An Angelman syndrome substitution in the HECT E3 ubiquitin ligase C-terminal Lobe of E6AP affects protein stability and activity

Authors

Steven A. Beasley, Clark University
Chloe E. Kellum, Clark University
Rachel J. Orlomoski, Clark University
Feston Idrizi, Clark University
Donald E. Spratt, Clark UniversityFollow

Document Type

Article

Abstract

Angelman syndrome (AS) is a rare neurodevelopmental disorder characterized by speech impairment, intellectual disability, ataxia, and epilepsy. AS is caused by mutations in the maternal copy of UBE3A located on chromosome 15q11-13. UBE3A codes for E6AP (E6 Associated Protein), a prominent member of the HECT (Homologous to E6AP C-Terminus) E3 ubiquitin ligase family. E6AP catalyzes the posttranslational attachment of ubiquitin via its HECT domain onto various intracellular target proteins to regulate DNA repair and cell cycle progression. The HECT domain consists of an N-lobe, required for E2~ubiquitin recruitment, while the C-lobe contains the conserved catalytic cysteine required for ubiquitin transfer. Previous genetic studies of AS patients have identified point mutations in UBE3A that result in amino acid substitutions or premature termination during translation. An AS transversion mutation (codon change from ATA to AAA) within the region of the gene that codes for the catalytic HECT domain of E6AP has been annotated (I827K), but the molecular basis for this loss of function substitution remained elusive. Here, we demonstrate that the I827K substitution destabilizes the 3D fold causing protein aggregation of the C-terminal lobe of E6AP using a combination of spectropolarimetry and nuclear magnetic resonance (NMR) spectroscopy. Our fluorescent ubiquitin activity assays with E6AP-I827K show decreased ubiquitin thiolester formation and ubiquitin discharge. Using 3D models in combination with our biochemical and biophysical results, we rationalize why the I827K disrupts E6AP-dependent ubiquitylation. This work provides new insight into the E6AP mechanism and how its malfunction can be linked to the AS phenotype.

Publication Title

PLoS ONE

Publication Date

7-2020

Volume

15

Issue

7 July

ISSN

1932-6203

DOI

10.1371/journal.pone.0235925

Repository Citation

Beasley, Steven A.; Kellum, Chloe E.; Orlomoski, Rachel J.; Idrizi, Feston; and Spratt, Donald E., "An Angelman syndrome substitution in the HECT E3 ubiquitin ligase C-terminal Lobe of E6AP affects protein stability and activity" (2020). Chemistry. 147.
https://commons.clarku.edu/chemistry/147

Cross Post Location

Student Publications

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Copyright Conditions

Beasley, S. A., Kellum, C. E., Orlomoski, R. J., Idrizi, F., & Spratt, D. E. (2020). An Angelman syndrome substitution in the HECT E3 ubiquitin ligase C-terminal Lobe of E6AP affects protein stability and activity. PLoS One, 15(7), e0235925.