ADAR1p150 prevents MDA5 and PKR activation via distinct mechanisms to avert fatal autoinflammation

Shi-Bin Hu; Jacki Heraud-Farlow; Tao Sun; Zhen Liang; Ankita Goradia; Scott Taylor; Carl R Walkley; Jin Billy Li

doi:10.1016/j.molcel.2023.09.018

ADAR1p150 prevents MDA5 and PKR activation via distinct mechanisms to avert fatal autoinflammation

Mol Cell. 2023 Nov 2;83(21):3869-3884.e7. doi: 10.1016/j.molcel.2023.09.018. Epub 2023 Oct 4.

Authors

Shi-Bin Hu¹, Jacki Heraud-Farlow², Tao Sun¹, Zhen Liang², Ankita Goradia³, Scott Taylor³, Carl R Walkley⁴, Jin Billy Li⁵

Affiliations

¹ Department of Genetics, Stanford University, Stanford, CA 94305, USA.
² St. Vincent's Institute of Medical Research, Fitzroy, VIC 3065, Australia; Department of Medicine, Eastern Hill Precinct, Melbourne Medical School, University of Melbourne, Fitzroy, VIC 3065, Australia.
³ St. Vincent's Institute of Medical Research, Fitzroy, VIC 3065, Australia.
⁴ St. Vincent's Institute of Medical Research, Fitzroy, VIC 3065, Australia; Department of Medicine, Eastern Hill Precinct, Melbourne Medical School, University of Melbourne, Fitzroy, VIC 3065, Australia. Electronic address: cwalkley@svi.edu.au.
⁵ Department of Genetics, Stanford University, Stanford, CA 94305, USA. Electronic address: jin.billy.li@stanford.edu.

PMID: 37797622
DOI: 10.1016/j.molcel.2023.09.018

Abstract

Effective immunity requires the innate immune system to distinguish foreign nucleic acids from cellular ones. Cellular double-stranded RNAs (dsRNAs) are edited by the RNA-editing enzyme ADAR1 to evade being recognized as viral dsRNA by cytoplasmic dsRNA sensors, including MDA5 and PKR. The loss of ADAR1-mediated RNA editing of cellular dsRNA activates MDA5. Additional RNA-editing-independent functions of ADAR1 have been proposed, but a specific mechanism has not been delineated. We now demonstrate that the loss of ADAR1-mediated RNA editing specifically activates MDA5, whereas loss of the cytoplasmic ADAR1p150 isoform or its dsRNA-binding activity enabled PKR activation. Deleting both MDA5 and PKR resulted in complete rescue of the embryonic lethality of Adar1p150^-/- mice to adulthood, contrasting with the limited or no rescue by removing MDA5 or PKR alone. Our findings demonstrate that MDA5 and PKR are the primary in vivo effectors of fatal autoinflammation following the loss of ADAR1p150.

Keywords: ADAR1; MDA5; PKR; RNA editing; dsRNA; innate immunity.

MeSH terms

Adenosine Deaminase / genetics
Adenosine Deaminase / metabolism
Animals
Cytoplasm / metabolism
Immunity, Innate* / genetics
Mice
RNA, Double-Stranded* / genetics

Substances

ADAR1 protein, mouse
Adenosine Deaminase
RNA, Double-Stranded
protein kinase R, mouse
Ifih1 protein, mouse