DTX3L induced NLRP3 ubiquitination inhibit R28 cell pyroptosis in OGD/R injury
Ziyu Zhou, Lei Shang, Qi Zhang, Ximin Hu, Ju-fang Huang, Kun Xiong
Journal:BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR CELL RESEARCH
IF:5.1
DOI:10.1016/j.bbamcr.2023.119433
PMID:36706922
Published:2023-01-24
research field:神经科学药理学眼科学
Abstract
Ischemia/reperfusion (I/R) injury is one of the most common etiologies in many diseases. Retinal I/R leads to cytokine storm , resulting in tissue damage and cell death. Pyroptosis , a novel type of regulated cell death, occurs after cellular I/R injury. In this study, we established an oxygen glucose deprivation (OGD/R) cellular model (R28) to simulate retinal I/R injury. We conducted an LDH assay, and EthD-III and PI staining procedures to confirm pyroptosis. Mass spectrometry and bioinformatics analysis were used to identify the possible proteins interacting with NLRP3 . Co-IP and various molecular biology techniques were used to investigate the possible modes regulating NLRP3 by DTX3L. EthD-III, PI staining and LDH assays demonstrated pyroptosis induced by OGD/R injury, mediated via NLRP3 pathway. Mass spectrometry and bioinformatics analysis screened out three candidate proteins interacting with NLRP3, and further Co-IP experiment indicated that DTX-3L may interact with NLRP3 to regulate its protein levels after injury. Co-IP experiments and various molecular biology methods demonstrated that DTX3L ubiquitinates NLRP3 resulting in pyroptosis after R28 OGD/R injury. Further, NLRP3 LRR and DTX3L RING domains interact with each other. Our study demonstrated that DTX3L may ubiquitinate NLRP3 to regulate OGD/R-induced pyroptosis globally in R28 cells.
本文使用的Yeasen产品


