Diabetic liver-enriched secretory dipeptidyl peptidase 4 (DPP4) fuels gut inflammation via attenuation of autophagy

bioRxiv Pub Date : 2024-08-08 DOI:10.1101/2024.08.06.606776
Mohammad Athar, Ratulananda Bhadury, Chayanika Gogoi, Pooja Mishra, Prity Kumari, Manisha Yadav, J. Maras, Devram S. Ghorpade
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Abstract

The recurrent pathological inflammation of the gut is a major concern in diabetic patients. With the failure of anti-inflammatory or diabetic drugs to limit relapse of colon inflammation demands the unearthing of mechanistic details underlying higher incidences of colitis in diabetic patients. Here we report the enrichment of DPP4 in the livers and blood samples of diabetic humans and mice models of diabesity that is in parallel to the development of colitis. Overexpression of DPP4 exacerbates or hepatic silencing of DPP4 impairs experimental colitis induced by DSS and STM. Mechanistically, we identified liver DPP4 attenuates gut-autophagic response to trigger enteric cell apoptosis, reduced mucin secretion, and compromised gut barrier leading to high infiltration of immune cells secreting inflammatory cytokines establishing pathological gut inflammation. Thus, liver-DPP4-mediated gut autophagy inhibition is a key pathway in diabesitic colitis.
糖尿病肝脏富含的分泌型二肽基肽酶 4 (DPP4) 通过抑制自噬助长肠道炎症
糖尿病患者肠道反复出现病理炎症是一个主要问题。由于抗炎药物或糖尿病药物无法限制结肠炎症的复发,因此需要找出糖尿病患者结肠炎发病率较高的机理细节。在此,我们报告了在糖尿病人和糖尿病小鼠模型的肝脏和血液样本中 DPP4 的富集情况,这与结肠炎的发展是同步的。过量表达 DPP4 会加重 DSS 和 STM 诱导的实验性结肠炎,而肝脏沉默 DPP4 则会损害实验性结肠炎。从机理上讲,我们发现肝脏 DPP4 可减弱肠道自噬反应,从而引发肠道细胞凋亡、粘蛋白分泌减少和肠道屏障受损,导致大量分泌炎性细胞因子的免疫细胞浸润,形成病理性肠道炎症。因此,肝脏-DPP4 介导的肠道自噬抑制是糖尿病性结肠炎的一个关键途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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