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Acetylation modulates the Fanconi anemia pathway by protecting FAAP20 from ubiquitin-mediated proteasomal degradation

Bhavika Nagareddy, Arafat Khan, Hyungjin Kim

2020Journal of Biological Chemistry15 citationsDOIOpen Access PDF

Abstract

isomerization and phosphorylation at a consensus phosphodegron motif is essential for preserving the integrity of the FA core complex, and thus FANCD2 monoubiquitination. However, how ubiquitin-dependent FAAP20 degradation is modulated to fine-tune FA pathway activation remains largely un-known. Here, we present evidence that FAAP20 is acetylated by the acetyltransferase p300/CBP on lysine 152, the key residue that when polyubiquitinated results in the degradation of FAAP20. Acetylation or mutation of the lysine residue stabilizes FAAP20 by preventing its ubiquitination, thereby protecting it from proteasome-dependent FAAP20 degradation. Consequently, disruption of the FAAP20 acetylation pathway impairs FANCD2 activation. Together, our study reveals a competition mechanism between ubiquitination and acetylation of a common lysine residue that controls FAAP20 stability and highlights a complex balancing between different posttranslational modifications as a way to refine the FA pathway signaling required for DNA ICL repair and genome stability.

Topics & Concepts

Fanconi anemiaUbiquitinAcetylationCell biologyProteasomeChemistryDegradation (telecommunications)Ubiquitin-Protein LigasesCancer researchDNABiologyDNA repairUbiquitin ligaseBiochemistryGeneComputer scienceTelecommunicationsUbiquitin and proteasome pathwaysHistone Deacetylase Inhibitors ResearchAutophagy in Disease and Therapy
Acetylation modulates the Fanconi anemia pathway by protecting FAAP20 from ubiquitin-mediated proteasomal degradation | Litcius