Journal
SCIENCE ADVANCES
Volume 8, Issue 14, Pages -Publisher
AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.abk0942
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Funding
- NIH [R01 DC016807, 1P20GM139762-01]
- Bellucci Depaoli Family Foundation
- Beijing Natural Science Foundation [Z20J00122]
- National Natural Science Foundation of China [81970838, 81870718, 81770996]
- NIGMS
- Bellucci Depaoli Family Foundation (The Imaging and Molecular Biology Cores at the Translational Hearing Research Center of Creighton University School of Medicine)
- NIH/NIDCD Grant [U24: 1U24DC015910-01]
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This study reveals the role of autophagy-lysosomal dysfunction in syndromic hearing and vision loss in mice and humans caused by the mutation of SLC7A14 protein.
Lysosomes contribute to cellular homeostasis via processes including macromolecule degradation, nutrient sensing, and autophagy. Defective proteins related to lysosomal macromolecule catabolism are known to cause a range of lysosomal storage diseases; however, it is unclear whether mutations in proteins involved in homeostatic nutrient sensing mechanisms cause syndromic sensory disease. Here, we show that SLC7A14, a transporter protein mediating lysosomal uptake of cationic amino acids, is evolutionarily conserved in vertebrate mechanosensory hair cells and highly expressed in lysosomes of mammalian cochlear inner hair cells (IHCs) and retinal photoreceptors. Autosomal recessive mutation of SLC7A14 caused loss of IHCs and photoreceptors, leading to presynaptic auditory neuropathy and retinitis pigmentosa in mice and humans. Loss-of-function mutation altered protein trafficking and increased basal autophagy, leading to progressive cell degeneration. This study implicates autophagy-lysosomal dysfunction in syndromic hearing and vision loss in mice and humans.
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