Effect of Acarbose on the 24-Hour Blood Glucose Profile and Pattern of Carbohydrate Absorption

Taylor, R.; Jenkins, D. J. A.; Barker, Helen M.; Fielden, Hashmein; Goff, D V; Misiewicz, J. J.; Lee, D. A.; Allen, H. B.; Macdonald, G.; Wallrabe, H.

doi:10.2337/diacare.5.2.92

Cited by 39 publications

(24 citation statements)

References 8 publications

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“…Assuming that the mean 2-h post-load glucose level in patients with IGT, when treated with placebo, increases 0.25 mmol/L in 3 years, that the mean level in patients treated with acarbose decreases 0.25 mmol/L in 3 years [21,22], and that the standard deviation of the levels is stable in both groups and remains equal to the standard deviation in the comparable subpopulation of the Hoorn Study survey (0.67 mmol/L) [3], we determined that we would need 47 participants in each treatment group to demonstrate the resulting 0.5-mmol/L difference as statistically significant with alpha (two-sided) = 0.05 and beta = 0.05. Thus, we needed complete data from 94 participants to provide sufficient statistical power.…”

Section: Methodsmentioning

confidence: 99%

“…We selected this dose because previous studies had demonstrated that it significantly lowered postprandial blood glucose with fewer side effects than a dose of 300 mg/day [20][21][22]. Participants were instructed to take their tablets with the first bite of a meal.…”

Section: Methodsmentioning

confidence: 99%

“…However, those results have been disputed as questions arose about the study's methods, analyses, and interpretations. Not only do the postprandial glucose levels decrease, but also the fasting glucose levels [20][21][22]. It was therefore questioned if acarbose also improved insulin secretion or insulin sensitivity.…”

Section: Introductionmentioning

confidence: 99%

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A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

Nijpels

Boorsma

Dekker

et al. 2008

Diabetes Metabolism Res

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

Nijpels

Boorsma

Dekker

et al. 2008

Diabetes Metabolism Res

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“…Taylor et al [26] have shown that substi tuting starch for sucrose may reduce carbo hydrate malabsorption with small doses of acarbose. The same group found that 50 mg of miglitol almost blunted the glycemic re sponse after 50 g potato starch over 4 h with only slight increases in breath hydrogen ex halation and symptoms [21], Moreover, dia betic patients on adequate diets reported only slight symptoms of carbohydrate mal absorption after 50 or 100 mg of miglitol [27].…”

Section: Discussionmentioning

confidence: 99%

Inhibition of Glycemic and Hormonal Responses after Repetitive Sucrose and Starch Loads by Different Doses of the α-Glucosidase Inhibitor Miglitol (BAY m 1099) in Man

Lembcke

Fölsch²,

Gatzemeier³

et al. 1991

Pharmacology

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In two randomized, placebo-controlled, double-blind studies, the efficacy, duration of action and tolerability of a single morning dose of 25, 50, and 100 mg miglitol (BAY m 1099), an absorbable inhibitor of intestinal α-glucosidases, were assessed after repetitive sucrose or maize-starch loads (50 g of carbohydrates in 400 ml of water each at 08.00, 12.00, and 17.00 h). With sucrose, miglitol reduced the postprandial rise in blood glucose, serum insulin and serum gastric inhibitory polypeptide concentrations at any dosage. This effect was dose-dependent and confined to the first carbohydrate load in the morning, thus indicating the duration of α-glucosidase inhibition of less than 4 h. Sucrose malabsorption, indicated by breath hydrogen responses, occurred dose-dependently with 50 and 100 mg, but not with 25 mg of miglitol. Similarly, symptoms of carbohydrate malabsorption were absent with 25 mg of the inhibitor and mild to moderate after 50 and 100 mg of miglitol. With starch as the substrate, BAY m 1099 led to a significant amelioration of glycemic and hormonal rises after the first meal, but not thereafter. A numerical dose dependency was recognized, but this was not significant at the 5 % level. Symptoms of carbohydrate malabsorption were absent with 25 mg and negligible with 50 mg BAY m 1099, but occurred almost regularly with the 100-mg dose. Breath hydrogen concentrations increased gradually with the dose of miglitol administered. A single morning dose of 25–100 mg of miglitol thus may be useful for the control of postprandial hyperglycemia after breakfast. Due to the duration of action of less than 4 h, this substance should be given with the three main meals.

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“…This digestion process is important for glucose absorption from the intestine to the blood, and in principle, control of HPA activity can be used as a means of controlling blood glucose levels. In fact, HPA activity has been correlated to post-prandial blood glucose levels (17)(18)(19), and inhibitors of ␣-amylase have been successfully used in the treatment of diseases such as diabetes or obesity where control of the blood glucose level is essential (20).…”

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confidence: 99%

In Situ Extension as an Approach for Identifying Novel α-Amylase Inhibitors

Numao

Damager

Li³

et al. 2004

Journal of Biological Chemistry

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A new approach for the discovery and subsequent structural elucidation of oligosaccharide-based inhibitors of ␣-amylases based upon autoglucosylation of known ␣-glucosidase inhibitors is presented. This concept, highly analogous to what is hypothesized to occur with acarbose, is demonstrated with the known ␣-glucosidase inhibitor, D-gluconohydroximino-1,5-lactam. This was transformed from an inhibitor of human pancreatic ␣-amylase with a K i value of 18 mM to a trisaccharide analogue with a K i value of 25 M. The three-dimensional structure of this complex was determined by x-ray crystallography and represents the first such structure determined with this class of inhibitors in any ␣-glycosidase. This approach to the discovery and structural analysis of amylase inhibitors should be generally applicable to other endoglucosidases and readily adaptable to a high throughput format.

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Effect of Acarbose on the 24-Hour Blood Glucose Profile and Pattern of Carbohydrate Absorption

Cited by 39 publications

References 8 publications

A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

Inhibition of Glycemic and Hormonal Responses after Repetitive Sucrose and Starch Loads by Different Doses of the α-Glucosidase Inhibitor Miglitol (BAY m 1099) in Man

In Situ Extension as an Approach for Identifying Novel α-Amylase Inhibitors

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Effect of Acarbose on the 24-Hour Blood Glucose Profile and Pattern of Carbohydrate Absorption

Cited by 39 publications

References 8 publications

A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

A study of the effects of acarbose on glucose metabolism in patients predisposed to developing diabetes: the Dutch acarbose intervention study in persons with impaired glucose tolerance (DAISI)

Inhibition of Glycemic and Hormonal Responses after Repetitive Sucrose and Starch Loads by Different Doses of the &alpha;-Glucosidase Inhibitor Miglitol (BAY m 1099) in Man

In Situ Extension as an Approach for Identifying Novel α-Amylase Inhibitors

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Inhibition of Glycemic and Hormonal Responses after Repetitive Sucrose and Starch Loads by Different Doses of the α-Glucosidase Inhibitor Miglitol (BAY m 1099) in Man