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克罗恩病中自噬相关基因16样蛋白1(ATG16L1)稳定性的改变

An alteration in ATG16L1 stability in Crohn disease.

作者信息

Lassen Kara G, Xavier Ramnik J

机构信息

Broad Institute; Cambridge, MA USA; Center for Computational and Integrative Biology; Massachusetts General Hospital; Boston, MA USA.

Broad Institute; Cambridge, MA USA; Center for Computational and Integrative Biology; Massachusetts General Hospital; Boston, MA USA; Gastrointestinal Unit and Center for the Study of Inflammatory Bowel Disease; Massachusetts General Hospital; Harvard Medical School; Boston, MA USA.

出版信息

Autophagy. 2014 Oct 1;10(10):1858-60. doi: 10.4161/auto.29963. Epub 2014 Aug 12.

DOI:10.4161/auto.29963
PMID:25136803
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4198368/
Abstract

Individuals who harbor a common coding polymorphism (Thr300Ala) within a structurally unclassified region of ATG16L1 are at increased risk for the development of Crohn disease. Recently, we reported on the generation and characterization of knockin mice carrying the ATG16L1 T300A variant. We demonstrate that multiple cell types from T300A knock-in mice exhibit reduced selective autophagy, and we mechanistically link this phenotype with an increased susceptibility of ATG16L1 T300A to CASP3- and CASP7-mediated cleavage. These findings demonstrate how a single polymorphism can result in cell type- and pathway-specific disruptions of selective autophagy and alterations in the inflammatory milieu that can contribute to disease.

摘要

在自噬相关基因16样蛋白1(ATG16L1)结构未分类区域存在常见编码多态性(苏氨酸300变为丙氨酸,即Thr300Ala)的个体患克罗恩病的风险增加。最近,我们报道了携带ATG16L1 T300A变体的基因敲入小鼠的产生及特性研究。我们证明,来自T300A基因敲入小鼠的多种细胞类型表现出选择性自噬减少,并且我们从机制上把这种表型与ATG16L1 T300A对胱天蛋白酶3(CASP3)和胱天蛋白酶7(CASP7)介导的切割的易感性增加联系起来。这些发现表明了单个多态性如何导致选择性自噬的细胞类型和途径特异性破坏以及炎症环境的改变,而这些改变可能促成疾病的发生。

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