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炎症刺激将组织蛋白酶活性募集至人树突状细胞的晚期内体区室。

Inflammatory stimuli recruit cathepsin activity to late endosomal compartments in human dendritic cells.

作者信息

Lautwein Alfred, Burster Timo, Lennon-Duménil Ana-Maria, Overkleeft Herman S, Weber Ekkehard, Kalbacher Hubert, Driessen Christoph

机构信息

Medical and Natural Sciences Research Center, University of Tübingen, Tübingen, Germany.

出版信息

Eur J Immunol. 2002 Dec;32(12):3348-57. doi: 10.1002/1521-4141(200212)32:12<3348::AID-IMMU3348>3.0.CO;2-S.

Abstract

Proteolysis by endocytic cysteine proteases is a central element of the antigen-presentation machinery in dendritic cells (DC). It controls the generation of immunogenic peptides, guides the transit of both MHC class II and MHC-like molecules through the endocytic compartment and converts class II into a peptide-receptive state - features closely linked to DC maturation. Differential activity of endocytic proteases, in particular cathepsins, in subcellular compartments has been implicated as a key regulatory element in controlling this machinery in murine DC. We analyzed the expression and subcellular distribution of the major endocytic cysteine proteases (cathepsins S, B, L and H) along with their major endogenous inhibitor, Cystatin C, in resting and stimulated human DC. Although the majority of cathepsin activity was restricted to lysosomes in resting DC, cathepsins selectively accumulated in late endosomes after LPS-induced stimulation. Surprisingly, expression and distribution of Cystatin C was unaffected by DC maturation. Thus, late endosomes represent a specialized compartment where proteolytic activity is developmentally regulated in DC. This could facilitate the conversion of exogenous protein into MHC class II-peptide complexes.

摘要

内吞性半胱氨酸蛋白酶介导的蛋白水解是树突状细胞(DC)抗原呈递机制的核心要素。它控制免疫原性肽的产生,引导MHC II类分子和MHC样分子通过内吞区室转运,并将II类分子转化为肽接受状态——这些特征与DC成熟密切相关。内吞蛋白酶,特别是组织蛋白酶,在亚细胞区室中的差异活性被认为是控制小鼠DC中这一机制的关键调节因素。我们分析了主要内吞性半胱氨酸蛋白酶(组织蛋白酶S、B、L和H)及其主要内源性抑制剂胱抑素C在静息和活化的人DC中的表达及亚细胞分布。尽管在静息DC中,大多数组织蛋白酶活性局限于溶酶体,但在脂多糖诱导的刺激后,组织蛋白酶选择性地在晚期内体中积累。令人惊讶的是,胱抑素C的表达和分布不受DC成熟的影响。因此,晚期内体代表了一个特殊的区室,在DC中蛋白水解活性在此受到发育调控。这可能有助于将外源性蛋白质转化为MHC II类-肽复合物。

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