Small molecule induced STING degradation facilitated by the HECT ligase HERC4-Reference-Cited by-同舟云学术

Small molecule induced STING degradation facilitated by the HECT ligase HERC4

Published:2024-05-29 Issue:1 Volume:15 Page:
ISSN:2041-1723
Container-title:Nature Communications
language:en
Short-container-title:Nat Commun

Author:

Mutlu Merve^ORCID,Schmidt Isabel^ORCID,Morrison Andrew I.^ORCID,Goretzki Benedikt,Freuler Felix,Begue Damien,Simic Oliver,Pythoud Nicolas,Ahrne Erik,Kapps Sandra,Roest Susan,Bonenfant Debora,Jeanpierre Delphine,Tran Thi-Thanh-Thao,Maher Rob,An Shaojian^ORCID,Rietsch Amandine,Nigsch Florian^ORCID,Hofmann Andreas^ORCID,Reece-Hoyes John,Parker Christian N.,Guerini Danilo

Abstract

AbstractStimulator of interferon genes (STING) is a central component of the cytosolic nucleic acids sensing pathway and as such master regulator of the type I interferon response. Due to its critical role in physiology and its’ involvement in a variety of diseases, STING has been a focus for drug discovery. Targeted protein degradation (TPD) has emerged as a promising pharmacology for targeting previously considered undruggable proteins by hijacking the cellular ubiquitin proteasome system (UPS) with small molecules. Here, we identify AK59 as a STING degrader leveraging HERC4, a HECT-domain E3 ligase. Additionally, our data reveals that AK59 is effective on the common pathological STING mutations, suggesting a potential clinical application of this mechanism. Thus, these findings introduce HERC4 to the fields of TPD and of compound-induced degradation of STING, suggesting potential therapeutic applications.

Publisher

Springer Science and Business Media LLC

Link

https://www.nature.com/articles/s41467-024-48922-w.pdf

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