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An Innovative Short-Clustered Maltodextrin as Starch Substitute for Ameliorating Postprandial Glucose Homeostasis

机译:一种创新的短簇麦芽糊精,作为淀粉替代品质后葡萄糖稳定性

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Dietary starch is usually associated with elevated postprandial glycemic response. This is a potential risk factor of type 2 diabetes. Here, a 1,4-α-glucan branching enzyme (GBE) was employed to reassemble α-1,4 and α-1,6 glycosidic bonds in starch molecules. Structural characterization showed that GBE-catalyzed molecular reassembly created an innovative short-clustered maltodextrin (SCMD), which showed a dense internal framework along with shortened external chains. Such short-clustered molecules obstructed digestive enzymes attack and displayed dramatically reduced digestibility. Therefore, SCMD was served as a dietary starch substitute to improve postprandial glucose homeostasis. A 22.3% decrease in glycemic peak was therefore detected in ICR mice following SCMD intake (10.7 mmol/L), compared with that in the control (13.8 mmol/L). Moreover, an attenuated insulin response (40.5% lower than that in control) to SCMD intake was regarded suitable for diabetes management. These novel discoveries demonstrate that enzymatically rebuilding starch molecules may be a meaningful strategy for diabetes management.
机译:膳食淀粉通常与餐后血糖反应升高有关。这是2型糖尿病的潜在危险因素。在这里,1,4-α-葡聚糖分支酶(GBE)被用于重组淀粉分子中的α-1,4和α-1,6糖苷键。结构表征表明,GBE催化的分子重组产生了一种创新的短簇麦芽糊精(SCMD),其内部结构致密,外部链缩短。这种短簇状分子阻碍了消化酶的攻击,并表现出显著的消化率降低。因此,SCMD被用作膳食淀粉替代品,以改善餐后葡萄糖稳态。因此,与对照组(13.8 mmol/L)相比,摄入SCMD(10.7 mmol/L)后,ICR小鼠的血糖峰值下降了22.3%。此外,对SCMD摄入的胰岛素反应减弱(比对照组低40.5%)被认为适合糖尿病管理。这些新发现表明,酶法重建淀粉分子可能是糖尿病管理的一个有意义的策略。

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