The Postprandial Anti-Hyperglycemic Effect of Pyridoxine and Its Derivatives Using In Vitro and In Vivo Animal Models

Hyuk Hwa Kim; Yu-Ri Kang; Jung-Yun Lee; Hung-Bae Chang; Ki Won Lee; Emmanouil Apostolidis; Young-In Kwon

doi:10.3390/nu10030285

Nutrients (Feb 2018)

The Postprandial Anti-Hyperglycemic Effect of Pyridoxine and Its Derivatives Using In Vitro and In Vivo Animal Models

Hyuk Hwa Kim,
Yu-Ri Kang,
Jung-Yun Lee,
Hung-Bae Chang,
Ki Won Lee,
Emmanouil Apostolidis,
Young-In Kwon

Affiliations

Hyuk Hwa Kim: Department of Food and Animal Biotechnology, Seoul National University, 08826 Seoul, Korea
Yu-Ri Kang: Department of Food and Nutrition, Hannam University, 34049 Daejeon, Korea
Jung-Yun Lee: Department of Food and Nutrition, Hannam University, 34049 Daejeon, Korea
Hung-Bae Chang: Department of Bio Quality Control, Korea Bio Polytechnic, 32943 Chungnam, Korea
Ki Won Lee: Department of Food and Animal Biotechnology, Seoul National University, 08826 Seoul, Korea
Emmanouil Apostolidis: Department of Chemistry and Food Science, Framingham State University, Framingham, MA 01701, USA
Young-In Kwon: Department of Food and Nutrition, Hannam University, 34049 Daejeon, Korea

DOI: https://doi.org/10.3390/nu10030285
Journal volume & issue: Vol. 10, no. 3
p. 285

Abstract

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In the current study, we investigated the inhibitory activity of pyridoxine, pyridoxal, and pyridoxamine, against various digestive enzymes such as α-glucosidases, sucrase, maltase, and glucoamylase. Inhibition of these enzymes involved in the absorption of disaccharide can improve post-prandial hyperglycemia due to a carbohydrate-based diet. Pyridoxal (4.14 mg/mL of IC50) had the highest rat intestinal α-glucosidase inhibitory activity, followed by pyridoxamine and pyridoxine (4.85 and 5.02 mg/mL of IC50, respectively). Pyridoxal demonstrated superior inhibition against maltase (0.38 mg/mL IC50) and glucoamylase (0.27 mg/mLIC50). In addition, pyridoxal showed significant higher α-amylase inhibitory activity (10.87 mg/mL of IC50) than that of pyridoxine (23.18 mg/mL of IC50). This indicates that pyridoxal can also inhibit starch hydrolyzing by pancreatic α-amylase in small intestine. Based on these in vitro results, the deeper evaluation of the anti-hyperglycemic potential of pyridoxine and its derivatives using Sprague-Dawley (SD) rat models, was initiated. The post-prandial blood glucose levels were tested two hours after sucrose/starch administration, with and without pyridoxine and its derivatives. In the animal trial, pyridoxal (p < 0.05) had a significantly reduction to the postprandial glucose levels, when compared to the control. The maximum blood glucose levels (Cmax) of pyridoxal administration group were decreased by about 18% (from 199.52 ± 22.93 to 164.10 ± 10.27, p < 0.05) and 19% (from 216.92 ± 12.46 to 175.36 ± 10.84, p < 0.05) in sucrose and starch loading tests, respectively, when compared to the control in pharmacodynamics study. The pyridoxal administration significantly decreased the minimum, maximum, and mean level of post-prandial blood glucose at 0.5 h after meals. These results indicate that water-soluble vitamin pyridoxine and its derivatives can decrease blood glucose level via the inhibition of carbohydrate-hydrolyzing and absorption-linked enzymes. Therefore, pyridoxal may have the potential to be used as a food ingredient for the prevention of prediabetes progression to type 2 diabetes.

Published in Nutrients

ISSN: 2072-6643 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Technology: Home economics: Nutrition. Foods and food supply
Website: https://www.mdpi.com/journal/nutrients

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