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乳糜泻中麸质不耐受的结构基础。

Structural basis for gluten intolerance in celiac sprue.

作者信息

Shan Lu, Molberg Øyvind, Parrot Isabelle, Hausch Felix, Filiz Ferda, Gray Gary M, Sollid Ludvig M, Khosla Chaitan

机构信息

Department of Chemical Engineering, Stanford University, Stanford, CA 94305-5025, USA.

出版信息

Science. 2002 Sep 27;297(5590):2275-9. doi: 10.1126/science.1074129.

Abstract

Celiac Sprue, a widely prevalent autoimmune disease of the small intestine, is induced in genetically susceptible individuals by exposure to dietary gluten. A 33-mer peptide was identified that has several characteristics suggesting it is the primary initiator of the inflammatory response to gluten in Celiac Sprue patients. In vitro and in vivo studies in rats and humans demonstrated that it is stable toward breakdown by all gastric, pancreatic, and intestinal brush-border membrane proteases. The peptide reacted with tissue transglutaminase, the major autoantigen in Celiac Sprue, with substantially greater selectivity than known natural substrates of this extracellular enzyme. It was a potent inducer of gut-derived human T cell lines from 14 of 14 Celiac Sprue patients. Homologs of this peptide were found in all food grains that are toxic to Celiac Sprue patients but are absent from all nontoxic food grains. The peptide could be detoxified in in vitro and in vivo assays by exposure to a bacterial prolyl endopeptidase, suggesting a strategy for oral peptidase supplement therapy for Celiac Sprue.

摘要

乳糜泻是一种广泛流行的小肠自身免疫性疾病,在遗传易感性个体中,因接触膳食中的麸质而诱发。已鉴定出一种33肽,它具有多种特性,表明它是乳糜泻患者对麸质炎症反应的主要引发剂。在大鼠和人类身上进行的体外和体内研究表明,它对所有胃蛋白酶、胰蛋白酶和肠刷状缘膜蛋白酶的分解作用具有稳定性。该肽与组织转谷氨酰胺酶(乳糜泻中的主要自身抗原)反应,其选择性远高于这种细胞外酶的已知天然底物。它是14名乳糜泻患者中14例肠道来源的人T细胞系的强效诱导剂。在所有对乳糜泻患者有毒的谷物中都发现了该肽的同源物,而在所有无毒谷物中则不存在。通过暴露于细菌脯氨酰内肽酶,该肽在体外和体内试验中均可解毒,这为乳糜泻的口服肽酶补充疗法提供了一种策略。

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