010

31. Systemic activation of the transient receptor potential vanilloid subtype 4 channel causes endothelial failure and circulatory collapse: Part 2

Author

Robert N. Willette, Sandhya S. Nerurkar, Cindy E. Fishman, Gregory H. Turner, Kevin S. Thorneloe, Weike Bao, Gerald Stankus, Robert W. Marquis, Tian-Li Yue, David J. Figueroa, David J. Behm, Robert E. Lee Trout, Bartholomew J. Votta, Xiaoping Xu, Anthony Sulpizio, Erin S. R. Lashinger, Heath Thomas, Chris P. Doe, Linda N. Casillas, Zuojun Lin, Irina M. Lozinskaya, Sandra J. Hoffman, Haisong Ju, and Min Lin

Subjects

TRPV4, Male, medicine.medical_specialty, Circulatory collapse, Patch-Clamp Techniques, Endothelium, TRPV Cation Channels, Vascular permeability, Aorta, Thoracic, Endothelial NOS, Ventricular Function, Left, Cell Line, Endothelial activation, Capillary Permeability, Rats, Sprague-Dawley, Transient receptor potential channel, Mice, Dogs, Enos, Leucine, Internal medicine, medicine, Cell Adhesion, Animals, Humans, Pharmacology, Mice, Knockout, Sulfonamides, biology, Dose-Response Relationship, Drug, Molecular Structure, Hemodynamics, biology.organism_classification, medicine.disease, Immunohistochemistry, Rats, Endocrinology, medicine.anatomical_structure, Vasoconstriction, Anesthesia, Molecular Medicine, Female, Endothelium, Vascular

Abstract

The transient receptor potential (TRP) vanilloid subtype 4 (V4) is a nonselective cation channel that exhibits polymodal activation and is expressed in the endothelium, where it contributes to intracellular Ca2+ homeostasis and regulation of cell volume. The purpose of the present study was to evaluate the systemic cardiovascular effects of GSK1016790A, a novel TRPV4 activator, and to examine its mechanism of action. In three species (mouse, rat, and dog), the i.v. administration of GSK1016790A induced a dose-dependent reduction in blood pressure, followed by profound circulatory collapse. In contrast, GSK1016790A had no acute cardiovascular effects in the TRPV4-/- null mouse. Hemodynamic analyses in the dog and rat demonstrate a profound reduction in cardiac output. However, GSK1016790A had no effect on rate or contractility in the isolated, buffer-perfused rat heart, and it produced potent endothelial-dependent relaxation of rodent-isolated vascular ring segments that were abolished by nitric-oxide synthase (NOS) inhibition (N-nitro-L-arginine methyl ester; L-NAME), ruthenium red, and endothelial NOS (eNOS) gene deletion. However, the in vivo circulatory collapse was not altered by NOS inhibition (L-NAME) or eNOS gene deletion but was associated with (concentration and time appropriate) profound vascular leakage and tissue hemorrhage in the lung, intestine, and kidney. TRPV4 immunoreactivity was localized in the endothelium and epithelium in the affected organs. GSK1016790A potently induced rapid electrophysiological and morphological changes (retraction/condensation) in cultured endothelial cells. In summary, inappropriate activation of TRPV4 produces acute circulatory collapse associated with endothelial activation/injury and failure of the pulmonary microvascular permeability barrier. It will be important to determine the role of TRPV4 in disorders associated with edema and microvascular congestion.

Published

2008

32. Chronic inhibition of 11beta‐hydroxysteroid dehydrogenase activity reduces cardiovascular comorbidities in corpulent and stroke‐prone SHR

Author

Jianqi Cui, Chris P. Doe, Robert N. Willette, Marianne E. Eybye, Ross G. Bentley, Christine G. Schnackenberg, Kristeen Maniscalco, Tian-Li Yue, and Melissa H. Costell

Subjects

medicine.medical_specialty, 11beta hydroxysteroid dehydrogenase, Endocrinology, business.industry, Internal medicine, Genetics, medicine, medicine.disease, business, Molecular Biology, Biochemistry, Stroke, Biotechnology

Published

2008

33. Serum and glucocorticoid‐regulated kinase mediates hypertension and end organ damage in DOCA‐salt hypertension

Author

Christine G. Schnackenberg, Graham Duddy, Robert N. Willette, Bao Hoang, and Melissa H. Costell

Subjects

medicine.medical_specialty, business.industry, End organ damage, Kinase, Doca salt, medicine.disease, Biochemistry, Endocrinology, Internal medicine, Pathophysiology of hypertension, Genetics, medicine, business, Molecular Biology, Glucocorticoid, Biotechnology, medicine.drug

Published

2008

34. In vivo activation of peroxisome proliferator-activated receptor-delta protects the heart from ischemia/reperfusion injury in Zucker fatty rats

Author

Beat M. Jucker, Weike Bao, Eliot H. Ohlstein, Tian-Li Yue, Lea Sarov-Blat, Klaudia Steplewski, Sandhya S. Nerurkar, and Robert N. Willette

Subjects

Male, medicine.medical_specialty, Cardiotonic Agents, Ischemia, Peroxisome proliferator-activated receptor, Blood Pressure, Myocardial Reperfusion Injury, Biology, GW0742, Internal medicine, medicine, Animals, PPAR delta, RNA, Messenger, Receptor, Beta oxidation, Pharmacology, chemistry.chemical_classification, Cardioprotection, Metabolic Syndrome, Fatty Acids, Troponin I, Heart, Ketones, medicine.disease, Rats, Rats, Zucker, Disease Models, Animal, Thiazoles, Endocrinology, chemistry, Lipotoxicity, Molecular Medicine, Cytokines, Reperfusion injury, Proto-Oncogene Proteins c-akt

Abstract

Peroxisome proliferator-activated receptor (PPAR)-delta is a transcription factor that belongs to the PPAR family. PPAR-delta is abundantly expressed in the heart, and its role in the heart is largely unknown. We tested whether pharmacological activation of PPAR-delta protects the heart from ischemia/reperfusion (I/R) injury in male Zucker fatty rats, a rodent model of obesity and dyslipidemia. A highly selective PPAR-delta agonist, [4-[[[2-[3-fluoro-4-(trifluoromethyl)phenyl]-4-methyl-5-thiazolyl]methyl] thio]-2-methylphenoxy]acetic acid (GW0742), was administered for 7 days at 10 mg/kg/day (p.o., once a day). Ischemic injury was produced by occlusion of the left anterior descending artery for 30 min followed by reperfusion for up to 24 h. Treatment with GW0742 reduced serum levels of cardiac troponin-I and infarct size by 63% (p < 0.01) and 32% (p < 0.01), respectively, and improved left ventricular function. Treatment with GW0742 up-regulated gene expression involved in cardiac fatty acid oxidation, increased fat use in the heart, and reduced serum levels of free fatty acids. The enhanced cardiac expression of interleukin (IL)-6, IL-8, intercellular adhesion molecule-1, and monocyte chemoattractant protein-1 induced by I/R were significantly attenuated by GW0742. Treatment with GW0742 also reduced apoptotic cardiomyocytes by 34% and cardiac caspase-3 activity by 61% (both p < 0.01 versus vehicle). GW0742 differentially regulated Bcl family members, favoring cell survival, and attenuated I/R-induced cardiac mitochondrial damage. In addition, GW0742 treatment augmented the cardiac Akt signaling pathway, as reflected by enhanced phospho-3-phosphoinositide-dependent kinase-1 and p-Akt. The results indicate that activation of PPAR-delta protected the heart from I/R injury in Zucker fatty rats, and multiple mechanisms including amelioration of lipotoxicity, anti-inflammation, and up-regulation of prosurvival signaling contribute together to the cardioprotection.

Published

2008

35. Vasodilation induced by endothelin: role of EDRF and prostanoids in rat hindquarters

Author

C F Sauermelch, Eliot H. Ohlstein, L. Vickery, and Robert N. Willette

Subjects

Male, medicine.medical_specialty, Physiology, Vasodilator Agents, Hemodynamics, Vasodilation, Buffers, In Vitro Techniques, Nitric Oxide, Methoxamine, chemistry.chemical_compound, Physiology (medical), Internal medicine, medicine, Animals, Anesthesia, Skin, Chemistry, Endothelins, Microcirculation, Muscles, Endothelium-derived relaxing factor, Rats, Inbred Strains, Hindlimb, Rats, Perfusion, Endocrinology, medicine.anatomical_structure, Regional Blood Flow, Circulatory system, Prostaglandins, Cardiology and Cardiovascular Medicine, Endothelin receptor, Blood vessel, medicine.drug

Abstract

Hemodynamic responses to endothelin (ET-1) were studied in hindquarters of anesthetized rats and also in isolated buffer-perfused hindquarters of pithed rats. ET-1 (10-100 pmol ia) produced brief dose-related increases in hindquarter blood flow. Acetylcholine (ACh. 0.3-1 micrograms ia) produced similar vasodilator responses. Hemodynamic responses elicited by either ET-1 or ACh were not significantly altered by pretreatment with indomethacin. ET-1 produced dose-dependent increases in skeletal muscle microvascular perfusion, whereas ET-1 had no effect on cutaneous microvascular perfusion, suggesting that vasodilation in the skeletal muscle of the hindlimb contributes to the increase in hindquarter blood flow induced by ET-1. Hemodynamic effects of ET-1 and ACh were studied in the isolated in situ buffer-perfused hindquarters of pithed rats. ET-1 (0.01-300 pmol ia) produced only dose-dependent increases in hindquarter perfusion pressure under basal conditions or when the vascular preparation was precontracted with methoxamine. ET-1 induced vasorelaxation was not observed. ACh (3 microgram ia) produced a 64% reduction in hindquarter perfusion pressure; indicative of endothelium-dependent relaxation. ET-3 (0.1-300 pmol) produced only dose-dependent increases in hindquarter perfusion pressure. When hemodynamic effects of ET-1 were studied under conditions of constant pressure, results were similar to those obtained under constant flow. This study demonstrates that in the rat hindquarters endothelium-derived relaxing factors and prostanoids do not appear to be mediators of endothelin-induced vasodilation.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1990

36. PPARdelta activation normalizes cardiac substrate metabolism and reduces right ventricular hypertrophy in congestive heart failure

Author

Stephen C. Lenhard, Christopher P. Doe, Melissa H. Costell, Lea Sarov-Blat, Tom C.-C. Hu, Beat M. Jucker, Robert N. Willette, Klaudia Steplewski, Kristeen Maniscalco, Carolyn Williams, Alan R. Olzinski, Christine G. Schnackenberg, and Roberta E. Bernard

Subjects

Cardiac function curve, Male, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Myocardial Infarction, Gene Expression, Pulmonary Edema, Biology, Ventricular Function, Left, Muscle hypertrophy, Rats, Sprague-Dawley, Right ventricular hypertrophy, Internal medicine, medicine, Animals, PPAR delta, Pharmacology, Heart Failure, Ejection fraction, Dose-Response Relationship, Drug, Hypertrophy, Right Ventricular, Reverse Transcriptase Polymerase Chain Reaction, Biological Transport, medicine.disease, Lipids, Diuresis, Rats, Endocrinology, medicine.anatomical_structure, Lipotoxicity, Ventricle, Heart failure, Cardiology, Myocardial infarction complications, Cardiology and Cardiovascular Medicine, Energy Metabolism, Oxidation-Reduction

Abstract

Previously, it was shown that selective deletion of peroxisome proliferator activated receptor delta (PPARdelta) in the heart resulted in a cardiac lipotoxicity, hypertrophy, and heart failure. The aim of the present study was to determine the effects of chronic and selective pharmacological activation of PPARdelta in a model of congestive heart failure. PPARdelta-specific agonist treatment (GW610742X at 30 and 100 mg/kg/day for 6-9 weeks) was initiated immediately postmyocardial infarction (MI) in Sprague-Dawley rats. Magnetic resonance imaging/spectroscopy was used to assess cardiac function and energetics. A 1-(13)C glucose clamp was performed to assess relative cardiac carbohydrate versus fat oxidation. Additionally, cardiac hemodynamics and reverse-transcription polymerase chain reaction gene expression analysis was performed. MI rats had significantly reduced left ventricle (LV) ejection fractions and whole heart phosphocreatine/adenosine triphosphate ratio compared with Sham animals (reduction of 43% and 14%, respectively). However, GW610742X treatment had no effect on either parameter. In contrast, the decrease in relative fat oxidation rate observed in both LV and right ventricle (RV) following MI (decrease of 58% and 54%, respectively) was normalized in a dose-dependent manner following treatment with GW610742X. These metabolic changes were associated with an increase in lipid transport/metabolism target gene expression (eg, CD36, CPT1, UCP3). Although there was no difference between groups in LV weight or infarct size measured upon necropsy, there was a dramatic reduction in RV hypertrophy and lung congestion (decrease of 22-48%, P0.01) with treatment which was associated with a7-fold decrease (P0.05) in aterial natriuretic peptide gene expression in RV. Diuretic effects were not observed with GW610742X. In conclusion, chronic treatment with a selective PPARdelta agonist normalizes cardiac substrate metabolism and reduces RV hypertrophy and pulmonary congestion consistent with improvement in congestive heart failure.

Published

2007

37. Effects of p38 MAPK Inhibitor on angiotensin II-dependent hypertension, organ damage, and superoxide anion production

Author

Zhaohui Ao, Douglas G. Johns, Sandhya S. Nerurkar, Tina N Woods, Stephen A. Douglas, Robert N. Willette, Robert W. Coatney, Weike Bao, Rosanna C. Mirabile, Tian-Li Yue, Christopher P. Doe, Ross G. Bentley, David J. Behm, and Jason F Ohlstein

Subjects

Male, medicine.medical_specialty, Endothelium, p38 mitogen-activated protein kinases, Blood Pressure, Protein Serine-Threonine Kinases, p38 Mitogen-Activated Protein Kinases, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Superoxides, Internal medicine, medicine, Animals, Aorta, Abdominal, Endothelial dysfunction, Enzyme Inhibitors, Pharmacology, chemistry.chemical_classification, Mice, Knockout, Reactive oxygen species, NADPH oxidase, Membrane Glycoproteins, biology, Ventricular Remodeling, Superoxide, Angiotensin II, Myocardium, Imidazoles, Intracellular Signaling Peptides and Proteins, NADPH Oxidases, medicine.disease, Rats, Vasodilation, medicine.anatomical_structure, Endocrinology, Carotid Arteries, Pyrimidines, chemistry, Echocardiography, Knockout mouse, Hypertension, NADPH Oxidase 2, cardiovascular system, biology.protein, Endothelium, Vascular, Cardiology and Cardiovascular Medicine, Protein Kinases

Abstract

Angiotensin II (Ang II) activates p38 mitogen-activated protein kinase (p38 MAPK) and increases reactive oxygen species (ROS), but the nature of the relationship in vivo is not fully understood. We assess the effect of SB239063AN, a highly selective, orally active, p38 MAPK inhibitor, on Ang II-dependent hypertension, target-organ damage and ROS production. Sprague-Dawley rats and MAPKAP kinase-2 knockout mice were infused with Ang II. Ang II infusion increased the levels of phosphorylated p38 MAPK in the heart and aorta. Production of superoxide anion and expression of NAD(P)H oxidase subunit gp91 in the aorta were increased 4- and 5-fold, respectively. In addition, Ang II infusion led to endothelial dysfunction, progressive and sustained hypertension, and cardiac hypertrophy. Treatment with SB239063AN (800 ppm in the diet) significantly attenuated the levels of phosphorylated p38 MAPK in the heart and aorta, reduced superoxide anion generation by 57% (P < 0.01), markedly suppressed gp91 mRNA expression, prevented endothelial dysfunction, and blunted both the hypertension and cardiac hypertrophy. Ang II-dependent hypertension was also significantly attenuated in MAPKAP kinase-2 knockout mice. The results suggest that Ang II induced hypertension, organ damage, and ROS production are possibly mediated by p38 MAPK and inhibition of p38 MAPK may offer a therapeutic approach for cardiovascular disease.

Published

2007

38. Cardioprotection Resulting from Glucagon-Like Peptide-1 Administration Involves Shifting Metabolic Substrate Utilization to Increase Energy Efficiency in the Rat Heart

Author

Mark R. Harpel, Weike Bao, Karpagam Aravindhan, Robert N. Willette, John J. Lepore, and Beat M. Jucker

Subjects

medicine.medical_specialty, Cardiotonic Agents, Magnetic Resonance Spectroscopy, Glucose uptake, Ischemia, lcsh:Medicine, Biology, Carbohydrate metabolism, chemistry.chemical_compound, Oxygen Consumption, Glucagon-Like Peptide 1, Internal medicine, Cyclic AMP, medicine, Animals, Myocytes, Cardiac, lcsh:Science, Cardioprotection, Carbon Isotopes, Multidisciplinary, Fatty acid metabolism, Glycogen, Myocardium, lcsh:R, Fatty Acids, Hydrogen-Ion Concentration, medicine.disease, Rats, Glucose, Endocrinology, chemistry, Anaerobic glycolysis, Reperfusion Injury, lcsh:Q, Energy Metabolism, Reperfusion injury, Research Article

Abstract

Previous studies have shown that glucagon-like peptide-1 (GLP-1) provides cardiovascular benefits independent of its role on peripheral glycemic control. However, the precise mechanism(s) by which GLP-1 treatment renders cardioprotection during myocardial ischemia remain unresolved. Here we examined the role for GLP-1 treatment on glucose and fatty acid metabolism in normal and ischemic rat hearts following a 30 min ischemia and 24 h reperfusion injury, and in isolated cardiomyocytes (CM). Relative carbohydrate and fat oxidation levels were measured in both normal and ischemic hearts using a 1-13C glucose clamp coupled with NMR-based isotopomer analysis, as well as in adult rat CMs by monitoring pH and O2 consumption in the presence of glucose or palmitate. In normal heart, GLP-1 increased glucose uptake (↑64%, p

Published

2015

39. Carvedilol prevents and reverses hypertrophy-induced cardiac dysfunction

Author

David P. Brooks, Allen H. Nelson, Robert W. Coatney, Frank C. Barone, Robert N. Willette, and Eliot H. Ohlstein

Subjects

Male, medicine.medical_specialty, Cardiac output, Vasodilator Agents, Adrenergic beta-Antagonists, Cardiomyopathy, Carbazoles, Administration, Oral, Cardiomegaly, Rats, Inbred WKY, Antioxidants, Muscle hypertrophy, Propanolamines, Internal medicine, Rats, Inbred SHR, medicine, Animals, Carvedilol, Ultrasonography, Pharmacology, Ejection fraction, Dose-Response Relationship, Drug, Ventricular Remodeling, business.industry, food and beverages, General Medicine, Stroke volume, medicine.disease, Diet, Rats, Disease Models, Animal, Endocrinology, Treatment Outcome, Heart failure, Cardiac hypertrophy, Cardiology, business, medicine.drug

Abstract

Background/Aims: Histological studies have provided evidence that carvedilol can prevent cardiac hypertrophy in spontaneously hypertensive-stroke prone rats (SP) fed a high-fat and -salt diet. However, the effects of carvedilol on cardiac function have not been studied in these animals. In addition, the ability of carvedilol to reverse established cardiac hypertrophy and dysfunction under these conditions remains to be determined. Here we have evaluated the ability of carvedilol to prevent and reverse cardiac hypertrophy and progressive dysfunction using echocardiography. Methods: Two echocardiology studies were conducted to determine the effects of carvedilol treatment on cardiac hypertrophy and dysfunction. In the first prevention study, four groups of rats were evaluated. SP were fed a high-fat (24.5% in food) and high-salt (1% in water) diet (SFD) without (SP-SFD control group) or with carvedilol (SP-SFD carvedilol group; carvedilol concentration 2,400 parts per million) for 18 weeks. Carvedilol was administered in the food at an optimum concentration (i.e. known to provide clinically relevant blood concentrations and reduce cardiac hypertrophy determined from previous studies). In addition, SP and WKY rats were fed a normal diet (SP normal diet group and WKY normal diet group). These groups are known to not develop the same significant cardiac hypertrophy and dysfunction within this limited time of study, and provided two more normal control groups for comparison. In the second reversal study, one group of SP was fed SFD for 12 weeks (SP-SFD pretreatment period) to induce cardiac hypertrophy. Carvedilol (2,400 parts per million) was then added to the diet for an additional 6 weeks (SP-SFD carvedilol treatment period). Results: In the first prevention study, carvedilol prolonged longevity (p < 0.05) and prevented left-ventricular hypertrophy and dysfunction (p < 0.05; SP-SFD control vs. SP-SFD carvedilol group). M-mode-measured and -calculated parameters demonstrated that carvedilol treatment in the SP-SFD carvedilol group prevented increases in left-ventricular wall thickness (p < 0.05) and decreases in diastolic chamber diameter and volume, stroke volume, ejection fraction and cardiac output (all p < 0.05) that occurred in the SP-SFD control group. Further, cardiac measurements in the SP-SFD carvedilol group were normalized to levels similar to those in the SP and WKY normal diet groups. All SFD-fed groups exhibited similar, significantly elevated blood pressure during the study. In the second reversal study, carvedilol treatment for 6 weeks reversed the cardiac hypertrophy and dysfunction that developed in SP-fed SFD for 12 weeks prior to carvedilol intervention. Under these conditions, carvedilol improved/normalized left-ventricular wall thickness, diastolic ventricular-chamber diameter and volume, stroke volume, ejection fraction and cardiac output (all p < 0.05). Conclusions: These data indicate that carvedilol provides protection from and facilitates reversal of progressive cardiac remodeling and dysfunction in this SP-SFD model of cardiac hypertrophy/heart failure. Since these effects occurred in the absence of effects on blood pressure, other known actions of carvedilol, especially its antioxidant activity, for example, may explain this significant cardiac protection. In addition, research using this SP-SFD model of cardiac hypertrophy/end-organ injury appears to translate well to human cardiovascular disease.

Published

2006

40. Assessing the effects of LXR agonists on cellular cholesterol handling: a stable isotope tracer study

Author

Avijit Ghosh, Robert N. Willette, Karpagam Aravindhan, Christine L. Webb, N. John DiNardo, Michael Jaye, and Beat M. Jucker

Subjects

medicine.medical_specialty, HepG2, Benzylamines, Hydrocarbons, Fluorinated, Gene Expression, Receptors, Cytoplasmic and Nuclear, QD415-436, Cholesterol 7 alpha-hydroxylase, Biochemistry, Benzoates, Models, Biological, Culture Media, Serum-Free, chemistry.chemical_compound, mass isotopomer distribution analysis, Endocrinology, Internal medicine, Cell Line, Tumor, medicine, Humans, Protein Isoforms, Liver X receptor, Liver X Receptors, Carbon Isotopes, Sulfonamides, biology, Cholesterol, Catabolism, turnover, compartmental, Cell Biology, Orphan Nuclear Receptors, DNA-Binding Proteins, Kinetics, chemistry, ABCG1, Liver, ABCA1, HMG-CoA reductase, biology.protein, lipids (amino acids, peptides, and proteins), Efflux, Cholesterol Esters, liver X receptor

Abstract

The liver X receptors (LXRs) alpha and beta are responsible for the transcriptional regulation of a number of genes involved in cholesterol efflux from cells and therefore may be molecular targets for the treatment of cardiovascular disease. However, the effects of LXR ligands on cholesterol turnover in cells has not been examined comprehensively. In this study, cellular cholesterol handling (e.g., synthesis, catabolism, influx, and efflux) was examined using a stable isotope labeling study and a two-compartment modeling scheme. In HepG2 cells, the incorporation of 13C into cholesterol from [1-13C]acetate was analyzed by mass isotopomer distribution analysis in conjunction with nonsteady state, multicompartment kinetic analysis to calculate the cholesterol fluxes. Incubation with synthetic, nonsteroidal LXR agonists (GW3965, T0901317, and SB742881) increased cholesterol synthesis (approximately 10-fold), decreased cellular cholesterol influx (71-82%), and increased cellular cholesterol efflux (1.7- to 1.9-fold) by 96 h. As a consequence of these altered cholesterol fluxes, cellular cholesterol decreased (36-39%) by 96 h. The increased cellular cholesterol turnover was associated with increased expression of the LXR-activated genes ABCA1, ABCG1, FAS, and sterol-regulatory element binding protein 1c. In summary, the mathematical model presented allows time-dependent calculations of cellular cholesterol fluxes. These data demonstrate that all of the cellular cholesterol fluxes were altered by LXR activation and that the increase in cholesterol synthesis did not compensate for the increased cellular cholesterol efflux, resulting in a net cellular cholesterol loss.

Published

2006

41. Eprosartan improves cardiac performance, reduces cardiac hypertrophy and mortality and downregulates myocardial monocyte chemoattractant protein-1 and inflammation in hypertensive heart disease

Author

Jonathan Sackner-Bernstein, Frank C. Barone, Marinela Berova, Thomas M. Behr, Robert N. Willette, Christiane E. Angermann, Karen M. Anderson, and Robert W. Coatney

Subjects

Vasculitis, medicine.medical_specialty, Heart disease, Normal diet, Physiology, Down-Regulation, Thiophenes, Article, Muscle hypertrophy, Internal medicine, Rats, Inbred SHR, Internal Medicine, medicine, Animals, RNA, Messenger, Antihypertensive Agents, Chemokine CCL2, Ultrasonography, business.industry, Angiotensin II, Macrophages, Myocardium, Hypertrophic cardiomyopathy, Imidazoles, Eprosartan, medicine.disease, Immunohistochemistry, Myocardial Contraction, Hypertensive heart disease, Rats, Endocrinology, Acrylates, Heart failure, Hypertension, Hypertrophy, Left Ventricular, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Objective The purpose of this investigation was to determine whether angiotensin II receptor (AII1 R) antagonism interferes with cardiac monocyte chemoattractant protein-1 (MCP-1) expression in hypertrophic cardiomyopathy and failure. Design We studied the effects of the AII1 R antagonist eprosartan on MCP-1 expression, and on the recruitment of macrophages into the myocardium in a model of cardiac hypertrophy and morbidity/mortality. Methods Stroke-prone spontaneously hypertensive rats fed a high-salt, high-fat diet (SFD) developed heart failure characterized by left ventricular (LV) hypertrophy/ pathology and hypocontractility. These rats received either normal diet, SFD, or SFD with the daily administration of 30 mg/kg eprosartan for 28 weeks. LV function and wall thickness was assessed by echocardiography, MCP-1 expression was measured by TaqMan real-time polymerase chain reaction, enzyme-linked immunosorbent assay and immunohistochemistry, and macrophage infiltration into the LV was determined by microscopy. Results Eprosartan reduced the rate of morbidity/ mortality (P = 0.001), LV MCP-1 mRNA (P < 0.05) and protein expression (P< 0.01), and LV macrophage infiltration (P< 0.01), while preserving ventricular function (P< 0.05). Eprosartan also produced a moderate (16%; P< 0.05) decrease in blood pressure. Conclusions These data demonstrate that AII1R antagonism in an animal model of hypertensive heart disease reduces MCP-1 expression in the myocardium that results in reduced macrophage recruitment. These effects parallel the preservation of LV systolic function and the reduction in cardiac remodeling/disease progression and reduced morbidity/mortality. Suppression of MCP-1 expression might explain in part the beneficial effects of AII1R antagonism in this model.

Published

2004

42. Antioxidative, antinitrative, and vasculoprotective effects of a peroxisome proliferator-activated receptor-gamma agonist in hypercholesterolemia

Author

Robert N. Willette, Bernard L. Lopez, Huirong Liu, Zhi-Ping Teng, Eliot H. Ohlstein, Tian-Li Yue, Erhe Gao, Xin-Liang Ma, Ines Batinic-Haberle, Ling Tao, and Theodore A. Christopher

Subjects

Agonist, Male, medicine.medical_specialty, Endothelium, medicine.drug_class, Hypercholesterolemia, Peroxisome proliferator-activated receptor, Receptors, Cytoplasmic and Nuclear, Inflammation, Vasodilation, In Vitro Techniques, Nitric Oxide, Antioxidants, Nitric oxide, Rosiglitazone, chemistry.chemical_compound, Physiology (medical), Internal medicine, medicine, Cyclic GMP-Dependent Protein Kinases, Animals, Receptor, Cyclic GMP, Nitrites, chemistry.chemical_classification, Nitrates, business.industry, Lipids, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Carotid Arteries, chemistry, Blood Vessels, Tyrosine, Thiazolidinediones, Rabbits, medicine.symptom, Cardiology and Cardiovascular Medicine, business, medicine.drug, Signal Transduction, Transcription Factors

Abstract

Background— Peroxisome proliferator–activated receptor (PPAR) signaling pathways have been reported to exert anti-inflammatory effects and attenuate atherosclerosis formation. However, the mechanisms responsible for their anti-inflammatory and antiatherosclerotic effects remain largely unknown. The present study tested the hypothesis that a PPARγ agonist may exert significant endothelial protection by antioxidative and antinitrative effects. Methods and Results— Male New Zealand White rabbits were randomized to receive a normal (control) or a high-cholesterol diet and treated with vehicle or rosiglitazone (a PPARγ agonist) 3 mg · kg −1 · d −1 for 5 weeks beginning 3 weeks after the high-cholesterol diet. At the end of 8 weeks of a high-cholesterol diet, the rabbits were killed, and the carotid arteries were isolated. Bioactive nitric oxide was determined functionally (endothelium-dependent vasodilatation) and biochemically (the phosphorylation of vasodilator-stimulated phosphoprotein, or P-VASP). Vascular superoxide production, PPARγ, gp91 phox , and inducible nitric oxide synthase (iNOS) expression, and vascular ONOO − formation were determined. Hypercholesterolemia caused severe endothelial dysfunction and reduced P-VASP, despite a marked increase in iNOS expression and total NO x production. Treatment with rosiglitazone enhanced PPARγ expression, improved endothelium-dependent vasodilatation, preserved P-VASP, suppressed gp91 phox and iNOS expression, reduced superoxide and total NO x production, and inhibited nitrotyrosine formation. Conclusions— The PPARγ agonist rosiglitazone exerted a significant vascular protective effect in hypercholesterolemic rabbits, most likely by attenuation of oxidative and nitrative stresses. The endothelial protective effects of PPARγ agonists may reduce leukocyte accumulation in vascular walls and contribute to their antiatherosclerotic effect.

Published

2003

43. Effect of human urotensin-II infusion on hemodynamics and cardiac function

Author

Fu Hu, Ghada S Hassan, Fazila Chouiali, Adel Giaid, Stephen A. Douglas, Eliot H. Ohlstein, Zhaohui Ao, Robert N. Willette, and Takashi Saito

Subjects

Cardiac function curve, Mean arterial pressure, medicine.medical_specialty, Physiology, Urotensins, Hemodynamics, Blood Pressure, Ventricular Function, Left, Contractility, Physiology (medical), Internal medicine, Heart rate, Medicine, Animals, Humans, Infusion Pumps, Pharmacology, Dose-Response Relationship, Drug, business.industry, General Medicine, medicine.disease, Myocardial Contraction, Rats, Endocrinology, Blood pressure, Heart failure, Circulatory system, Injections, Intravenous, business

Abstract

Recent studies have shown that the vasoactive peptide urotensin-II (U-II) exerts a wide range of action on the cardiovascular system of various species. In the present study, we determined the in vivo effects of U-II on basal hemodynamics and cardiac function in the anesthetized intact rat. Intravenous bolus injection of human U-II resulted in a dose-dependent decrease in mean arterial pressure and left ventricular systolic pressure. Cardiac contractility represented by ±dP/dt was decreased after injection of U-II. However, there was no significant change in heart rate or diastolic pressure. The present study suggests that upregulation of myocardial U-II may contribute to impaired myocardial function in disease conditions such as congestive heart failure.Key words: urotensin-II, rat, infusion, heart.

Published

2003

44. Enrasentan improves survival, limits left ventricular remodeling, and preserves myocardial performance in hypertensive cardiac hypertrophy and dysfunction

Author

Alan R. Olzinski, Nambi Aiyar, Robert N. Willette, Allen H. Nelson, Robert W. Coatney, Eliot H. Ohlstein, Karen M. Anderson, Tina N Woods, and Frank C. Barone

Subjects

Endothelin Receptor Antagonists, Male, medicine.medical_specialty, Heart disease, Cardiac index, Carboxylic Acids, Blood Pressure, Muscle hypertrophy, Heart Rate, Internal medicine, Rats, Inbred SHR, Heart rate, Medicine, Animals, Protein Precursors, Ventricular remodeling, Aldosterone, Pharmacology, Ventricular Remodeling, business.industry, Myocardium, medicine.disease, Rats, Survival Rate, Endocrinology, Blood pressure, Heart failure, Hypertension, Indans, Cardiology, Hypertrophy, Left Ventricular, Cardiology and Cardiovascular Medicine, business, Endothelin receptor, Atrial Natriuretic Factor

Abstract

Summary: Evidence suggests that endothelin receptor antagonists may have therapeutic potential for the chronic treatment of heart failure. In the current study, the effects of an orally active mixed endothelin-A/endothelin-B (ET A /ET B ) receptor antagonist (enrasentan) were assessed in a model of cardiac hypertrophy and dysfunction (spontaneously hypertensive stroke prone rats) maintained on a high-salt/high-fat diet. Echocardiography was used to quantify cardiac performance and left ventricular dimensions. Enrasentan (1,200 and 2,400 parts per million in the high-salt/high-fat diet) had no significant effects on body weight and systolic blood pressure. However, increases in heart rate were not observed in the enrasentan-treated groups at 12 weeks (p < 0.05). Enrasentan-treated groups exhibited significantly improved survival (90–95% vs. 30% [control rats] at 18 weeks; p < 0.001). Enrasentan treatments also increased stroke volume (at 8, 12, and 16 weeks) and cardiac index (at 8 and 16 weeks) 33–50% and 45–63%, respectively. Enrasentan treatments reduced the relative wall thickness (14–27% at 8 and 12 weeks), ratio of left ventricular mass to body weight (20% at 12 weeks), and ratio of terminal heart weight to body weight (16–23%, p < 0.05). Finally, circulating aldosterone concentration (54–57%) and proANF fragment (33%) were reduced in enrasentan-treated groups (54–57% and 33%, respectively). Mixed ET A /ET B receptor antagonism improves cardiac performance and attenuates ventricular remodeling and premature mortality in an aggressive hypertension model.

Published

2001

45. Eprosartan reduces cardiac hypertrophy, protects heart and kidney, and prevents early mortality in severely hypertensive stroke-prone rats

Author

Wallace G. Campbell, Sudeep Chandra, Eliot H. Ohlstein, David P. Brooks, Susanta K. Sarkar, Frank C. Barone, Robert N. Willette, Lisa C. Contino, Robert W. Coatney, and Allen H. Nelson

Subjects

Cardiac function curve, Male, medicine.medical_specialty, Cardiac output, Normal diet, Physiology, Natriuresis, Blood Pressure, Cardiomegaly, Thiophenes, Kidney, Heart Rate, Physiology (medical), Internal medicine, Rats, Inbred SHR, medicine, Animals, Protein Precursors, Antihypertensive Agents, Ejection fraction, Ventricular Remodeling, business.industry, Myocardium, Body Weight, Imidazoles, Eprosartan, Organ Size, medicine.disease, Angiotensin II, Magnetic Resonance Imaging, Peptide Fragments, Rats, Stroke, Survival Rate, Proteinuria, Endocrinology, Blood pressure, Acrylates, Heart failure, Hypertension, Cardiology, Cardiology and Cardiovascular Medicine, business, Atrial Natriuretic Factor, medicine.drug

Abstract

Objective: Eprosartan is a selective angiotensin II type I receptor antagonist approved for the treatment of hypertension. In the present studies, eprosartan's ability to provide end-organ protection was evaluated in a model of cardiomyopathy and renal failure in stroke-prone rats (SP). Methods: SP were fed a high fat (24.5% in food) and high salt (1% in water) diet (SFD). Eprosartan (60 mg/kg/day) or vehicle (saline control) ( n =25/group) was administered by intraperitoneally-implanted minipumps to these SP on the SFD for 12 weeks. Normal diet fed SP and WKY rats ( n =25/group) were also included for comparison (i.e. served as normal controls). Mortality, hemodynamics, and both renal and cardiac function and histopathology were monitored in all treatment groups. Results : Eprosartan decreased the severely elevated arterial pressure (−12%; P

Published

2001

46. The myocardial beta-adrenergic system in spontaneously hypertensive heart failure (SHHF) rats

Author

Walter J. Koch, Andrea D. Eckhart, Karen M. Anderson, and Robert N. Willette

Subjects

Male, medicine.medical_specialty, Aging, Heart disease, Heart Ventricles, Hemodynamics, Adrenergic, Left ventricular hypertrophy, Ventricular Function, Left, Muscle hypertrophy, Rats, Sprague-Dawley, GTP-Binding Proteins, Heart Rate, Internal medicine, Heart rate, Receptors, Adrenergic, beta, Internal Medicine, medicine, Animals, Humans, Heart Failure, biology, business.industry, Beta adrenergic receptor kinase, Myocardium, Isoproterenol, Gene Expression Regulation, Developmental, Heart, Rats, Inbred Strains, Organ Size, medicine.disease, Cyclic AMP-Dependent Protein Kinases, Myocardial Contraction, Rats, Disease Models, Animal, Endocrinology, beta-Adrenergic Receptor Kinases, Heart failure, Hypertension, biology.protein, business

Abstract

Abstract —Responsiveness to β-adrenergic stimulation is reduced in the failing human myocardium. This results principally from reduced β-adrenergic receptor (βAR) density, elevated β-adrenergic receptor kinase 1 (βARK1) levels, and functional uncoupling of remaining receptors. The temporal nature of changes in the human myocardial β-adrenergic system relative to onset of symptomatic heart failure (HF) has been difficult to discern. A relatively new model of HF, the spontaneously hypertensive heart failure (SHHF) rat spontaneously and reproducibly develops left ventricular hypertrophy (LVH) and progresses to HF, thus enabling longitudinal studies to examine the cellular and molecular bases for hypertension-induced cardiac hypertrophy and subsequent HF. The purpose of this study was to examine age-dependent changes in the βAR system in this model. Lean male SHHF rats at 3, 7, 14, and 20 months were compared with age-matched Sprague-Dawley (SD) control rats ([C]; 4 animals/group). At all ages the SHHF rats had elevated blood pressures and left ventricular end-diastolic pressure relative to the SD control rats ( P

Published

1999

47. Plasma- and cerebrospinal fluid-immunoreactive endothelin-1: effects of nonpeptide endothelin receptor antagonists with diverse affinity profiles for endothelin-A and endothelin-B receptors

Author

Luengo Juan Ignacio, John D. Elliott, Jia-Ning Xiang, Stephanie Guiney, Eliot H. Ohlstein, Robert N. Willette, Barbara L. Storer, and Charles F. Sauermelch

Subjects

Agonist, Endothelin Receptor Antagonists, Male, medicine.medical_specialty, medicine.drug_class, Carboxylic Acids, Viper Venoms, Nitric oxide, chemistry.chemical_compound, Dogs, Internal medicine, Blood plasma, medicine, Animals, Vasoconstrictor Agents, Enzyme Inhibitors, Receptor, Benzofurans, Injections, Intraventricular, Pharmacology, Endothelin-1, Receptors, Endothelin, Antagonist, respiratory system, Receptor, Endothelin A, Endothelin 1, Receptor, Endothelin B, Endocrinology, NG-Nitroarginine Methyl Ester, chemistry, Indans, Injections, Intravenous, cardiovascular system, Systemic administration, Nitric Oxide Synthase, Propionates, Cardiology and Cardiovascular Medicine, Endothelin receptor, circulatory and respiratory physiology

Abstract

Some endothelin (ET) receptor antagonists have been reported to elevate plasma immunoreactive endothelin-1 (irET-1). However, there is no information regarding the effects of ET receptor antagonists on cerebrospinal fluid (CSF) levels. To better understand the regulation of circulating and CSF ET-1, the effects of several nonpeptide antagonists with high, intermediate, or low affinity at the ETB receptor, as well as the potent ETB selective agonist sarafotoxin 6c (S6c), were characterized and compared. The effects of SB209670 (Ki ETA = 0.2 nM; Ki ETB = 12 nM), SB217242 (Ki ETA = 1.1 nM; Ki ETB = 111 nM), SB234551 (Ki ETA = 0.1 nM; Ki ETB = 500 nM), SB247083 (Ki ETA = 0.4 nM; Ki ETB = 467 nM), and S6c (Ki ETA = 950 nM; Ki ETB = 1 nM) on plasma irET-1 were determined by ELISA in the anesthetized dog after i.v. administration. Systemic administration of equivalent doses of the nonpeptide ET receptor antagonists produced dose-related elevations in plasma irET-1 which were correlated (p = 0.019) with affinity at the ETB receptor. There was no significant correlation with affinity at the ETA receptor. In addition, the plasma irET-1 and ET antagonist concentrations were linearly correlated (r = 0.98) throughout the time course after antagonist administration. There was no evidence of densensitization after three bolus administrations performed at 2-h intervals (SB209670, 1 and 3 mg/kg i.v.). Elevations in plasma irET-1 (four- to fivefold) were also observed after systemic administration of S6c (1 nmol/kg i.v.). The administration of L-NAME (200 micrograms/kg/min for 30 min), an inhibitor of nitric oxide (NO) synthase, increased blood pressure (33%) but did not alter plasma irET-1. In contrast, systemic administration of the ET receptor antagonists had little or no effect on the on irET-1 in the CSF. However, intracerebroventricular (i.c.v.) administration of SB209670 produced a dose-related (3-100 micrograms) increase in cisternal CSF levels of irET-1 without altering plasma irET-1. Systemic administration of ETB receptor antagonists and agonists rapidly increased plasma irET-1. These ETB receptor antagonist effects correlate linearly with affinity at the cloned human ETB receptor, do not exhibit desensitization, and do not appear to reflect inhibition of ETB-mediated NO production. The endothelial ETB receptor may represent a high-capacity storage/clearance site for circulating ET-1. ET receptor antagonists may also act extravascularly/abluminally to increase irET-1 in the CNS.

Published

1998

48. Discovery of adrenomedullin in rat ischemic cortex and evidence for its role in exacerbating focal brain ischemic damage

Author

A. C. Sulpizio, Raymond F. White, Tian-Li Yue, Robert R. Ruffolo, Xinkang Wang, Nambi Aiyar, Giora Z. Feuerstein, Frank C. Barone, Robert N. Willette, and R. K. Clark

Subjects

medicine.medical_specialty, DNA, Complementary, Time Factors, Vasodilator Agents, Cerebral arteries, Molecular Sequence Data, Vasodilation, Calcitonin gene-related peptide, Brain Ischemia, Brain ischemia, Adrenomedullin, Dogs, Cortex (anatomy), Internal medicine, Rats, Inbred SHR, medicine, Animals, Amino Acid Sequence, RNA, Messenger, Stroke, Gene Library, Cerebral Cortex, Multidisciplinary, Base Sequence, business.industry, Drug Administration Routes, Cerebral Arteries, medicine.disease, Immunohistochemistry, Rats, Up-Regulation, medicine.anatomical_structure, Endocrinology, Cerebral cortex, business, Peptides, Research Article

Abstract

Focal brain ischemia is the most common event leading to stroke in humans. To understand the molecular mechanisms associated with brain ischemia, we applied the technique of mRNA differential display and isolated a gene that encodes a recently discovered peptide, adrenomedullin (AM), which is a member of the calcitonin gene-related peptide (CGRP) family. Using the rat focal stroke model of middle cerebral artery occlusion (MCAO), we determined that AM mRNA expression was significantly increased in the ischemic cortex up to 17.4-fold at 3 h post-MCAO (P < 0.05) and 21.7-fold at 6 h post-MCAO (P < 0.05) and remained elevated for up to 15 days (9.6-fold increase; P < 0.05). Immunohistochemical studies localized AM to ischemic neuronal processes, and radioligand (125I-labeled CGRP) displacement revealed high-affinity (IC50 = 80.3 nmol) binding of AM to CGRP receptors in brain cortex. The cerebrovascular function of AM was studied using synthetic AM microinjected onto rat pial vessels using a cranial window or applied to canine basilar arteries in vitro. AM, applied abluminally, produced dose-dependent relaxation of preconstricted pial vessels (P < 0.05). Intracerebroventricular (but not systemic) AM administration at a high dose (8 nmol), prior to and after MCAO, increased the degree of focal ischemic injury (P < 0.05). The ischemia-induced expression of both AM mRNA and peptide in ischemic cortical neurons, the demonstration of the direct vasodilating effects of the peptide on cerebral vessels, and the ability of AM to exacerbate ischemic brain damage suggests that AM plays a significant role in focal ischemic brain injury.

Published

1995

49. Therapeutic effects of endothelin receptor antagonists in stroke

Author

Frank C. Barone, Tian-Li Yue, Giora Feurestein, and Robert N. Willette

Subjects

medicine.hormone, Endothelin Receptor Antagonists, medicine.medical_specialty, Endothelium, Neuroprotection, Brain Ischemia, Endothelins, Internal medicine, Neuromodulation, medicine, Animals, Humans, cardiovascular diseases, Stroke, Brain Chemistry, Neurons, business.industry, Endothelin receptor antagonist, Vasospasm, General Medicine, medicine.disease, Cerebrovascular Disorders, Endocrinology, medicine.anatomical_structure, Neurology, Ischemic Attack, Transient, Cerebrovascular Circulation, cardiovascular system, Neurology (clinical), Endothelium, Vascular, business, Endothelin receptor

Abstract

The presence of the endothelin isopeptides and endothelin receptors on neurons, glial cells and brain capillary endothelium suggests that endothelins may play a significant role in neuromodulation, astrocytic function and in regulation of cerebral blood flow. Furthermore, endothelins may play a significant role in the central regulation of neuroendocrine and autonomic nervous system functions (i.e., plasma volume, cardiovascular and respiratory control). Endothelin has potent cerebrovascular and proliferative effects suggesting a pathogenic role in cerebrovascular diseases. Endothelin receptors may represent important therapeutic targets for the treatment of both hemorrhagic and ischemic stroke. A review of the available data on endothelin levels and the effects of endothelin antagonists in cerebrovascular diseases is provided in the present report. Most notably is evidence in support of increased brain endothelin levels in hemorrhagic and ischemic stroke both in animal models and in humans. Also, endothelin receptor antagonists exert significant efficacy in animal models of cerebrovascular disease. For example, SB 209670, a rationally designed, potent, nonpeptide endothelin receptor antagonist, exerts therapeutic efficacy in reducing vasospasm following subarachnoid hemorrhage and neuroprotection following ischemic stroke. Certainly the available data warrants further evaluation of novel, selective endothelin receptor antagonists or endothelin converting enzyme inhibitors in cerebrovascular diseases.

Published

1995

50. Clinical perspectives of calcitonin gene related peptide pharmacology

Author

Nambi Aiyar, Robert N. Willette, and Glora Feuerstein

Subjects

medicine.medical_specialty, Physiology, Calcitonin Gene-Related Peptide, Migraine Disorders, Amylin, Neuropeptide, Inflammation, Vasodilation, Coronary Disease, Calcitonin gene-related peptide, Pharmacology, Physiology (medical), Internal medicine, medicine, Humans, Receptor, Heart Failure, Neurogenic inflammation, integumentary system, business.industry, Vasospasm, General Medicine, Subarachnoid Hemorrhage, medicine.disease, Shock, Septic, Endocrinology, Hypertension, medicine.symptom, business

Abstract

Calcitonin gene related peptide (CGRP), a potent vasoactive and cardiotonic peptide, interacts with specific G-protein-coupled receptors. CGRP is synthesized and released from small, capsaicin-sensitive sensory nerves. This extensive network of sensory nerves, found in virtually all organs, suggest a potential role for CGRP in diverse physiologic and pathophysiologic processes. The potent vasodilation elicited by CGRP in the cerebral, coronary, and peripheral vasculature has led to its therapeutic evaluation in the treatment of cerebral vasospasm following subarachnoid hemorrhage, stable angina, and Raynaud's phenomenon. The potential inotropic action and coronary vasodilation have also led to a potential beneficial effect in congestive heart failure. The enriched localization of CGRP in trigeminal sensory ganglia may indicate a role in the neurogenic inflammation associated with migraine. Thus, CGRP antagonists may represent a novel therapeutic approach to the treatment of migraine. In addition, CGRP and amylin (homologous pancreatic peptide) reduce the tissue–glucose response to insulin. It has been suggested that a CGRP antagonist may therefore improve insulin sensitivity in non-insulin-dependent diabetes, NIDDM. This brief review provides a preliminary exploration of the potential therapeutic opportunities surrounding CGRP and CGRP antagonists. Future advances are dependent on a better understanding of the structure and function of CGRP receptor(s) and the concomitant identification of selective and potent agonists and antagonists useful for addressing therapeutic hypotheses.Key words: calcitonin gene related peptide, congestive heart failure, diabetes, therapy, vasospasm, migraine.

Published

1995