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维生素D受体(VDR)通过自噬相关蛋白16样蛋白1(ATG16L1)调节自噬活性。

VDR/vitamin D receptor regulates autophagic activity through ATG16L1.

作者信息

Sun Jun

机构信息

a Department of Biochemistry , Rush University, Cohn Research Building , Chicago , IL , USA.

出版信息

Autophagy. 2016 Jun 2;12(6):1057-8. doi: 10.1080/15548627.2015.1072670. Epub 2015 Jul 28.

DOI:10.1080/15548627.2015.1072670
PMID:26218741
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4922437/
Abstract

The Paneth cell is a unique intestinal epithelial cell that can sense the gut microbiome and secrete anti-microbial peptides, thereby playing critical roles in the maintenance of homeostasis at the intestinal-microbial interface. These roles in regulating innate immunity and intestinal microbial ecology are dependent on a functional autophagy pathway through ATG16L1. ATG16L1 is a regulator for autophagy and a risk gene for inflammatory bowel disease (IBD). We demonstrated that a low VDR/vitamin D receptor level in the intestine is associated with abnormal Paneth cells, impaired autophagy function, and imbalanced bacterial profile (dysbiosis), accompanied by a reduction of ATG16L1. We determined that VDR transcriptionally regulates ATG16L1 as a VDR target gene. Administration of the bacterial product butyrate increases intestinal VDR expression and suppresses inflammation in a colitis model. Thus, our study indicates that VDR may be a determinant of IBD risk through its actions on ATG16L1. These insights can be leveraged to define therapeutic targets for restoring Paneth cells and autophagy through VDR in chronic inflammation. It may also have applicability for infectious diseases and autoimmune diseases associated with skin or lung, where the host is in contact with bacteria.

摘要

潘氏细胞是一种独特的肠道上皮细胞,能够感知肠道微生物群并分泌抗菌肽,从而在维持肠道-微生物界面的稳态中发挥关键作用。这些在调节先天免疫和肠道微生物生态方面的作用依赖于通过ATG16L1的功能性自噬途径。ATG16L1是自噬的调节因子,也是炎症性肠病(IBD)的风险基因。我们证明,肠道中低水平的维生素D受体(VDR)与潘氏细胞异常、自噬功能受损和细菌谱失衡(生态失调)有关,同时伴有ATG16L1的减少。我们确定VDR作为VDR靶基因转录调控ATG16L1。在结肠炎模型中,给予细菌产物丁酸盐可增加肠道VDR表达并抑制炎症。因此,我们的研究表明,VDR可能通过其对ATG16L1的作用成为IBD风险的决定因素。这些见解可用于确定通过VDR恢复慢性炎症中潘氏细胞和自噬的治疗靶点。它也可能适用于宿主与细菌接触的与皮肤或肺部相关的传染病和自身免疫性疾病。