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乳铁蛋白和骨桥蛋白的络合或复杂共凝聚对模拟婴儿胃肠道消化、肠道炎症和骨骼发育的影响。

The impact of complexation or complex coacervation of lactoferrin and osteopontin on simulated infant gastrointestinal digestion, intestinal inflammation, and bone development.

机构信息

School of Food and Nutritional Sciences, University College Cork, Cork, Ireland.

Nestlé Development Centre Nutrition, Wyeth Nutritionals Ireland, Askeaton, Co. Limerick, V94 E7P9, Ireland.

出版信息

Food Funct. 2024 Sep 30;15(19):9928-9940. doi: 10.1039/d4fo02790f.

Abstract

Lactoferrin (LF) and osteopontin (OPN) are bioactive milk proteins which can form heteroprotein complexes and complex coacervates. This research studied the effect of LF-OPN complexation and complex coacervation on the simulated infant gastrointestinal digestion of LF with subsequent examination of gut and bone health bioactivities in preclinical models. In an infant digestion model, the proteolytic profile of LF was unaltered by the pre-association of LF and OPN. Gastric proteolysis of LF was increased when the model gastric pH was reduced from 5.3 to 4.0, but less so when complexed with OPN. In a model of intestinal inflammation, undigested (79% inhibition) and gastric digestates (26% inhibition) of LF, but not gastrointestinal digestates, inhibited lipopolysaccharide (LPS)-induced NF-κB activation in intestinal epithelial cells. LF-OPN complexation sustained the inhibitory effect (21-43% of the undigested effect, depending on the type of complex) of LF after gastrointestinal digestion, suggesting that the peptides produced were different. In a neonatal rodent model used to study bone development, coacervating LF and OPN improved bone structures with a significant increase of trabecular proportion (BV/TV increase by 21.7%). This resulted in an 11.3% increase in stiffness of bones. Feeding the LF and OPN proteins in coacervate format also increased the levels of OPN, P1NP and M-CSF in blood, signifying a more pronounced impact on bone development. This research demonstrated that LF-OPN complexation and complex coacervation can delay simulated infant gastrointestinal digestion of LF and protect or improve the bioactivity of the proteins.

摘要

乳铁蛋白(LF)和骨桥蛋白(OPN)是具有生物活性的牛奶蛋白,可形成异源蛋白复合物和复合凝聚物。本研究探讨了 LF-OPN 复合和复合凝聚对 LF 模拟婴儿胃肠道消化的影响,并随后在临床前模型中检查了肠道和骨骼健康的生物活性。在婴儿消化模型中,LF 与 OPN 预先结合并未改变 LF 的蛋白水解谱。当模型胃 pH 值从 5.3 降低至 4.0 时,LF 的胃蛋白酶解增加,但与 OPN 复合时则增加较少。在肠道炎症模型中,未消化(抑制 79%)和胃消化物(抑制 26%)的 LF 但不是胃肠道消化物可抑制肠上皮细胞中脂多糖(LPS)诱导的 NF-κB 激活。LF-OPN 复合化维持了 LF 经胃肠道消化后的抑制作用(未消化作用的 21-43%,取决于复合的类型),这表明产生的肽不同。在用于研究骨骼发育的新生啮齿动物模型中,凝聚的 LF 和 OPN 改善了骨骼结构,使小梁比例(BV/TV 增加 21.7%)显著增加。这导致骨骼刚度增加 11.3%。以凝聚形式喂养 LF 和 OPN 蛋白也增加了血液中 OPN、P1NP 和 M-CSF 的水平,表明对骨骼发育的影响更为明显。本研究表明,LF-OPN 复合和复合凝聚可以延缓 LF 的模拟婴儿胃肠道消化,并保护或提高蛋白质的生物活性。

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