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胰腺分泌性胰蛋白酶抑制剂是人类母乳中的一种主要促运动和保护因子。

Pancreatic secretory trypsin inhibitor is a major motogenic and protective factor in human breast milk.

作者信息

Marchbank Tania, Weaver Gillian, Nilsen-Hamilton Marit, Playford Raymond J

机构信息

Centre for Gastroenterology, Institute of Cell and Molecular Science, Barts & The London School of Medicine and Dentistry, Queen Mary University of London, and Queen Charlotte's Hospital, Turner St., London E1 2AD, UK.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2009 Apr;296(4):G697-703. doi: 10.1152/ajpgi.90565.2008. Epub 2009 Jan 15.

Abstract

Colostrum is the first milk produced after birth and is rich in immunoglobulins and bioactive molecules. We examined whether human colostrum and milk contained pancreatic secretory trypsin inhibitor (PSTI), a peptide of potential relevance for mucosal defense and, using in vitro and in vivo models, determined whether its presence influenced gut integrity and repair. Human milk was collected from individuals over various times from parturition and PSTI concentrations determined with the use of immunoassay. Human milk samples were analyzed for proliferation and promigratory activity (wounded monolayers) and antiapoptotic activity (caspase-3 activity) with the use of intestinal HT29 cells with or without neutralizing antibodies to PSTI and epidermal growth factor (EGF). Rats were restrained and given indomethacin to induce gastric injury. Effect of gavage with human breast milk with or without neutralizing antibodies on amount of injury were compared with animals receiving a commercial formula feed. PSTI is secreted into human milk, with colostrum containing a much higher concentration of PSTI than human milk obtained later. Human milk stimulated migration and proliferation about threefold and reduced indomethacin-induced apoptosis by about 70-80%. Sixty-five percent of the migratory effect of human milk could be removed by immunoneutralization of PSTI. PSTI worked synergistically with EGF in mediating these effects. Gastric damage in rats was reduced by about 75% in the presence of human milk and was more efficacious than the formula feed (P<0.001). Protective effects of the milk were reduced by about 60% by PSTI immunoneutralization. We concluded that PSTI is secreted into human milk at concentrations that have probable pathophysiological relevance.

摘要

初乳是产后产生的第一份乳汁,富含免疫球蛋白和生物活性分子。我们研究了人初乳和乳汁中是否含有胰腺分泌性胰蛋白酶抑制剂(PSTI),这是一种与黏膜防御可能相关的肽,并使用体外和体内模型确定其存在是否会影响肠道完整性和修复。在分娩后的不同时间从个体采集人乳,并使用免疫测定法测定PSTI浓度。使用带有或不带有针对PSTI和表皮生长因子(EGF)的中和抗体的肠道HT29细胞,分析人乳样品的增殖和促迁移活性(损伤单层)以及抗凋亡活性(半胱天冬酶 - 3活性)。对大鼠进行束缚并给予吲哚美辛以诱导胃损伤。将灌胃含或不含中和抗体的人母乳对损伤量的影响与接受商业配方饲料的动物进行比较。PSTI分泌到人乳中,初乳中PSTI的浓度比后期获得的人乳高得多。人乳刺激迁移和增殖约三倍,并使吲哚美辛诱导的细胞凋亡减少约70 - 80%。通过PSTI免疫中和可消除人乳65%的迁移作用。PSTI与EGF协同作用介导这些效应。在有人乳存在的情况下,大鼠的胃损伤减少了约75%,并且比配方饲料更有效(P<0.001)。通过PSTI免疫中和,乳汁的保护作用降低了约60%。我们得出结论,PSTI以可能具有病理生理学相关性的浓度分泌到人乳中。

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