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Self-guarding of MORC3 enables virulence factor-triggered immunity

Moritz M. Gaidt (), Alyssa Morrow, Marian R. Fairgrieve, Jonathan P. Karr, Nir Yosef and Russell E. Vance ()
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Moritz M. Gaidt: University of California
Alyssa Morrow: University of California
Marian R. Fairgrieve: University of California
Jonathan P. Karr: University of California
Nir Yosef: University of California
Russell E. Vance: University of California

Nature, 2021, vol. 600, issue 7887, 138-142

Abstract: Abstract Pathogens use virulence factors to inhibit the immune system1. The guard hypothesis2,3 postulates that hosts monitor (or ‘guard’) critical innate immune pathways such that their disruption by virulence factors provokes a secondary immune response1. Here we describe a ‘self-guarded’ immune pathway in human monocytes, in which guarding and guarded functions are combined in one protein. We find that this pathway is triggered by ICP0, a key virulence factor of herpes simplex virus type 1, resulting in robust induction of anti-viral type I interferon (IFN). Notably, induction of IFN by ICP0 is independent of canonical immune pathways and the IRF3 and IRF7 transcription factors. A CRISPR screen identified the ICP0 target MORC34 as an essential negative regulator of IFN. Loss of MORC3 recapitulates the IRF3- and IRF7-independent IFN response induced by ICP0. Mechanistically, ICP0 degrades MORC3, which leads to de-repression of a MORC3-regulated DNA element (MRE) adjacent to the IFNB1 locus. The MRE is required in cis for IFNB1 induction by the MORC3 pathway, but is not required for canonical IFN-inducing pathways. As well as repressing the MRE to regulate IFNB1, MORC3 is also a direct restriction factor of HSV-15. Our results thus suggest a model in which the primary anti-viral function of MORC3 is self-guarded by its secondary IFN-repressing function—thus, a virus that degrades MORC3 to avoid its primary anti-viral function will unleash the secondary anti-viral IFN response.

Date: 2021
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DOI: 10.1038/s41586-021-04054-5

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