Wdfy3 regulates glycophagy, mitophagy, and synaptic plasticity-Reference-Cited by-同舟云学术

Wdfy3 regulates glycophagy, mitophagy, and synaptic plasticity

Published:2021-06-29 Issue:12 Volume:41 Page:3213-3231
ISSN:0271-678X
Container-title:Journal of Cerebral Blood Flow & Metabolism
language:en
Short-container-title:J Cereb Blood Flow Metab

Author:

Napoli Eleonora¹,Panoutsopoulos Alexios A²³,Kysar Patricia⁴,Satriya Nathaniel¹,Sterling Kira¹,Shibata Bradley⁴,Imai Denise⁵,Ruskin David N⁶,Zarbalis Konstantinos S²³⁷,Giulivi Cecilia¹⁷^ORCID

Affiliation:

1. Department of Molecular Biosciences, School of Veterinary Medicine, University of California, Davis, CA, USA

2. Department of Pathology and Laboratory Medicine, University of California, Davis, Sacramento, CA, USA

3. Institute for Pediatric Regenerative Medicine, Shriners Hospitals for Children, Sacramento, CA, USA

4. Department of Cell Biology and Human Anatomy, School of Medicine, University of California, Davis, CA, USA

5. Anatomic Pathology Service, Veterinary Medical Teaching Hospital, University of California, Davis, CA, USA

6. Department of Psychology and Neuroscience Program, Trinity College, Hartford, CT, USA

7. Medical Investigations of Neurodevelopmental Disorders (MIND) Institute, University of California Davis, CA, USA

Abstract

Autophagy is essential to cell function, as it enables the recycling of intracellular constituents during starvation and in addition functions as a quality control mechanism by eliminating spent organelles and proteins that could cause cellular damage if not properly removed. Recently, we reported on Wdfy3’s role in mitophagy, a clinically relevant macroautophagic scaffold protein that is linked to intellectual disability, neurodevelopmental delay, and autism spectrum disorder. In this study, we confirm our previous report that Wdfy3 haploinsufficiency in mice results in decreased mitophagy with accumulation of mitochondria with altered morphology, but expanding on that observation, we also note decreased mitochondrial localization at synaptic terminals and decreased synaptic density, which may contribute to altered synaptic plasticity. These changes are accompanied by defective elimination of glycogen particles and a shift to increased glycogen synthesis over glycogenolysis and glycophagy. This imbalance leads to an age-dependent higher incidence of brain glycogen deposits with cerebellar hypoplasia. Our results support and further extend Wdfy3’s role in modulating both brain bioenergetics and synaptic plasticity by including glycogen as a target of macroautophagic degradation.

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine,Clinical Neurology,Neurology

Link

http://journals.sagepub.com/doi/pdf/10.1177/0271678X211027384

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