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易患回肠炎的 SAMP1/YitFc 小鼠中潘氏细胞 CRS4C 的高表达:区域分布、亚细胞定位和作用机制。

Elevated expression of Paneth cell CRS4C in ileitis-prone SAMP1/YitFc mice: regional distribution, subcellular localization, and mechanism of action.

机构信息

Department of Microbiology and Molecular Genetics, School of Medicine, College of Health Sciences, University of California, Irvine, California 92697-4800, USA.

出版信息

J Biol Chem. 2010 Mar 5;285(10):7493-504. doi: 10.1074/jbc.M109.083220. Epub 2010 Jan 7.

Abstract

Paneth cells at the base of small intestinal crypts of Lieberkühn secrete host defense peptides and proteins, including alpha-defensins, as mediators of innate immunity. Mouse Paneth cells also express alpha-defensin-related Defcr-rs genes that code for cysteine-rich sequence 4C (CRS4C) peptides that have a unique CPX triplet repeat motif. In ileitis-prone SAMP1/YitFc mice, Paneth cell levels of CRS4C mRNAs and peptides are induced more than a 1000-fold relative to non-prone strains as early as 4 weeks of age, with the mRNA and peptide levels highest in distal ileum and below detection in duodenum. CRS4C-1 peptides are found exclusively in Paneth cells where they occur only in dense core granules and thus are secreted to function in the intestinal lumen. CRS4C bactericidal peptide activity is membrane-disruptive in that it permeabilizes Escherichia coli and induces rapid microbial cell K(+) efflux, but in a manner different from mouse alpha-defensin cryptdin-4. In in vitro studies, inactive pro-CRS4C-1 is converted to bactericidal CRS4C-1 peptide by matrix metalloproteinase-7 (MMP-7) proteolysis of the precursor proregion at the same residue positions that MMP-7 activates mouse pro-alpha-defensins. The absence of processed CRS4C in protein extracts of MMP-7-null mouse ileum demonstrates the in vivo requirement for intracellular MMP-7 in pro-CRS4C processing.

摘要

小肠隐窝底部的潘氏细胞分泌宿主防御肽和蛋白质,包括α-防御素,作为先天免疫的介质。小鼠潘氏细胞还表达α-防御素相关的 Defcr-rs 基因,这些基因编码含有独特 CPX 三重复基序的富含半胱氨酸序列 4C (CRS4C) 肽。在易患回肠炎的 SAMP1/YitFc 小鼠中,潘氏细胞 CRS4C mRNA 和肽的水平在 4 周龄时就相对于非易患菌株诱导了 1000 多倍,mRNA 和肽水平在回肠远端最高,在十二指肠中无法检测到。CRS4C-1 肽仅存在于潘氏细胞中,它们仅存在于致密核心颗粒中,因此被分泌到肠腔中发挥作用。CRS4C 杀菌肽的活性是破坏膜的,因为它使大肠杆菌透化,并诱导快速的微生物细胞 K+外流,但方式与小鼠α-防御素 cryptdin-4 不同。在体外研究中,无活性的 pro-CRS4C-1 通过基质金属蛋白酶-7 (MMP-7) 在相同的残基位置对前体 pro-region 的蛋白水解,转化为杀菌性 CRS4C-1 肽,MMP-7 激活小鼠 pro-α-防御素。MMP-7 缺失小鼠回肠蛋白提取物中没有处理过的 CRS4C,证明了 MMP-7 在 pro-CRS4C 加工中的体内必需性。

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