Sweet Biotechnology: Enzymatic Production and Digestibility Screening of Novel Kojibiose and Nigerose Analogues

Dhaene, Shari; Laar, Amar van; Doncker, Marc De; Beul, Emma De; Beerens, Koen; Grootaert, Charlotte; Caroen, Jurgen; Eycken, Johan Van der; Camp, John Van; Desmet, Tom

doi:10.1021/acs.jafc.1c07709

Cited by 3 publications

(1 citation statement)

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“…This is confirmed by the HPAEC-PAD findings, while these analyses also showed that the monosaccharide composition has an impact. Although the decreased glucose levels upon exposure to D-Glc-α1,2-D-Gal, D-Glc-α1,2-D-Rib and D-Glc-α1,3-L-Ara could be related to the fact that only one molecule of glucose is released during their digestion, we have previously demonstrated that cellular ATP production and the change in disaccharide concentration over time is similar for these sugars in comparison to a mannitol control [ 38 ]. Therefore, the decrease in glucose concentration during exposure to Glc-α1,2-D-Gal, D-Glc-α1,2-D-Rib and D-Glc-α1,3-L-Ara is most likely a result of both a lower glucose content of the sugar and delayed digestion.…”

Section: Discussionmentioning

confidence: 99%

Rare Sugar Metabolism and Impact on Insulin Sensitivity along the Gut–Liver–Muscle Axis In Vitro

et al. 2023

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Rare sugars have recently attracted attention as potential sugar replacers. Understanding the biochemical and biological behavior of these sugars is of importance in (novel) food formulations and prevention of type 2 diabetes. In this study, we investigated whether rare sugars may positively affect intestinal and liver metabolism, as well as muscle insulin sensitivity, compared to conventional sugars. Rare disaccharide digestibility, hepatic metabolism of monosaccharides (respirometry) and the effects of sugars on skeletal muscle insulin sensitivity (impaired glucose uptake) were investigated in, respectively, Caco-2, HepG2 and L6 cells or a triple coculture model with these cells. Glucose and fructose, but not l-arabinose, acutely increased extracellular acidification rate (ECAR) responses in HepG2 cells and impaired glucose uptake in L6 cells following a 24 h exposure at 28 mM. Cellular bioenergetics and digestion experiments with Caco-2 cells indicate that especially trehalose (α1-1α), D-Glc-α1,2-D-Gal, D-Glc-α1,2-D-Rib and D-Glc-α1,3-L-Ara experience delayed digestion and reduced cellular impact compared to maltose (α1-4), without differences on insulin-stimulated glucose uptake in a short-term setup with a Caco-2/HepG2/L6 triple coculture. These results suggest a potential for l-arabinose and specific rare disaccharides to improve metabolic health; however, additional in vivo research with longer sugar exposures should confirm their beneficial impact on insulin sensitivity in humans.

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Section: Discussionmentioning

confidence: 99%