AZIN1 RNA editing alters protein interactions, leading to nuclear translocation and worse outcomes in prostate cancer Journal Article


Authors: Ghalali, A.; Wang, L.; Stopsack, K. H.; Rice, J. M.; Wu, S.; Wu, C. L.; Zetter, B. R.; Rogers, M. S.
Article Title: AZIN1 RNA editing alters protein interactions, leading to nuclear translocation and worse outcomes in prostate cancer
Abstract: The transcript encoding Antizyme Inhibitor 1 (AZIN1) is frequently edited in various cancers, and this editing is associated with enhanced tumor aggressiveness. After comparison of wild-type AZIN1 (wtAZIN1) and edited AZIN1 (edAZIN1, which contains a Ser367Gly substitution), we report differential binding of edAZIN1 to a small set of proteins; specifically, edAZIN1 binds to alpha-smooth muscle actin (ACTA2), gamma actin 1 (ACTG1), and myosin9, whereas wtAZIN1 does not. This binding enables nuclear translocation of edAZIN1. In contrast to overexpression of edAZIN1 and, to a lesser extent, (editable) wtAZIN1, overexpression of an uneditable AZIN1 allele does not promote a cellular phenotype associated with increased tumorigenicity. In patients, both editing and nuclear localization of AZIN1 are common and are associated with tumor aggressiveness, i.e., a higher Gleason score, higher genomic instability, and a shorter progression-free survival time. In conclusion, the data indicate that binding of edAZIN1 to the actin/myosin9 complex supports its nuclear translocation, leading to enhanced cellular aggressiveness, and is associated with worse prostate cancer outcomes. © 2022, The Author(s).
Keywords: carrier protein; genetics; metabolism; actin; prostatic neoplasms; prostate tumor; carrier proteins; actins; rna editing; humans; human; male; azin1 protein, human
Journal Title: Experimental and Molecular Medicine
Volume: 54
Issue: 10
ISSN: 1226-3613
Publisher: Springer Nature  
Date Published: 2022-10-01
Start Page: 1713
End Page: 1726
Language: English
DOI: 10.1038/s12276-022-00845-6
PUBMED: 36202978
PROVIDER: scopus
PMCID: PMC9636422
DOI/URL:
Notes: Article -- Export Date: 1 December 2022 -- Source: Scopus
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