Beneficial Effect of Long-Term Combined Treatment with Voglibose and Pioglitazone on Pancreatic Islet Function of Genetically Diabetic GK Rats

H. Ishida; S. Kato; M. Nishimura; N. Mizuno; S. Fujimoto; E. Mukai; M. Kajikawa; Y. Yamada; H. Odaka; H. Ikeda; Y. Seino

doi:10.1055/s-2007-978956

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Horm Metab Res 1998; 30(11): 673-678
DOI: 10.1055/s-2007-978956

Originals Clinical

Beneficial Effect of Long-Term Combined Treatment with Voglibose and Pioglitazone on Pancreatic Islet Function of Genetically Diabetic GK Rats

H. Ishida¹ ^, ² , S. Kato¹ , M. Nishimura¹ , N. Mizuno¹ , S. Fujimoto¹ , E. Mukai¹ , M. Kajikawa¹ , Y. Yamada³ , H. Odaka³ , H. Ikeda³ , Y. Seino¹

¹Department of Metabolism and Clinical Nutrition, Kyoto University School of Medicine, Kyoto, Japan
²Third Department of Internal Medicine, Kyorin University School of Medicine, Tokyo, Japan
³Pharmaceutical Research Laboratories-II, Takeda Chemical Industries, Osaka, Japan

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1997

1998

Publication Date:
20 April 2007 (online)

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Effects of voglibose (an α-glucosidase inhibitor) and pioglitazone (an insulin sensitizer) on glycemic control and on the function of pancreatic islets were evaluated using Goto-Kakizaki (GK) rats with non-insulin-dependent diabetes mellitus (NIDDM). Five week administration (8-13 weeks of age in GK rats) of voglibose alone (added to the chow at a concentration of 10 ppm), pioglitazone alone (10 mg/kg daily p.o.), or both of the agents together significantly improved fasting plasma glucose levels and those at 120 min in oral glucose tolerance tests. Insulin secretory capacity in response to glucose of the isolated islets, assessed by batch incubation, was significantly improved in the voglibose and in the voglibose plus pioglitazone groups. Eight-week administration (5-13 weeks of age) of voglibose and voglibose plus pioglitazone successfully lowered the fasting levels of plasma glucose and triglyceride. The glucose-responsiveness in insulin release from the islets was also significantly recovered by the therapy. The treatment increased the insulin content of the islets to almost twice that in untreated controls. Thus, treatment by these drugs can not only effectively ameliorate the metabolic derangement of NIDDM in GK rats, but it can also restore the deteriorated islet function, possibly through protection from glucose toxicity.

Key words

Insulin Secretion - Insulin Resistance - α-Glucosidase Inhibitor - GK Rats - Glucose Toxicity