The effects of sitagliptin on gastric emptying in healthy humans - a randomised, controlled study
Date
2012
Authors
Stevens, J.
Horowitz, M.
Deacon, C.
Nauck, M.
Rayner, C.
Jones, K.
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Journal article
Citation
Alimentary Pharmacology and Therapeutics, 2012; 36(4):379-390
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J. E. Stevens, M. Horowitz, C. F. Deacon, M. Nauck, C. K. Rayner & K. L. Jones
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Abstract
Background The rate of gastric emptying (GE) and subsequent release of the incretin hormones, glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic peptide (GIP) are critical determinants of postprandial glycaemia in health and type 2 diabetes. Slowing of GE may be the dominant mechanism by which exogenous GLP-1, and some GLP-1 analogues, improve postprandial glycaemia. Aim To determine the effect of sitagliptin on GE in healthy subjects, and the relationships between GE with glycaemia and incretin hormone secretion. Methods Fifteen volunteers (22.8+/-0.7years) were studied on two occasions following 2days dosing with sitagliptin (100mg/day) or placebo. GE (scintigraphy), glycaemia and plasma GLP-1 and GIP (total and intact), insulin and glucagon were measured for 240min following a mashed potato meal (1808kJ). Results There was no difference in GE between sitgaliptin and placebo [50% emptying time (T50): P=0.4]. Mean blood glucose was slightly less (P=0.02) on sitagliptin. Sitagliptin reduced plasma glucagon between 75 and 120min (P<0.05), and increased intact GLP-1 (P=0.0002) and intact GIP (P=0.0001) by approximately twofold, but reduced total GIP (P=0.0003) and had no effect on total GLP-1 (P=0.16) or insulin (P=0.75). On sitagliptin the initial rise in blood glucose (r=-0.66, P=0.008) and the intact GIP response (r=-0.66, P=0.007) were inversely related, whereas the intact GLP-1 response was related directly (r=0.52, P=0.05) to the T50. Conclusions While the effects of sitagliptin on glycaemic control are unlikely to relate to slowing of GE in healthy humans, the rate of GE is a significant determinant of postprandial glycaemia on sitagliptin (Clinical Trial:NCT00501657).
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© 2012 Blackwell Publishing Ltd.