Interaction of insulin with prokinetic drugs in STZ-induced diabetic mice

doi:10.4292/wjgpt.v4.i2.28

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World Journal of Gastrointestinal Pharmacology and Therapeutics

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2150-5349

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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World J Gastrointest Pharmacol Ther. May 6, 2013; 4(2): 28-38
Published online May 6, 2013. doi: 10.4292/wjgpt.v4.i2.28

Interaction of insulin with prokinetic drugs in STZ-induced diabetic mice

Mohamed A Fouad Shalaby, Hekma A Abd El Latif, Mostafa E El Sayed

Mohamed A Fouad Shalaby, Department of Pharmacology, Kahira Pharmaceutical Company, Cairo 793, Egypt

Hekma A Abd El Latif, Mostafa E El Sayed, Faculty of Pharmacy, Cairo University, Cairo 11562, Egypt

Author contributions: Shalaby MAF designed the study, wrote the manuscript and performed all experiments; El Latif HAA and El Sayed ME were involved in editing the manuscript.

Supported by Pharmacology Department, Kahira Pharmaceutical Company and Pharmacology and Toxicology Department, Faculty of Pharmacy, Cairo University, Egypt

Correspondence to: Dr. Mohamed A Fouad Shalaby, Research Specialist Pharmacist, Department of Pharmacology, Kahira Pharmaceutical Company, 4 Abd El-Hamed El-Deeb st., Shobra, Cairo 793, Egypt. mafrec10@yahoo.com

Telephone: +20-22-997029 Fax: +20-22-025477

Received: August 25, 2012
Revised: October 29, 2012
Accepted: January 17, 2013
Published online: May 6, 2013

Abstract

AIM: To study the possible interactions of metoclopramide, domperidone and erythromycin in streptozotocin-induced diabetic mice treated with insulin by various parameters.

METHODS: Effects of the individual as well as combined drugs were studied in diabetic mice via estimation of the blood glucose and serum insulin levels, small intestinal transit (SIT), gastric emptying (GE), xylose absorption and glucose tolerance tests. Groups were given insulin 2 IU/kg s.c., metoclopramide 20 mg/kg p.o., domperidone 20 mg/kg p.o. and erythromycin 6 mg/kg p.o. individually and in combination. There were also normal and diabetic control groups. The first set of experiments was carried out to investigate the subchronic effect on blood glucose and serum insulin levels in diabetic mice of one week of daily dose administration of the tested drugs individually as well as the combination of insulin with each prokinetic drug. The other five sets of experiments were carried out to investigate the acute effect of a single dose of each drug individually and in combination on blood glucose and serum insulin levels, SIT, GE, oral xylose absorption and glucose tolerance tests.

RESULTS: The study included the prokinetic drugs metoclopramide (20 mg/kg), domperidone (20 mg/kg) and erythromycin (6 mg/kg), as well as insulin (2 IU/kg), which was individually effective in decreasing SIT, enhancing GE and increasing xylose absorption significantly in diabetic mice. Erythromycin tended to decrease blood glucose level and increase serum insulin level after 1 wk of daily administration in diabetic mice. Erythromycin potentiated the effect of insulin on blood glucose level and serum insulin level whereas other prokinetic agents failed to do so after repeated dose administration in diabetic mice. Metoclopramide or erythromycin in combination with insulin significantly decreased SIT, in diabetic mice, to lower levels than with insulin alone. Administration of prokinetic drugs along with insulin antagonized the action of insulin on xylose absorption. These combinations also increased the rate of glucose absorption from the gut.

CONCLUSION: The present study suggests that prokinetic drugs could potentially improve glycemic control in diabetic gastroparesis by allowing a more predictable absorption of nutrients, matched to the action of exogenous insulin. The use of prokinetics, such as erythromycin, may be interesting in the clinic in decreasing the need for insulin in diabetic patients. The dose of insulin may be safely decreased with erythromycin in chronic treatments.

Keywords: Streptozotocin, Gastrointestinal motility, Insulin, Prokinetic drugs, Intestinal absorption