Your search keyword '"Andrew D Howard"' showing total 112 results

1. GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent.

Author

Michele J Pachanski, Melissa E Kirkland, Daniel T Kosinski, Joel Mane, Boonlert Cheewatrakoolpong, Jiyan Xue, Daphne Szeto, Gail Forrest, Corin Miller, Michelle Bunzel, Christopher W Plummer, Harry R Chobanian, Michael W Miller, Sarah Souza, Brande S Thomas-Fowlkes, Aimie M Ogawa, Adam B Weinglass, Jerry Di Salvo, Xiaoyan Li, Yue Feng, Daniel A Tatosian, Andrew D Howard, Steven L Colletti, and Maria E Trujillo

Subjects

Medicine, Science

Abstract

GPR40 agonists are effective antidiabetic agents believed to lower glucose through direct effects on the beta cell to increase glucose stimulated insulin secretion. However, not all GPR40 agonists are the same. Partial agonists lower glucose through direct effects on the pancreas, whereas GPR40 AgoPAMs may incorporate additional therapeutic effects through increases in insulinotrophic incretins secreted by the gut. Here we describe how GPR40 AgoPAMs stimulate both insulin and incretin secretion in vivo over time in diabetic GK rats. We also describe effects of AgoPAMs in vivo to lower glucose and body weight beyond what is seen with partial GPR40 agonists in both the acute and chronic setting. Further comparisons of the glucose lowering profile of AgoPAMs suggest these compounds may possess greater glucose control even in the presence of elevated glucagon secretion, an unexpected feature observed with both acute and chronic treatment with AgoPAMs. Together these studies highlight the complexity of GPR40 pharmacology and the potential additional benefits AgoPAMs may possess above partial agonists for the diabetic patient.

Published

2017

2. GPR120 suppresses adipose tissue lipolysis and synergizes with GPR40 in antidiabetic efficacy

Author

Santhosh Satapati, Ying Qian, Margaret S. Wu, Aleksandr Petrov, Ge Dai, Sheng-ping Wang, Yonghua Zhu, Xiaolan Shen, Eric S. Muise, Ying Chen, Emanuel Zycband, Adam Weinglass, Jerry Di Salvo, John S. Debenham, Jason M. Cox, Ping Lan, Vinit Shah, Stephen F. Previs, Mark Erion, David E. Kelley, Liangsu Wang, Andrew D. Howard, and Jin Shang

Subjects

lipolysis and fatty acid metabolism, insulin resistance, diabetes, fatty acid, Biochemistry, QD415-436

Abstract

GPR40 and GPR120 are fatty acid sensors that play important roles in glucose and energy homeostasis. GPR40 potentiates glucose-dependent insulin secretion and demonstrated in clinical studies robust glucose lowering in type 2 diabetes. GPR120 improves insulin sensitivity in rodents, albeit its mechanism of action is not fully understood. Here, we postulated that the antidiabetic efficacy of GPR40 could be enhanced by coactivating GPR120. A combination of GPR40 and GPR120 agonists in db/db mice, as well as a single molecule with dual agonist activities, achieved superior glycemic control compared with either monotherapy. Compared with a GPR40 selective agonist, the dual agonist improved insulin sensitivity in ob/ob mice measured by hyperinsulinemic-euglycemic clamp, preserved islet morphology, and increased expression of several key lipolytic genes in adipose tissue of Zucker diabetic fatty rats. Novel insights into the mechanism of action for GPR120 were obtained. Selective GPR120 activation suppressed lipolysis in primary white adipocytes, although this effect was attenuated in adipocytes from obese rats and obese rhesus, and sensitized the antilipolytic effect of insulin in rat and rhesus primary adipocytes. In conclusion, GPR120 agonism enhances insulin action in adipose tissue and yields a synergistic efficacy when combined with GPR40 agonism.

Published

2017

3. Design, synthesis and biological evaluation of indane derived GPR40 agoPAMs

Author

Barbara Pio, Ravi P. Nargund, Yan Guo, Daniel Kosinski, Josien Hubert B, Michael Wright, Michele Pachanski, Harry R. Chobanian, Xiaoping Zhang, Richard Tschirret-Guth, Melissa Kirkland, Andrew D. Howard, Sarah Souza, Eric R. Ashley, Robert K. Orr, Steven L. Colletti, Joel Mane, Jerry Di Salvo, Michael W. Miller, Boonlert Cheewatrakoolpong, Koppara Samuel, William K. Hagmann, James Lamca, Juliann Ehrhart, Maria E. Trujillo, Jackie Shang, Qing Chen, Adam B. Weinglass, and Randal M. Bugianesi

Subjects

Agonist, endocrine system, medicine.drug_class, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Enteroendocrine cell, 01 natural sciences, Biochemistry, Receptors, G-Protein-Coupled, Free fatty acid receptor 1, Drug Discovery, medicine, Humans, Receptor, Mode of action, Molecular Biology, geography, geography.geographical_feature_category, 010405 organic chemistry, Chemistry, Organic Chemistry, Islet, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Mechanism of action, Drug Design, Indans, Molecular Medicine, medicine.symptom

Abstract

GPR40 (FFAR1 or FFA1) is a G protein-coupled receptor, primarily expressed in pancreatic islet β-cells and intestinal enteroendocrine cells. When activated by fatty acids, GPR40 elicits increased insulin secretion from islet β-cells only in the presence of elevated glucose levels. Towards this end, studies were undertaken towards discovering a novel GPR40 Agonist whose mode of action is via Positive Allosteric Modulation of the GPR40 receptor (AgoPAM). Efforts were made to identify a suitable GPR40 AgoPAM tool molecule to investigate mechanism of action and de-risk liver toxicity of GPR40 AgoPAMs due to reactive acyl-glucuronide (AG) metabolites.

Published

2019

4. Implications of the End-Stage Renal Disease Treatment Choices Model among U.S. Dialysis Providers

Author

Amber B, Paulus, Andrew D, Howard, and Brandy A, Vinson

Subjects

Prospective Payment System, Renal Dialysis, Humans, Kidney Failure, Chronic, Medicare, United States, Aged

Abstract

The End Stage Renal Disease Treatment Choices (ETC) Model is a mandatory payment model designed to encourage greater use of home dialysis and kidney transplantation among Medicare beneficiaries with kidney failure and to reduce Medicare expenditures while enhancing the quality of care offered to patients with kidney failure. The ETC model will run for six years, from January 1, 2021, to June 30, 2027. This article provides an overview of the ETC Model and analyzes its implications for dialysis providers.

Published

2021

5. Targeting a ceramide double bond improves insulin resistance and hepatic steatosis

Author

Ying Li, Renato Felipe Pereira, J. Alan Maschek, Joseph L. Wilkerson, Annelise M Poss, Scott A. Summers, Vincent A. Kaddai, David E. Kelley, Xiaolan Shen, William L. Holland, Doris Hissako Sumida, Jared Rutter, Margaret Wu, Ying Qian, Jun Yao, Aleksandr Petrov, Graeme I. Lancaster, David G. McLaren, Trevor S. Tippetts, Liangsu Wang, Santhosh Satapati, Mackenzie J. Pearson, Christian N. Nunes, Rafael Mayoral Monibas, Heather Zhou, Liping Wang, Monowarul Mobin Siddique, Mark D. Erion, Stephen F. Previs, Bhagirath Chaurasia, C. Rufus Sweeney, Jinqi Liu, Ying Chen, James E. Cox, Andrew D. Howard, University of Utah, Merck, Universidade Estadual Paulista (Unesp), Baker IDI Heart and Diabetes Institute, University of Brunei Darussalam, Sciex, Howard Hughes Medical Institute, Bristol Myers Squibb, Morphic Therapeutic, and Johnson and Johnson

Subjects

0301 basic medicine, Leptin, medicine.medical_specialty, Ceramide, Double bond, Adipose tissue, 030209 endocrinology & metabolism, Ceramides, Diet, High-Fat, Article, 03 medical and health sciences, Mice, chemistry.chemical_compound, 0302 clinical medicine, Insulin resistance, Internal medicine, Diabetes Mellitus, medicine, Humans, Animals, chemistry.chemical_classification, Sphingolipids, Multidisciplinary, Leptin Deficiency, Membrane Proteins, Dihydroceramide desaturase, medicine.disease, Sphingolipid, Mice, Mutant Strains, Fatty Liver, 030104 developmental biology, Endocrinology, Lipotoxicity, chemistry, Insulin Resistance, Steatosis, Oxidoreductases, Gene Deletion

Abstract

Made available in DSpace on 2019-10-06T17:15:07Z (GMT). No. of bitstreams: 0 Previous issue date: 2019-07-26 American Diabetes Association American Heart Association Ben B. and Iris M. Margolis Foundation Diabetes Research Center, University of Washington Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP) Preeclampsia Research Laboratories U.S. Department of Agriculture Juvenile Diabetes Research Foundation United Kingdom Agricultural Research Service National Institutes of Health Norges Idrettshøgskole Ceramides contribute to the lipotoxicity that underlies diabetes, hepatic steatosis, and heart disease. By genetically engineering mice, we deleted the enzyme dihydroceramide desaturase 1 (DES1), which normally inserts a conserved double bond into the backbone of ceramides and other predominant sphingolipids. Ablation of DES1 from whole animals or tissue-specific deletion in the liver and/or adipose tissue resolved hepatic steatosis and insulin resistance in mice caused by leptin deficiency or obesogenic diets. Mechanistic studies revealed ceramide actions that promoted lipid uptake and storage and impaired glucose utilization, none of which could be recapitulated by (dihydro)ceramides that lacked the critical double bond. These studies suggest that inhibition of DES1 may provide a means of treating hepatic steatosis and metabolic disorders. Department of Nutrition and Integrative Physiology Diabetes and Metabolism Research Center University of Utah Merck Research Laboratories Merck School of Dentistry São Paulo State University (UNESP) Department of Biochemistry and the Diabetes and Metabolism Research Center University of Utah Baker IDI Heart and Diabetes Institute Faculty of Science University of Brunei Darussalam Sciex Howard Hughes Medical Institute Bristol Myers Squibb Morphic Therapeutic Johnson and Johnson School of Dentistry São Paulo State University (UNESP) FAPESP: 2014/17619-6 U.S. Department of Agriculture: 2019-67018-29250 Juvenile Diabetes Research Foundation United Kingdom: 3-SRA-2019-768-A-B Agricultural Research Service: 5T32DK091317 National Institutes of Health: DK108833 National Institutes of Health: DK112826 National Institutes of Health: DK115824 National Institutes of Health: DK116450 Norges Idrettshøgskole: P30DK020579

Published

2020

6. Optimization of Preclinical Metabolism for Somatostatin Receptor Subtype 5-Selective Antagonists

Author

Weiguo Liu, Ramzi F. Sweis, Feroze Ujjainwalla, Remond Moningka, F. Anthony Romero, Yi Zang, Paul E. Finke, Zahid Hussain, Karen H. Dingley, Michael A. Plotkin, Andrew D. Howard, Jin Shang, Beth Ann Murphy, Jianming Bao, Gino Salituro, Harold B. Wood, and Joseph L. Duffy

Subjects

0301 basic medicine, Somatostatin receptor, Chemistry, Organic Chemistry, 030209 endocrinology & metabolism, Metabolism, Pharmacology, Biochemistry, In vitro, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Somatostatin, Pharmacokinetics, In vivo, Pharmacodynamics, Drug Discovery, Lead compound

Abstract

[Image: see text] A series of structurally diverse azaspirodecanone and spirooxazolidinone analogues were designed and synthesized as potent and selective somatostatin receptor subtype 5 (SSTR5) antagonists. Four optimized compounds each representing a subseries showed improvement in their metabolic stability and pharmacokinetic profiles compared to those of the original lead compound 1 while maintaining pharmacodynamic efficacy. The optimized cyclopropyl analogue 13 demonstrated efficacy in a mouse oral glucose tolerance test and an improved metabolic profile and pharmacokinetic properties in rhesus monkey studies. In this Communication, we discuss the relationship among structure, in vitro and in vivo activity, metabolic stability, and ultimately the potential of these compounds as therapeutic agents for the treatment of type 2 diabetes. Furthermore, we show how the use of focused libraries significantly expanded the structural class and provided new directions for structure–activity relationship optimization.

Published

2018

7. Discovery and Pharmacology of a Novel Somatostatin Subtype 5 (SSTR5) Antagonist: Synergy with DPP-4 Inhibition

Author

Daniel Metzger, Joseph L. Duffy, Weiguo Liu, Jiafang He, Garry Chicchi, Gino Salituro, Ann E. Weber, Margaret Wu, Cai Li, John Wang, Taro E. Akiyama, Andrew D. Howard, Shao Pengcheng Patrick, John Bawiec, Beth Ann Murphy, Gui-Bai Liang, Yun-Ping Zhou, Susan D. Aster, Kwei-Lan Tsao, and Jin Shang

Subjects

0301 basic medicine, Chemistry, Insulin, medicine.medical_treatment, Organic Chemistry, Glucose challenge, Antagonist, 030209 endocrinology & metabolism, Glucose excursion, Pharmacology, Biochemistry, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Somatostatin, Incretin Hormone, Drug Discovery, medicine, Potency, Dipeptidyl peptidase-4

Abstract

[Image: see text] We report new SSTR5 antagonists with enhanced potency, subtype selectivity, and minimal off-target activities as compared to previously reported compounds. Starting from the reported SSTR5 antagonist 1, we systematically surveyed changes in the central core and head piece while maintaining the diphenyl tail group constant. From this study the azaspirodecanone 10 emerged as a new highly potent and selective SSTR5 antagonist. Compound 10 lowered glucose excursion by 94% in an oral glucose tolerance test (OGTT) in mice following a 3 mg/kg oral dose. The compound increased both total and active circulating incretin hormone GLP-1 levels in mice at a dose of 10 mg/kg. A synergistic effect was also demonstrated when compound 10 was coadministered with a DPP-4 inhibitor, substantially increasing circulating active GLP-1[7–36] amide and insulin in response to a glucose challenge.

Published

2018

8. GPR120 suppresses adipose tissue lipolysis and synergizes with GPR40 in antidiabetic efficacy

Author

Jerry Di Salvo, Santhosh Satapati, Mark D. Erion, Jin Shang, Stephen F. Previs, Adam B. Weinglass, John S. Debenham, Margaret Wu, Sheng-Ping Wang, Andrew D. Howard, Ying Chen, Aleksandr Petrov, Ge Dai, Yonghua Zhu, Liangsu Wang, David E. Kelley, Ying Qian, Xiaolan Shen, Eric S. Muise, Jason M. Cox, Ping Lan, Vinit Shah, and Emanuel Zycband

Subjects

Male, 0301 basic medicine, Agonist, endocrine system, medicine.medical_specialty, medicine.drug_class, Lipolysis, medicine.medical_treatment, Adipose tissue, 030209 endocrinology & metabolism, QD415-436, CHO Cells, Biochemistry, Diabetes Mellitus, Experimental, Receptors, G-Protein-Coupled, Islets of Langerhans, Mice, 03 medical and health sciences, Cricetulus, 0302 clinical medicine, Endocrinology, Insulin resistance, Cricetinae, Internal medicine, Free fatty acid receptor 1, medicine, Animals, Research Articles, diabetes, Chemistry, Insulin, GPR120, Cell Biology, medicine.disease, lipolysis and fatty acid metabolism, Rats, 030104 developmental biology, Adipose Tissue, Gene Expression Regulation, Mechanism of action, fatty acid, Insulin Resistance, medicine.symptom

Abstract

GPR40 and GPR120 are fatty acid sensors that play important roles in glucose and energy homeostasis. GPR40 potentiates glucose-dependent insulin secretion and demonstrated in clinical studies robust glucose lowering in type 2 diabetes. GPR120 improves insulin sensitivity in rodents, albeit its mechanism of action is not fully understood. Here, we postulated that the antidiabetic efficacy of GPR40 could be enhanced by coactivating GPR120. A combination of GPR40 and GPR120 agonists in db/db mice, as well as a single molecule with dual agonist activities, achieved superior glycemic control compared with either monotherapy. Compared with a GPR40 selective agonist, the dual agonist improved insulin sensitivity in ob/ob mice measured by hyperinsulinemic-euglycemic clamp, preserved islet morphology, and increased expression of several key lipolytic genes in adipose tissue of Zucker diabetic fatty rats. Novel insights into the mechanism of action for GPR120 were obtained. Selective GPR120 activation suppressed lipolysis in primary white adipocytes, although this effect was attenuated in adipocytes from obese rats and obese rhesus, and sensitized the antilipolytic effect of insulin in rat and rhesus primary adipocytes. In conclusion, GPR120 agonism enhances insulin action in adipose tissue and yields a synergistic efficacy when combined with GPR40 agonism.

Published

2017

9. GPR40 reduces food intake and body weight through GLP-1

Author

Judith N. Gorski, Maria E. Trujillo, Brande Thomas-Fowlkes, Adam B. Weinglass, Jerry Di Salvo, Aimie M. Ogawa, Sarah Souza, Christopher W. Plummer, Joel Mane, Michele Pachanski, Boonlert Cheewatrakoolpong, Andrew D. Howard, and Steven L. Colletti

Subjects

Male, 0301 basic medicine, Agonist, endocrine system, medicine.medical_specialty, Physiology, medicine.drug_class, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Gastric motility, Biology, Partial agonist, Receptors, G-Protein-Coupled, Eating, Mice, 03 medical and health sciences, Glucagon-Like Peptide 1, Weight loss, Physiology (medical), Internal medicine, Free fatty acid receptor 1, Weight Loss, medicine, Animals, Mice, Knockout, Appetite Regulation, Insulin, Body Weight, Glucagon-like peptide-1, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, medicine.symptom, Weight gain

Abstract

G protein-coupled receptor 40 (GPR40) partial agonists lower glucose through the potentiation of glucose-stimulated insulin secretion, which is believed to provide significant glucose lowering without the weight gain or hypoglycemic risk associated with exogenous insulin or glucose-independent insulin secretagogues. The class of small-molecule GPR40 modulators, known as AgoPAMs (agonist also capable of acting as positive allosteric modulators), differentiate from partial agonists, binding to a distinct site and functioning as full agonists to stimulate the secretion of both insulin and glucagon-like peptide-1 (GLP-1). Here we show that GPR40 AgoPAMs significantly increase active GLP-1 levels and reduce acute and chronic food intake and body weight in diet-induced obese (DIO) mice. These effects of AgoPAM treatment on food intake are novel and required both GPR40 and GLP-1 receptor signaling pathways, as demonstrated in GPR40 and GLP-1 receptor-null mice. Furthermore, weight loss associated with GPR40 AgoPAMs was accompanied by a significant reduction in gastric motility in these DIO mice. Chronic treatment with a GPR40 AgoPAM, in combination with a dipeptidyl peptidase IV inhibitor, synergistically decreased food intake and body weight in the mouse. The effect of GPR40 AgoPAMs on GLP-1 secretion was recapitulated in lean, healthy rhesus macaque demonstrating that the putative mechanism mediating weight loss translates to higher species. Together, our data indicate effects of AgoPAMs that go beyond glucose lowering previously observed with GPR40 partial agonist treatment with additional potential for weight loss.

Published

2017

10. Structural basis for the cooperative allosteric activation of the free fatty acid receptor GPR40

Author

Adam B Weinglass, Nicholas B Hastings, Bradley S Sherborne, Jennifer M. Johnston, Andrew D Howard, Maria Webb, Steven L. Colletti, Clemens Vonrhein, Kevin J. Lumb, Srivanya Tummala, Frank K Brown, Jennifer Hadix, Hubert Josien, Stephen M. Soisson, Guo Yan, Harry R. Chobanian, John Wang, Michael W. Miller, Brande Thomas-Fowlkes, Dawn L. Hall, Jeffrey D. Hermes, Thu Ho, Barbara Pio, Payal R. Sheth, Sujata Sharma, Maria Kornienko, Samantha J Allen, Sangita B. Patel, Jerry Di Salvo, Sarah Souza, Gérard Bricogne, Christopher W Plummer, Jun Lu, and Noel Byrne

Subjects

Models, Molecular, 0301 basic medicine, Binding Sites, biology, Protein Conformation, Allosteric regulation, Cooperativity, Crystallography, X-Ray, Partial agonist, Receptors, G-Protein-Coupled, 03 medical and health sciences, Transmembrane domain, 030104 developmental biology, Allosteric Regulation, Allosteric enzyme, Biochemistry, Structural Biology, Free fatty acid receptor 1, biology.protein, Free fatty acid receptor, Biophysics, Humans, Binding site, Molecular Biology, Protein Binding

Abstract

Clinical studies indicate that partial agonists of the G-protein-coupled, free fatty acid receptor 1 GPR40 enhance glucose-dependent insulin secretion and represent a potential mechanism for the treatment of type 2 diabetes mellitus. Full allosteric agonists (AgoPAMs) of GPR40 bind to a site distinct from partial agonists and can provide additional efficacy. We report the 3.2-Å crystal structure of human GPR40 (hGPR40) in complex with both the partial agonist MK-8666 and an AgoPAM, which exposes a novel lipid-facing AgoPAM-binding pocket outside the transmembrane helical bundle. Comparison with an additional 2.2-Å structure of the hGPR40-MK-8666 binary complex reveals an induced-fit conformational coupling between the partial agonist and AgoPAM binding sites, involving rearrangements of the transmembrane helices 4 and 5 (TM4 and TM5) and transition of the intracellular loop 2 (ICL2) into a short helix. These conformational changes likely prime GPR40 to a more active-like state and explain the binding cooperativity between these ligands.

Published

2017

11. Design and Synthesis of Novel, Selective GPR40 AgoPAMs

Author

Melissa Kirkland, Randal M. Bugianesi, Melodie Christensen, Maria E. Trujillo, Michele Pachanski, Richard Tschirret-Guth, Josien Hubert B, Adam B. Weinglass, Sarah Souza, Ravi P. Nargund, Christopher W. Plummer, Andrew D. Howard, Joel Mane, Louis-Charles Campeau, Robert K. Orr, Daniel Kosinski, Xiaoping Zhang, Boonlert Cheewatrakoolpong, Jerry Di Salvo, Michael W. Miller, William K. Hagmann, Helen Chen, Steven L. Colletti, Andrew Nolting, Michael Wright, Matthew J. Clements, and Murali Rajagopalan

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, business.industry, Pancreatic islets, Organic Chemistry, Tachyphylaxis, Hypoglycemia, medicine.disease, Biochemistry, Partial agonist, 03 medical and health sciences, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Tolerability, Internal medicine, Diabetes mellitus, Free fatty acid receptor 1, Drug Discovery, medicine, Receptor, business

Abstract

GPR40 is a G-protein-coupled receptor expressed primarily in pancreatic islets and intestinal L-cells that has been a target of significant recent therapeutic interest for type II diabetes. Activation of GPR40 by partial agonists elicits insulin secretion only in the presence of elevated blood glucose levels, minimizing the risk of hypoglycemia. GPR40 agoPAMs have shown superior efficacy to partial agonists as assessed in a glucose tolerability test (GTT). Herein, we report the discovery and optimization of a series of potent, selective GPR40 agoPAMs. Compound 24 demonstrated sustained glucose lowering in a chronic study of Goto Kakizaki rats, showing no signs of tachyphylaxis for this mechanism.

Published

2017

12. GPR119, a Major Enteroendocrine Sensor of Dietary Triglyceride Metabolites Coacting in Synergy With FFA1 (GPR40)

Author

Birgitte Holst, Anna-Sofie Husted, Jeppe H. Ekberg, Thue W. Schwartz, Frank Reiman, Line Vildbrad Kristensen, Kristoffer L. Egerod, Fiona M. Gribble, Maja S. Engelstoft, Timothy J. Kowalski, Rasmus M. Sichlau, Harald S. Hansen, Andrew D. Howard, Andreas N. Madsen, Pascal Timshel, and Maria Hauge

Subjects

0301 basic medicine, Agonist, endocrine system, medicine.medical_specialty, Colon, medicine.drug_class, Incretin, Biology, Article, Receptors, G-Protein-Coupled, Mice, 03 medical and health sciences, chemistry.chemical_compound, Endocrinology, Glucagon-Like Peptide 1, Free fatty acid receptor 1, Internal medicine, medicine, Animals, Sulfones, Receptor, Triglycerides, Benzofurans, Mice, Knockout, Bombesin, GPR120, Dietary Fats, Peptide Fragments, 030104 developmental biology, GPR119, chemistry, Secretagogue

Abstract

Triglycerides (TGs) are among the most efficacious stimulators of incretin secretion; however, the relative importance of FFA1 (G Protein-coupled Receptor [GPR] 40), FFA4 (GPR120), and GPR119, which all recognize TG metabolites, ie, long-chain fatty acid and 2-monoacylglycerol, respectively, is still unclear. Here, we find all 3 receptors to be highly expressed and highly enriched in fluorescence-activated cell sorting-purified GLP-1 and GIP cells isolated from transgenic reporter mice. In vivo, the TG-induced increase in plasma GIP was significantly reduced in FFA1-deficient mice (to 34%, mean of 4 experiments each with 8-10 animals), in GPR119-deficient mice (to 24%) and in FFA1/FFA4 double deficient mice (to 15%) but not in FFA4-deficient mice. The TG-induced increase in plasma GLP-1 was only significantly reduced in the GPR119-deficient and the FFA1/FFA4 double deficient mice, but not in the FFA1, and FFA4-deficient mice. In mouse colonic crypt cultures the synthetic FFA1 agonists, TAK-875 stimulated GLP-1 secretion to a similar extent as the prototype GLP-1 secretagogue neuromedin C; this, however, only corresponded to approximately half the maximal efficiency of the GPR119 agonist AR231453, whereas the GPR120 agonist Metabolex-209 had no effect. Importantly, when the FFA1 agonist was administered on top of appropriately low doses of the GPR119 agonist, a clear synergistic, ie, more than additive, effect was observed. It is concluded that the 2-monoacylglycerol receptor GPR119 is at least as important as the long-chain fatty acid receptor FFA1 in mediating the TG-induced secretion of incretins and that the 2 receptors act in synergy, whereas FFA4 plays a minor if any role.

Published

2016

13. Duodenal-jejunal bypass surgery induces hepatic lipidomic alterations associated with ameliorated hepatic steatosis in mice

Author

Yonghua Zhu, David E. Kelley, Jin Shang, Ying Qian, Liangsu Wang, Mark D. Erion, Stephen F. Previs, Andrew D. Howard, Haiying Liu, Xiaolan Shen, and Jose Castro-Perez

Subjects

0301 basic medicine, chemistry.chemical_classification, medicine.medical_specialty, Nutrition and Dietetics, Endocrinology, Diabetes and Metabolism, Medicine (miscellaneous), Fatty acid, Phosphatidic acid, Metabolism, Lipidome, medicine.disease, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Endocrinology, Insulin resistance, chemistry, Weight loss, Internal medicine, medicine, Steatosis, medicine.symptom, Diacylglycerol kinase

Abstract

Objective Bariatric surgery induces weight loss and improvement of insulin resistance; one aspect of both is an amelioration of hepatic steatosis. This study was undertaken to assess the changes in the hepatic lipidome after duodenal-jejunal bypass (DJB) surgery. Methods A DJB surgical model was developed and characterized in diet-induced obese mice. In comparison with sham-operated mice, an unbiased lipidomic profiling of hepatic lipids was performed together with measurements of gene expression within key pathways of hepatic lipid metabolism. Results In the liver of DJB mice, a dramatic reduction (by 77%) in hepatic triacylglycerols was observed. Global lipidomic profiling identified marked decreases of triacylglycerols comprised of medium length fatty acids and with low double bond content. Specific diacylglycerol species were also among the most dramatic decreases in hepatic lipids, whereas lysophosphatidic acids and phosphatidic acids were increased. Expression of fatty acid transporter and lipogenic genes was down-regulated. Conclusions From in-depth analysis of hepatic lipid composition, specific lipid intermediates were identified that are preferentially changed following DJB surgery. These changes were most likely due to DJB-induced weight loss, and only further studies will be able to distinguish weight loss-dependent from weight loss-independent changes.

Published

2016

14. Neurotensin Is Coexpressed, Coreleased, and Acts Together With GLP-1 and PYY in Enteroendocrine Control of Metabolism

Author

Felix Sommer, Cecilia F. Ratner, Stefan Offermanns, Kaare V. Grunddal, Andreas N. Madsen, Mark K. Nøhr, Jens J. Holst, Timothy J. Kowalski, Andrea R. Nawrocki, Steen Seier Poulsen, Jens Pedersen, Fredrik Bäckhed, Kristoffer L. Egerod, Andrew D. Howard, Berit Svendsen, Maja S. Engelstoft, Thue W. Schwartz, and Birgitte Holst

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Enteroendocrine Cells, Recombinant Fusion Proteins, Neuropeptide, Mice, Transgenic, Enteroendocrine cell, Biology, digestive system, Receptors, G-Protein-Coupled, Tissue Culture Techniques, 03 medical and health sciences, chemistry.chemical_compound, Endocrinology, Genes, Reporter, Glucagon-Like Peptide 1, Ileum, Internal medicine, medicine, Animals, Humans, Glucose homeostasis, Peptide YY, Intestinal Mucosa, Rats, Wistar, Neurotensin, Gastric emptying, Secretory Vesicles, digestive, oral, and skin physiology, Proglucagon, Glucagon-like peptide-1, Peptide Fragments, Mice, Inbred C57BL, Luminescent Proteins, 030104 developmental biology, Gene Expression Regulation, chemistry, Bombesin, Female, Biomarkers, hormones, hormone substitutes, and hormone antagonists

Abstract

The 2 gut hormones glucagon-like peptide-1 (GLP-1) and peptide YY (PYY) are well known to be coexpressed, costored, and released together to coact in the control of key metabolic target organs. However, recently, it became clear that several other gut hormones can be coexpressed in the intestinal-specific lineage of enteroendocrine cells. Here, we focus on the anatomical and functional consequences of the coexpression of neurotensin with GLP-1 and PYY in the distal small intestine. Fluorescence-activated cell sorting analysis, laser capture, and triple staining demonstrated that GLP-1 cells in the crypts become increasingly multihormonal, ie, coexpressing PYY and neurotensin as they move up the villus. Proglucagon promoter and pertussis toxin receptor-driven cell ablation and reappearance studies indicated that although all the cells die, the GLP-1 cells reappear more quickly than PYY- and neurotensin-positive cells. High-resolution confocal fluorescence microscopy demonstrated that neurotensin is stored in secretory granules distinct from GLP-1 and PYY storing granules. Nevertheless, the 3 peptides were cosecreted from both perfused small intestines and colonic crypt cultures in response to a series of metabolite, neuropeptide, and hormonal stimuli. Importantly, neurotensin acts synergistically, ie, more than additively together with GLP-1 and PYY to decrease palatable food intake and inhibit gastric emptying, but affects glucose homeostasis in a more complex manner. Thus, neurotensin is a major gut hormone deeply integrated with GLP-1 and PYY, which should be taken into account when exploiting the enteroendocrine regulation of metabolism pharmacologically.

Published

2016

15. The aromatic amino acid sensor GPR142 controls metabolism through balanced regulation of pancreatic and gut hormones

Author

Maja S. Engelstoft, Jacek Mokrosinski, Alexander Munk, Natalia Petersen, Yue Feng, Fiona M. Gribble, Margaret Wu, Jens J. Holst, Jin Shang, Yun-Ping Zhou, Thue W. Schwartz, Andrew D. Howard, Jeppe P. Ekberg, Siv A. Hjorth, Jonas T. Treebak, Kristoffer L. Egerod, Frank Reimann, Jens F. Rehfeld, Olga Rudenko, Peter Thams, Mokrosinski, Jacek [0000-0001-5008-0457], Reimann, Frank [0000-0001-9399-6377], Gribble, Fiona [0000-0002-4232-2898], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Blood Glucose, Male, medicine.medical_treatment, Mice, Obese, Enteroendocrine cell, Glucose homeostasis, Trp, Receptors, G-Protein-Coupled, chemistry.chemical_compound, Mice, 0302 clinical medicine, Glucagon-Like Peptide 1, Insulin-Secreting Cells, Receptors, Glucagon, Insulin, Mice, Knockout, Glycogen, Chemistry, Tryptophan, medicine.anatomical_structure, hormones, hormone substitutes, and hormone antagonists, Agonist, endocrine system, medicine.medical_specialty, G-protein-coupled receptor, GPR142, medicine.drug_class, 030209 endocrinology & metabolism, Glucagon, Glucagon-Like Peptide-1 Receptor, Receptors, Gastrointestinal Hormone, 03 medical and health sciences, Amino Acids, Aromatic, Islets of Langerhans, Receptor-Interacting Protein Serine-Threonine Kinase 2, Internal medicine, medicine, Animals, Amino acid sensing, Molecular Biology, Pancreatic islets, Cell Biology, Rats, Rats, Zucker, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Glucose, Glucagon-Secreting Cells, Hormone

Abstract

OBJECTIVES: GPR142, which is highly expressed in pancreatic islets, has recently been deorphanized as a receptor for aromatic amino acids; however, its physiological role and pharmacological potential is unclear.METHODS AND RESULTS: We find that GPR142 is expressed not only in β- but also in α-cells of the islets as well as in enteroendocrine cells, and we confirm that GPR142 is a highly selective sensor of essential aromatic amino acids, in particular Trp and oligopeptides with N-terminal Trp. GPR142 knock-out mice displayed a very limited metabolic phenotype but demonstrated that L-Trp induced secretion of pancreatic and gut hormones is mediated through GPR142 but that the receptor is not required for protein-induced hormone secretion. A synthetic GPR142 agonist stimulated insulin and glucagon as well as GIP, CCK, and GLP-1 secretion. In particular, GIP secretion was sensitive to oral administration of the GPR142 agonist an effect which in contrast to the other hormones was blocked by protein load. Oral administration of the GPR142 agonist increased [3H]-2-deoxyglucose uptake in muscle and fat depots mediated through insulin action while it lowered liver glycogen conceivably mediated through glucagon, and, consequently, it did not lower total blood glucose. Nevertheless, acute administration of the GPR142 agonist strongly improved oral glucose tolerance in both lean and obese mice as well as Zucker fatty rat. Six weeks in-feed chronic treatment with the GPR142 agonist did not affect body weight in DIO mice, but increased energy expenditure and carbohydrate utilization, lowered basal glucose, and improved insulin sensitivity.CONCLUSIONS: GPR142 functions as a sensor of aromatic amino acids, controlling GIP but also CCK and GLP-1 as well as insulin and glucagon in the pancreas. GPR142 agonists could have novel interesting potential in modifying metabolism through a balanced action of gut hormones as well as both insulin and glucagon.

Published

2018

16. GPR40 (FFAR1) – Combined Gs and Gq signaling in vitro is associated with robust incretin secretagogue action ex vivo and in vivo

Author

Birgitte Holst, Jerry Di Salvo, Michael Lückmann, Marie A. Vestmar, Maja S. Engelstoft, Andrew D. Howard, Michael W. Miller, Thue W. Schwartz, Adam B. Weinglass, Thomas M. Frimurer, Andreas N. Madsen, Maria E. Trujillo, Michael Wright, Anna Sofie Husted, Jeppe P. Ekberg, and Maria Hauge

Subjects

Agonist, endocrine system, medicine.medical_specialty, Ago-allosteric agonist, medicine.drug_class, Incretin, Pharmacology, In vivo, Internal medicine, Free fatty acid receptor 1, medicine, Secretion, G protein-coupled receptor, Receptor, Molecular Biology, Glucagon like peptide 1 (GLP-1), Long chain fatty acids (LCFAs), business.industry, digestive, oral, and skin physiology, Cell Biology, Biased signaling, Endocrinology, Original Article, Secretagogue, business, hormones, hormone substitutes, and hormone antagonists, Ex vivo

Abstract

Objectives GPR40 (FFAR1), a clinically proven anti-diabetes target, is a Gq-coupled receptor for long chain fatty acids (LCFA) stimulating insulin secretion directly and mediating a major part of the dietary triglyceride-induced secretion of the incretins GLP-1 and GIP. In phase-II studies the GPR40 agonist TAK-875 decreased blood glucose but surprisingly without stimulating incretins. Methods and results Here we find that GPR40 can signal through not only Gq and IP3 but also Gs and cAMP when stimulated with certain agonists such as AM-1638 and AM-5262 in contrast to the endogenous LCFA ligands and agonists such as TAK-875 and AM-837, which only signal through Gq. In competition binding against [3H]AM-1638 and [3H]L358 the Gq + Gs and the Gq-only agonists either competed for or showed positive cooperativity by increasing the binding of the two different radio-ligands, in opposite ways. Nevertheless, both the Gq-only and the Gq + Gs agonists all docked surprisingly well into the binding site for TAK-875 in the X-ray structure of GPR40. In murine intestinal primary cell-cultures the endogenous LCFAs and the Gq-only agonists stimulated GLP-1 secretion with rather poor efficacy as compared with the high efficacy Gq + Gs GPR40 agonists and a prototype GPR119 agonist. Similarly, in fasting both male and female mice the Gq + Gs agonists showed significantly higher efficacy than the Gq-only agonists in respect of increasing plasma GLP-1 and plasma GIP in a GPR40-dependent manner. Conclusions It is concluded that stimulation of GPR40 by endogenous LCFAs or by Gq-only synthetic agonists result in a rather limited incretin response, whereas Gq + Gs GPR40 agonists stimulate incretin secretion robustly.

Published

2015

17. Corrigendum to 'Discovery of benzofuran propanoic acid GPR120 agonists: From uHTS hit to mechanism-based pharmacodynamic effects' [Bioorg. Med. Chem. Lett. 26 (2016) 5724-5728]

Author

Matthew Lombardo, Eric N. Johnson, John Cummings, Jerry Di Salvo, Thomas Roussel, James R. Tata, Melissa Kirkland, Michael A. Plotkin, Christopher Joseph Sinz, Feroze Ujjainwalla, Dennis Leung, Dorina Trusca, Joel Mane, Taro E. Akiyama, Alejandro Crespo, Mary Ann Powles, Kate Bender, Michael F.A. Finley, Joanna Pols, Candice Alleyne, Michele Pachanski, Andrew D. Howard, Wayne M. Geissler, Ying Lei, Bahanu Habulihaz, Victor N. Uebele, Clare London, and Maria Madeira

Subjects

Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Mechanism based, GPR120, Biochemistry, chemistry.chemical_compound, Propanoic acid, chemistry, Drug Discovery, Molecular Medicine, Benzofuran, Molecular Biology

Published

2017

18. Investigation of Cardiovascular Effects of Tetrahydro-β-carboline sstr3 antagonists

Author

Donald Nelson, Gary G. Chicchi, James Dellureficio, Ravi P. Nargund, Peter H. Dobbelaar, Liangqin Guo, Kwei-Lan Tsao, Janet S. Kerr, Bei Zhang, Zhong Lai, Patricia R. Bunting, Shrenik K. Shah, Raman K. Bakshi, Qingmei Hong, Hongbo Qi, Guillermo Fernandez, Mikhail Reibarkh, Qing Shao, Quang Truong, Koppara Samuel, Jian Liu, Sylvia Volksdorf, Zhixiong Ye, Yun-Ping Zhou, Margaret Wu, Cai Li, Stan Mitelman, Andrew D. Howard, Wu Du, Maria E. Trujillo, George J. Eiermann, Shuwen He, Vijay Bhasker G. Reddy, Tianying Jian, Pierre Morissette, Patrick Fitzgerald, Dorina Trusca, Sharon Tong, and William K. Hagmann

Subjects

biology, business.industry, Organic Chemistry, hERG, Antagonist, In vitro toxicology, Type 2 diabetes, Pharmacology, medicine.disease, Biochemistry, QT interval, Somatostatin, Drug Discovery, biology.protein, Medicine, cardiovascular diseases, Receptor, business, Antagonism

Abstract

Antagonism of somatostatin subtype receptor 3 (sstr3) has emerged as a potential treatment of Type 2 diabetes. Unfortunately, the development of our first preclinical candidate, MK-4256, was discontinued due to a dose-dependent QTc (QT interval corrected for heart rate) prolongation observed in a conscious cardiovascular (CV) dog model. As the fate of the entire program rested on resolving this issue, it was imperative to determine whether the observed QTc prolongation was associated with hERG channel (the protein encoded by the human Ether-à-go-go-Related Gene) binding or was mechanism-based as a result of antagonizing sstr3. We investigated a structural series containing carboxylic acids to reduce the putative hERG off-target activity. A key tool compound, 3A, was identified from this SAR effort. As a potent sstr3 antagonist, 3A was shown to reduce glucose excursion in a mouse oGTT assay. Consistent with its minimal hERG activity from in vitro assays, 3A elicited little to no effect in an anesthetized, vagus-intact CV dog model at high plasma drug levels. These results afforded the critical conclusion that sstr3 antagonism is not responsible for the QTc effects and therefore cleared a path for the program to progress.

Published

2014

19. Discovery and Optimization of a Novel Triazole Series of GPR142 Agonists for the Treatment of Type 2 Diabetes

Author

John S. Debenham, Dann L. Parker, Birgit T. Priest, Ravi P. Nargund, Feroze Ujjainwalla, Randal M. Bugianesi, Michele Pachanski, Liangqin Guo, William K. Hagmann, George J. Eiermann, Yi Zang, Ramzi F. Sweis, Andrew D. Howard, Jenna L. Terebetski, Melissa Kirkland, Yue Feng, Gino Salituro, Derun Li, Christopher Joseph Sinz, Stan Mitelman, Maria E. Trujillo, Scott D. Edmondson, Karen H. Dingley, Jin Shang, Nicole Buist, Xiaofang Li, Weiguo Liu, Mary Ann Powles, Terri M. Kelly, and Edward C. Sherer

Subjects

0301 basic medicine, medicine.medical_specialty, Organic Chemistry, Triazole, Type 2 Diabetes Mellitus, Glucose excursion, Type 2 diabetes, Metabolic stability, medicine.disease, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Endocrinology, chemistry, Internal medicine, Drug Discovery, medicine, Deficient mouse, Potency, Lead compound

Abstract

GPR142 has been identified as a potential glucose-stimulated insulin secretion (GSIS) target for the treatment of type 2 diabetes mellitus (T2DM). A class of triazole GPR142 agonists was discovered through a high throughput screen. The lead compound 4 suffered from poor metabolic stability and poor solubility. Lead optimization strategies to improve potency, efficacy, metabolic stability, and solubility are described. This optimization led to compound 20e, which showed significant reduction of glucose excursion in wild-type but not in GPR142 deficient mice in an oral glucose tolerance test (oGTT) study. These studies provide strong evidence that reduction of glucose excursion through treatment with 20e is GPR142-mediated, and GPR142 agonists could be used as a potential treatment for type 2 diabetes.

Published

2016

20. The ESRD Quality Incentive Program: The Current Limitations of Evidence and Data to Develop Measures, Drive Improvement, and Incentivize Outcomes

Author

Andrew D. Howard and Louis H. Diamond

Subjects

Process management, Health information technology, business.industry, media_common.quotation_subject, 030232 urology & nephrology, 030204 cardiovascular system & hematology, Payment, Clinical decision support system, Quality Improvement, Centers for Medicare and Medicaid Services, U.S, United States, 03 medical and health sciences, 0302 clinical medicine, Nephrology, Health care, Medicine, Humans, Kidney Failure, Chronic, Incentive program, Quality (business), business, Medicaid, Delivery of Health Care, Strengths and weaknesses, media_common

Abstract

This article describes the current state of facilitating the integration of evidence into practice to support initiatives focused on patients with ESRD. We will use the Centers for Medicare and Medicaid Services (CMS) ESRD Quality Incentive Program (QIP) as an example, including a description of the health information infrastructure needed to support the translation of evidence into practice and some of the challenges encountered. The process from the generation of evidence to integration of this evidence into practice includes policy development leading to clinical practice guidelines, clinical performance measures, and clinical decision support tools. The ESRD QIP is the most mature program outside the hospital initiatives in the CMS Quality Payment Program and currently contains 16 measures. ESRD data to support these measures are aggregated at the dialysis facility level and reported through the CMS Consolidated Renal Operations in a Web-enabled Network (CROWNWeb) and the Centers for Disease Control and Prevention using the National Healthcare Safety Network. We review these measures and the health information infrastructure used to report the data, focusing on the inherent strengths and weaknesses of the ESRD QIP along with opportunities for improvement of the program.

Published

2016

21. Discovery of benzofuran propanoic acid GPR120 agonists: From uHTS hit to mechanism-based pharmacodynamic effects

Author

Christopher Joseph Sinz, Feroze Ujjainwalla, Joel Mane, Eric N. Johnson, John Cummings, Jerry Di Salvo, Michele Pachanski, Michael A. Plotkin, Joanna Pols, Taro E. Akiyama, Andrew D. Howard, Matthew Lombardo, James R. Tata, Maria Madeira, Ying Lei, Wayne M. Geissler, Victor N. Uebele, Michael F.A. Finley, Clare London, Candice Alleyne, Thomas Roussel, Kate Bender, Dennis Leung, Bahanu Habulihaz, Mary Ann Powles, Melissa Kirkland, Dorina Trusca, and Alejandro Crespo

Subjects

0301 basic medicine, Blood Glucose, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Pharmacology, 01 natural sciences, Biochemistry, Receptors, G-Protein-Coupled, 03 medical and health sciences, chemistry.chemical_compound, Mice, Pharmacokinetics, In vivo, Free fatty acid receptor 1, Drug Discovery, Potency, Animals, Humans, Hypoglycemic Agents, Benzofuran, Molecular Biology, Benzofurans, chemistry.chemical_classification, 010405 organic chemistry, Organic Chemistry, Fatty acid, GPR120, 0104 chemical sciences, High-Throughput Screening Assays, 030104 developmental biology, Propanoic acid, chemistry, Diabetes Mellitus, Type 2, Molecular Medicine, Propionates

Abstract

The transformation of an aryloxybutanoic acid ultra high-throughput screening (uHTS) hit into a potent and selective series of G-protein coupled receptor 120 (GPR120) agonists is reported. uHTS hit 1 demonstrated an excellent rodent pharmacokinetic profile and selectivity over the related fatty acid receptor GPR40, but only modest GPR120 potency. Optimization of the "left-hand" aryl group led to compound 6, which demonstrated a GPR120 mechanism-based pharmacodynamic effect in a mouse oral glucose tolerance test (oGTT). Further optimization gave rise to the benzofuran propanoic acid series (exemplified by compound 37), which demonstrated acute mechanism-based pharmacodynamic effects. The combination of in vivo efficacy and attractive rodent pharmacodynamic profiles suggests compounds generated from this series may afford attractive candidates for the treatment of Type 2 diabetes.

Published

2016

22. The Role of Voltage-Gated Potassium Channels Kv2.1 and Kv2.2 in the Regulation of Insulin and Somatostatin Release from Pancreatic Islets

Author

Yusheng Xiong, Bei B. Zhang, Mette V. Jensen, George J. Eiermann, Maria L. Garcia, Christopher B. Newgard, Andrew D. Howard, Nancy A. Thornberry, Lan Ge, Xiaoyan Nina Li, Gregory J. Kaczorowski, Michael Wagner, Yun-Ping Zhou, Aleksandr Petrov, Hans E. Hohmeier, and James Herrington

Subjects

Adult, Male, endocrine system, medicine.medical_specialty, Patch-Clamp Techniques, medicine.medical_treatment, Spider Venoms, Biology, Arthropod Proteins, Mice, Young Adult, Shab Potassium Channels, Insulin-Secreting Cells, Internal medicine, Insulin Secretion, Potassium Channel Blockers, medicine, Animals, Humans, Insulin, Receptors, Somatostatin, education, Cells, Cultured, Mice, Knockout, Pharmacology, Delta cell, geography, education.field_of_study, geography.geographical_feature_category, Somatostatin receptor-5, Pancreatic islets, Voltage-gated potassium channel, Middle Aged, Islet, Electrophysiological Phenomena, Insulin oscillation, Mice, Inbred C57BL, Glucose, Somatostatin, Endocrinology, medicine.anatomical_structure, Benzamides, Molecular Medicine, Female, Peptides, Protein Binding

Abstract

The voltage-gated potassium channels Kv2.1 and Kv2.2 are highly expressed in pancreatic islets, yet their contribution to islet hormone secretion is not fully understood. Here we investigate the role of Kv2 channels in pancreatic islets using a combination of genetic and pharmacologic approaches. Pancreatic β-cells from Kv2.1(-/-) mice possess reduced Kv current and display greater glucose-stimulated insulin secretion (GSIS) relative to WT β-cells. Inhibition of Kv2.x channels with selective peptidyl [guangxitoxin-1E (GxTX-1E)] or small molecule (RY796) inhibitors enhances GSIS in isolated wild-type (WT) mouse and human islets, but not in islets from Kv2.1(-/-) mice. However, in WT mice neither inhibitor improved glucose tolerance in vivo. GxTX-1E and RY796 enhanced somatostatin release in isolated human and mouse islets and in situ perfused pancreata from WT and Kv2.1(-/-) mice. Kv2.2 silencing in mouse islets by adenovirus-small hairpin RNA (shRNA) specifically enhanced islet somatostatin, but not insulin, secretion. In mice lacking somatostatin receptor 5, GxTX-1E stimulated insulin secretion and improved glucose tolerance. Collectively, these data show that Kv2.1 regulates insulin secretion in β-cells and Kv2.2 modulates somatostatin release in δ-cells. Development of selective Kv2.1 inhibitors without cross inhibition of Kv2.2 may provide new avenues to promote GSIS for the treatment of type 2 diabetes.

Published

2012

23. Duodenal-jejunal bypass surgery induces hepatic lipidomic alterations associated with ameliorated hepatic steatosis in mice

Author

Jin, Shang, Jose M, Castro-Perez, Xiaolan, Shen, Yonghua, Zhu, Haiying, Liu, Ying, Qian, Stephen, Previs, Andrew D, Howard, Mark, Erion, David E, Kelley, and Liangsu, Wang

Subjects

Blood Glucose, Fatty Liver, Male, Mice, Jejunum, Duodenum, Gastric Bypass, Animals, Bariatric Surgery, Insulin Resistance

Abstract

Bariatric surgery induces weight loss and improvement of insulin resistance; one aspect of both is an amelioration of hepatic steatosis. This study was undertaken to assess the changes in the hepatic lipidome after duodenal-jejunal bypass (DJB) surgery.A DJB surgical model was developed and characterized in diet-induced obese mice. In comparison with sham-operated mice, an unbiased lipidomic profiling of hepatic lipids was performed together with measurements of gene expression within key pathways of hepatic lipid metabolism.In the liver of DJB mice, a dramatic reduction (by 77%) in hepatic triacylglycerols was observed. Global lipidomic profiling identified marked decreases of triacylglycerols comprised of medium length fatty acids and with low double bond content. Specific diacylglycerol species were also among the most dramatic decreases in hepatic lipids, whereas lysophosphatidic acids and phosphatidic acids were increased. Expression of fatty acid transporter and lipogenic genes was down-regulated.From in-depth analysis of hepatic lipid composition, specific lipid intermediates were identified that are preferentially changed following DJB surgery. These changes were most likely due to DJB-induced weight loss, and only further studies will be able to distinguish weight loss-dependent from weight loss-independent changes.

Published

2015

24. SAR exploration at the C-3 position of tetrahydro-β-carboline sstr3 antagonists

Author

Janet Kerr, Gary G. Chicchi, Margaret Wu, Cai Li, Shuwen He, Vijay Bhasker G. Reddy, Sharon Tong, William K. Hagmann, Patrick Fitzgerald, Guillermo Fernandez, Andrew D. Howard, Tianying Jian, Zhe Feng, Raman K. Bakshi, Dorina Trusca, Peter H. Dobbelaar, Donald Nelson, Mikhail Reibarkh, Qing Shao, Liangqin Guo, Yun-Ping Zhou, Ravi P. Nargund, Kwei-Lan Tsao, Edward C. Sherer, Stan Mitelman, Pierre Morissette, Maria E. Trujillo, Quang Truong, Zhixiong Ye, James D. Dellureficio, Hongbo Qi, Melissa Lin, Shrenik K. Shah, Sylvia Volksdorf, Jian Liu, Qingmei Hong, Koppara Samuel, Alexander Pasternak, George J. Eiermann, Patricia B. Bunting, Wu Du, and Bei B. Zhang

Subjects

QTC PROLONGATION, congenital, hereditary, and neonatal diseases and abnormalities, Clinical Biochemistry, hERG, Pharmaceutical Science, Pharmacology, 010402 general chemistry, 01 natural sciences, Biochemistry, Mice, Structure-Activity Relationship, Dogs, Drug Discovery, Animals, Humans, cardiovascular diseases, Receptors, Somatostatin, Molecular Biology, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Antagonist, 0104 chemical sciences, Rats, biology.protein, Molecular Medicine, Antagonism, Carbolines

Abstract

MK-4256, a tetrahydro-β-carboline sstr3 antagonist, was discontinued due to a cardiovascular (CV) adverse effect observed in dogs. Additional investigations revealed that the CV liability (QTc prolongation) was caused by the hERG off-target activity of MK-4256 and was not due to sstr3 antagonism. In this Letter, we describe our extensive SAR effort at the C3 position of the tetrahydro-β-carboline structure. This effort resulted in identification of 5-fluoro-pyridin-2-yl as the optimal substituent on the imidazole ring to balance sstr3 activity and the hERG off-target liability.

Published

2015

25. Discovery of substituted biphenyl imidazoles as potent, bioavailable bombesin receptor subtype-3 agonists

Author

Marc L. Reitman, Cheng Guo, Theresa M. Kelly, Constantin Tamvakopoulos, Joseph M. Metzger, Tianying Jian, Howard Y. Chen, Arthur A. Patchett, Oksana C. Palyha, Alison M. Strack, Allan J. Goodman, Ravi P. Nargund, Peter H. Dobbelaar, Yanqing Kan, Mark Hadden, Larry Yet, Peter R. Guzzo, Qianping Peng, Linus S. Lin, Shuwen He, Lauren P. Shearman, Alan J. Henderson, Carina P. Tan, Sargent Bruce J, Xiao-Ming Guan, Scott D. Feighner, Iyassu K. Sebhat, Jie Pan, Jian Liu, Donald J. Marsh, Matthew J. Wyvratt, Andrew D. Howard, and Megan Ruenz

Subjects

Agonist, medicine.drug_class, Clinical Biochemistry, Biological Availability, Pharmaceutical Science, Pharmacology, Biochemistry, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Animals, Humans, Potency, Structure–activity relationship, Molecular Biology, Biphenyl, Chemistry, Drug discovery, fungi, Organic Chemistry, Imidazoles, Rats, Bombesin receptor, Bioavailability, Receptors, Bombesin, Molecular Medicine, Bombesin Receptor Subtype-3

Abstract

We report SAR studies on a novel non-peptidic bombesin receptor subtype-3 (BRS-3) agonist lead series derived from high-throughput screening hit RY-337. This effort led to the discovery of compound 22e with significantly improved potency at both rodent and human BRS-3.

Published

2010

26. Discovery of 5-aryloxy-2,4-thiazolidinediones as potent GPR40 agonists

Author

Aleksandr Petrov, Lihu Yang, Ralph T. Mosley, Carina P. Tan, George J. Eiermann, Joel P. Berger, Sanjeev Kumar, Peter T. Meinke, Eric Chang, Sander G. Mills, Nancy A. Thornberry, Cheng Tang, Monica Einstein, Eric Cline, Yun-Ping Zhou, Min Ge, Songnian Lin, Andrew D. Howard, Yue Feng, Changyou Zhou, Taro E. Akiyama, and Gino Salituro

Subjects

Agonist, endocrine system, medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Receptors, G-Protein-Coupled, Mice, Structure-Activity Relationship, Pharmacokinetics, Oral administration, Internal medicine, Free fatty acid receptor 1, Diabetes mellitus, Drug Discovery, medicine, Animals, Molecular Biology, Pancreatic hormone, Mice, Knockout, Glucose tolerance test, medicine.diagnostic_test, Chemistry, Insulin, Organic Chemistry, medicine.disease, Endocrinology, Molecular Medicine, Thiazolidinediones, Protein Binding

Abstract

Systematic structure-activity relationship (SAR) studies of a screening lead led to the discovery of a series of thiazolidinediones (TZDs) as potent GPR40 agonists. Among them, compound C demonstrated an acute mechanism-based glucose-lowering in an intraperitoneal glucose tolerance test (IPGTT) in lean mice, while no effects were observed in GPR40 knock-out mice.

Published

2010

27. Obesity and genetics regulate microRNAs in islets, liver, and adipose of diabetic mice

Author

Eric E. Schadt, Danielle M. Greenawalt, Ping Wang, Elias Chaibub Neto, John S. Tsang, Jin Shang, Enpeng Zhao, Jee-Young Moon, Andrew D. Howard, Brian S. Yandell, Michele A. Cleary, Nancy A. Thornberry, Christina Kendziorski, Yun-Ping Zhou, Angie T. Oler, Kathryn L. Schueler, Alan D. Attie, Robert R. Kleinhanz, I-Ming Wang, Irena Ivanovska, Mark P. Keller, Mary E. Rabaglia, YounJeong Choi, Pek Yee Lum, Bei B. Zhang, and Donnie S. Stapleton

Subjects

Male, Gene Dosage, Mice, Obese, Adipose tissue, Biology, Article, Islets of Langerhans, Mice, Insulin resistance, microRNA, Gene expression, Genetics, medicine, Animals, Humans, Gene silencing, Obesity, Regulation of gene expression, Gene Expression Profiling, Pancreatic islets, medicine.disease, Gene expression profiling, Disease Models, Animal, MicroRNAs, medicine.anatomical_structure, Adipose Tissue, Diabetes Mellitus, Type 2, Gene Expression Regulation, Liver, Female

Abstract

Type 2 diabetes results from severe insulin resistance coupled with a failure of b cells to compensate by secreting sufficient insulin. Multiple genetic loci are involved in the development of diabetes, although the effect of each gene on diabetes susceptibility is thought to be small. MicroRNAs (miRNAs) are noncoding 19-22-nucleotide RNA molecules that potentially regulate the expression of thousands of genes. To understand the relationship between miRNA regulation and obesity-induced diabetes, we quantitatively profiled approximately 220 miRNAs in pancreatic islets, adipose tissue, and liver from diabetes-resistant (B6) and diabetes-susceptible (BTBR) mice. More than half of the miRNAs profiled were expressed in all three tissues, with many miRNAs in each tissue showing significant changes in response to genetic obesity. Furthermore, several miRNAs in each tissue were differentially responsive to obesity in B6 versus BTBR mice, suggesting that they may be involved in the pathogenesis of diabetes. In liver there were approximately 40 miRNAs that were downregulated in response to obesity in B6 but not BTBR mice, indicating that genetic differences between the mouse strains play a critical role in miRNA regulation. In order to elucidate the genetic architecture of hepatic miRNA expression, we measured the expression of miRNAs in genetically obese F2 mice. Approximately 10% of the miRNAs measured showed significant linkage (miR-eQTLs), identifying loci that control miRNA abundance. Understanding the influence that obesity and genetics exert on the regulation of miRNA expression will reveal the role miRNAs play in the context of obesity-induced type 2 diabetes.

Published

2009

28. Phosphodiesterase 3 and 4 comprise the major cAMP metabolizing enzymes responsible for insulin secretion in INS-1 (832/13) cells and rat islets

Author

Chris M. Thompson, Weizhen Wu, Michael Wu, Joseph A. Mancini, Yun-Ping Zhou, Deena Waddleton, Jing Li, Andrew D. Howard, Yue Feng, and Nancy A. Thornberry

Subjects

medicine.medical_specialty, Phosphodiesterase 3, Biology, Biochemistry, Rats, Sprague-Dawley, Islets of Langerhans, chemistry.chemical_compound, Cell Line, Tumor, Internal medicine, Insulin Secretion, Cyclic AMP, medicine, Animals, Insulin, Secretion, RNA, Messenger, Pharmacology, Gene knockdown, Phosphoric Diester Hydrolases, Pancreatic islets, Trequinsin, Rat Insulinoma, Phosphodiesterase, Rats, Cell biology, Glucose, Endocrinology, medicine.anatomical_structure, chemistry, PDE10A

Abstract

cAMP is a key modulator for glucose-dependent insulin secretion (GDIS). Members of the phosphodiesterase (PDEs) gene family regulate intracellular levels of cAMP by hydrolyzing cAMP to the corresponding inactive 5'AMP derivative. These studies examined the expression and function of all 18 cAMP-specific PDEs in the rat insulinoma derived INS-1 (832/13) cell and isolated rat islets using quantitative PCR and siRNA-mediated gene-specific knockdown. PDE1C, PDE3B, PDE4C, PDE8B, PDE10A, and PDE11A were significantly expressed in rat islets and INS-1 (832/13) cells at the mRNA level. PDE1C, PDE10A and PDE11A were also expressed in brain, along with PDE3B, PDE4C and PDE8B which were also highly expressed in liver, and PDE3B was present in adipose tissue and PDE4C in skeletal muscle. siRNA mediated knockdown of PDE1C, PDE3B, PDE8B and PDE4C, but not PDE10A and PDE11A, significantly enhanced GDIS in rat INS-1 (832/13) cells. Also, selective inhibitors of PDE3 (trequinsin) and PDE4 (roflumilast and L-826,141) significantly augmented GDIS in both INS-1 (832/13) cells and rat islets. The combination of PDE3 and PDE4 selective inhibitors demonstrate that these enzymes comprise a significant proportion of the cAMP metabolizing activity in INS-1 cells and rat islets.

Published

2008

29. Selective Small-Molecule Agonists of G Protein–Coupled Receptor 40 Promote Glucose-Dependent Insulin Secretion and Reduce Blood Glucose in Mice

Author

Lihu Yang, Ralph T. Mosley, Peter T. Meinke, Yue Feng, Nancy A. Thornberry, Monica Einstein, Carina P. Tan, George J. Eiermann, Changyou Zhou, Sander G. Mills, Sanjeev Kumar, Songnian Lin, Andrew D. Howard, Joel P. Berger, Aleksandr Petrov, Yun Ping Zhou, Gino Salituro, and Taro E. Akiyama

Subjects

Blood Glucose, Male, Agonist, endocrine system, medicine.medical_specialty, medicine.drug_class, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, CHO Cells, Inositol 1,4,5-Trisphosphate, Type 2 diabetes, Fatty Acids, Nonesterified, In Vitro Techniques, Biology, Cell Line, Diabetes Mellitus, Experimental, Receptors, G-Protein-Coupled, Islets of Langerhans, Mice, Cricetulus, Pregnancy, Cricetinae, Internal medicine, Free fatty acid receptor 1, Diabetes mellitus, Insulin Secretion, Internal Medicine, medicine, Animals, Humans, Insulin, Obesity, Rats, Wistar, Receptor, Pancreatic hormone, Mice, Knockout, geography, geography.geographical_feature_category, Fatty Acids, Islet, medicine.disease, Dietary Fats, Pharmacology and Therapeutics, Rats, Mice, Inbred C57BL, Endocrinology, Animals, Newborn, Female

Abstract

OBJECTIVE— Acute activation of G protein–coupled receptor 40 (GPR40) by free fatty acids (FFAs) or synthetic GPR40 agonists enhances insulin secretion. However, it is still a matter of debate whether activation of GPR40 would be beneficial for the treatment of type 2 diabetes, since chronic exposure to FFAs impairs islet function. We sought to evaluate the specific role of GPR40 in islets and its potential as a therapeutic target using compounds that specifically activate GPR40. RESEARCH DESIGN AND METHODS— We developed a series of GPR40-selective small-molecule agonists and studied their acute and chronic effects on glucose-dependent insulin secretion (GDIS) in isolated islets, as well as effects on blood glucose levels during intraperitoneal glucose tolerance tests in wild-type and GPR40 knockout mice (GPR40−/−). RESULTS— Small-molecule GPR40 agonists significantly enhanced GDIS in isolated islets and improved glucose tolerance in wild-type mice but not in GPR40−/− mice. While a 72-h exposure to FFAs in tissue culture significantly impaired GDIS in islets from both wild-type and GPR40−/− mice, similar exposure to the GPR40 agonist did not impair GDIS in islets from wild-type mice. Furthermore, the GPR40 agonist enhanced insulin secretion in perfused pancreata from neonatal streptozotocin-induced diabetic rats and improved glucose levels in mice with high-fat diet–induced obesity acutely and chronically. CONCLUSIONS— GPR40 does not mediate the chronic toxic effects of FFAs on islet function. Pharmacological activation of GPR40 may potentiate GDIS in humans and be beneficial for overall glucose control in patients with type 2 diabetes.

Published

2008

30. Novel Ghrelin Assays Provide Evidence for Independent Regulation of Ghrelin Acylation and Secretion in Healthy Young Men

Author

Ralf Nass, Mary C. Oliveri, Michael O. Thorner, Andrew D. Howard, Bruce D. Gaylinn, Catherine E. Prudom, H. Mario Geysen, Michael L. Johnson, David A. Gordon, Derrick R. Witcher, Paula P. Veldhuis, Suzan S. Pezzoli, and Jianhua Liu

Subjects

Adult, Male, medicine.medical_specialty, Acylation, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Clinical Biochemistry, Enzyme-Linked Immunosorbent Assay, Context (language use), Peptide hormone, Biology, Sensitivity and Specificity, Biochemistry, Endocrinology, Internal medicine, medicine, Humans, media_common, Immune Sera, digestive, oral, and skin physiology, Biochemistry (medical), Appetite, Fasting, Metabolism, medicine.disease, Obesity, Ghrelin, Butyrylcholinesterase, Original Article, Sample collection, Body mass index, hormones, hormone substitutes, and hormone antagonists

Abstract

Context: Ghrelin, an acylated peptide hormone secreted from the gut, regulates appetite and metabolism. Elucidating its pattern of secretion in the fed and fasted states is important in the face of the obesity epidemic. Objective: Our objective was to examine changes in circulating ghrelin and des-acyl ghrelin in response to meals and fasting using newly developed two-site sandwich assays and sample preservation protocols to allow specific detection of full-length forms. Design: Ten-minute sampling was done for 26.5 h during a fed admission with standardized meals and on a separate admission during the final 24 h of a 61.5-h fast and continuing for 2.5 h after terminating the fast. Setting: The study was conducted at the University Hospital General Clinical Research Center. Participants: Eight male volunteers participated, mean ± sd age 24.5 ± 3.7 yr and body mass index 24 ± 2.1 kg/m2. Main Outcome Measures: Ten-minute sampling profiles were assessed for ghrelin and des-acyl ghrelin, fed and fasting. Results: In the fed state, ghrelin and des-acyl ghrelin showed similar dynamics; both were sharply inhibited by meals and increased at night. During fasting, ghrelin decreased to nadir levels seen postprandially, and des-acyl ghrelin remained near peak levels seen preprandially. Total full-length ghrelin (acyl plus des-acyl) levels remained unchanged. Conclusions: Meals inhibited secretion of both ghrelin and des-acyl ghrelin, yet long-term fasting inhibited acylation but not total secretion. Acylation may be regulated independently of secretion by nutrient availability in the gut or by esterases that cleave the acyl group. These studies highlight the importance of stringent conditions for sample collection and evaluation of full-length ghrelin and des-acyl ghrelin using specific two-site assays.

Published

2008

31. Identification of Glucose-Dependant Insulin Secretion Targets in Pancreatic β Cells by Combining Defined-Mechanism Compound Library Screening and siRNA Gene Silencing

Author

Sarah Horwitz, Kevin T. Chapman, Chris M. Thompson, Euan Macintyre, Nancy A. Thornberry, Jing Li, Jin Shang, Yun-Ping Zhou, Andrew D. Howard, John R. Thompson, Yue Feng, and Weizhen Wu

Subjects

medicine.medical_treatment, Biology, Pharmacology, Biochemistry, Receptors, Dopamine, Analytical Chemistry, Rats, Sprague-Dawley, RNA interference, Insulin-Secreting Cells, Insulin Secretion, medicine, Animals, Insulin, Gene silencing, Gene Silencing, RNA, Messenger, RNA, Small Interfering, Receptor, Cells, Cultured, Gene Library, Gene knockdown, Adenosine, Rats, Glucose, Drug development, Dopamine receptor, Dopamine Antagonists, Molecular Medicine, Metabolic Networks and Pathways, Biotechnology, medicine.drug

Abstract

Identification and validation of novel drug targets continues to be a major bottleneck in drug development, particularly for polygenic complex diseases such as type 2 diabetes. Here, the authors describe an approach that allows researchers to rapidly identify and validate potential drug targets by combining chemical tools and RNA interference technology. As a proof-of-concept study, the known mechanism Sigma LOPAC library was used to screen for glucose-dependent insulin secretion (GDIS) in INS-1 832/13 cells. In addition to several mechanisms that are known to regulate GDIS (such as cyclic adenosine monophosphate-specific phosphodiesterases, adrenoceptors, and Ca(2+) channels), the authors find that several of the dopamine receptor (DRD) antagonists significantly enhance GDIS, whereas DRD agonists profoundly inhibit GDIS. Subsequent siRNA studies in the same cell line indicate that knockdown of DRD2 enhanced GDIS. Furthermore, selective DRD2 antagonists and agonists also enhance or suppress, respectively, GDIS in isolated rat islets. The data support that the approach described here offers a rapid and effective way for target identification and validation.

Published

2008

32. Induction of miR-132 and miR-212 Expression by Glucagon-Like Peptide 1 (GLP-1) in Rodent and Human Pancreatic β-Cells

Author

Yong Wang, Mary E. Rabaglia, Xiaolan Shen, Andrew D. Howard, Yue Feng, Christopher B. Newgard, Hans E. Hohmeier, Mufaddal S. Soni, Heather Zhou, Jing Li, Alan D. Attie, Nancy A. Thornberry, Mark P. Keller, Jin Shang, and Yun Ping Zhou

Subjects

medicine.medical_specialty, endocrine system, medicine.medical_treatment, Biology, Rats, Sprague-Dawley, miR-132, Mice, Endocrinology, Glucagon-Like Peptide 1, Internal medicine, Cell Line, Tumor, Insulin-Secreting Cells, Insulin Secretion, medicine, Cyclic AMP, Animals, Humans, Insulin, Protein kinase A, Molecular Biology, Protein Kinase Inhibitors, Original Research, Sulfonamides, Activator (genetics), General Medicine, Isoquinolines, Glucagon-like peptide-1, Cyclic AMP-Dependent Protein Kinases, Protein Kinase A Inhibitor, Rats, Mice, Inbred C57BL, MicroRNAs, medicine.anatomical_structure, Glucose, Diabetes Mellitus, Type 2, Cell culture, Pancreas

Abstract

Better understanding how glucagon-like peptide 1 (GLP-1) promotes pancreatic β-cell function and/or mass may uncover new treatment for type 2 diabetes. In this study, we investigated the potential involvement of microRNAs (miRNAs) in the effect of GLP-1 on glucose-stimulated insulin secretion. miRNA levels in INS-1 cells and isolated rodent and human islets treated with GLP-1 in vitro and in vivo (with osmotic pumps) were measured by real-time quantitative PCR. The role of miRNAs on insulin secretion was studied by transfecting INS-1 cells with either precursors or antisense inhibitors of miRNAs. Among the 250 miRNAs surveyed, miR-132 and miR-212 were significantly up-regulated by GLP-1 by greater than 2-fold in INS-1 832/3 cells, which were subsequently reproduced in freshly isolated rat, mouse, and human islets, as well as the islets from GLP-1 infusion in vivo in mice. The inductions of miR-132 and miR-212 by GLP-1 were correlated with cAMP production and were blocked by the protein kinase A inhibitor H-89 but not affected by the exchange protein activated by cAMP activator 8-pCPT-2'-O-Me-cAMP-AM. GLP-1 failed to increase miR-132 or miR-212 expression levels in the 832/13 line of INS-1 cells, which lacks robust cAMP and insulin responses to GLP-1 treatment. Overexpression of miR-132 or miR-212 significantly enhanced glucose-stimulated insulin secretion in both 832/3 and 832/13 cells, and restored insulin responses to GLP-1 in INS-1 832/13 cells. GLP-1 increases the expression of miRNAs 132 and 212 via a cAMP/protein kinase A-dependent pathway in pancreatic β-cells. Overexpression of miR-132 or miR-212 enhances glucose and GLP-1-stimulated insulin secretion.

Published

2015

33. Discovery of substituted (4-phenyl-1H-imidazol-2-yl)methanamine as potent somatostatin receptor 3 agonists

Author

Kwei-Lan Tsao, Derun Li, Liangqing Guo, Richard G. Ball, Zhicai Wu, David X. Yang, Gary G. Chicchi, William K. Hagmann, Quang Tuang, Dorina Trusca, Yang Yu, Shuwen He, Qingmei Hong, Ravi P. Nargund, Edward C. Sherer, Yun-Ping Zhou, Zhong Lai, and Andrew D. Howard

Subjects

Agonist, medicine.drug_class, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Biochemistry, Methylamines, Structure-Activity Relationship, Drug Discovery, medicine, Somatostatin receptor 3, Molecular Medicine, Humans, Receptors, Somatostatin, Antagonism, Molecular Biology

Abstract

We report SAR studies on a novel non-peptidic somatostatin receptor 3 (SSTR3) agonist lead series derived from (4-phenyl-1H-imidazol-2-yl)methanamine. This effort led to the discovery of a highly potent low molecular weight SSTR3 agonist 5c (EC50=5.2 nM, MW=359). The results from molecular overlays of 5c onto the L-129 structure indicate good alignment, and two main differences of the proposed overlays of the antagonist MK-4256 onto the conformation of 5c lead to inversion of antagonism to agonism.

Published

2015

34. The IL-1β Converting Enzyme as a Therapeutic Target

Author

Nancy A. Thornberry, Matthew J. Kostura, Andrew D. Howard, Susan M. Molineaux, Kevin T. Chapman, Douglas K. Miller, and Jimmy R. Calaycay

Subjects

chemistry.chemical_classification, business.industry, Chemistry, General Neuroscience, Caspase 1, Molecular Sequence Data, Metalloendopeptidases, Computational biology, General Biochemistry, Genetics and Molecular Biology, Text mining, Enzyme, History and Philosophy of Science, Animals, Humans, Amino Acid Sequence, business, Interleukin-1

Published

2006

35. 2-Aminoquinoline melanin-concentrating hormone (MCH)1R antagonists

Author

Mark T. Goulet, Lex H.T. Van der Ploeg, Junying Wang, Scott D. Feighner, Jonathan R. Young, Oksana C. Palyha, Douglas J. MacNeil, Cherilyn Turner, Donna L. Hreniuk, Ronsar Eid, Andreas W. Sailer, Robert J. DeVita, Xinchun Tong, Danny Chaung, Myle Hoang, Lauren P. Shearman, Carina P. Tan, Peter Lin, Jie Pan, Sloan Stribling, Alison M. Strack, Andrew D. Howard, Ramon E. Camacho, and Jinlong Jiang

Subjects

Male, Quinuclidines, Melanin-concentrating hormone, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Binding, Competitive, Biochemistry, Chemical synthesis, Rats, Sprague-Dawley, Aminoquinoline, Eating, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Drug Discovery, medicine, Animals, Humans, Receptors, Somatostatin, Molecular Biology, Molecular Structure, Organic Chemistry, Quinoline, Antagonist, Stereoisomerism, In vitro, Rats, chemistry, Quinolines, Molecular Medicine, Biological Assay, Energy Metabolism, medicine.drug

Abstract

A series of 2-aminoquinoline compounds was prepared and evaluated in MCH1R binding and functional antagonist assays. Small dialkyl, methylalkyl, methylcycloalkyl, and cyclic amines were tolerated at the quinoline 2-position. The in vivo efficacy of compound 12 was explored and compared to that of a related inactive analog to determine their effects on food intake and body weight in rodents.

Published

2006

36. 4-Aminoquinoline melanin-concentrating hormone 1-receptor (MCH1R) antagonists

Author

Lex H.T. Van der Ploeg, Mark T. Goulet, Lehua Chang, Carina P. Tan, Donna L. Hreniuk, Andreas W. Sailer, Scott D. Feighner, Jinlong Jiang, Robert J. DeVita, Jie Pan, Peter Lin, Oksana C. Palyha, Douglas J. MacNeil, Nancy R. Morin, Myle Hoang, and Andrew D. Howard

Subjects

Melanin-concentrating hormone, medicine.drug_class, Stereochemistry, High-throughput screening, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Carboxamide, In Vitro Techniques, Binding, Competitive, Biochemistry, Chemical synthesis, Cell Line, Structure-Activity Relationship, chemistry.chemical_compound, mental disorders, Drug Discovery, medicine, Humans, Receptors, Somatostatin, Receptor, Molecular Biology, Molecular Structure, Organic Chemistry, Antagonist, Stereoisomerism, Combinatorial chemistry, In vitro, chemistry, 4-Aminoquinoline, Aminoquinolines, Molecular Medicine

Abstract

Structure-activity relationships of a 4-aminoquinoline MCH1R antagonist lead series were explored by synthesis of analogs with modifications at the 2-, 4-, and 6-positions of the original HTS hit. Improvements to the original screening lead included lipophilic groups at the 2-position and biphenyl, cyclohexyl phenyl, and hydrocinnamyl carboxamides at the 6-position. Modifications of the 4-amino group were not well tolerated.

Published

2006

37. Chronic Inhibition of Dipeptidyl Peptidase-4 With a Sitagliptin Analog Preserves Pancreatic β-Cell Mass and Function in a Rodent Model of Type 2 Diabetes

Author

Cai Li, James Mu, Nancy A. Thornberry, Yue Feng, Yun-Ping Zhou, Zhihua Li, Lan Zhu, Andrew D. Howard, Bei B. Zhang, John Woods, David E. Moller, Ranabir Sinha Roy, and Emanuel Zycband

Subjects

Blood Glucose, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Incretin, Type 2 diabetes, Biology, Sitagliptin Phosphate, Islets of Langerhans, Mice, Insulin-Secreting Cells, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Animals, Hypoglycemic Agents, Insulin, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Dipeptidyl peptidase-4, Dyslipidemias, Mice, Inbred ICR, Triazoles, Streptozotocin, medicine.disease, Immunohistochemistry, Disease Models, Animal, Sulfonylurea Compounds, Endocrinology, Diabetes Mellitus, Type 2, Pyrazines, Sitagliptin, Glipizide, medicine.drug

Abstract

Inhibitors of dipeptidyl peptidase-4 (DPP-4), a key regulator of the actions of incretin hormones, exert antihyperglycemic effects in type 2 diabetic patients. A major unanswered question concerns the potential ability of DPP-4 inhibition to have beneficial disease-modifying effects, specifically to attenuate loss of pancreatic beta-cell mass and function. Here, we investigated the effects of a potent and selective DPP-4 inhibitor, an analog of sitagliptin (des-fluoro-sitagliptin), on glycemic control and pancreatic beta-cell mass and function in a mouse model with defects in insulin sensitivity and secretion, namely high-fat diet (HFD) streptozotocin (STZ)-induced diabetic mice. Significant and dose-dependent correction of postprandial and fasting hyperglycemia, HbA(1c), and plasma triglyceride and free fatty acid levels were observed in HFD/STZ mice following 2-3 months of chronic therapy. Treatment with des-fluoro-sitagliptin dose dependently increased the number of insulin-positive beta-cells in islets, leading to the normalization of beta-cell mass and beta-cell-to-alpha-cell ratio. In addition, treatment of mice with des-fluoro-sitagliptin, but not glipizide, significantly increased islet insulin content and improved glucose-stimulated insulin secretion in isolated islets. These findings suggest that DPP-4 inhibitors may offer long-lasting efficacy in the treatment of type 2 diabetes by modifying the courses of the disease.

Published

2006

38. Long-Term Posttransplantation Care: The Expanding Role of Community Nephrologists

Author

Andrew D. Howard

Subjects

Nephrology, medicine.medical_specialty, Interprofessional Relations, Population, Disease, Medicare, Internal medicine, medicine, Humans, Community Health Services, Intensive care medicine, education, Adverse effect, Kidney transplantation, education.field_of_study, business.industry, Communication, Continuity of Patient Care, medicine.disease, Kidney Transplantation, Long-Term Care, Transplantation, Long-term care, surgical procedures, operative, Insurance, Health, Reimbursement, Transplant surgeon, business, Immunosuppressive Agents

Abstract

Improvements in transplantation practices, immunosuppressive agents, and management of comorbid conditions have led to better outcomes for kidney transplant recipients. Transplantation has become the treatment of choice for patients with end-stage renal disease (ESRD). This has resulted in continued growth in the number of patients living with a functioning kidney allograft as a percentage of the total ESRD population. These patients require long-term follow-up care, which already is straining the limited resources of transplant centers. Community nephrologists are the logical choice to assume responsibility for the posttransplantation care of these patients after discharge from transplant centers when they are stabilized. Optimal management of kidney transplant recipients depends on regular interactive communication between the patient's community nephrologist and the transplant center. Open communication will not only facilitate the initial transition of care, it also will decrease the frequency of referrals back to the transplant center. In an ideal situation, the transplant center and community nephrologist would develop and discuss plans for discharge and transition of care for the individual patient before the actual kidney transplantation. Important issues for effective communication include changes in laboratory results and kidney function; pretransplantation and posttransplantation comorbid conditions, surgical complications, or adverse effects of medications; modifications to immunosuppressive therapy or other medications; recurrent hospitalizations or emergency care; and changes in biopsy results.

Published

2006

39. Ghrelin Neutralization by a Ribonucleic Acid-SPM Ameliorates Obesity in Diet-Induced Obese Mice

Author

Lauren P. Shearman, Liyang Wang, Alison M. Strack, D. Sloan Stribling, Paul Mazur, Sven Klussmann, Andrew D. Howard, D. Euan MacIntyre, Steffen Helmling, Lan Ge, and Sheng-Ping Wang

Subjects

Male, Agonist, medicine.medical_specialty, Time Factors, medicine.drug_class, Peptide Hormones, Oligonucleotides, Radioimmunoassay, Mice, Obese, Enzyme-Linked Immunosorbent Assay, CHO Cells, Biology, beta-Lactamases, Polyethylene Glycols, Inhibitory Concentration 50, Mice, Endocrinology, Genes, Reporter, In vivo, Cricetinae, Internal medicine, medicine, Animals, Humans, Obesity, Receptor, Behavior, Animal, Dose-Response Relationship, Drug, NFATC Transcription Factors, Body Weight, digestive, oral, and skin physiology, Feeding Behavior, Ghrelin, Mice, Inbred C57BL, Dose–response relationship, Hypothalamus, RNA, Secretagogue, Anti-Obesity Agents, Peptides, Diet-induced obese, hormones, hormone substitutes, and hormone antagonists, Protein Binding

Abstract

Ghrelin, an acylated peptide secreted from the stomach, acts as a short-term signal of nutrient depletion. Ghrelin is an endogenous ligand for the GH secretagogue receptor 1a, a G protein-coupled receptor expressed in the hypothalamus and pituitary. We used a synthetic oligonucleotide, NOX-B11-2, capable of specific high-affinity binding to bioactive ghrelin to determine whether ghrelin neutralization would alter indices of energy balance in vivo. This novel type of ghrelin-blocking agent, called an RNA Spiegelmer (SPM), is a polyethylene glycol-modified l-RNA oligonucleotide, the nonnatural configuration of which confers in vivo stability. NOX-B11-2 blocked ghrelin mediated activation of GH secretagogue receptor 1a in cell culture (IC50 approximately 5 nm). We explored the effects of acute NOX-B11-2 administration on ghrelin-induced feeding in mice. NOX-B11-2 (66 mg/kg, sc) blocked ghrelin-induced feeding and was without effect on feeding evoked by an orally active nonpeptide ghrelin receptor agonist. We demonstrated that selective ghrelin blockade effectively promoted weight loss in diet-induced obese (DIO) mice. Chronic infusion of NOX-B11-2 (33 mg/kg.d, sc) to DIO mice evoked body weight loss for 13 d and reduced food intake and fat mass relative to control SPM-infused mice. In a 7-d study, DIO mice infused with NOX-B11-2 (33 mg/kg.d, sc) showed body weight loss, compared with animals receiving control SPM. This effect was directly mediated by SPM neutralization of ghrelin because NOX-B11-2 administration to ghrelin-deficient mice resulted in no weight loss. The decreased obesity observed in SPM-treated DIO mice provides validation for ghrelin neutralization as a potential antiobesity therapy.

Published

2006

40. Discovery of MK-1421, a Potent, Selective sstr3 Antagonist, as a Development Candidate for Type 2 Diabetes

Author

Yang Yu, Gary G. Chicchi, Frederick Wong, Janet S. Kerr, Sharon Tong, Zhe Feng, Guillermo Fernandez, Edward C. Sherer, Kwei-Lan Tsao, Qing Shao, Bei B. Zhang, Yun-Ping Zhou, Pierre Morissette, Shuwen He, Shrenik K. Shah, Vijay Bhasker G. Reddy, Liangqin Guo, Ravi P. Nargund, Margaret Wu, Cai Li, Zhixiong Ye, Alexander Pasternak, George J. Eiermann, Patricia R. Bunting, Hongbo Qi, Michele Pachanski, Stan Mitelman, Maria E. Trujillo, Quang Truong, Maria Madiera, Andrew D. Howard, Donald Nelson, Qingmei Hong, Zhong Lai, Yue Feng, Bindhu V. Karanam, Jian Liu, Koppara Samuel, Wu Du, William K. Hagmann, Tianying Jian, Dorina Trusca, Sylvia Volksdorf, and Peter H. Dobbelaar

Subjects

business.industry, Murine model, Organic Chemistry, Drug Discovery, Antagonist, Qtc interval prolongation, medicine, Type 2 diabetes, Glucose excursion, Pharmacology, medicine.disease, business, Biochemistry

Abstract

The imidazolyl-tetrahydro-β-carboline class of sstr3 antagonists have demonstrated efficacy in a murine model of glucose excursion and may have potential as a treatment for type 2 diabetes. The first candidate in this class caused unacceptable QTc interval prolongation in oral, telemetrized cardiovascular (CV) dogs. Herein, we describe our efforts to identify an acceptable candidate without CV effects. These efforts resulted in the identification of (1R,3R)-3-(4-(5-fluoropyridin-2-yl)-1H-imidazol-2-yl)-1-(1-ethyl-pyrazol-4-yl)-1-(3-methyl-1,3,4-oxadiazol-3H-2-one-5-yl)-2,3,4,9-tetrahydro-1H-β-carboline (17e, MK-1421).

Published

2014

41. Fistula First Breakthrough Initiative (FFBI): Lessons About Arteriovenous Fistula Prevalence Goals

Author

Andrew D. Howard, Klemens B. Meyer, Stuart L. Goldstein, and Robin S. Howard

Subjects

medicine.medical_specialty, business.industry, Fistula, MEDLINE, Arteriovenous fistula, medicine.disease, United States, Surgery, Arteriovenous Shunt, Surgical, Renal Dialysis, Nephrology, Humans, Medicine, business, Goals

Published

2013

42. Activation of melanocortin MC4 receptors increases erectile activity in rats ex copula

Author

Doreen E. Cashen, Erin McGowan, Jennifer E. Drisko, Ravi P. Nargund, William J. Martin, D. Euan MacIntyre, Gary J Hom, Iyassu K. Sebhat, Lex H.T. Van der Ploeg, Liza Gantert, and Andrew D. Howard

Subjects

Male, Agonist, medicine.medical_specialty, medicine.drug_class, Binding, Competitive, Peptides, Cyclic, Piperazines, Rats, Sprague-Dawley, Tetrahydroisoquinolines, Internal medicine, medicine, Animals, Agouti-Related Protein, ACTH receptor, Receptor, Pharmacology, Camphanes, Dose-Response Relationship, Drug, Chemistry, Penile Erection, digestive, oral, and skin physiology, Antagonist, Triazoles, Isoquinolines, Receptor antagonist, Peptide Fragments, Rats, Apomorphine, Endocrinology, Receptors, Corticotropin, THIQ, Receptor, Melanocortin, Type 4, Melanocortin, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Melanocortin peptide agonists, alpha-melanocyte stimulating hormone (alpha-MSH) and melanotan-II, stimulate erectile activity in a variety of species, including man. Since neither peptide discriminates amongst melanocortin receptors, it is not clear which subtype mediates these pro-erectile effects. Here, we present data that melanocortin-induced erectogenesis is mediated by melanocortin MC(4) receptors. Systemic administration of a melanocortin MC(4) receptor agonist (N-[(3R)-1,2,3,4-tetrahydroisoquinolinium-3-ylcarbonyl]-(1R)-1-(4-chlorobenzyl)-2-[4-cyclohexyl-4-(1H-1,2,4-triazol-1ylmethyl)piperidin-1-yl]-2-oxoethylamine; THIQ) with high selectivity over other melanocortin receptors enhanced intracavernosal pressure and stimulated erectile activity in rats ex copula. THIQ dose-dependently (1-5 mg/kg, i.v.) increased the total number of erections, to an extent comparable or greater than that produced by apomorphine (0.025 mg/kg, s.c.). Central administration of THIQ (20 microg, intracerebroventricular (i.c.v.)) increased the number of reflexive penile erections; whereas administration of both a nonselective endogenous melanocortin MC(4) receptor antagonist (agouti-related protein (AgRP), 5.5. microg, i.c.v.) and a melanocortin MC(4) receptor preferring antagonist (MPB10, 1 mg/kg, i.v.) blocked THIQ-induced erectogenesis. These pro-erectile effects were also attenuated by systemic or central administration of an oxytocin antagonist (L-368899, 1 mg/kg, i.v.). Thus, melanocortin MC(4) receptor activation is sufficient for erectogenesis and these effects may involve oxytocinergic pathways.

Published

2002

43. Design and Pharmacology of N-[(3R)-1,2,3,4-Tetrahydroisoquinolinium- 3-ylcarbonyl]-(1R)-1-(4-chlorobenzyl)- 2-[4-cyclohexyl-4-(1H-1,2,4-triazol- 1-ylmethyl)piperidin-1-yl]-2-oxoethylamine (1), a Potent, Selective, Melanocortin Subtype-4 Receptor Agonist

Author

Ralph A. Stearns, Randy R. Miller, William J. Martin, Ravi P. Nargund, Erin McGowan, Lex H.T. Van der Ploeg, and Arthur A. Patchett, Andrew D. Howard, David B. R. Johnston, D. Euan MacIntyre, Rubana N. Kalyani, Khaled Barakat, Raman K. Bakshi, Ralph T. Mosley, Jennifer E. Drisko, Constantin Tamvakopoulos, Rui Tang, Alison M. Strack, Zhixiong Ye, Doreen E. Cashen, Tanya MacNeil, David H. Weinberg, Palucki Brenda, Gary J Hom, and Iyassu K. Sebhat

Subjects

Agonist, Chemistry, medicine.drug_class, Biological activity, Pharmacology, Melanocortin receptor, THIQ, Drug Discovery, medicine, Anorectic, Molecular Medicine, Structure–activity relationship, Melanocortin, Receptor, medicine.drug

Abstract

Synthetic and natural peptides that act as nonselective melanocortin receptor agonists have been found to be anorexigenic and to stimulate erectile activity. We report the design and development of 1, a potent, selective (1184-fold vs MC3R, 350-fold vs MC5R), small-molecule agonist of the MC4 receptor. Pharmacological testing confirms the food intake lowering effects of MC4R agonism and suggests another role for the receptor in the stimulation of erectile activity.

Published

2002

44. A role for the melanocortin 4 receptor in sexual function

Author

Christopher P. Austin, Doreen E. Cashen, Sheng-Shung Pong, Brian D. Spar, Brett Connolly, Tung Ming Fong, D. Euan MacIntyre, Carina P. Tan, Michael R. Tota, Ravi P. Nargund, R. S. L. Chang, Oksana C. Palyha, Constantin Tamvakopoulos, Deborah L. Drazen, Anthony G. DiLella, Jennifer E. Drisko, David J. Figueroa, Tanya MacNeil, Andreas W. Sailer, David H. Weinberg, Randy J. Nelson, Charles Rosenblum, Cathy R.-R.C. Huang, Rui Tang, Arthur A. Patchett, Xiao-Ming Guan, Hong Yu, George J. Christ, Andrew D. Howard, Lex H.T. Van der Ploeg, William J. Martin, Aurawan Vongs, Iyassu K. Sebhat, and Ralph A. Stearns

Subjects

Male, Agonist, medicine.medical_specialty, DNA, Complementary, Intracranial Pressure, medicine.drug_class, Blood Pressure, In Vitro Techniques, Biology, Somatosensory system, Mice, Sexual Behavior, Animal, Nerve Fibers, Internal medicine, Copulation, medicine, Animals, Glans, In Situ Hybridization, DNA Primers, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Human penis, Feeding Behavior, Ribonuclease, Pancreatic, Biological Sciences, Spinal cord, Electric Stimulation, Mice, Inbred C57BL, Melanocortin 4 receptor, medicine.anatomical_structure, Endocrinology, Receptors, Corticotropin, Models, Animal, Receptor, Melanocortin, Type 4, Brainstem, Energy Metabolism, Penis

Abstract

By using a combination of genetic, pharmacological, and anatomical approaches, we show that the melanocortin 4 receptor (MC4R), implicated in the control of food intake and energy expenditure, also modulates erectile function and sexual behavior. Evidence supporting this notion is based on several findings: ( i ) a highly selective non-peptide MC4R agonist augments erectile activity initiated by electrical stimulation of the cavernous nerve in wild-type but not Mc4r -null mice; ( ii ) copulatory behavior is enhanced by administration of a selective MC4R agonist and is diminished in mice lacking Mc4r; ( iii ) reverse transcription (RT)-PCR and non-PCR based methods demonstrate MC4R expression in rat and human penis, and rat spinal cord, hypothalamus, brainstem, pelvic ganglion (major autonomic relay center to the penis), but not in rat primary corpus smooth muscle cavernosum cells; and ( iv ) in situ hybridization of glans tissue from the human and rat penis reveal MC4R expression in nerve fibers and mechanoreceptors in the glans of the penis. Collectively, these data implicate the MC4R in the modulation of penile erectile function and provide evidence that MC4R-mediated proerectile responses may be activated through neuronal circuitry in spinal cord erectile centers and somatosensory afferent nerve terminals of the penis. Our results provide a basis for the existence of MC4R-controlled neuronal pathways that control sexual function.

Published

2002

45. The role of melanocortins in body weight regulation: opportunities for the treatment of obesity

Author

Michael R. Tota, Ravi P. Nargund, Xiao-Ming Guan, Howard Y. Chen, Douglas J. MacNeil, David H. Weinberg, Tanya MacNeil, Euan Macintyre, Alison M. Strack, Charles Rosenblum, Maria A. Bednarek, Andrew D. Howard, Chun-Pyn Shen, Tung M. Fong, Mark T. Goulet, Lex H.T. Van der Ploeg, Airu S. Chen, and Donald J. Marsh

Subjects

endocrine system, medicine.medical_specialty, Gene Expression, Biology, Melanocortin receptor, Proopiomelanocortin, Internal medicine, medicine, Animals, Humans, Melanocyte-Stimulating Hormones, Obesity, Receptor, Melanocortins, Pharmacology, integumentary system, Receptors, Melanocortin, digestive, oral, and skin physiology, Body Weight, Melanocortin 3 receptor, Melanocortin 4 receptor, Endocrinology, Receptors, Corticotropin, biology.protein, Anti-Obesity Agents, Melanocortin, hormones, hormone substitutes, and hormone antagonists, Melanocortin 1 receptor

Abstract

Five G-protein-coupled melanocortin receptors (MC(1)-MC(5)) are expressed in mammalian tissues. The melanocortin receptors support diverse physiological functions, including the regulation of hair color, adrenal function, energy homeostasis, feed efficiency, sebaceous gland lipid production and immune and sexual function. The melanocortins (adrenocorticotropic hormone (ACTH), alpha-melanocyte-stimulating hormone (alpha-MSH), beta-MSH and gamma-MSH) are agonist peptide ligands for the melanocortin receptors and these peptides are processed from the pre-prohormone proopiomelanocortin (POMC). Peptide antagonists for the melanocortin MC(1), MC(3) and MC(4) receptors include agouti-related protein (AgRP) and agouti. Diverse lines of evidence, including genetic and pharmacological data obtained in rodents and humans, support a role for the melanocortin MC(3) and MC(4) receptors in the regulation of energy homeostasis. Recent advances in the development of potent and selective peptide and non-peptide melanocortin receptor ligands are anticipated to help unravel the roles for the melanocortin receptors in humans and to accelerate the clinical use of small molecule melanocortin mimetics.

Published

2002

46. GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent

Author

Sarah Souza, Boonlert Cheewatrakoolpong, Christopher W. Plummer, Joel Mane, Steven L. Colletti, Jiyan Xue, Corin O. Miller, Yue Feng, Jerry Di Salvo, Gail Forrest, Harry R. Chobanian, Brande Thomas-Fowlkes, Daniel Kosinski, Daniel Tatosian, Daphne Szeto, Michele Pachanski, Melissa Kirkland, Andrew D. Howard, Xiaoyan Li, Adam B. Weinglass, Michelle Bunzel, Aimie M. Ogawa, Maria E. Trujillo, and Michael W. Miller

Subjects

Male, 0301 basic medicine, Partial Agonists, Physiology, Peptide Hormones, medicine.medical_treatment, lcsh:Medicine, Biochemistry, Receptors, G-Protein-Coupled, Mice, Endocrinology, 0302 clinical medicine, Insulin Secretion, Medicine and Health Sciences, Insulin, lcsh:Science, Glucose tolerance test, Multidisciplinary, medicine.diagnostic_test, Organic Compounds, Monosaccharides, Glucagon secretion, Drugs, Blood Sugar, Body Fluids, Chemistry, Blood, Physical Sciences, Anatomy, Beta cell, Research Article, endocrine system, medicine.medical_specialty, Carbohydrates, Blood sugar, Incretin, 030209 endocrinology & metabolism, CHO Cells, Biology, Incretins, Partial agonist, Glucagon, Blood Plasma, Cell Line, Islets of Langerhans, 03 medical and health sciences, Cricetulus, Internal medicine, medicine, Animals, Humans, Secretion, Pharmacology, Diabetic Endocrinology, Endocrine Physiology, lcsh:R, Organic Chemistry, Chemical Compounds, Biology and Life Sciences, Glucose Tolerance Test, Hormones, Rats, Glucose, 030104 developmental biology, lcsh:Q, Physiological Processes

Abstract

GPR40 agonists are effective antidiabetic agents believed to lower glucose through direct effects on the beta cell to increase glucose stimulated insulin secretion. However, not all GPR40 agonists are the same. Partial agonists lower glucose through direct effects on the pancreas, whereas GPR40 AgoPAMs may incorporate additional therapeutic effects through increases in insulinotrophic incretins secreted by the gut. Here we describe how GPR40 AgoPAMs stimulate both insulin and incretin secretion in vivo over time in diabetic GK rats. We also describe effects of AgoPAMs in vivo to lower glucose and body weight beyond what is seen with partial GPR40 agonists in both the acute and chronic setting. Further comparisons of the glucose lowering profile of AgoPAMs suggest these compounds may possess greater glucose control even in the presence of elevated glucagon secretion, an unexpected feature observed with both acute and chronic treatment with AgoPAMs. Together these studies highlight the complexity of GPR40 pharmacology and the potential additional benefits AgoPAMs may possess above partial agonists for the diabetic patient.

Published

2017

47. Diamine Derivatives as Novel Small-Molecule, Potent, and Subtype-Selective Somatostatin SST3 Receptor Agonists

Author

Richard G. Ball, Liangqin Guo, Zhicai Wu, Quang Truong, Gary G. Chicchi, Ravi P. Nargund, Dorina Trusca, Kwei-Lan Tsao, Qingmei Hong, Yang Yu, George J. Eiermann, Shuwen He, Yun-Ping Zhou, Bei B. Zhang, William K. Hagmann, Maria E. Trujillo, Michele Pachanski, Hongbo Qi, David X. Yang, Andrew D. Howard, Derun Li, Zhong Lai, and Edward C. Sherer

Subjects

Agonist, medicine.drug_class, business.industry, Organic Chemistry, Antagonist, Pharmacology, Biochemistry, Partial agonist, HYDIA, Somatostatin, In vivo, Drug Discovery, medicine, Receptor, business, G protein-coupled receptor

Abstract

A novel class of small-molecule, highly potent, and subtype-selective somatostatin SST3 agonists was discovered through modification of a SST3 antagonist. As an example, (1R,2S)-9 demonstrated not only potent in vitro SST3 agonist activity but also in vivo SST3 agonist activity in a mouse oral glucose tolerance test (OGTT). These agonists may be useful reagents for studying the physiological roles of the SST3 receptor and may potentially be useful as therapeutic agents.

Published

2014

48. Long-term management of the renal transplant recipient: Optimizing the relationship between the transplant center and the community nephrologist

Author

Andrew D. Howard

Subjects

Adult, Graft Rejection, Male, Nephrology, Health Knowledge, Attitudes, Practice, medicine.medical_specialty, medicine.medical_treatment, Malignancy, Internal medicine, Diabetes Mellitus, Humans, Medicine, Community Health Services, Risk factor, Intensive care medicine, Adverse effect, Kidney transplantation, Monitoring, Physiologic, Immunosuppression Therapy, business.industry, Immunosuppression, Continuity of Patient Care, medicine.disease, Kidney Transplantation, Long-Term Care, United States, Transplantation, Long-term care, surgical procedures, operative, Female, Clinical Competence, business

Abstract

Rapid growth in the number of kidney transplant recipients along with improved viability of transplanted organs and increased patient survival have all led to the need for effective long-term management of these patients. The increasing numbers of transplants and the duration of posttransplant medical care can overwhelm the resources of a transplant center. These factors highlight the need for optimizing the relationship between the transplant center and the community nephrologist. There are several factors that affect the timing for transitioning patients from the transplant center to the community nephrologist and no standard timing has yet been established. Continued management of pretransplant comorbid conditions is important as are monitoring for adverse effects of failure of immunosuppressive therapy and the development of posttransplant complications. An array of testing that can be useful in monitoring these patients as well as the suggested frequency for their use are reviewed. Guidelines for the optimal interaction between the transplant center and the community nephrologist are provided to include circumstances concerning adjustment or conversion of immunosuppressive medications, evidence of allograft dysfunction, and the development of malignancy.

Published

2001

49. Identification of Peptide Ligand-binding Domains within the Human Motilin Receptor Using Photoaffinity Labeling

Author

Laurence J. Miller, Bernard Coulie, Elizabeth M. Hadac, Maoqing Dong, Scott D. Feighner, Andrew D. Howard, Bunzo Matsuura, and Delia I. Pinon

Subjects

Receptors, Neuropeptide, Agonist, medicine.drug_class, Motilin receptor, Molecular Sequence Data, Peptide, CHO Cells, Photoaffinity Labels, Ligands, Biochemistry, Receptors, Gastrointestinal Hormone, Motilin, chemistry.chemical_compound, Cricetinae, medicine, Animals, Humans, Amino Acid Sequence, Receptor, Molecular Biology, chemistry.chemical_classification, Photoaffinity labeling, Chemistry, Chinese hamster ovary cell, digestive, oral, and skin physiology, Cell Biology, Cyanogen bromide, Peptides, hormones, hormone substitutes, and hormone antagonists

Abstract

The cDNA encoding the human motilin receptor was recently cloned and found to represent a G protein-coupled receptor that is structurally related to the growth hormone secretagogue receptors. Together, these represent a new Class I receptor family. Our aim in the present work is to gain insight into the molecular basis of binding of motilin to its receptor using photoaffinity labeling. To achieve this, we developed a Chinese hamster ovary cell line that overexpressed functional motilin receptor (CHO-MtlR; 175,000 sites per cell, with K(i) = 2.3 +/- 0.4 nm motilin and EC(50) = 0.3 +/- 0.1 nm motilin) and a radioiodinatable peptide analogue of human motilin that incorporated a photolabile p-benzoyl-l-phenylalanine (Bpa) residue into its pharmacophoric domain. This probe, [Bpa(1),Ile(13)]motilin, was a full agonist at the motilin receptor that increased intracellular calcium in a concentration-dependent manner (EC(50) = 1.5 +/- 0.4 nm). This photolabile ligand bound specifically and with high affinity to the motilin receptor (K(i) = 12.4 +/- 1.0 nm), and covalently labeled that molecule within its M(r) = 45,000 deglycosylated core. Cyanogen bromide cleavage demonstrated its covalent attachment to fragments of the receptor having apparent M(r) = 6,000 and M(r) = 31,000. These were demonstrated to represent fragments that included both the first and the large second extracellular loop domains, with the latter representing a unique structural feature of this receptor. The spatial approximation of the pharmacophoric domain of motilin with these receptor domains support their functional importance as well.

Published

2001

50. Short Segment of Human Melanin-Concentrating Hormone That Is Sufficient for Full Activation of Human Melanin-Concentrating Hormone Receptors 1 and 2

Author

Donna L. Hreniuk, Oksana C. Palyha, Van der Ploeg Lh, Douglas J. MacNeil, Andrew D. Howard, Scott D. Feighner, Maria A. Bednarek, Nancy R. Morin, and Sadowski Sj

Subjects

medicine.medical_specialty, Growth-hormone-releasing hormone receptor, Melanin-concentrating hormone, Protein Conformation, Molecular Sequence Data, Peptides, Cyclic, Biochemistry, Cell Line, Receptors, G-Protein-Coupled, chemistry.chemical_compound, Isomerism, Thyrotropin-releasing hormone receptor, Internal medicine, medicine, Humans, Amino Acid Sequence, Cysteine, Disulfides, Receptors, Pituitary Hormone, Receptor, Melanins, Alanine, Hypothalamic Hormones, Thyroid hormone receptor, integumentary system, Peptide Fragments, Pituitary Hormones, Endocrinology, Amino Acid Substitution, chemistry, Hormone receptor, sense organs, Melanocortin 1 receptor, Hormone

Abstract

Human melanin-concentrating hormone (hMCH) is a potent but nonselective agonist at human melanin-concentrating hormone receptors 1 and 2 (hMCH-1R and hMCH-2R, respectively). To determine the structural features of this neuropeptide which are necessary for efficient binding to and activation of the receptors, Ala-substituted, open-chain, and truncated analogues were synthesized and tested in the binding assays in CHO cells expressing hMCH-1R and hMCH-2R, and in functional assays measuring the level of intracellular calcium mobilization in human HEK-293 cells expressing these receptors. A compound consisting merely of the cyclic core of hMCH with the Arg attached to the N-terminus of the disulfide ring was found to activate both hMCH-1R and hMCH-2R about as effectively as full-length hMCH. Thus, the sequence Arg-cyclo(S-S)(Cys-Met-Leu-Gly-Arg-Val-Tyr-Arg-Pro-Cys) appears to constitute the "active core" that is necessary for agonist potency at hMCH-1R and hMCH-2R. A potent and approximately 4-fold more selective agonist at hMCH-1R than at hMCH-2R is also reported.

Published

2001