CPL207280, a Novel G Protein-Coupled Receptor 40/Free Fatty Acid Receptor 1-Specific Agonist, Shows a Favorable Safety Profile and Exerts Antidiabetic Effects in Type 2 Diabetic Animals.

Bazydlo-Guzenda, Katarzyna; Buda, Pawel; Matloka, Mikolaj; Mach, Mateusz; Stelmach, Filip; Dzida, Radoslaw; Smuga, Damian; Hucz-Kalitowska, Joanna; Teska-Kaminska, Malgorzata; Vialichka, Varvara; Dubiel, Krzysztof; Kaminska, Bozena; Wieczorek, Maciej; Pieczykolan, Jerzy

Bazydlo-Guzenda, Katarzyna; Buda, Pawel; Matloka, Mikolaj; Mach, Mateusz; Stelmach, Filip; Dzida, Radoslaw; Smuga, Damian; Hucz-Kalitowska, Joanna; Teska-Kaminska, Malgorzata; Vialichka, Varvara; Dubiel, Krzysztof; Kaminska, Bozena; Wieczorek, Maciej; Pieczykolan, Jerzy.

Afiliação

Bazydlo-Guzenda K; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.). katarzyna.bazydlo@celonpharma.c
Buda P; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Matloka M; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Mach M; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Stelmach F; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Dzida R; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Smuga D; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Hucz-Kalitowska J; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Teska-Kaminska M; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Vialichka V; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Dubiel K; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Kaminska B; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Wieczorek M; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).
Pieczykolan J; Research and Development Centre, Celon Pharma SA, Kazun Nowy, Poland (K.B.-G., P.B., Mi.M., Ma.M., F.S., R.D., D.S., J.H.-K., M.T.-K., V.V., K.D., M.W., J.P.), and Postgraduate School of Molecular Medicine, Medical University of Warsaw, Warsaw, Poland (K.B.-G., B.K.).

Mol Pharmacol ; 100(4): 335-347, 2021 10.

Article em En | MEDLINE | ID: mdl-34349026

RESUMO

G protein-coupled receptor (GPR) 40 is a free fatty acid receptor mainly expressed in pancreatic ß-cells activated by medium- and long-chain fatty acids and regulating insulin secretion via an increase in cytosolic free calcium ([Ca2+]i). Activation of GPR40 in pancreatic ß-cells may improve glycemic control in type 2 diabetes through enhancement of glucose-stimulated insulin secretion. However, the most clinically advanced GPR40 agonist-TAK-875 (fasiglifam)-was withdrawn from phase III because of its hepatotoxicity resulting from the inhibition of pivotal bile acid transporters. Here, we present a new, potent CPL207280 agonist and compare it with fasiglifam in numerous in vitro and in vivo studies. CPL207280 showed greater potency than fasiglifam in a Ca2+ influx assay with a human GPR40 protein (EC50 = 80 vs. 270 nM, respectively). At the 10 µM concentration, it showed 3.9 times greater enhancement of glucose-stimulated insulin secretion in mouse MIN6 pancreatic ß-cells. In Wistar Han rats and C57BL6 mice challenged with glucose, CPL207280 stimulated 2.5 times greater insulin secretion without causing hypoglycemia at 10 mg/kg compared with fasiglifam. In three diabetic rat models, CPL207280 improved glucose tolerance and increased insulin area under the curve by 212%, 142%, and 347%, respectively. Evaluation of potential off-target activity (Safety47) and selectivity of CPL207280 (at 10 µM) did not show any significant off-target activity. We conclude that CPL207280 is a potent enhancer of glucose-stimulated insulin secretion in animal disease models with no risk of hypoglycemia at therapeutic doses. Therefore, we propose the CPL207280 compound as a compelling candidate for type 2 diabetes treatment. SIGNIFICANCE STATEMENT: GPR40 is a well-known and promising target for diabetes. This study is the first to show the safety and effects of CPL207280, a novel GPR40/free fatty acid receptor 1 agonist, on glucose homeostasis both in vitro and in vivo in different diabetic animal models. Therefore, we propose the CPL207280 compound as a novel, glucose-lowering agent, overcoming the unmet medical needs of patients with type 2 diabetes.

Assuntos

Diabetes Mellitus Tipo 2/sangue; Diabetes Mellitus Tipo 2/tratamento farmacológico; Hipoglicemiantes/uso terapêutico; Receptores Acoplados a Proteínas G/agonistas; Receptores Acoplados a Proteínas G/metabolismo; Animais; Benzofuranos/química; Benzofuranos/farmacologia; Benzofuranos/uso terapêutico; Glicemia/efeitos dos fármacos; Glicemia/metabolismo; Células CHO; Cricetinae; Cricetulus; Humanos; Hipoglicemiantes/química; Hipoglicemiantes/farmacologia; Masculino; Camundongos; Camundongos Endogâmicos C57BL; Ratos; Ratos Sprague-Dawley; Ratos Wistar; Ratos Zucker; Sulfonas/química; Sulfonas/farmacologia; Sulfonas/uso terapêutico

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Receptores Acoplados a Proteínas G / Diabetes Mellitus Tipo 2 / Hipoglicemiantes Tipo de estudo: Prognostic_studies Limite: Animals / Humans / Male Idioma: En Revista: Mol Pharmacol Ano de publicação: 2021 Tipo de documento: Article

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