Open Access
Treatment with CNX-011-67, a novel GPR40 agonist, delays onset and progression of diabetes and improves beta cell preservation and function in male ZDF rats
Nagesh Gowda
1
,
Anilkumar Dandu
1
,
Jaideep Singh
1
,
Sanghamitra Biswas
1
,
Vijaya Raghav
1
,
Mudigere N Lakshmi
1
,
Pavagada C Shilpa
1
,
Sunil Venkategowda
1
,
Ashokkumar Reddy
1
,
Manojkumar Sadasivuni
1
,
Kumaraswamy Aparna
1
,
Mahesh Kumar Verma
1
,
Yoganand Moolemath
1
,
Mammen O Anup
1
,
Marikunte V Venkataranganna
1
,
Baggavalli P. Somesh
1
,
Madanahalli R Jagannath
1
1
Connexios Life Sciences Pvt Ltd, JP Nagar, India
|
Publication type: Journal Article
Publication date: 2013-05-21
scimago Q2
wos Q2
SJR: 0.814
CiteScore: 4.7
Impact factor: 2.7
ISSN: 20506511
PubMed ID:
23692921
Pharmacology
Pharmacology (medical)
Abstract
The role of G protein-coupled receptor (GPR40), which is highly expressed in pancreatic beta cells, has been studied extensively in the amelioration of beta cell dysfunction in T2D using rat and mouse islets, beta cell lines and in animal models of diabetes. But its potential as a therapeutic target has not been fully explored. This aim of the study is to evaluate the therapeutic potential of CNX-011-67, a highly selective, potent and orally bioavailable GPR40 agonist, in controlling diabetes and other metabolic parameters. Seven week old male ZDF rats were treated with either vehicle or CNX-011-67, 5 mg/kg twice daily, for seven weeks. The animals were subjected to oral glucose tolerance and insulin tolerance tests. Plasma glucose, insulin, triglyceride, HbA1c, fructosamine and free fatty acids were measured at selected time points. Pancreas from control and treated animals were subjected to insulin and pancreatic and duodenal homeobox 1 (PDX1) immunohistochemistry and were also evaluated by electron microscopy. Also the potential impact of CNX-011-67 on islet insulin secretion, content, ATP levels and markers of both glucose oxidation, beta cell health in rat islets under chronic glucolipotoxic conditions was evaluated. Treatment of male ZDF rats with CNX-011-67 for 7 weeks significantly enhanced insulin secretion in response to oral glucose load, delayed the onset of fasting hyperglycemia by 3 weeks, reduced nonfasting glucose excursions, fasting free fatty acids and triglyceride levels. A significant increase in PDX1 expression and insulin content and reduction in plasma fructosamine, HOMA-IR, and beta cell apoptosis were observed. CNX-011-67 improves glucose mediated insulin secretion, insulin gene transcription and islet insulin content in cultured rat islets under chronic glucolipotoxic condition. Also enhanced glucose oxidation in the form of increased islet ATP content and overall improvement in beta cell health in the form of reduced expression of stress markers (TXNIP and CHOP mRNA) were observed. These findings, suggest that long-term oral therapy with CNX-011-67 could be of clinical value to provide good glycemic control and improve islet beta cell function.
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Citations from 2024:
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GOST
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Gowda N. et al. Treatment with CNX-011-67, a novel GPR40 agonist, delays onset and progression of diabetes and improves beta cell preservation and function in male ZDF rats // BMC pharmacology & toxicology. 2013. Vol. 14. No. 1. 28
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Gowda N., Dandu A., Singh J., Biswas S., Raghav V., Lakshmi M. N., Shilpa P. C., Venkategowda S., Reddy A., Sadasivuni M., Aparna K., Verma M. K., Moolemath Y., Anup M. O., Venkataranganna M. V., Somesh B. P., Jagannath M. R. Treatment with CNX-011-67, a novel GPR40 agonist, delays onset and progression of diabetes and improves beta cell preservation and function in male ZDF rats // BMC pharmacology & toxicology. 2013. Vol. 14. No. 1. 28
Cite this
RIS
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TY - JOUR
DO - 10.1186/2050-6511-14-28
UR - https://doi.org/10.1186/2050-6511-14-28
TI - Treatment with CNX-011-67, a novel GPR40 agonist, delays onset and progression of diabetes and improves beta cell preservation and function in male ZDF rats
T2 - BMC pharmacology & toxicology
AU - Gowda, Nagesh
AU - Dandu, Anilkumar
AU - Singh, Jaideep
AU - Biswas, Sanghamitra
AU - Raghav, Vijaya
AU - Lakshmi, Mudigere N
AU - Shilpa, Pavagada C
AU - Venkategowda, Sunil
AU - Reddy, Ashokkumar
AU - Sadasivuni, Manojkumar
AU - Aparna, Kumaraswamy
AU - Verma, Mahesh Kumar
AU - Moolemath, Yoganand
AU - Anup, Mammen O
AU - Venkataranganna, Marikunte V
AU - Somesh, Baggavalli P.
AU - Jagannath, Madanahalli R
PY - 2013
DA - 2013/05/21
PB - Springer Nature
IS - 1
VL - 14
PMID - 23692921
SN - 2050-6511
ER -
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@article{2013_Gowda,
author = {Nagesh Gowda and Anilkumar Dandu and Jaideep Singh and Sanghamitra Biswas and Vijaya Raghav and Mudigere N Lakshmi and Pavagada C Shilpa and Sunil Venkategowda and Ashokkumar Reddy and Manojkumar Sadasivuni and Kumaraswamy Aparna and Mahesh Kumar Verma and Yoganand Moolemath and Mammen O Anup and Marikunte V Venkataranganna and Baggavalli P. Somesh and Madanahalli R Jagannath},
title = {Treatment with CNX-011-67, a novel GPR40 agonist, delays onset and progression of diabetes and improves beta cell preservation and function in male ZDF rats},
journal = {BMC pharmacology & toxicology},
year = {2013},
volume = {14},
publisher = {Springer Nature},
month = {may},
url = {https://doi.org/10.1186/2050-6511-14-28},
number = {1},
pages = {28},
doi = {10.1186/2050-6511-14-28}
}