Quantitative transportomics identifies Kif5a as a major regulator of neurodegeneration

Author:

Shah Sahil H123ORCID,Schiapparelli Lucio M2,Ma Yuanhui4,Yokota Satoshi1ORCID,Atkins Melissa1,Xia Xin1,Cameron Evan G1,Huang Thanh5,Saturday Sarah2,Sun Catalina B1,Knasel Cara1,Blackshaw Seth5ORCID,Yates John R4ORCID,Cline Hollis T2ORCID,Goldberg Jeffrey L1ORCID

Affiliation:

1. Byers Eye Institute and Spencer Center for Vision Research, Stanford University

2. Scripps Research, Neuroscience Department and the Dorris Neuroscience Center

3. Neuroscience Graduate Program and Medical Scientist Training Program, University of California, San Diego

4. Scripps Research, Department of Molecular Medicine

5. Department of Neuroscience, Johns Hopkins University School of Medicine

Abstract

Many neurons in the adult central nervous system, including retinal ganglion cells (RGCs), degenerate and die after injury. Early axon protein and organelle trafficking failure is a key component in many neurodegenerative disorders yet changes to axoplasmic transport in disease models have not been quantified. We analyzed early changes in the protein ‘transportome’ from RGC somas to their axons after optic nerve injury and identified transport failure of an anterograde motor protein Kif5a early in RGC degeneration. We demonstrated that manipulating Kif5a expression affects anterograde mitochondrial trafficking in RGCs and characterized axon transport in Kif5a knockout mice to identify proteins whose axon localization was Kif5a-dependent. Finally, we found that knockout of Kif5a in RGCs resulted in progressive RGC degeneration in the absence of injury. Together with expression data localizing Kif5a to human RGCs, these data identify Kif5a transport failure as a cause of RGC neurodegeneration and point to a mechanism for future therapeutics.

Funder

National Institutes of Health

Hahn Family Foundation

Glaucoma Research Foundation

Research to Prevent Blindness

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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