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在婴儿模拟胃肠道条件下牛血清白蛋白的ABBOS表位未完全消除。

Incomplete elimination of the ABBOS epitope of bovine serum albumin under simulated gastrointestinal conditions of infants.

作者信息

Alting A C, Meijer R J, van Beresteijn E C

机构信息

Department of Biophysical Chemistry, Netherlands Institute for Dairy Research, Ede, The Netherlands.

出版信息

Diabetes Care. 1997 May;20(5):875-80. doi: 10.2337/diacare.20.5.875.

Abstract

OBJECTIVE

Because the bovine serum albumin residues 126-144 (ABBOS) have been reported to be responsible for the autoimmune reaction directed against pancreatic islet cells, it was our aim to study the potential survival of the ABBOS epitope during digestion in the gastrointestinal tract.

RESEARCH DESIGN AND METHODS

Either nontreated (commercially available) or heat-treated bovine serum albumin (BSA) was hydrolyzed in vitro with pepsin at a pH of 2.0, 3.0, and 4.0 and subsequently with pancreatic enzymes at a pH of 7.5. Cross-reactivity between the ABBOS peptide and the BSA hydrolysates was determined by competitive enzyme-linked immunosorbent assay (ELISA) using a rabbit polyclonal antibody raised against the ABBOS peptide in BSA.

RESULTS

Biochemical findings clearly showed that the degradation of BSA during simulated physiological digestion depended on its conformation and on the pH of its pepsin-catalyzed hydrolysis. Raising the pH of the pepsin-catalyzed hydrolysis from 2.0 to 4.0 decreased the efficiency of the process, especially when BSA had first been denatured by heat treatment. As a consequence, a large proportion of the cross-reactive anti-ABBOS antibody-binding sites was still intact in the final hydrolysates.

CONCLUSIONS

The present results suggest that the ABBOS epitope of BSA will not be completely eliminated during digestion under conditions that prevail in the stomach of infants (pH 3-4).

摘要

目的

由于据报道牛血清白蛋白126 - 144位残基(ABBOS)是针对胰岛细胞的自身免疫反应的原因,我们的目的是研究ABBOS表位在胃肠道消化过程中的潜在存活情况。

研究设计与方法

将未处理的(市售的)或经热处理的牛血清白蛋白(BSA)在体外于pH 2.0、3.0和4.0条件下用胃蛋白酶水解,随后在pH 7.5条件下用胰酶水解。使用针对BSA中ABBOS肽产生的兔多克隆抗体,通过竞争性酶联免疫吸附测定(ELISA)来确定ABBOS肽与BSA水解产物之间的交叉反应性。

结果

生化结果清楚地表明,在模拟生理消化过程中BSA的降解取决于其构象以及胃蛋白酶催化水解的pH值。将胃蛋白酶催化水解的pH值从2.0提高到4.0会降低该过程的效率,特别是当BSA首先经过热处理变性时。因此,在最终的水解产物中,很大一部分交叉反应性抗ABBOS抗体结合位点仍然完整。

结论

目前的结果表明,在婴儿胃中占主导的条件(pH 3 - 4)下消化期间,BSA的ABBOS表位不会被完全消除。

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