Increased polyubiquitination and proteasomal degradation of a Munc18-1 disease-linked mutant causes temperature-sensitive defect in exocytosis
Sally Martin, Andreas Papadopulos, Vanesa M Tomatis, Emma Sierecki, Nancy T Malintan, Rachel S Gormal, Nichole Giles, Wayne A Johnston, Kirill Alexandrov, Yann Gambin, Brett M Collins, Frederic A Meunier, Sally Martin, Andreas Papadopulos, Vanesa M Tomatis, Emma Sierecki, Nancy T Malintan, Rachel S Gormal, Nichole Giles, Wayne A Johnston, Kirill Alexandrov, Yann Gambin, Brett M Collins, Frederic A Meunier
Abstract
Munc18-1 is a critical component of the core machinery controlling neuroexocytosis. Recently, mutations in Munc18-1 leading to the development of early infantile epileptic encephalopathy have been discovered. However, which degradative pathway controls Munc18-1 levels and how it impacts on neuroexocytosis in this pathology is unknown. Using neurosecretory cells deficient in Munc18, we show that a disease-linked mutation, C180Y, renders the protein unstable at 37°C. Although the mutated protein retains its function as t-SNARE chaperone, neuroexocytosis is impaired, a defect that can be rescued at a lower permissive temperature. We reveal that Munc18-1 undergoes K48-linked polyubiquitination, which is highly increased by the mutation, leading to proteasomal, but not lysosomal, degradation. Our data demonstrate that functional Munc18-1 levels are controlled through polyubiquitination and proteasomal degradation. The C180Y disease-causing mutation greatly potentiates this degradative pathway, rendering Munc18-1 unable to facilitate neuroexocytosis, a phenotype that is reversed at a permissive temperature.
Copyright © 2014 The Authors. Published by Elsevier Inc. All rights reserved.
Source: PubMed