1. Academic Validation
  2. XBP1 mRNA splicing triggers an autophagic response in endothelial cells through BECLIN-1 transcriptional activation

XBP1 mRNA splicing triggers an autophagic response in endothelial cells through BECLIN-1 transcriptional activation

  • J Biol Chem. 2013 Jan 11;288(2):859-72. doi: 10.1074/jbc.M112.412783.
Andriana Margariti 1 Hongling Li Ting Chen Daniel Martin Gema Vizcay-Barrena Saydul Alam Eirini Karamariti Qingzhong Xiao Anna Zampetaki Zhongyi Zhang Wen Wang Zhixin Jiang Chan Gao Benyu Ma Ye-Guang Chen Gillian Cockerill Yanhua Hu Qingbo Xu Lingfang Zeng
Affiliations

Affiliation

  • 1 Cardiovascular Division, King's College London BHF Centre, 125 Coldharbour Lane, London SE5 9NU, United Kingdom. andriani.margariti@kcl.ac.uk
Abstract

Sustained activation of X-box-binding protein 1 (XBP1) results in endothelial cell (EC) Apoptosis and atherosclerosis development. The present study provides evidence that XBP1 mRNA splicing triggered an autophagic response in ECs by inducing autophagic vesicle formation and markers of Autophagy BECLIN-1 and microtubule-associated protein 1 light chain 3β (LC3-βII). Endostatin activated autophagic gene expression through XBP1 mRNA splicing in an inositol-requiring Enzyme 1α (IRE1α)-dependent manner. Knockdown of XBP1 or IRE1α by shRNA in ECs ablated endostatin-induced autophagosome formation. Importantly, data from arterial vessels from XBP1 EC conditional knock-out (XBP1eko) mice demonstrated that XBP1 deficiency in ECs reduced the basal level of LC3β expression and ablated response to endostatin. Chromatin immunoprecipitation assays further revealed that the spliced XBP1 isoform bound directly to the BECLIN-1 promoter at the region from nt -537 to -755. BECLIN-1 deficiency in ECs abolished the XBP1-induced Autophagy response, whereas spliced XBP1 did not induce transcriptional activation of a truncated BECLIN-1 promoter. These results suggest that XBP1 mRNA splicing triggers an autophagic signal pathway through transcriptional regulation of BECLIN-1.

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