AI Article Synopsis
- * The study reveals that CSPalpha deficiency leads to rapid degeneration of retinal photoreceptor terminals, causing early blindness, while other retinal synapses remain unaffected initially.
- * Unlike photoreceptor cells, auditory hair cells express CSPbeta, which prevents neurodegeneration in their ribbon synapses, indicating that specific CSP isoforms are vital for protecting certain types of synapses from damage.
Article Abstract
Cysteine string protein (CSP) alpha is an abundant synaptic vesicle protein that contains a DNA-J domain characteristic of Hsp40-type cochaperones. Previous studies showed that deletion of CSPalpha in mice leads to massive lethal neurodegeneration but did not clarify how the neurodegeneration affects specific subpopulations of neurons. Here, we analyzed the effects of the CSPalpha deficiency on tonically active ribbon synapses of the retina and the inner ear. We show that CSPalpha-deficient photoreceptor terminals undergo dramatic and rapidly progressive neurodegeneration that starts before eye opening and initially does not affect other retinal synapses. These changes are associated with progressive blindness. In contrast, ribbon synapses of auditory hair cells did not exhibit presynaptic impairments in CSPalpha-deficient mice. Hair cells, but not photoreceptor cells or central neurons, express CSPbeta, thereby accounting for the lack of a hair-cell phenotype in CSPalpha knockout mice. Our data demonstrate that tonically active ribbon synapses in retina are particularly sensitive to the deletion of CSPalpha and that expression of at least one CSP isoform is essential to protect such tonically active synapses from neurodegeneration.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1413794 | PMC |
| http://dx.doi.org/10.1073/pnas.0510060103 | DOI Listing |
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