Localized molecular chaperone synthesis maintains neuronal dendrite proteostasis

Author:

Ugalde Maria Vera1,Alecki Célia1,Rizwan Javeria1,Le Phuong2ORCID,Jacob-Tomas Suleima1,Xu Jia Ming1,Minotti Sandra1,Wu Tad1,Durham Heather1,Yeo Gene2

Affiliation:

1. McGill University

2. University of California, San Diego

Abstract

Abstract Proteostasis is maintained through regulated protein synthesis and degradation and chaperone-assisted protein folding. However, this is challenging in neuronal projections because of their polarized morphology and constant synaptic proteome remodeling. Using high-resolution fluorescence microscopy, we discovered that neurons localize a subset of chaperone mRNAs to their dendrites and use microtubule-based transport to increase this asymmetric localization following proteotoxic stress. The most abundant dendritic chaperone mRNA encodes a constitutive heat shock protein 70 family member (HSPA8). Proteotoxic stress also enhanced HSPA8 mRNA translation efficiency in dendrites. Stress-mediated HSPA8 mRNA localization to the dendrites was impaired by depleting fused in sarcoma—an amyotrophic lateral sclerosis-related protein—in cultured mouse motor neurons and expressing a pathogenic variant of heterogenous nuclear ribonucleoprotein A2/B1 in neurons derived from human induced pluripotent stem cells. These results reveal a crucial and unexpected neuronal stress response in which RNA-binding proteins increase the dendritic localization of HSPA8 mRNA to maintain proteostasis and prevent neurodegeneration.

Publisher

Research Square Platform LLC

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