| Literature DB >> 26590345 |
Valerie Uytterhoeven1, Elsa Lauwers2, Ine Maes1, Katarzyna Miskiewicz1, Manuel N Melo3, Jef Swerts1, Sabine Kuenen1, Rafaël Wittocx1, Nikky Corthout4, Siewert-Jan Marrink3, Sebastian Munck4, Patrik Verstreken5.
Abstract
Synapses are often far from their cell bodies and must largely independently cope with dysfunctional proteins resulting from synaptic activity and stress. To identify membrane-associated machines that can engulf synaptic targets destined for degradation, we performed a large-scale in vitro liposome-based screen followed by functional studies. We identified a presynaptically enriched chaperone Hsc70-4 that bends membranes based on its ability to oligomerize. This activity promotes endosomal microautophagy and the turnover of specific synaptic proteins. Loss of microautophagy slows down neurotransmission while gain of microautophagy increases neurotransmission. Interestingly, Sgt, a cochaperone of Hsc70-4, is able to switch the activity of Hsc70-4 from synaptic endosomal microautophagy toward chaperone activity. Hence, Hsc70-4 controls rejuvenation of the synaptic protein pool in a dual way: either by refolding proteins together with Sgt, or by targeting them for degradation by facilitating endosomal microautophagy based on its membrane deforming activity.Entities:
Mesh:
Substances:
Year: 2015 PMID: 26590345 DOI: 10.1016/j.neuron.2015.10.012
Source DB: PubMed Journal: Neuron ISSN: 0896-6273 Impact factor: 17.173