Your search keyword '"Huaibing, He"' showing total 62 results

1. Discovery of MK-1462: GLP-1 and Glucagon Receptor Dual Agonist for the Treatment of Obesity and Diabetes

Author

Anandan Palani, Andrea R. Nawrocki, Federica Orvieto, Elisabetta Bianchi, Emanuela Mandić, Antonello Pessi, Chunhui Huang, Qiaolin Deng, Nathalie Toussaint, Erika Walsh, Vijay Reddy, Eric Ashley, Huaibing He, Sheena Mumick, Brian Hawes, Donald Marsh, Mark Erion, Ravi Nargund, and Paul E. Carrington

Subjects

Organic Chemistry, Drug Discovery, Biochemistry

Abstract

Peptide-based analogues of the gut-derived incretin hormone, glucagon-like peptide 1 (GLP1), stimulate insulin secretion in a glucose-dependent manner. Currently marketed GLP1 receptor (GLP1R) agonists are safe and effective in the management of Type 2 diabetes but often offer only modest weight loss. This has prompted the search for safe and effective alternatives to enhance the weight loss component of these treatments. We have demonstrated that concomitant activation GLP1R and the glucagon receptor (GCGR) can improve glucose metabolism and provide superior weight loss when compared to selective GLP1R agonism in preclinical species. This paper will highlight chemistry structure-activity relationship optimization and summarize in vivo efficacy studies toward the discovery of a once daily balanced dual agonist

Published

2022

2. Pharmacological AMPK activation induces transcriptional responses congruent to exercise in skeletal and cardiac muscle, adipose tissues and liver.

Author

Eric S Muise, Hong-Ping Guan, Jinqi Liu, Andrea R Nawrocki, Xiaodong Yang, Chuanlin Wang, Carlos G Rodríguez, Dan Zhou, Judith N Gorski, Marc M Kurtz, Danqing Feng, Kenneth J Leavitt, Lan Wei, Robert R Wilkening, James M Apgar, Shiyao Xu, Ku Lu, Wen Feng, Ying Li, Huaibing He, Stephen F Previs, Xiaolan Shen, Margaret van Heek, Sandra C Souza, Mark J Rosenbach, Tesfaye Biftu, Mark D Erion, David E Kelley, Daniel M Kemp, Robert W Myers, and Iyassu K Sebhat

Subjects

Medicine, Science

Abstract

Physical activity promotes metabolic and cardiovascular health benefits that derive in part from the transcriptional responses to exercise that occur within skeletal muscle and other organs. There is interest in discovering a pharmacologic exercise mimetic that could imbue wellness and alleviate disease burden. However, the molecular physiology by which exercise signals the transcriptional response is highly complex, making it challenging to identify a single target for pharmacological mimicry. The current studies evaluated the transcriptome responses in skeletal muscle, heart, liver, and white and brown adipose to novel small molecule activators of AMPK (pan-activators for all AMPK isoforms) compared to that of exercise. A striking level of congruence between exercise and pharmacological AMPK activation was observed across the induced transcriptome of these five tissues. However, differences in acute metabolic response between exercise and pharmacologic AMPK activation were observed, notably for acute glycogen balances and related to the energy expenditure induced by exercise but not pharmacologic AMPK activation. Nevertheless, intervention with repeated daily administration of short-acting activation of AMPK was found to mitigate hyperglycemia and hyperinsulinemia in four rodent models of metabolic disease and without the cardiac glycogen accretion noted with sustained pharmacologic AMPK activation. These findings affirm that activation of AMPK is a key node governing exercise mediated transcription and is an attractive target as an exercise mimetic.

Published

2019

3. A Series of Novel, Highly Potent, and Orally Bioavailable Next-Generation Tricyclic Peptide PCSK9 Inhibitors

Author

Thomas J. Tucker, Nianyu Li, Scott P. Salowe, Harold B. Wood, Danila Branca, Alan S. Bass, Rupesh P. Amin, BethAnn Murphy, Aurash Shahripour, Angela Kerekes, Abbas Walji, Nicole Buist, Jeffrey T. Kuethe, Huaibing He, Rodger Tracy, Kenneth A. Koeplinger, Weixun Wang, Bhavana Bhatt, Candice Alleyne, Sookhee Ha, Douglas G. Johns, Elisabetta Bianchi, Chengwei Wu, Peter Orth, Tjerk Bueters, Yusheng Xiong, Hratch J. Zokian, Michael J. Hafey, Mark W. Embrey, and John Higgins

Subjects

chemistry.chemical_classification, Molecular Structure, biology, PCSK9, PCSK9 Inhibitors, Administration, Oral, Biological Availability, Peptide, Pharmacology, Crystallography, X-Ray, Proprotein convertase, Peptides, Cyclic, Rats, Bioavailability, Macaca fascicularis, Structure-Activity Relationship, chemistry, Drug Discovery, biology.protein, Animals, Molecular Medicine, Kexin, Dosing, Antibody, Tricyclic

Abstract

Proprotein convertase subtilisin-like/kexin type 9 (PCSK9) is a key regulator of plasma LDL-cholesterol (LDL-C) and a clinically validated target for the treatment of hypercholesterolemia and coronary artery disease. Starting from second-generation lead structures such as 2, we were able to refine these structures to obtain extremely potent bi- and tricyclic PCSK9 inhibitor peptides. Optimized molecules such as 44 demonstrated sufficient oral bioavailability to maintain therapeutic levels in rats and cynomolgus monkeys after dosing with an enabled formulation. We demonstrated target engagement and LDL lowering in cynomolgus monkeys essentially identical to those observed with the clinically approved, parenterally dosed antibodies. These molecules represent the first report of highly potent and orally bioavailable macrocyclic peptide PCSK9 inhibitors with overall profiles favorable for potential development as once-daily oral lipid-lowering agents. In this manuscript, we detail the design criteria and multiparameter optimization of this novel series of PCSK9 inhibitors.

Published

2021

4. Dipeptidyl Peptidase 4 Inhibition Stimulates Distal Tubular Natriuresis and Increases in Circulating SDF-1α1-67 in Patients With Type 2 Diabetes

Author

Amy Locke, Julie A. Lovshin, David Z.I. Cherney, Leif E. Lovblom, Weixun Wang, Yulyia Lytvyn, Daniel J. Drucker, Vesta Lai, Shajiha Khan, Huaibing He, Lucinda Hittle, Robel Alemu, and Harindra Rajasekeran

Subjects

Advanced and Specialized Nursing, medicine.medical_specialty, Fractional excretion of sodium, business.industry, Endocrinology, Diabetes and Metabolism, Hemodynamics, 030209 endocrinology & metabolism, Type 2 diabetes, 030204 cardiovascular system & hematology, medicine.disease, Natriuresis, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Sitagliptin, Internal medicine, Internal Medicine, medicine, Empagliflozin, business, Dipeptidyl peptidase-4, medicine.drug, Tubuloglomerular feedback

Abstract

OBJECTIVE Antihyperglycemic agents, such as empagliflozin, stimulate proximal tubular natriuresis and improve cardiovascular and renal outcomes in patients with type 2 diabetes. Because dipeptidyl peptidase 4 (DPP-4) inhibitors are used in combination with sodium–glucose cotransporter 2 (SGLT2) inhibitors, we examined whether and how sitagliptin modulates fractional sodium excretion and renal and systemic hemodynamic function. RESEARCH DESIGN AND METHODS We studied 32 patients with type 2 diabetes in a prospective, double-blind, randomized, placebo-controlled trial. Measurements of renal tubular function and renal and systemic hemodynamics were obtained at baseline, then hourly after one dose of sitagliptin or placebo, and repeated at 1 month. Fractional excretion of sodium and lithium and renal hemodynamic function were measured during clamped euglycemia. Systemic hemodynamics were measured using noninvasive cardiac output monitoring, and plasma levels of intact versus cleaved stromal cell–derived factor (SDF)-1α were quantified using immunoaffinity and tandem mass spectrometry. RESULTS Sitagliptin did not change fractional lithium excretion but significantly increased total fractional sodium excretion (1.32 ± 0.5 to 1.80 ± 0.01% vs. 2.15 ± 0.6 vs. 2.02 ± 1.0%, P = 0.012) compared with placebo after 1 month of treatment. Moreover, sitagliptin robustly increased intact plasma SDF-1α1-67 and decreased truncated plasma SDF-1α3-67. Renal hemodynamic function, systemic blood pressure, cardiac output, stroke volume, and total peripheral resistance were not adversely affected by sitagliptin. CONCLUSIONS DPP-4 inhibition promotes a distal tubular natriuresis in conjunction with increased levels of intact SDF-1α1-67. Because of the distal location of the natriuretic effect, DPP-4 inhibition does not affect tubuloglomerular feedback or impair renal hemodynamic function, findings relevant to using DPP-4 inhibitors for treating type 2 diabetes.

Published

2017

5. Late-stage lipidation of fully elaborated tryptophan-containing peptides for improved pharmacokinetics

Author

Songnian Lin, Cannon B. Wille, Chunhui Huang, Vijay Bhasker G. Reddy, Huaibing He, Anandan Palani, and Ravi P. Nargund

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Organic Chemistry, Tryptophan, Late stage, Fatty acid, Peptide, Lipid-anchored protein, 010402 general chemistry, 01 natural sciences, Biochemistry, Glucagon, 0104 chemical sciences, Pharmacokinetics, In vivo, Drug Discovery

Abstract

The late-stage modification of native peptides to alter and/or enhance their properties and functions is attractive but formidably challenging. Peptide lipidation is one of the effective strategies to overcome short half-life and rapid clearance. Herein, we report a late-stage installation of a fatty acid lipid onto fully elaborated peptides, using glucagon as an example, through regio- and chemoselective functionalization of tryptophan with high potency and remarkable in vivo half-life extension.

Published

2017

6. The discovery of novel 5,6,5- and 5,5,6-tricyclic pyrrolidines as potent and selective DPP-4 inhibitors

Author

Hong D. Chu, Huaibing He, Ying-Duo Gao, Xiaohua Li, Aleksandr Petrov, Tesfaye Biftu, Joseph M. Metzger, Jeffrey T. Kuethe, Kathryn A. Lyons, Jason M. Cox, Ranabir SinhaRoy, George J. Eiermann, Ann E. Weber, Shiyao Xu, Giovanna Scapin, and Joseph K. Wu

Subjects

Models, Molecular, 0301 basic medicine, Pyrrolidines, Dipeptidyl Peptidase 4, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Crystallography, X-Ray, Omarigliptin, 01 natural sciences, Biochemistry, Pyrrolidine, Dipeptidyl peptidase, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Molecular Biology, Dipeptidyl peptidase-4, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, Protease, Dose-Response Relationship, Drug, Molecular Structure, Drug discovery, Organic Chemistry, Rats, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, chemistry, Molecular Medicine, Tricyclic

Abstract

Novel potent and selective 5,6,5- and 5,5,6-tricyclic pyrrolidine dipeptidyl peptidase IV (DPP-4) inhibitors were identified. Structure-activity relationship (SAR) efforts focused on improving the intrinsic DPP-4 inhibition potency, increasing protease selectivity, and demonstrating clean ion channel and cytochrome P450 profiles while trying to achieve a pharmacokinetic profile suitable for once weekly dosing in humans.

Published

2016

7. A Series of Novel, Highly Potent, and Orally Bioavailable Next-Generation Tricyclic Peptide PCSK9 Inhibitors.

Author

Tucker, Thomas J., Embrey, Mark W., Alleyne, Candice, Amin, Rupesh P., Bass, Alan, Bhatt, Bhavana, Bianchi, Elisabetta, Branca, Danila, Bueters, Tjerk, Buist, Nicole, Ha, Sookhee N., Hafey, Mike, Huaibing He, Higgins, John, Johns, Douglas G., Kerekes, Angela D., Koeplinger, Kenneth A., Kuethe, Jeffrey T., Nianyu Li, and Murphy, BethAnn

Published

2021

8. Pharmacological AMPK activation induces transcriptional responses congruent to exercise in skeletal and cardiac muscle, adipose tissues and liver

Author

Hong-Ping Guan, Wen Feng, Daniel M. Kemp, Judith N. Gorski, Shiyao Xu, Ying Li, Dan Zhou, Ku Lu, Tesfaye Biftu, David E. Kelley, Chuanlin Wang, Sandra C. Souza, Lan Wei, Danqing Feng, Robert R. Wilkening, Andrea R. Nawrocki, Iyassu K. Sebhat, Mark J. Rosenbach, Margaret van Heek, Carlos G. Rodriguez, Eric S. Muise, Xiaodong Yang, Mark D. Erion, Jinqi Liu, Stephen F. Previs, James M. Apgar, Marc M. Kurtz, Huaibing He, Robert W. Myers, Xiaolan Shen, and Kenneth J. Leavitt

Subjects

0301 basic medicine, Glycogens, Glycobiology, Adipose tissue, Cardiovascular Medicine, AMP-Activated Protein Kinases, Biochemistry, Transcriptome, chemistry.chemical_compound, 0302 clinical medicine, Medicine and Health Sciences, Hyperinsulinemia, Homeostasis, Public and Occupational Health, Musculoskeletal System, Multidisciplinary, Glycogen, Organic Compounds, Pharmaceutics, Muscles, Monosaccharides, Fatty Acids, Cardiac muscle, Heart, Sports Science, Chemistry, medicine.anatomical_structure, Adipose Tissue, Liver, Physical Sciences, Medicine, Anatomy, Oxidation-Reduction, Research Article, medicine.medical_specialty, Drug Administration, Science, DNA transcription, Carbohydrates, Cardiovascular Pharmacology, 03 medical and health sciences, Drug Therapy, Physical Conditioning, Animal, Internal medicine, Genetics, medicine, Animals, Sports and Exercise Medicine, Muscle, Skeletal, Exercise, Pharmacology, business.industry, Myocardium, Organic Chemistry, Chemical Compounds, Biology and Life Sciences, Skeletal muscle, AMPK, Physical Activity, medicine.disease, Enzyme Activation, Mice, Inbred C57BL, Glucose, 030104 developmental biology, Endocrinology, Skeletal Muscles, Gene Expression Regulation, chemistry, Physical Fitness, Cardiovascular Anatomy, Gene expression, Energy Metabolism, business, 030217 neurology & neurosurgery

Abstract

Physical activity promotes metabolic and cardiovascular health benefits that derive in part from the transcriptional responses to exercise that occur within skeletal muscle and other organs. There is interest in discovering a pharmacologic exercise mimetic that could imbue wellness and alleviate disease burden. However, the molecular physiology by which exercise signals the transcriptional response is highly complex, making it challenging to identify a single target for pharmacological mimicry. The current studies evaluated the transcriptome responses in skeletal muscle, heart, liver, and white and brown adipose to novel small molecule activators of AMPK (pan-activators for all AMPK isoforms) compared to that of exercise. A striking level of congruence between exercise and pharmacological AMPK activation was observed across the induced transcriptome of these five tissues. However, differences in acute metabolic response between exercise and pharmacologic AMPK activation were observed, notably for acute glycogen balances and related to the energy expenditure induced by exercise but not pharmacologic AMPK activation. Nevertheless, intervention with repeated daily administration of short-acting activation of AMPK was found to mitigate hyperglycemia and hyperinsulinemia in four rodent models of metabolic disease and without the cardiac glycogen accretion noted with sustained pharmacologic AMPK activation. These findings affirm that activation of AMPK is a key node governing exercise mediated transcription and is an attractive target as an exercise mimetic.

Published

2019

9. Measurement of catecholamines in rat and mini-pig plasma and urine by liquid chromatography–tandem mass spectrometry coupled with solid phase extraction

Author

Xinchun Tong, Lucinda H. Cohen, Huaibing He, and Ester Carballo-Jane

Subjects

Blood Glucose, Analyte, Swine, Clinical Biochemistry, Urine, Tandem mass spectrometry, Sensitivity and Specificity, Biochemistry, High-performance liquid chromatography, Analytical Chemistry, Catecholamines, Pharmacokinetics, Tandem Mass Spectrometry, Liquid chromatography–mass spectrometry, Animals, Solid phase extraction, Chromatography, High Pressure Liquid, Chromatography, Chemistry, Solid Phase Extraction, Extraction (chemistry), Reproducibility of Results, Cell Biology, General Medicine, Rats, Linear Models, Swine, Miniature

Abstract

A tandem mass spectrometry method combined with an ion-pair chromatographic separation after weak cation exchange solid phase sample extraction for epinephrine (E), norepinephrine (NE) and dopamine (DA) has been developed. Two surrogate matrixes for plasma and urine as well as stable isotope labeled internal standards were utilized for quantitation. The observed dynamic range of E, NE and DA was 0.025-100ng/ml for plasma, and 0.25-1000ng/ml for urine with a r(2) regression coefficient >0.99. Extraction recoveries were greater than 60% and the lower limit of quantitation was 25pg/ml for all three analytes in plasma. This method provided excellent sensitivity and selectivity for use with small sample volumes (≤25uL), enabling high-throughput pharmacodynamic animal model development and screening of adverse effects.

Published

2015

10. Discovery and optimization of orally active cyclohexane-based prolylcarboxypeptidase (PrCP) inhibitors

Author

Yong Zhang, Jeffrey J. Hale, Andreas Verras, Shirly Pinto, Huaibing He, Zhu Shen, Urmi R. Bhatt, Elaine C. Tung, John S. Debenham, Matthew J. Clements, Dunlu Chen, Dong-Ming Shen, Wayne M. Geissler, Thomas H. Graham, JeanMarie Lisnock, Qing Chen, Suoyu Xu, Xiaohua Li, Margarita Garcia-Calvo, Wensheng Liu, Xinchun Tong, Judyann Wiltsie, Christina B. Madsen-Duggan, and Jeffrey T. Kuethe

Subjects

Male, Oral dose, Cyclohexane, High-throughput screening, Clinical Biochemistry, Pharmaceutical Science, Carboxypeptidases, Pharmacology, Biochemistry, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Pharmacokinetics, Cyclohexanes, Drug Discovery, Animals, Obesity, Enzyme Inhibitors, Molecular Biology, Binding affinities, Serine protease, Molecular Structure, biology, Organic Chemistry, Mice, Inbred C57BL, Orally active, chemistry, biology.protein, Molecular Medicine, Ex vivo

Abstract

The synthesis, SAR, binding affinities and pharmacokinetic profiles are described for a series of cyclohexane-based prolylcarboxypeptidase (PrCP) inhibitors discovered by high throughput screening. Compounds show high levels of ex vivo target engagement in mouse plasma 20 h post oral dose.

Published

2013

11. Systemic pan-AMPK activator MK-8722 improves glucose homeostasis but induces cardiac hypertrophy

Author

Aleksandr Petrov, Wen Feng, Ann E. Weber, Effie Tozzo, Lisa LaFranco Scheuch, Shiyao Xu, Wei Zhu, Nancy A. Thornberry, Dinko Gonzalez Trotter, Rory J. Rohm, Franklin Liu, Ku Lu, Michelle Bunzel, David E. Kelley, Stacey Conarello, Jinqi Liu, Corin O. Miller, Xiaoda Niu, Huaibing He, Ronald E. Painter, Ying Li, Daniel M. Kemp, Ying Qian, Maria E. Trujillo, Mark D. Erion, Liyang Wang, Iyassu K. Sebhat, Gaochao Zhou, Michael Klimas, Marie A. Holahan, Marc M. Kurtz, George J. Eiermann, Guillermo Fernandez, Bindu Bennet, Juliann Ehrhart, Tesfaye Biftu, Aimie Ogawa, Sandra C. Souza, Cai Li, Srinivasa Prahalada, James A. Milligan, Hong-Ping Guan, Danqing Feng, Robert W. Myers, Douglas Wisniewski, Xiaodong Yang, Daniel Rubins, Hongwu Wang, and Margaret van Heek

Subjects

0301 basic medicine, Blood Glucose, Male, medicine.medical_specialty, Pyridines, Glucose uptake, Cardiomegaly, Biology, AMP-Activated Protein Kinases, Energy homeostasis, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Internal medicine, medicine, Glucose homeostasis, Animals, Homeostasis, Insulin, Glycogen synthase, Protein kinase A, Muscle, Skeletal, Multidisciplinary, Glycogen, Activator (genetics), Imidazoles, AMPK, Fasting, Macaca mulatta, Hypoglycemia, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Glucose, chemistry, biology.protein, Benzimidazoles, 030217 neurology & neurosurgery

Abstract

Hitting a dozen enzymes with one drug The adenosine monophosphate-activated protein kinase (AMPK) controls cellular energy status. AMPK is activated when energy levels fall. This stimulates adenosine triphosphate (ATP)-generating pathways that promote glucose uptake and inhibits ATP-consuming pathways associated with glucose synthesis. In principle, these effects would be beneficial in metabolic diseases, including diabetes. Pharmacological activation of AMPK has been challenging, however, because in mammals, the enzyme exists as 12 distinct complexes. Myers et al. describe an orally available compound (MK-8722) that activates all 12 complexes (see the Perspective by Hardie). In animal models, MK-8722 ameliorated diabetes, but it also caused enlargement of the heart. MK-8722 may be a useful tool compound for laboratory research on AMPK function. Science , this issue p. 507 ; see also p. 455

Published

2016

12. Aminopiperidine-fused imidazoles as dipeptidyl peptidase-IV inhibitors

Author

Sangita B. Patel, Scott D. Edmondson, Ann E. Weber, Reshma A. Patel, Aleksandr Petrov, Kathryn A. Lyons, Bing Zhu, Joseph K. Wu, Anthony Mastracchio, Shiyao Xu, George J. Eiermann, Ranabir Sinha Roy, Giovanna Scapin, Nancy A. Thornberry, Jason M. Cox, and Huaibing He

Subjects

Benzimidazole, Imidazopyridine, animal structures, Pyridines, Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Inhibitory Concentration 50, Mice, chemistry.chemical_compound, Dogs, Piperidines, Glucagon-Like Peptide 1, In vivo, Drug Discovery, Animals, Humans, Potency, education, Molecular Biology, Dipeptidyl peptidase-4, Dipeptidyl-Peptidase IV Inhibitors, education.field_of_study, biology, Hydrolysis, Sitagliptin Phosphate, Organic Chemistry, Imidazoles, Triazoles, Macaca mulatta, Dipeptidyl peptidase 8, Rats, chemistry, Enzyme inhibitor, Drug Design, Pyrazines, biology.protein, Molecular Medicine, Benzimidazoles

Abstract

A new series of DPP-4 inhibitors derived from piperidine-fused benzimidazoles and imidazopyridines is described. Optimization of this class of DPP-4 inhibitors led to the discovery of imidazopyridine 34. The potency, selectivity, cross-species DMPK profiles, and in vivo efficacy of 34 is reported.

Published

2009

13. Discovery of Potent and Selective Dipeptidyl Peptidase IV Inhibitors Derived from β-Aminoamides Bearing Subsituted Triazolopiperazines

Author

Nancy A. Thornberry, Michael H. Fisher, Dooseop Kim, Bei B. Zhang, Huaibing He, Xiaoping Zhang, Barbara Leiting, Kathryn A. Lyons, Joseph K. Wu, Emma R. Parmee, Matthew J. Wyvratt, Linda Brockunier, KellyAnn D. Pryor, Ann E. Weber, Sangita B. Patel, George J. Eiermann, Ranabir Sinha Roy, Giovanna Scapin, Aleksandr Petrov, Lan Zhu, and Jennifer E. Kowalchick

Subjects

Male, Stereochemistry, Dipeptidyl Peptidase 4, Crystallography, X-Ray, Chemical synthesis, Piperazines, Dipeptidyl peptidase, Mice, Structure-Activity Relationship, Dogs, In vivo, Drug Discovery, Animals, Humans, Potency, Structure–activity relationship, IC50, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, biology, Stereoisomerism, Haplorhini, Glucose Tolerance Test, Triazoles, Amides, Rats, Mice, Inbred C57BL, Enzyme, chemistry, Enzyme inhibitor, Pyrazines, biology.protein, Molecular Medicine

Abstract

A series of beta-aminoamides bearing triazolopiperazines have been discovered as potent, selective, and orally active dipeptidyl peptidase IV (DPP-4) inhibitors by extensive structure-activity relationship (SAR) studies around the triazolopiperazine moiety. Among these, compound 34b with excellent in vitro potency (IC50 = 4.3 nM) against DPP-4, high selectivity over other enzymes, and good pharmacokinetic profiles exhibited pronounced in vivo efficacy in an oral glucose tolerance test (OGTT) in lean mice. On the basis of these properties, compound 34b has been profiled in detail. Further refinement of the triazolopiperazines resulted in the discovery of a series of extremely potent compounds with subnanomolar activity against DPP-4 (42b- 49b), that is, 4-fluorobenzyl-substituted compound 46b, which is notable for its superior potency (IC50 = 0.18 nM). X-ray crystal structure determination of compounds 34b and 46b in complex with DPP-4 enzyme revealed that (R)-stereochemistry at the 8-position of triazolopiperazines is strongly preferred over (S) with respect to DPP-4 inhibition.

Published

2008

14. Design, synthesis, and biological evaluation of triazolopiperazine-based β-amino amides as potent, orally active dipeptidyl peptidase IV (DPP-4) inhibitors

Author

Ann E. Weber, Reshma A. Patel, Joseph K. Wu, Aleksandr Petrov, Frank Marsilio, Jennifer E. Kowalchick, KellyAnn D. Pryor, Nancy A. Thornberry, Barbara Leiting, Kathryn A. Lyons, Giovanna Scapin, Huaibing He, George J. Eiermann, and Dooseop Kim

Subjects

Models, Molecular, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, Piperazines, Dipeptidyl peptidase, Pharmacokinetics, In vivo, Drug Discovery, Animals, Protease Inhibitors, Beta (finance), Molecular Biology, Dipeptidyl-Peptidase IV Inhibitors, Chemistry, DPP-4 Inhibitors, Organic Chemistry, Amides, Rats, Bioavailability, Orally active, Design synthesis, Drug Design, Molecular Medicine

Abstract

Various beta-amino amides containing triazolopiperazine heterocycles have been prepared and evaluated as potent, selective, orally active dipeptidyl peptidase IV (DPP-4) inhibitors. These compounds display excellent oral bioavailability and good overall pharmacokinetic profiles in preclinical species. Moreover, in vivo efficacy in an oral glucose tolerance test in lean mice is demonstrated.

Published

2007

15. 4-Arylcyclohexylalanine analogs as potent, selective, and orally active inhibitors of dipeptidyl peptidase IV

Author

Reshma A. Patel, Huaibing He, David E. Kaelin, Barbara Leiting, Kathryn A. Lyons, Nancy A. Thornberry, Sangita B. Patel, Ann E. Weber, Abigail Lee Smenton, Alexsandr Petrov, George J. Eiermann, Giovanna Scapin, Joseph L. Duffy, and Joseph K. Wu

Subjects

Models, Molecular, animal structures, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Biochemistry, Dipeptidyl peptidase, Mice, Pharmacokinetics, Oral administration, In vivo, Drug Discovery, medicine, Animals, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, Glucose tolerance test, Alanine, biology, medicine.diagnostic_test, Chemistry, Organic Chemistry, Enzyme, Enzyme inhibitor, Area Under Curve, biology.protein, Molecular Medicine, Triazolopyridine

Abstract

A novel series of 4-arylcyclohexylalanine DPP-4 inhibitors was synthesized and tested for inhibitory activity as well as selectivity over the related proline-specific enzymes DPP-8 and DPP-9. Optimization of this series led to 28 (DPP-4 IC(50)=4.8 nM), which showed an excellent pharmacokinetic profile across several preclinical species. Evaluation of 28 in an oral glucose tolerance test demonstrated that this compound effectively reduced glucose excursion in lean mice.

Published

2007

16. Discovery of 3-aminopiperidines as potent, selective, and orally bioavailable dipeptidyl peptidase IV inhibitors

Author

Joseph K. Wu, Reshma A. Patel, Nancy A. Thornberry, Ann E. Weber, Jason M. Cox, Shiyao Xu, Bing Zhu, Barbara Leiting, Kathryn A. Lyons, Scott D. Edmondson, Ranabir Sinha Roy, Bart Harper, Huaibing He, and Anthony Mastracchio

Subjects

CYP2D6, animal structures, Clinical Biochemistry, hERG, Biological Availability, Pharmaceutical Science, Biochemistry, Structure-Activity Relationship, Piperidines, Drug Discovery, Animals, Humans, Hypoglycemic Agents, Potency, Molecular Biology, Dipeptidyl peptidase-4, Dipeptidyl-Peptidase IV Inhibitors, Molecular Structure, biology, Chemistry, Calcium channel, Organic Chemistry, Biological activity, Potassium channel, Rats, Enzyme inhibitor, Area Under Curve, biology.protein, Molecular Medicine, Half-Life

Abstract

Substituted 3-aminopiperidines 3 were evaluated as DPP-4 inhibitors. The inhibitors showed good DPP-4 potency with superb selectivity over other peptidases (QPP, DPP8, and DPP9). Selected DPP-4 inhibitors were further evaluated for their hERG potassium channel, calcium channel, Cyp2D6, and pharmacokinetic profiles.

Published

2007

17. Triazolopiperazine-amides as dipeptidyl peptidase IV inhibitors: Close analogs of JANUVIA™ (sitagliptin phosphate)

Author

Joseph K. Wu, KellyAnn D. Pryor, Ann E. Weber, George J. Eiermann, Reshma A. Patel, Dooseop Kim, Jinyou Xu, Nancy A. Thornberry, Anthony Mastracchio, Scott D. Edmondson, Jennifer E. Kowalchick, Huaibing He, Barbara Leiting, and Kathryn A. Lyons

Subjects

Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Piperazines, Dipeptidyl peptidase, Sitagliptin Phosphate, Structure-Activity Relationship, Oral administration, Drug Discovery, medicine, Animals, Structure–activity relationship, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, biology, Chemistry, Organic Chemistry, Triazoles, Amides, Rats, Enzyme, Enzyme inhibitor, Pyrazines, Sitagliptin, biology.protein, Molecular Medicine, medicine.drug

Abstract

A series of beta-aminoamides bearing triazolopiperazines has been prepared and evaluated as potent, selective, orally active dipeptidyl peptidase IV (DPP-4) inhibitors. Efforts at optimization of the beta-aminoamide series, which ultimately led to the discovery of JANUVIA (sitagliptin phosphate, compound 1), are described.

Published

2007

18. Optimization of 1,4-diazepan-2-one containing dipeptidyl peptidase IV inhibitors for the treatment of type 2 diabetes

Author

Joseph K. Wu, Xiaoxia Qian, Barbara Leiting, Ranabir SinhaRoy, Dennis Feng, Huaibing He, Aleksandr Petrov, Nancy A. Thornberry, Ann E. Weber, Bei Zhang, Gui-Bai Liang, Tesfaye Biftu, Xiaoping Zhang, George J. Eiermann, and Kathy Lyons

Subjects

Male, animal structures, Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Molecular Conformation, Administration, Oral, Pharmaceutical Science, Pharmacology, Biochemistry, Chemical synthesis, Rats, Sprague-Dawley, Inhibitory Concentration 50, Mice, chemistry.chemical_compound, Oral administration, Drug Discovery, Animals, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, biology, Organic Chemistry, Azepines, In vitro, Rats, Enzyme, Diabetes Mellitus, Type 2, Models, Chemical, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Lactam, Molecular Medicine, Pharmacophore, Derivative (chemistry)

Abstract

Following the discovery of N-acyl-1,4-diazepan-2-one as a novel pharmacophore for potent and selective DPP-4 inhibitors, optimization of this new lead with different substitution on the seven-membered ring resulted in several highly potent and selective, orally bioavailable, and efficacious DPP-4 inhibitors, such as 3R-methyl-1-cyclopropyl-1,4-diazepan-2-one derivative 9i (DPP-4 IC50 = 8.0 nM) and 3R,6R-dimethyl-1,4-diazepan-2-one derivative 14a (DPP-4 IC50 = 9.7 nM).

Published

2007

19. (3R)-4-[(3R)-3-Amino-4-(2,4,5-trifluorophenyl)butanoyl]-3-(2,2,2-trifluoroethyl)-1,4-diazepan-2-one, a selective dipeptidyl peptidase IV inhibitor for the treatment of type 2 diabetes

Author

Huaibing He, George J. Eiermann, Nancy A. Thornberry, Dennis Feng, Bei Zhang, Xiaoping Zhang, Tesfaye Biftu, Suresh B. Singh, Ranabir SinhaRoy, Kathy Lyons, Ann E. Weber, Ying-Duo Gao, Joseph K. Wu, Barbara Leiting, Gui-Bai Liang, Sangita B. Patel, Aleksandr Petrov, Xiaoxia Qian, Gerard R. Kieczykowski, and Giovanna Scapin

Subjects

medicine.medical_specialty, animal structures, Protein Conformation, Dipeptidyl Peptidase 4, Clinical Biochemistry, Pharmaceutical Science, Type 2 diabetes, Crystallography, X-Ray, Biochemistry, Dipeptidyl peptidase, Internal medicine, Diabetes mellitus, Drug Discovery, medicine, Animals, Hypoglycemic Agents, Protease Inhibitors, Oral glucose tolerance, Molecular Biology, Dipeptidyl-Peptidase IV Inhibitors, Chemistry, Sitagliptin Phosphate, Organic Chemistry, Rats, Inbred Strains, Azepines, Triazoles, medicine.disease, Rats, Endocrinology, Diabetes Mellitus, Type 2, Pyrazines, Sitagliptin, Molecular Medicine, medicine.drug

Abstract

Replacement of the triazolopiperazine ring of sitagliptin (DPP-4 IC50 = 18 nM) with 3-(2,2,2-trifluoroethyl)-1,4-diazepan-2-one gave dipeptidyl peptidase IV (DPP-4) inhibitor 1 which is potent (DPP-4 IC50 = 2.6 nM), selective, and efficacious in an oral glucose tolerance test in mice. It was selected for extensive preclinical development as a potential back-up candidate to sitagliptin.

Published

2007

20. Structure-activity-relationship of amide and sulfonamide analogs of omarigliptin

Author

Joseph K. Wu, George J. Eiermann, Jeffrey T. Kuethe, Robert R. Wilkening, Aleksandr Petrov, Xiaohua Li, Ann E. Weber, Jason M. Cox, Ping Chen, Tesfaye Biftu, Kathryn A. Lyons, Joseph M. Metzger, Dennis Feng, Huaibing He, Ying-Duo Gao, Youwei Yan, James M. Apgar, Shiyao Xu, Ranabir Sinha Roy, Giovanna Scapin, Xiaoxia Qian, and George A. Doss

Subjects

Stereochemistry, Dipeptidyl Peptidase 4, Clinical Biochemistry, Pharmaceutical Science, Omarigliptin, Biochemistry, Heterocyclic Compounds, 2-Ring, chemistry.chemical_compound, Structure-Activity Relationship, Dogs, Amide, Drug Discovery, Structure–activity relationship, Animals, Molecular Biology, Dipeptidyl-Peptidase IV Inhibitors, Pyrans, chemistry.chemical_classification, Sulfonamides, Binding Sites, Organic Chemistry, Amides, Sulfonamide, Protein Structure, Tertiary, Rats, Molecular Docking Simulation, Orally active, Long acting, chemistry, Molecular Medicine, Half-Life

Abstract

A series of novel substituted-[(3R)-amino-2-(2,5-difluorophenyl)]tetrahydro-2H-pyran analogs have been prepared and evaluated as potent, selective and orally active DPP-4 inhibitors. These efforts lead to the discovery of a long acting DPP-4 inhibitor, omarigliptin (MK-3102), which recently completed phase III clinical development and has been approved in Japan.

Published

2015

21. Discovery of potent, selective, and orally bioavailable pyridone-based dipeptidyl peptidase-4 inhibitors

Author

Reshma A. Patel, Aleksandr Petrov, Frank Marsilio, Barbara Leiting, Kathryn A. Lyons, Anthony Mastracchio, Lan Wei, Jinyou Xu, Ann E. Weber, Nancy A. Thornberry, George J. Eiermann, Joseph F. Leone, Joseph K. Wu, Scott D. Edmondson, Huaibing He, and Robert J. Mathvink

Subjects

Adenosine Deaminase, Nitrogen, Pyridones, Dipeptidyl Peptidase 4, Clinical Biochemistry, Administration, Oral, Biological Availability, Pharmaceutical Science, Sensitivity and Specificity, Biochemistry, Chemical synthesis, Substrate Specificity, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Oral administration, Drug Discovery, Adenosine Deaminase Inhibitors, Animals, Humans, Structure–activity relationship, Protease Inhibitors, Molecular Biology, Dipeptidyl peptidase-4, Glycoproteins, chemistry.chemical_classification, Molecular Structure, biology, Organic Chemistry, Amides, Macaca mulatta, Rats, Bioavailability, Enzyme, chemistry, Enzyme inhibitor, Lactam, biology.protein, Molecular Medicine

Abstract

anti-Substituted beta-methylphenylalanine derived amides have been shown to be potent DPP-IV inhibitors exhibiting excellent selectivity over both DPP8 and DPP9. The optimized compound exhibited good pharmacokinetic profiles in three preclinical species.

Published

2006

22. Dipeptidyl Peptidase IV Inhibition for the Treatment of Type 2 Diabetes

Author

Hyun O. Ok, Tesfaye Biftu, Ann E. Weber, Scott D. Edmondson, William P. Feeney, Joseph K. Wu, Kelly Ann Pryor, George R. Lankas, Reshma A. Patel, Aleksandr Petrov, Xiaoping Zhang, Xiaoxia Qian, Nancy A. Thornberry, Dooseop Kim, Andrea Woods, Ranabir Sinha Roy, George J. Eiermann, Chi-Chung Chan, Dawn E. Ippolito, Maria G. Beconi, Lan Zhu, Leah Bitalac Reigle, Huaibing He, Dennis M. Zaller, Barbara Leiting, and Kathryn A. Lyons

Subjects

Dipeptidase, medicine.medical_specialty, education.field_of_study, animal structures, biology, Endocrinology, Diabetes and Metabolism, Incretin, medicine.disease, Dipeptidyl peptidase 8, Dipeptidyl peptidase, Dipeptidyl Peptidase 9, Endocrinology, Internal medicine, Toxicity, Internal Medicine, medicine, biology.protein, Reticulocytopenia, education, Dipeptidyl peptidase-4

Abstract

Dipeptidyl peptidase (DPP)-IV inhibitors are a new approach to the treatment of type 2 diabetes. DPP-IV is a member of a family of serine peptidases that includes quiescent cell proline dipeptidase (QPP), DPP8, and DPP9; DPP-IV is a key regulator of incretin hormones, but the functions of other family members are unknown. To determine the importance of selective DPP-IV inhibition for the treatment of diabetes, we tested selective inhibitors of DPP-IV, DPP8/DPP9, or QPP in 2-week rat toxicity studies and in acute dog tolerability studies. In rats, the DPP8/9 inhibitor produced alopecia, thrombocytopenia, reticulocytopenia, enlarged spleen, multiorgan histopathological changes, and mortality. In dogs, the DPP8/9 inhibitor produced gastrointestinal toxicity. The QPP inhibitor produced reticulocytopenia in rats only, and no toxicities were noted in either species for the selective DPP-IV inhibitor. The DPP8/9 inhibitor was also shown to attenuate T-cell activation in human in vitro models; a selective DPP-IV inhibitor was inactive in these assays. Moreover, we found DPP-IV inhibitors that were previously reported to be active in models of immune function to be more potent inhibitors of DPP8/9. These results suggest that assessment of selectivity of potential clinical candidates may be important to an optimal safety profile for this new class of antihyperglycemic agents.

Published

2005

23. Discovery of potent and selective phenylalanine based dipeptidyl peptidase IV inhibitors

Author

Jinyou, Xu, Lan, Wei, Robert, Mathvink, Jiafang, He, You-Jung, Park, Huaibing, He, Barbara, Leiting, Kathryn A, Lyons, Frank, Marsilio, Reshma A, Patel, Joseph K, Wu, Nancy A, Thornberry, and Ann E, Weber

Subjects

Dipeptidyl Peptidase 4, Phenylalanine, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Protease Inhibitors, Molecular Biology, Biochemistry

Abstract

anti-Substituted beta-methylphenylalanine derived amides have been shown to be potent DPP-IV inhibitors exhibiting excellent selectivity over both DPP8 and DPP9. These are among the most potent compounds reported to date lacking an electrophilic trap. The most potent compound among these is 5-oxo-1,2,4-oxadiazole 44, which is a 3 nM DPP-IV inhibitor.

Published

2005

24. Dipeptidyl peptidase IV inhibitors derived from β-aminoacylpiperidines bearing a fused thiazole, oxazole, isoxazole, or pyrazole

Author

Reshma A. Patel, Hong Dong, Ann E. Weber, Joseph K. Wu, Wallace T. Ashton, George A. Doss, Huaibing He, Nancy A. Thornberry, Barbara Leiting, Kathryn A. Lyons, Frank Marsilio, and Rosemary Sisco

Subjects

Stereochemistry, medicine.drug_class, Dipeptidyl Peptidase 4, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Pyrazole, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Piperidines, Drug Discovery, medicine, Protease Inhibitors, Isoxazole, Thiazole, Oxazoles, Molecular Biology, Oxazole, Bicyclic molecule, biology, Organic Chemistry, Isoxazoles, Thiazoles, chemistry, Enzyme inhibitor, biology.protein, Pyrazoles, Molecular Medicine

Abstract

A series of β-aminoacylpiperidines bearing various fused five-membered heterocyclic rings was synthesized as dipeptidyl peptidase IV inhibitors. Potent and relatively selective inhibition could be obtained, depending on choice of heterocycle, regioisomerism, and substitution. In particular, one analog (74, DPP-IV IC50 = 26 nM) exhibited good oral bioavailability and acceptable half-life in the rat, albeit with rather high clearance.

Published

2005

25. (2R)-4-Oxo-4-[3-(Trifluoromethyl)-5,6-dihydro[1,2,4]triazolo[4,3-a]pyrazin- 7(8H)-yl]-1-(2,4,5-trifluorophenyl)butan-2-amine: A Potent, Orally Active Dipeptidyl Peptidase IV Inhibitor for the Treatment of Type 2 Diabetes

Author

Ann E. Weber, Margaret E. McCann, Lan Zhu, Matthew J. Wyvratt, Sangita B. Patel, Gerard J. Hickey, Joseph K. Wu, Jennifer E. Kowalchick, Dooseop Kim, Bei B. Zhang, George J. Eiermann, Barbara Leiting, Kathryn A. Lyons, Huaibing He, Maria G. Beconi, Frank Marsilio, Nancy A. Thornberry, Reshma A. Patel, Aleksandr Petrov, Liping Wang, Michael H. Fisher, Ranabir Sinha Roy, and Giovanna Scapin

Subjects

Blood Glucose, Models, Molecular, Protein Conformation, medicine.drug_class, Stereochemistry, Dipeptidyl Peptidase 4, Drug Evaluation, Preclinical, Administration, Oral, Carboxamide, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Dipeptidyl peptidase, Sitagliptin Phosphate, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Glucagon-Like Peptide 1, Drug Discovery, medicine, Animals, Hypoglycemic Agents, Enzyme Inhibitors, Protein Precursors, Binding Sites, Trifluoromethyl, Dose-Response Relationship, Drug, biology, Bicyclic molecule, Glucose Tolerance Test, Triazoles, Glucagon, Peptide Fragments, Rats, Mice, Inbred C57BL, Diabetes Mellitus, Type 2, chemistry, Enzyme inhibitor, Pyrazines, biology.protein, Molecular Medicine, Amine gas treating

Abstract

A novel series of beta-amino amides incorporating fused heterocycles, i.e., triazolopiperazines, were synthesized and evaluated as inhibitors of dipeptidyl peptidase IV (DPP-IV) for the treatment of type 2 diabetes. (2R)-4-Oxo-4-[3-(trifluoromethyl)-5,6-dihydro[1,2,4]triazolo[4,3-a]pyrazin-7(8H)-yl]-1-(2,4,5-trifluorophenyl)butan-2-amine (1) is a potent, orally active DPP-IV inhibitor (IC(50) = 18 nM) with excellent selectivity over other proline-selective peptidases, oral bioavailability in preclinical species, and in vivo efficacy in animal models. MK-0431, the phosphate salt of compound 1, was selected for development as a potential new treatment for type 2 diabetes.

Published

2004

26. Discovery of potent and selective β-homophenylalanine based dipeptidyl peptidase IV inhibitors

Author

Ann E. Weber, Hyun O. Ok, Joseph K. Wu, Frank Marsilio, Lawrence F. Colwell, Huaibing He, Emma R. Parmee, Reshma A. Patel, Jinyou Xu, Bahanu Habulihaz, Edward Gonzalez, Nancy A. Thornberry, Barbara Leiting, and Kathryn A. Lyons

Subjects

Stereochemistry, Dipeptidyl Peptidase 4, Clinical Biochemistry, Biological Availability, Pharmaceutical Science, Peptide, Phenylalanine, Methylation, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Amide, Drug Discovery, Animals, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Aminobutyrates, Organic Chemistry, In vitro, Rats, Thiazoles, Enzyme, chemistry, Enzyme inhibitor, Electrophile, biology.protein, Molecular Medicine, Half-Life

Abstract

Modification of in-house screening lead beta-aminoacyl proline 8 gave an equipotent thiazolidide 9. Extensive SAR studies on the phenyl ring of 9 led to the discovery of a novel series of potent and selective DP-IV inhibitors. Introduction of a fluorine at the 2-position proved to be crucial for the potency of this series. The 2,5-difluoro (22q) and 2,4,5-trifluoro (22t) analogues were potent inhibitors of DP-IV (IC(50)=270, 119nM, respectively).

Published

2004

27. 4-Amino cyclohexylglycine analogues as potent dipeptidyl peptidase IV inhibitors

Author

Anthony Mastracchio, George J. Eiermann, Ann E. Weber, Reshma A. Patel, Aleksandr Petrov, Larry Colwell, Ruth Kilburn, Scott D. Edmondson, William P. Feeney, Joseph K. Wu, Huaibing He, Jiafang He, Emma R. Parmee, Nancy A. Thornberry, Barbara Leiting, Kathryn A. Lyons, Bahanu Habulihaz, Jerry Di Salvo, and Frank Marsilio

Subjects

Potassium Channels, Dipeptidyl Peptidase 4, Clinical Biochemistry, Glycine, Pharmaceutical Science, Biochemistry, Chemical synthesis, Mice, chemistry.chemical_compound, Pharmacokinetics, Oral administration, In vivo, Amide, Drug Discovery, Animals, Hypoglycemic Agents, Protease Inhibitors, Cation Transport Proteins, Molecular Biology, chemistry.chemical_classification, biology, Organic Chemistry, Ether-A-Go-Go Potassium Channels, In vitro, Rats, Enzyme, chemistry, Potassium Channels, Voltage-Gated, Enzyme inhibitor, biology.protein, Molecular Medicine, Protein Binding

Abstract

Substituted 4-amino cyclohexylglycine analogues were evaluated for DP-IV inhibitory properties. Bis-sulfonamide 15e was an extremely potent 2.6 nM inhibitor of the enzyme with excellent selectivity over all counterscreens. 2,4-difluorobenzenesulfonamide 15b and 1-naphthyl amide 16b, however, combined an acceptable in vitro profile with good pharmacokinetic properties in the rat, and 15b was orally efficacious at 3 mpk in an OGTT in lean mice.

Published

2004

28. Erratum. Dipeptidyl Peptidase 4 Inhibition Stimulates Distal Tubular Natriuresis and Increases in Circulating SDF-1α 1-67 in Patients With Type 2 Diabetes. Diabetes Care 2017;40:1073–1081

Author

Shajiha Khan, Weixun Wang, Lucinda Hittle, Amy Locke, David Z.I. Cherney, Robel Alemu, Huaibing He, Leif E. Lovblom, Vesta Lai, Harindra Rajasekeran, Daniel J. Drucker, Julie A. Lovshin, and Yulyia Lytvyn

Subjects

Advanced and Specialized Nursing, medicine.medical_specialty, Errata, business.industry, Endocrinology, Diabetes and Metabolism, Type 2 diabetes, medicine.disease, Natriuresis, Endocrinology, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, In patient, business, Dipeptidyl peptidase-4

Abstract

In the above-mentioned article, six asterisks were added to Fig. 2. In addition, the following information …

Published

2017

29. Omarigliptin (MK-3102): a novel long-acting DPP-4 inhibitor for once-weekly treatment of type 2 diabetes

Author

Xiaoping Zhang, Nancy A. Thornberry, Ann E. Weber, Sangita B. Patel, Annette Bak, Gino Salituro, Huaibing He, Ranabir SinhaRoy, Bei Zhang, Xiaoxia Qian, Jacqueline D. Hicks, Kathy Lyons, Ping Chen, Dennis Feng, Tesfaye Biftu, Davida Krueger, Jason M. Cox, Shiyao Sherrie Xu, Giovanna Scapin, Ying-Duo Gao, Sharon Tong, Charles Sewall, Youwei Yan, Aleksandr Petrov, Jeffrey T. Kuethe, George J. Eiermann, Joseph K. Wu, George A. Doss, and Jiafang He

Subjects

Dipeptidyl-Peptidase IV Inhibitors, Chemistry, Once weekly, Type 2 diabetes, Pharmacology, medicine.disease, Omarigliptin, Heterocyclic Compounds, 2-Ring, Structure-Activity Relationship, Long acting, Mechanism of action, Pharmacokinetics, Diabetes Mellitus, Type 2, Drug Discovery, medicine, Molecular Medicine, Animals, Humans, Hypoglycemic Agents, Dosing, medicine.symptom, Dipeptidyl peptidase-4, Pyrans

Abstract

In our effort to discover DPP-4 inhibitors with added benefits over currently commercially available DPP-4 inhibitors, MK-3102 (omarigliptin), was identified as a potent and selective dipeptidyl peptidase 4 (DPP-4) inhibitor with an excellent pharmacokinetic profile amenable for once-weekly human dosing and selected as a clinical development candidate. This manuscript summarizes the mechanism of action, scientific rationale, medicinal chemistry, pharmacokinetic properties, and human efficacy data for omarigliptin, which is currently in phase 3 clinical development.

Published

2014

30. Simultaneous determination of codeine and it seven metabolites in plasma and urine by high-performance liquid chromatography with ultraviolet and electrochemical detection

Author

Sheila Shay, Huaibing He, Margaret Wood, Alastair J. J. Wood, and Yoseph Caraco

Subjects

Normorphine, Detection limit, Chromatography, Codeine, Chemistry, Reproducibility of Results, General Chemistry, Urine, Sensitivity and Specificity, High-performance liquid chromatography, chemistry.chemical_compound, Norcodeine, Electrochemistry, medicine, Humans, Spectrophotometry, Ultraviolet, Solid phase extraction, Sodium dodecyl sulfate, Glucuronide, Chromatography, High Pressure Liquid, medicine.drug

Abstract

A sensitive and selective high-performance liquid chromatography method has been developed for the measurement of codeine and its seven metabolites, norcodeine, morphine, normorphine, codeine-6-glucuronide, morphine-6-glucuronide, morphine-3-glucuronide and norcodeine glucuronide, in plasma and urine. The compounds were recovered from plasma and urine using solid-phase extraction with C18 cartridges and separated on a reversed-phase C8 column with a mobile phase consisting of 77% buffer (5 mM sodium phosphate monobasic and 0.70 mM sodium dodecyl sulfate, pH 2.35) and 23% acetonitrile. Codeine, norcodeine, codeine-6-glucuronide, norcodeine glucuronide and morphine-3-glucuronide were detected by ultraviolet detection at 214 nm, with a detection limit of 0.02 nmol/ml for each compound in plasma. Morphine-6-glucuronide, normorphine and morphine were monitored by electrochemical detection at 350 mV, with a detection limit of 0.003 nmol/ml for each compound in plasma. The assay showed good reproducibility and accuracy using external standardization. The recovery and inter-day variation for all compounds in plasma samples were 63.40-77.90% and 3.49-16.77% (R.S.D.) and while in urine were 64.98-90.13% and 2.93-9.96% (R.S.D.), respectively.

Published

1998

31. Norepinephrine Release in the Human Forearm

Author

Charles M. Stein, Richard Nelson, Huaibing He, Margaret Wood, and Alastair J. J. Wood

Subjects

Adult, Male, medicine.medical_specialty, Sympathetic nervous system, Time Factors, Brachial Artery, Epinephrine, Norepinephrine (medication), Norepinephrine, Forearm, Reference Values, Internal medicine, medicine.artery, Internal Medicine, medicine, Humans, Brachial artery, Receptor, business.industry, medicine.anatomical_structure, Endocrinology, Injections, Intra-Arterial, Hypertension, Catecholamine, Blood Vessels, medicine.symptom, business, Vasoconstriction, medicine.drug

Abstract

Abstract It has been postulated that delayed facilitation of norepinephrine release by epinephrine is causally related to the development of hypertension. It has been proposed that a brief increase in epinephrine concentrations results in the uptake of epinephrine into the sympathetic nerve terminal. Subsequent rerelease of epinephrine stimulates presynaptic β-adrenergic receptors, resulting in a prolonged increase in plasma norepinephrine (NE) concentrations, with amplified sympathetic responses and vasoconstriction. To determine whether such epinephrine-induced, delayed facilitation of NE release occurs in a vascular bed draining resistance vessels and, if it occurs, whether that facilitation differs in hypertension, we used a radioisotope dilution method to measure unstimulated and isoproterenol-stimulated forearm NE spillover before, during, and after a 50 ng/min infusion of epinephrine for 30 minutes directly into the brachial artery. No delayed facilitatory effects of epinephrine on forearm NE spillover were observed in either 6 normotensive (NT) or 8 borderline hypertensive (BHT) subjects (NT unstimulated forearm NE spillover preepinephrine 1.79±0.41 ng/min versus postepinephrine 2.36±0.65 ng/min, P =.38; BHT preepinephrine 2.24±0.70 ng/min versus postepinephrine 1.93±0.46 ng/min, P =.51; NT isoproterenol-stimulated forearm NE spillover preepinephrine 4.61±1.01 ng/min versus postepinephrine 4.4±0.98 ng/min, P =.9; BHT preepinephrine 4.04±1.36 ng/min versus postepinephrine 4.69±1.49 ng/min P =.5). We conclude that the short-term local infusion of epinephrine does not have a delayed facilitatory effect on forearm NE spillover in NT or BHT subjects. Therefore, the prolonged increase in NE concentrations after epinephrine infusion previously shown systemically, and not seen locally in the forearm, suggests that the delayed facilitatory response to epinephrine may occur in other organs.

Published

1997

32. Cyclosporine Impairs Vasodilation Without Increased Sympathetic Activity in Humans

Author

Alastair J. J. Wood, C. M. Stein, Theodore Pincus, and Huaibing He

Subjects

Adult, Male, medicine.medical_specialty, Sympathetic nervous system, Sympathetic Nervous System, Vasodilation, Muscle, Smooth, Vascular, Veins, Nephrotoxicity, Norepinephrine (medication), Phenylephrine, Internal medicine, polycyclic compounds, Internal Medicine, medicine, Humans, Alprostadil, Aged, Dose-Response Relationship, Drug, business.industry, Isoproterenol, Middle Aged, Hand, Transplantation, medicine.anatomical_structure, Endocrinology, Cyclosporine, Female, medicine.symptom, business, Vasoconstriction, medicine.drug, Blood vessel

Abstract

Abstract Hypertension and nephrotoxicity frequently complicate treatment with cyclosporine; two suggested mechanisms are increased sympathetic activity and altered vascular reactivity. It is difficult to assess these mechanisms in patients receiving cyclosporine after transplantation because of the accompanying major physiological alterations. Therefore, we studied 12 patients with rheumatoid arthritis twice—while they were taking and not taking cyclosporine. We measured vascular response in the dorsal hand vein using the linear variable differential transformer technique. Cyclosporine treatment significantly attenuated vasodilation induced by 60 ng/min isoproterenol (no cyclosporine, 19.8±3.5% versus cyclosporine, 7.9±2.2%; P =.02) and prostaglandin E 1 at 1000 pg/min (no cyclosporine, 72.6±10.2% versus cyclosporine, 45.6±9.0%) and 2000 pg/min (no cyclosporine, 100.8±14.7% versus cyclosporine, 68.6±8.0%; F=5.47, P =.047). However, neither vascular response to phenylephrine or nitroglycerin nor sympathetic activity assessed by measurement of norepinephrine spillover with a radioisotope dilution technique was affected by cyclosporine (no cyclosporine, 516.1±47.9 ng/min versus cyclosporine, 476.6±51.8 ng/min; P =.42). Cyclosporine impaired venodilation in response to two agonists that act through adenylate cyclase without altering α-agonist–induced venoconstriction or sympathetic activity. Therefore, in humans impaired vasodilation rather than sympathetic activation or enhanced vasoconstriction may be an important mechanism for the alterations of vascular tone that occur after long-term cyclosporine administration.

Published

1995

33. A new class of prolylcarboxypeptidase inhibitors, part 1: discovery and evaluation

Author

Xinchun Tong, Zhu Shen, Huaibing He, Andreas Verras, Kelly Bleasby, Wensheng Liu, Elaine C. Tung, Urmi R. Bhatt, Thomas H. Graham, Jeffrey J. Hale, Xiaohua Li, Suoyu Xu, Iyassu K. Sebhat, Judyann Wiltsie, Dan Xie, Margarita Garcia-Calvo, Michael E. Lassman, Jianying Xiao, Dong-Ming Shen, JeanMarie Lisnock, Wayne M. Geissler, Judith N. Gorski, Yusheng Xiong, Shirly Pinto, and Qing Chen

Subjects

Male, Pyrrolidines, High-throughput screening, Butanols, Clinical Biochemistry, Pharmaceutical Science, Carboxypeptidases, Pharmacology, Biochemistry, Inhibitory Concentration 50, Mice, In vivo, Drug Discovery, Ic50 values, Animals, Obesity, Enzyme Inhibitors, Molecular Biology, biology, Molecular Structure, Chemistry, Organic Chemistry, Target engagement, Minimal activity, In vitro, Enzyme Activation, Mice, Inbred C57BL, Enzyme inhibitor, biology.protein, Molecular Medicine, Ex vivo

Abstract

A new structural class of potent prolylcarboxypeptidase (PrCP) inhibitors was discovered by high-throughput screening. The series possesses a tractable SAR profile with sub-nanomolar in vitro IC50 values. Compared to prior inhibitors, the new series demonstrated minimal activity shifts in pure plasma and complete ex vivo plasma target engagement in mouse plasma at the 20 h post-dose time point (po). In addition, the in vivo level of CNS and non-CNS drug exposure was measured.

Published

2012

34. A new class of prolylcarboxypeptidase inhibitors, part 2: the aminocyclopentanes

Author

Jianying Xiao, Kelly Bleasby, Dong-Ming Shen, Thomas H. Graham, Suoyu Xu, Jeffrey J. Hale, Judyann Wiltsie, Andreas Verras, Michael E. Lassman, Judith N. Gorski, Mikhail Reibarkh, JeanMarie Lisnock, Wensheng Liu, Margarita Garcia-Calvo, Qing Chen, Huaibing He, Shirly Pinto, Wayne M. Geissler, Elaine C. Tung, Urmi R. Bhatt, Xinchun Tong, Dan Xie, Xiaohua Li, and Zhu Shen

Subjects

Male, High-throughput screening, Clinical Biochemistry, Pharmaceutical Science, Carboxypeptidases, Cyclopentanes, Pharmacology, Biochemistry, Pyrrolidine, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Pharmacokinetics, Drug Discovery, Animals, Obesity, Amines, Enzyme Inhibitors, Molecular Biology, biology, Molecular Structure, Chemistry, Organic Chemistry, Target engagement, In vitro, Minimal activity, Enzyme Activation, Mice, Inbred C57BL, Enzyme inhibitor, Cyclization, biology.protein, Molecular Medicine, Ex vivo

Abstract

A series of potent inhibitors of prolylcarboxypeptidase (PrCP) was developed by modifying a lead structure that was discovered by high-throughput screening. The tert -butyl pyrrolidine was replaced by an aminocyclopentane to reduce the metabolic liabilities of the original lead. The compounds demonstrated sub-nanomolar in vitro IC 50 values, minimal activity shifts in pure plasma and improved pharmacokinetics. Complete ex vivo plasma target engagement was achieved with low brain exposure at the 20 h time point following p.o. dosing in a mouse. The results indicate that the aminocyclopentanes are useful tools for studying the therapeutic potential of peripheral (non-CNS) PrCP inhibition.

Published

2012

35. The discovery of non-benzimidazole and brain-penetrant prolylcarboxypeptidase inhibitors

Author

Andreas Verras, Zhu Shen, Huaibing He, Suoyu Xu, Urmi R. Bhatt, Hong C. Shen, Dunlu Chen, Wayne M. Geissler, Margarita Garcia-Calvo, Dong-Ming Shen, Qing Chen, Wensheng Liu, Michael E. Lassman, Shirly Pinto, Dan Xie, Thomas H. Graham, Steven L. Colletti, Elaine C. Tung, Jeffrey J. Hale, Yusheng Xiong, Kelly Bleasby, Xinchun Tong, Renee M. Chabin, and James R. Tata

Subjects

Benzimidazole, ATP Binding Cassette Transporter, Subfamily B, Pyrrolidines, Time Factors, Clinical Biochemistry, Pharmaceutical Science, Carboxypeptidases, Biochemistry, Pyrrolidine, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Benzylamine, In vivo, Amide, Drug Discovery, Animals, Humans, Obesity, Molecular Biology, P-glycoprotein, biology, Chemistry, Organic Chemistry, Body Weight, Brain, Biological Transport, Amides, Disease Models, Animal, Models, Chemical, Enzyme inhibitor, biology.protein, Molecular Medicine, Benzimidazoles, Bioisostere

Abstract

Novel prolylcarboxypeptidase (PrCP) inhibitors with nanomolar IC50 values were prepared by replacing the previously described dichlorobenzimidazole-substituted pyrrolidine amides with a variety of substituted benzylamine amides. In contrast to prior series, the compounds demonstrated minimal inhibition shift in whole serum and minimal recognition by P-glycoprotein (P-gp) efflux transporters. The compounds were also cell permeable and demonstrated in vivo brain exposure. The in vivo effect of compound (S)-6e on weight loss in an established diet-induced obesity (eDIO) mouse model was studied.

Published

2011

36. Synthesis and evaluation of [(1R)-1-amino-2-(2,5-difluorophenyl)ethyl]cyclohexanes and 4-[(1R)-1-amino-2-(2,5-difluorophenyl)ethyl]piperidines as DPP-4 inhibitors

Author

Ann E. Weber, Ping Chen, Kathryn A. Lyons, Charles G. Caldwell, Nancy A. Thornberry, Joseph K. Wu, Wallace T. Ashton, and Huaibing He

Subjects

animal structures, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biological Availability, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Piperidines, Cyclohexanes, Drug Discovery, Animals, Proline, Molecular Biology, Dipeptidyl-Peptidase IV Inhibitors, biology, Chemistry, Organic Chemistry, Biological activity, Rats, Enzyme inhibitor, biology.protein, Molecular Medicine, Amine gas treating, Piperidine, Selectivity, Half-Life

Abstract

A series of 4-amino cyclohexanes and 4-substituted piperidines were prepared and evaluated for inhibition of DPP-4. Analog 20q displayed both good DPP-4 potency and selectivity against other proteases, while derivative 20k displayed long half life and modest oral bioavailability in rat. The most potent analog, 3-(5-aminocarbonylpyridyl piperidine 53j, displayed excellent DPP-4 activity with good selectivity versus other proline enzymes.

Published

2010

37. Optimization of high-performance liquid chromatographic assay for catecholamines

Author

Robert J. Deegan, Huaibing He, Margaret Wood, and Alastair J. J. Wood

Subjects

chemistry.chemical_compound, Column chromatography, Chromatography, Chemistry, Phase composition, Sodium, Extraction (chemistry), chemistry.chemical_element, Separation method, MONOCHLOROACETIC ACID, General Chemistry, Acetonitrile, Sodium acetate

Abstract

This paper describes the application of a window diagram technique to optimize the four components of eluent (sodium acetate, sodium heptanesulfonate, acetonitrile and pH adjusted by monochloroacetic acid), for complete separation of five catecholamine compounds and the internal standard (3,4-dihydroxybenzylamine, DHBA). In addition, studies were performed to address the problem of the variable recovery of DHBA from dog plasma due to a time-dependent loss of DHBA. We found that this phenomenon can be prevented by pH adjustment prior to addition of DHBA, allowing development of an accurate high-performance liquid chromatographic assay for plasma catecholamines in dogs.

Published

1992

38. Utility of unbound plasma drug levels and P-glycoprotein transport data in prediction of central nervous system exposure

Author

Z. Yao, G. M. Salituro, L. H. Cohen, Michael J. Hafey, K.A. Lyons, Suoyu Xu, Xiaohua Li, X. Shen, Kelly Bleasby, Huaibing He, Grace Chan, and Wei Tang

Subjects

Drug, Central Nervous System, Male, endocrine system diseases, Health, Toxicology and Mutagenesis, media_common.quotation_subject, Central nervous system, Plasma protein binding, Pharmacology, Toxicology, Biochemistry, Cell Line, Drug levels, Mice, Cerebrospinal fluid, Tandem Mass Spectrometry, polycyclic compounds, medicine, Animals, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, media_common, P-glycoprotein, Mice, Knockout, integumentary system, biology, Chemistry, Biological Transport, General Medicine, Blood proteins, female genital diseases and pregnancy complications, In vitro, carbohydrates (lipids), Mice, Inbred C57BL, medicine.anatomical_structure, Pharmaceutical Preparations, biology.protein, Chromatography, Liquid

Abstract

Drug concentrations in cerebrospinal fluid have been assumed to be a natural surrogate for total drug exposures in the central nervous system. The present communication reports a data set from a study of 30 compounds in mice. An attempt was made to correlate cerebrospinal fluid and unbound plasma drug concentrations via incorporation of in vitro P-glycoprotein (Pgp)-mediated transport data. 2. Pgp-deficient (Pgp -/-) and wild-type mice were dosed with compounds of interest by oral gavage (orally) at 5 mg kg −1 . Plasma and cerebrospinal fluid samples were collected at 1 h post-dosing, and analysed by liquid chromatography-tandem mass spectrometry (LC-MS/MS) for drug concentrations. Mouse and human Pgp-mediated transport were evaluated in vitro by a bi-directional (B to A and A to B) transport assay using LLC-PK1 cells expressing mouse (mdr1a) and human (MDR1) forms of Pgp, respectively. 3. Compounds with B to A/A to B transport ratios < 2 were defined as non-substrates of Pgp, whereas those exhibiting B to A/A to B transport ratios ≥2 were considered Pgp substrates. Plasma protein bind- ing was also determined in vitro via equilibrium dialysis. Of the 30 compounds, 13 were identified to be mouse Pgp substrates, all of which were also human Pgp substrates, demonstrating a good agreement between mouse and human data. 4. In Pgp wild-type mice, the unbound plasma and cerebrospinal fluid concentrations of the non-Pgp sub - strates correlated well, with a regression slope of approximately 1.0. A similar relationship existed for Pgp substrates in Pgp -/- mice. On the other hand, an improved correlation of cerebrospinal fluid and systemic exposures of the Pgp substrates in Pgp wild-type mice was observed when the unbound plasma concentrations were normalized to the corresponding B to A/A to B transport ratios. 5. These results reinforce the premise that a combined use of unbound plasma drug concentrations and in vitro Pgp transport data may be of value for the estimation of central nervous system exposures.

Published

2009

39. Fluoroolefins as amide bond mimics in dipeptidyl peptidase IV inhibitors

Author

Sangita B. Patel, Jackie Shang, Joseph K. Wu, Huaibing He, Reshma A. Patel, Barbara Leiting, Kathryn A. Lyons, Lan Wei, Jinyou Xu, Ashok Chaudhary, Nancy A. Thornberry, Scott D. Edmondson, Maria G. Beconi, Dennis C. Dean, Ann E. Weber, Jianmei Pang, Shiyao Xu, and Giovanna Scapin

Subjects

Hydrocarbons, Fluorinated, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Alkenes, Biochemistry, Chemical synthesis, Substrate Specificity, chemistry.chemical_compound, Structure-Activity Relationship, Amide, Drug Discovery, Structure–activity relationship, Peptide bond, Animals, Hypoglycemic Agents, Molecular Biology, Dipeptidyl peptidase-4, Dipeptidyl-Peptidase IV Inhibitors, biology, Chemistry, Organic Chemistry, Molecular Mimicry, Stereoisomerism, Amides, Rats, Models, Chemical, Enzyme inhibitor, biology.protein, Microsomes, Liver, Molecular Medicine, Bioisostere, Drug metabolism

Abstract

The synthesis, selectivity, rat pharmacokinetic profile, and drug metabolism profiles of a series of potent fluoroolefin-derived DPP-4 inhibitors (4) are reported. A radiolabeled fluoroolefin 33 was shown to possess a high propensity to form reactive metabolites, thus revealing a potential liability for this class of DPP-4 inhibitors.

Published

2008

40. Rational design of a novel, potent, and orally bioavailable cyclohexylamine DPP-4 inhibitor by application of molecular modeling and X-ray crystallography of sitagliptin

Author

Sangita B. Patel, Joseph K. Wu, Joe W. Becker, Huaibing He, Xiaoping Zhang, Suresh B. Singh, Bei Zhang, Nancy A. Thornberry, Tesfaye Biftu, George A. Doss, Giovanna Scapin, Ranabir SinhaRoy, Ann E. Weber, George J. Eiermann, Kathy Lyons, Dennis Feng, and Aleksandr Petrov

Subjects

Models, Molecular, Molecular model, Stereochemistry, Dipeptidyl Peptidase 4, Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Cyclohexylamine, Crystallography, X-Ray, Biochemistry, Sitagliptin Phosphate, chemistry.chemical_compound, Inhibitory Concentration 50, Amide, Drug Discovery, medicine, Adenosine Deaminase Inhibitors, Moiety, Humans, Molecular Biology, Glycoproteins, Cyclohexylamines, Dipeptidyl-Peptidase IV Inhibitors, Binding Sites, biology, Chemistry, Organic Chemistry, Rational design, HIV Protease Inhibitors, Triazoles, Models, Chemical, Enzyme inhibitor, Sitagliptin, Drug Design, Pyrazines, biology.protein, Molecular Medicine, medicine.drug

Abstract

Molecular modeling was used to design a rigid analog of sitagliptin 1. The X-ray crystal structure of sitagliptin bound to DPP-4 suggested that the central beta-amino butyl amide moiety could be replaced with a cyclohexylamine group. This was confirmed by structural analysis and the resulting analog 2a was synthesized and found to be a potent DPP-4 inhibitor (IC(50)=21 nM) with excellent in vivo activity and pharmacokinetic profile.

Published

2007

41. 4-aminophenylalanine and 4-aminocyclohexylalanine derivatives as potent, selective, and orally bioavailable inhibitors of dipeptidyl peptidase IV

Author

Reshma A. Patel, Huaibing He, Nancy A. Thornberry, Ann E. Weber, Brian A. Kirk, Joseph K. Wu, Joseph L. Duffy, Giovanna Scapin, Barbara Leiting, Kathryn A. Lyons, George J. Eiermann, Liping Wang, Sangita B. Patel, and Alexsandr Petrov

Subjects

Models, Molecular, medicine.drug_class, Stereochemistry, Dipeptidyl Peptidase 4, Phenylalanine, Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Biological Availability, Carboxamide, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Dipeptidyl peptidase, Mice, Structure-Activity Relationship, Cyclohexanes, Drug Discovery, medicine, Animals, Enzyme Inhibitors, Molecular Biology, Dipeptidyl peptidase-4, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, Alanine, Binding Sites, biology, Molecular Structure, Organic Chemistry, Glucose Tolerance Test, Bioavailability, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine

Abstract

A novel series of 4-aminophenylalanine and 4-aminocyclohexylalanine derivatives were designed and evaluated as inhibitors of dipeptidyl peptidase IV (DPP-4). The phenylalanine series afforded compounds such as 10 that were potent and selective (DPP-4, IC50 = 28 nM), but exhibited limited oral bioavailability. The corresponding cyclohexylalanine derivatives such as 25 afforded improved PK exposure and efficacy in a murine OGTT experiment. The X-ray crystal structure of 25 bound to the DPP-4 active site is presented.

Published

2006

42. (2S,3S)-3-Amino-4-(3,3-difluoropyrrolidin-1-yl)-N,N-dimethyl-4-oxo-2-(4-[1,2,4]triazolo[1,5-a]-pyridin-6-ylphenyl)butanamide: a selective alpha-amino amide dipeptidyl peptidase IV inhibitor for the treatment of type 2 diabetes

Author

Joseph K. Wu, Anthony Mastracchio, Nancy A. Thornberry, Alexsandr Petrov, George J. Eiermann, Barbara Leiting, Ranabir Sinha Roy, Park Yj, Giovanna Scapin, Robert J. Mathvink, Suoyu Xu, Ann E. Weber, Dorothy Levorse, Jackie Shang, Joseph F. Leone, Reshma A. Patel, Huaibing He, Jiafang He, Scott D. Edmondson, Kathy Lyons, Shil Patel, Bart Harper, Adrian L. Smith, Di Salvo J, Bing Zhu, and Maria G. Beconi

Subjects

Male, Models, Molecular, Calcium Channels, L-Type, Stereochemistry, Dipeptidyl Peptidase 4, Phenylalanine, Administration, Oral, Biological Availability, Mice, Obese, Muscle Proteins, In Vitro Techniques, Crystallography, X-Ray, Dipeptidyl peptidase, Sodium Channels, Cell Line, NAV1.5 Voltage-Gated Sodium Channel, chemistry.chemical_compound, Mice, Structure-Activity Relationship, In vivo, Amide, Drug Discovery, Animals, Humans, Hypoglycemic Agents, Protease Inhibitors, Muscle, Skeletal, IC50, chemistry.chemical_classification, biology, Chemistry, Stereoisomerism, Glucose Tolerance Test, Triazoles, Bioavailability, Mice, Inbred C57BL, Enzyme, Diabetes Mellitus, Type 2, Enzyme inhibitor, biology.protein, Microsomes, Liver, Molecular Medicine, Triazolopyridine, Rabbits

Abstract

A series of beta-substituted biarylphenylalanine amides were synthesized and evaluated as inhibitors of dipeptidyl peptidase IV (DPP-4) for the treatment of type 2 diabetes. Optimization of the metabolic profile of early analogues led to the discovery of (2S,3S)-3-amino-4-(3,3-difluoropyrrolidin-1-yl)-N,N-dimethyl-4-oxo-2-(4-[1,2,4]triazolo[1,5-a]pyridin-6-ylphenyl)butanamide (6), a potent, orally active DPP-4 inhibitor (IC(50) = 6.3 nM) with excellent selectivity, oral bioavailability in preclinical species, and in vivo efficacy in animal models. Compound 6 was selected for further characterization as a potential new treatment for type 2 diabetes.

Published

2006

43. Discovery of potent, selective, and orally bioavailable oxadiazole-based dipeptidyl peptidase IV inhibitors

Author

George J. Eiermann, Sangita B. Patel, Nancy A. Thornberry, Joseph K. Wu, Ann E. Weber, Barbara Leiting, Kathryn A. Lyons, Joseph F. Leone, Jinyou Xu, Lan Wei, Scott D. Edmondson, Frank Marsilio, Giovanna Scapin, Reshma A. Patel, Aleksandr Petrov, Robert J. Mathvink, and Huaibing He

Subjects

Models, Molecular, animal structures, Stereochemistry, Protein Conformation, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Oxadiazole, Administration, Oral, Biological Availability, Stereoisomerism, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Dogs, Amide, Drug Discovery, Structure–activity relationship, Animals, Humans, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, Dipeptidyl-Peptidase IV Inhibitors, Oxadiazoles, Binding Sites, biology, Organic Chemistry, Ether-A-Go-Go Potassium Channels, Rats, Enzyme Activation, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Selectivity

Abstract

A novel series of oxadiazole based amides have been shown to be potent DPP-4 inhibitors. The optimized compound 43 exhibited excellent selectivity over a variety of DPP-4 homologs.

Published

2006

44. Hit-to-Lead Optimization and Discovery of 5-((5-([1,1'-Biphenyl]-4-yl)-6-chloro-1H-benzo[d]imidazol-2-yl)oxy)-2-methylbenzoic Acid (MK-3903): A Novel Class of Benzimidazole-Based Activators of AMP-Activated Protein Kinase.

Author

Ping Lan, Romero, F. Anthony, Wodka, Dariusz, Kassick, Andrew J., Qun Dang, Gibson, Tony, Cashion, Daniel, Gaochao Zhou, Yuli Chen, Xiaoping Zhang, Aihua Zhang, Ying Li, Trujillo, Maria E., Qing Shao, Wu, Margaret, Shiyao Xu, Huaibing He, MacKenna, Deidre, Staunton, Jocelyn, and Chapman, Kevin T.

Published

2017

45. Dipeptidyl peptidase IV inhibition for the treatment of type 2 diabetes: potential importance of selectivity over dipeptidyl peptidases 8 and 9

Author

George R, Lankas, Barbara, Leiting, Ranabir Sinha, Roy, George J, Eiermann, Maria G, Beconi, Tesfaye, Biftu, Chi-Chung, Chan, Scott, Edmondson, William P, Feeney, Huaibing, He, Dawn E, Ippolito, Dooseop, Kim, Kathryn A, Lyons, Hyun O, Ok, Reshma A, Patel, Aleksandr N, Petrov, Kelly Ann, Pryor, Xiaoxia, Qian, Leah, Reigle, Andrea, Woods, Joseph K, Wu, Dennis, Zaller, Xiaoping, Zhang, Lan, Zhu, Ann E, Weber, and Nancy A, Thornberry

Subjects

Male, Mice, Knockout, Dipeptidases, Dipeptidyl Peptidase 4, Recombinant Proteins, Rats, Mice, Inbred C57BL, Mice, Thiazoles, Dogs, Diabetes Mellitus, Type 2, Isomerism, Animals, Humans, Hypoglycemic Agents, Female, Protease Inhibitors, Isoleucine, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases

Abstract

Dipeptidyl peptidase (DPP)-IV inhibitors are a new approach to the treatment of type 2 diabetes. DPP-IV is a member of a family of serine peptidases that includes quiescent cell proline dipeptidase (QPP), DPP8, and DPP9; DPP-IV is a key regulator of incretin hormones, but the functions of other family members are unknown. To determine the importance of selective DPP-IV inhibition for the treatment of diabetes, we tested selective inhibitors of DPP-IV, DPP8/DPP9, or QPP in 2-week rat toxicity studies and in acute dog tolerability studies. In rats, the DPP8/9 inhibitor produced alopecia, thrombocytopenia, reticulocytopenia, enlarged spleen, multiorgan histopathological changes, and mortality. In dogs, the DPP8/9 inhibitor produced gastrointestinal toxicity. The QPP inhibitor produced reticulocytopenia in rats only, and no toxicities were noted in either species for the selective DPP-IV inhibitor. The DPP8/9 inhibitor was also shown to attenuate T-cell activation in human in vitro models; a selective DPP-IV inhibitor was inactive in these assays. Moreover, we found DPP-IV inhibitors that were previously reported to be active in models of immune function to be more potent inhibitors of DPP8/9. These results suggest that assessment of selectivity of potential clinical candidates may be important to an optimal safety profile for this new class of antihyperglycemic agents.

Published

2005

46. Discovery of potent and selective orally bioavailable beta-substituted phenylalanine derived dipeptidyl peptidase IV inhibitors

Author

Ann E. Weber, Anthony Mastracchio, Joseph F. Leone, Joseph L. Duffy, George J. Eiermann, Barbara Leiting, Kathryn A. Lyons, Joseph K. Wu, Nancy A. Thornberry, Scott D. Edmondson, Ida Ita, Amanda M. Makarewicz, Huaibing He, Reshma A. Patel, and Aleksandr Petrov

Subjects

Blood Glucose, Stereochemistry, Dipeptidyl Peptidase 4, Phenylalanine, Clinical Biochemistry, Substituent, Pharmaceutical Science, Administration, Oral, Biochemistry, Chemical synthesis, Substrate Specificity, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Transcriptional Regulator ERG, Drug Discovery, Animals, Humans, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Molecular Structure, Chemistry, Organic Chemistry, Biological activity, Glucose Tolerance Test, Rats, DNA-Binding Proteins, Enzyme, Enzyme inhibitor, biology.protein, Trans-Activators, Molecular Medicine, Selectivity, Derivative (chemistry)

Abstract

anti-Substituted biaryl beta-methylphenylalanine derived amides have been shown to be potent DPP-IV inhibitors that suffer from suboptimal selectivity and pharmacokinetics. This letter describes the substitution of the beta-methyl substituent with beta-polar substituents, culminating in the discovery of a beta-dimethylamide substituted phenylalanine derivative with an excellent potency, selectivity, and pharmacokinetic profile.

Published

2005

47. Potent and selective proline derived dipeptidyl peptidase IV inhibitors

Author

Lan Zhu, Reshma A. Patel, Lawrence F. Colwell, Nancy A. Thornberry, Anthony Mastracchio, Frank Marsilio, Bahanu Habulihaz, Joseph K. Wu, Emma R. Parmee, Maria G. Beconi, Scott D. Edmondson, Barbara Leiting, Kathryn A. Lyons, Ann E. Weber, Ann Mao, Huaibing He, and Sanjeev Kumar

Subjects

animal structures, Proline, Stereochemistry, Dipeptidyl Peptidase 4, Clinical Biochemistry, Thiazolidine, Pharmaceutical Science, Administration, Oral, Biological Availability, In Vitro Techniques, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Potency, Animals, Humans, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Organic Chemistry, In vitro, Rats, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Sample collection, Selectivity

Abstract

In-house screening of the Merck sample collection identified proline derived homophenylalanine 3 as a DPP-IV inhibitor with modest potency (DPP-IV IC50 = 1.9 μM). Optimization of 3 led to compound 37, which is among the most potent and selective DPP-IV inhibitors discovered to date.

Published

2004

48. Fluoropyrrolidine amides as dipeptidyl peptidase IV inhibitors

Author

Ann E. Weber, Barbara Leiting, Kathryn A. Lyons, Charles G. Caldwell, Frank Marsilio, Jiafang He, Emma R. Parmee, Huaibing He, George J. Eiermann, Ping Chen, Joseph K. Wu, Reshma A. Patel, Aleksandr Petrov, and Nancy A. Thornberry

Subjects

Pyrrolidines, Stereochemistry, Adenosine Deaminase, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Mice, Dogs, Pharmacokinetics, In vivo, Oral administration, Drug Discovery, medicine, Adenosine Deaminase Inhibitors, Animals, Protease Inhibitors, Molecular Biology, Glycoproteins, chemistry.chemical_classification, Glucose tolerance test, biology, medicine.diagnostic_test, Chemistry, Organic Chemistry, Fluorine, Amides, Rats, Isoenzymes, Mice, Inbred C57BL, Enzyme, Enzyme inhibitor, biology.protein, Molecular Medicine, Selectivity

Abstract

Amides derived from fluorinated pyrrolidines and 4-substituted cyclohexylglycine analogues have been prepared and evaluated as inhibitors of dipeptidyl dipeptidase IV (DP-IV). Analogues which incorporated (S)-3-fluoropyrrolidine showed good selectivity for DP-IV over quiescent cell proline dipeptidase (QPP). Compound 48 had good pharmacokinetic properties and was orally active in an oral glucose tolerance test in lean mice.

Published

2003

49. Quantitation of loperamide and N-demethyl-loperamide in human plasma using electrospray ionization with selected reaction ion monitoring liquid chromatography-mass spectrometry

Author

Abu J. M. Sadeque, Alastair J. J. Wood, John C.L Erve, David L. Hachey, and Huaibing He

Subjects

Adult, Spectrometry, Mass, Electrospray Ionization, Chromatography, Electrospray ionization, Metabolite, Selected reaction monitoring, Reproducibility of Results, General Chemistry, Mass spectrometry, High-performance liquid chromatography, Loperamide, Sensitivity and Specificity, Triple quadrupole mass spectrometer, chemistry.chemical_compound, chemistry, Liquid chromatography–mass spectrometry, Calibration, Humans, Ammonium acetate, Chromatography, High Pressure Liquid

Abstract

We report here the development and validation of an LC-MS method for quantitation of loperamide (LOP) and its N-demethyl metabolite (DMLOP) in human plasma. O-Acetyl-loperamide (A-LOP) was synthesized by us for use as an internal standard in the assay. After addition of the internal standard, the compounds of interest were extracted with methyl tert.-butylether and separated by HPLC on a C18 reversed-phase column using an acetonitrile-water gradient containing 20 mM ammonium acetate. The three compounds were well separated by HPLC and no interfering peaks were detected at the usual concentrations found in plasma. Analytes were quantitated using positive electrospray ionization in a triple quadrupole mass spectrometer operating in the MS-MS mode. Selected reaction monitoring was used to quantify LOP (m/z 477-266), DMLOP (m/z 463--252) and A-LOP (m/z 519--266) on ions formed by loss of the 4-(p-chlorophenyl)-4-hydroxy-piperidyl group upon low energy collision-induced dissociation. Calibration curves, which were linear over the range 1.04 to 41.7 pmol/ml (LOP) and 1.55 to 41.9 pmol/ml (DMLOP), were run contemporaneously with each batch of samples, along with low (4.2 pmol/ml), medium (16.7 pmol/ml) and high (33.4 pmol/ml) quality control samples. The lower limit of quantitation (LLQ) of LOP and DMLOP was about 0.25 pmol/ml in plasma. The extraction efficiency of LOP and DMLOP from human plasma was 72.3+/-1.50% (range: 70.7-73.7%) and 79.4+/-12.8% (64.9-88.8%), respectively. The intra- and inter-assay variability of LOP and DMLOP ranged from 2.1 to 14.5% for the low, medium and high quality control samples. The method has been used successfully to study loperamide pharmacokinetics in adult humans.

Published

2000

50. Determination of catecholamines in sheep plasma by high-performance liquid chromatography with electrochemical detection: comparison of deoxyepinephrine and 3,4-dihydroxybenzylamine as internal standard

Author

Brian W. Christman, C. Michael Stein, Alastair J. J. Wood, and Huaibing He

Subjects

Sodium, Dopamine, chemistry.chemical_element, High-performance liquid chromatography, Norepinephrine (medication), Norepinephrine, Catecholamines, Dogs, Blood plasma, medicine, Electrochemistry, Animals, Humans, Chromatography, High Pressure Liquid, Detection limit, Chromatography, Sheep, Extraction (chemistry), Reproducibility of Results, General Chemistry, Reference Standards, Deoxyepinephrine, chemistry, Catecholamine, Quantitative analysis (chemistry), medicine.drug

Abstract

3,4-Dihydroxybenzylamine (DHBA) is commonly used as the internal standard in HPLC catecholamine assays. Sheep are frequently used in studies of cardiovascular physiology and in such studies measurement of catecholamines is important. The recovery of DHBA from sheep plasma is, however variable and poor. Therefore, we have developed a reliable and sensitive HPLC-ED method with alumina extraction for measurement of catecholamines in sheep plasma using deoxyepinephrine (epinine) as the internal standard. Separation was performed on a muBondapak C18 column (300x3.9 mm, 10 microm) with a mobile phase containing 2% acetonitrile and 98% buffer (0.05% sodium acetate-0.02% EDTA-0.013% sodium heptanesulfonate), pH 3.25. The extraction of epinine from water, human plasma, dog plasma and sheep plasma did not differ (p0.05), but extraction of DHBA from sheep plasma was significantly impaired (p0.0001). The R2 of regression curves (n=5) of norepinephrine (NE) (25.02 pg/ml-1.00 ng/ml) and epinephrine (E) (25.82 pg/ml-1.03 ng/ml), using epinine as internal standard were greater than 0.99. The intra- and inter-day coefficients of variation were 2.11-11.15 and 0.88-12.60% for NE and 1.12-10.91 and 2.88-12.60% for E, respectively. The detection limits for NE and E are 12 pg/ml. The technique described has the advantage that it allows the simultaneous determination of both endogenous and [3H]norepinephrine in sheep plasma using a sensitive and reproducible HPLC technique.

Published

1997