Hypoglycaemic effects of the novel antidiabetic agent repaglinide in rats and dogs

• Published in: British journal of pharmacology Vol. 121; no. 8; pp. 1597 - 1604
• Main Authors: Mark, Michael, Grell, Wolfgang
• Format: Journal Article
• Language: English
• Published: Oxford, UK Blackwell Publishing Ltd 01.08.1997; Nature Publishing
• Subjects: Animals; antidiabetic agents; antihyperglycaemic effects; Biological and medical sciences; Carbamates - pharmacology; Dogs; Female; General and cellular metabolism. Vitamins; Glyburide - pharmacology; hypoglycaemic effects; Hypoglycemic Agents - pharmacology; Medical sciences; Pharmacology. Drug treatments; Piperidines - pharmacology; Rats; Rats, Wistar; Repaglinide; Stereoisomerism; Sulfonylurea Compounds - pharmacology; Fissipedia; Glimepiride; Carnivora; Intravenous administration; Rat; Rodentia; Oral administration; Biological activity; Vertebrata; Hypoglycemic agent; Mammalia; Structure activity relation; Animal; Enantiomer; Sulfonylureas; Repaglinide; Stereospecificity; Glibenclamide; Dog; Comparative study; Glycemia; Duration of action
• ISSN: 0007-1188; 1476-5381
• DOI: 10.1038/sj.bjp.0701307

1 Repaglinide, a novel compound with a nonsulphonylurea structure, is currently being clinically tested as a therapeutic agent. In the present study, the hypoglycaemic effects of repaglinide in rats and dogs were investigated. 2 Whereas the R‐enantiomer, AG‐EE 624 ZW, showed only weak hypoglycaemic activity, the S‐enantiomer, repaglinide, turned out to be a potent hypoglycaemic compound in rats after oral as well as after intravenous administration. Only 50% of the dose of repaglinide was needed to be equieffective with the racemic mixture AG‐EE 388 ZW. The corresponding ED50 values calculated for the effects after 120 min p.a. (intravenous administration) were 3.4 μg kg−1 (repaglinide) and 6 μg kg−1 (AG‐EE 388 ZW). 3 When compared to glimepiride or glibenclamide, repaglinide displayed a 18 to 25 times higher potency in fasted rats. The ED50 values calculated for the effects after 120 min p.a. (oral administration) were 10 μg kg−1 (repaglinide), 182 μg kg−1 (glimepiride) and 255 μg kg−1 (glibenclamide). 4 In glucose loaded rats (0.5, 1.0, 2.0 and 3.0 g kg−1 glucose, p.o.) repaglinide exerted a very strong antihyperglycaemic activity which was even more pronounced than under normoglycaemic conditions. So for a reduction in blood glucose of 1 mmol l−1, 10.3, 9.3, 7.0 8.4 and 7.2 μg kg−1 repaglinide were needed after glucose loads of 0.0, 0.5, 1.0, 2.0 and 3.0 g kg−1, respectively. 5 In beagle dogs repaglinide again showed a pronounced hypoglycaemic effect (ED50 28.3 μg kg−1) which lasted for up to 24 h. However, insulin levels were only transiently increased. 6 The in vivo data presented are well supported by recently published in vitro findings. From its activity profile, repaglinide appears to be a promising new therapeutic agent. British Journal of Pharmacology (1997) 121, 1597–1604; doi:10.1038/sj.bjp.0701307