Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.

Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.

Mutations in whirlin cause either Usher syndrome type II (USH2), a deafness-blindness disorder, or nonsyndromic deafness. The molecular basis for the variable disease expression is unknown. We show here that only the whirlin long isoform, distinct from a short isoform by virtue of having two N-termi...

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Main Authors: Jun Yang, Xiaoqing Liu, Yun Zhao, Michael Adamian, Basil Pawlyk, Xun Sun, D Randy McMillan, M Charles Liberman, Tiansen Li
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-05-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC2873905?pdf=render
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spelling doaj-d40cc87784f94e8599249d143577c1d02020-11-24T21:47:55ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042010-05-0165e100095510.1371/journal.pgen.1000955Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.Jun YangXiaoqing LiuYun ZhaoMichael AdamianBasil PawlykXun SunD Randy McMillanM Charles LibermanTiansen LiMutations in whirlin cause either Usher syndrome type II (USH2), a deafness-blindness disorder, or nonsyndromic deafness. The molecular basis for the variable disease expression is unknown. We show here that only the whirlin long isoform, distinct from a short isoform by virtue of having two N-terminal PDZ domains, is expressed in the retina. Both long and short isoforms are expressed in the inner ear. The N-terminal PDZ domains of the long whirlin isoform mediates the formation of a multi-protein complex that includes usherin and VLGR1, both of which are also implicated in USH2. We localized this USH2 protein complex to the periciliary membrane complex (PMC) in mouse photoreceptors that appears analogous to the frog periciliary ridge complex. The latter is proposed to play a role in photoreceptor protein trafficking through the connecting cilium. Mice carrying a targeted disruption near the N-terminus of whirlin manifest retinal and inner ear defects, reproducing the clinical features of human USH2 disease. This is in contrast to mice with mutations affecting the C-terminal portion of whirlin in which the phenotype is restricted to the inner ear. In mice lacking any one of the USH2 proteins, the normal localization of all USH2 proteins is disrupted, and there is evidence of protein destabilization. Taken together, our findings provide new insights into the pathogenic mechanism of Usher syndrome. First, the three USH2 proteins exist as an obligatory functional complex in vivo, and loss of one USH2 protein is functionally close to loss of all three. Second, defects in the three USH2 proteins share a common pathogenic process, i.e., disruption of the PMC. Third, whirlin mutations that ablate the N-terminal PDZ domains lead to Usher syndrome, but non-syndromic hearing loss will result if they are spared.http://europepmc.org/articles/PMC2873905?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jun Yang
Xiaoqing Liu
Yun Zhao
Michael Adamian
Basil Pawlyk
Xun Sun
D Randy McMillan
M Charles Liberman
Tiansen Li
spellingShingle Jun Yang
Xiaoqing Liu
Yun Zhao
Michael Adamian
Basil Pawlyk
Xun Sun
D Randy McMillan
M Charles Liberman
Tiansen Li
Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
PLoS Genetics
author_facet Jun Yang
Xiaoqing Liu
Yun Zhao
Michael Adamian
Basil Pawlyk
Xun Sun
D Randy McMillan
M Charles Liberman
Tiansen Li
author_sort Jun Yang
title Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
title_short Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
title_full Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
title_fullStr Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
title_full_unstemmed Ablation of whirlin long isoform disrupts the USH2 protein complex and causes vision and hearing loss.
title_sort ablation of whirlin long isoform disrupts the ush2 protein complex and causes vision and hearing loss.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2010-05-01
description Mutations in whirlin cause either Usher syndrome type II (USH2), a deafness-blindness disorder, or nonsyndromic deafness. The molecular basis for the variable disease expression is unknown. We show here that only the whirlin long isoform, distinct from a short isoform by virtue of having two N-terminal PDZ domains, is expressed in the retina. Both long and short isoforms are expressed in the inner ear. The N-terminal PDZ domains of the long whirlin isoform mediates the formation of a multi-protein complex that includes usherin and VLGR1, both of which are also implicated in USH2. We localized this USH2 protein complex to the periciliary membrane complex (PMC) in mouse photoreceptors that appears analogous to the frog periciliary ridge complex. The latter is proposed to play a role in photoreceptor protein trafficking through the connecting cilium. Mice carrying a targeted disruption near the N-terminus of whirlin manifest retinal and inner ear defects, reproducing the clinical features of human USH2 disease. This is in contrast to mice with mutations affecting the C-terminal portion of whirlin in which the phenotype is restricted to the inner ear. In mice lacking any one of the USH2 proteins, the normal localization of all USH2 proteins is disrupted, and there is evidence of protein destabilization. Taken together, our findings provide new insights into the pathogenic mechanism of Usher syndrome. First, the three USH2 proteins exist as an obligatory functional complex in vivo, and loss of one USH2 protein is functionally close to loss of all three. Second, defects in the three USH2 proteins share a common pathogenic process, i.e., disruption of the PMC. Third, whirlin mutations that ablate the N-terminal PDZ domains lead to Usher syndrome, but non-syndromic hearing loss will result if they are spared.
url http://europepmc.org/articles/PMC2873905?pdf=render
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