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首页> 外文期刊>Food Chemistry >Influence of structural and surface properties of whey-derived peptides on zinc-chelating capacity, and in vitro gastric stability and bioaccessibility of the zinc-peptide complexes
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Influence of structural and surface properties of whey-derived peptides on zinc-chelating capacity, and in vitro gastric stability and bioaccessibility of the zinc-peptide complexes

机译:乳清衍生肽的结构和表面性质对锌螯合能力,锌肽复合物的体外胃稳定性和生物可及性的影响

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摘要

Gastrointestinal stability of zinc-peptide complexes is essential for zinc delivery. As peptide surface charge can influence their metal complex stability, we evaluated the zinc-chelating capacity and stability of zinc complexes of whey protein hydrolysates (WPH), produced with Everlase (WPH-Ever; xi-potential, -39 mV) and papain (WPH-Pap; xi-potential, -7 mV), during simulated digestion. WPH-Ever had lower amount of zinc-binding amino acids but showed higher zinc-chelating capacity than WPH-Pap. This is attributable to the highly anionic surface charge of WPH-Ever for electrostatic interaction with zinc. Release of zinc during peptic digestion was lower for WPH-Ever-zinc, and over 50% of zinc remained bound in both peptide complexes after peptic-pancreatic digestion. Fourier transform infrared spectroscopy suggests the involvement of carboxylate ion, and sidechain carbon-oxygen of aspartate/glutamate and serine/threonine in zinc-peptide complexation. The findings indicate that strong zinc chelation can promote gastric stability and impede intestinal release, for peptides intended for use as dietary zinc carriers.
机译:锌肽复合物的胃肠道稳定性对于锌的递送至关重要。由于肽的表面电荷会影响其金属配合物的稳定性,因此我们评估了由Everlase(WPH-Ever; xi-potential,-39 mV)和木瓜蛋白酶( WPH-Pap; xi电位,-7 mV),在模拟消化过程中。与WPH-Pap相比,WPH-Ever具有更少的锌结合氨基酸,但显示出更高的锌螯合能力。这归因于WPH-Ever与锌的静电相互作用具有很高的阴离子表面电荷。对于WPH-Ever-锌,在消化过程中锌的释放量较低,在消化消化后,两种肽复合物中锌的结合率仍超过50%。傅里叶变换红外光谱表明,锌肽络合涉及到羧酸根离子,天冬氨酸/谷氨酸和丝氨酸/苏氨酸的侧链碳氧。这些发现表明,对于打算用作膳食锌载体的肽,强锌螯合可以促进胃的稳定性并阻止肠道释放。

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