EDK Editome Disease Knowledgebase

AZIN1 is antizyme inhibitor 1 protein, and the Ed-AZI (edited AZIN1) sequestrates antizyme and blocks the degradation of ODC (oncoproteins) and CCND1 (cyclin D1), that promotes cell proliferation and possibly the HCC (hepatocellular carcinoma) onset and progression. A-to-I editing event within the AZIN1 transcript, in tumor tissues from HCC patients when compared to paired non-tumor tissues. Serine at residue 367 of AZIN1 protein is recoded into Glycine and the editing level of this site increases during HCC pathogenesis.

The wild-type AZIN1 can promote the tumorigenicity, the edited AZIN1 conferred gain-of-function phenotypes that are manifested by more aggressive behaviors during ESCC progression. A recoding A-I editing events in AZIN1 gene, Serine at residue 367 of AZIN1 protein is recoded into Glycine are catalyzed by ADAR1. And the editing alterations in the AZIN1 may be responsible for the ADAR1-induced malignant phenotypes during ESCC progression.

The hyper-editing of AZIN1enhances the invasive potential of CAFs within the TME in colon and is an important predictor of tumor invasiveness in CRC.

AZIN1 RNA editing levels may be an important prognostic biomarker in GC patients, and may serve as a key clinical decision-making tool for determining preoperative treatment strategies in GC patients.