Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro

Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro

The Cx26 mRNA has not been reported to undergo alternative splicing. In expressing a series of human keratitis ichthyosis deafness (KID) syndrome mutations of Cx26 (A88V, N14K and A40V), we found the production of a truncated mRNA product. These mutations, although not creating a cryptic splice site...

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Main Authors: Jonathan Cook, Elizabeth de Wolf, Nicholas Dale
Format: Article
Language:English
Published: The Royal Society 2019-08-01
Series:Royal Society Open Science
Subjects:
connexin
connexon (hemichannel)
mrna
alternative splicing
keratitis ichthyosis deafness syndrome
Online Access:https://royalsocietypublishing.org/doi/pdf/10.1098/rsos.191128
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spelling doaj-b27d54084ab0434a8c4c711f3c3cebee2020-11-25T03:57:37ZengThe Royal SocietyRoyal Society Open Science2054-57032019-08-016810.1098/rsos.191128191128Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitroJonathan CookElizabeth de WolfNicholas DaleThe Cx26 mRNA has not been reported to undergo alternative splicing. In expressing a series of human keratitis ichthyosis deafness (KID) syndrome mutations of Cx26 (A88V, N14K and A40V), we found the production of a truncated mRNA product. These mutations, although not creating a cryptic splice site, appeared to activate a pre-existing cryptic splice site. The alternative splicing of the mutant Cx26 mRNA could be prevented by mutating the predicted 3′, 5′ splice sites and the branch point. The presence of a C-terminal fluorescent protein tag (mCherry or Clover) was necessary for this alternative splicing to occur. Strangely, Cx26A88V could cause the alternative splicing of co-expressed WT Cx26—suggesting a trans effect. The alternative splicing of Cx26A88V caused cell death, and this could be prevented by the 3′, 5′ and branch point mutations. Expression of the KID syndrome mutants could be rescued by combining them with removal of the 5′ splice site. We used this strategy to enable expression of Cx26A40V-5′ and demonstrate that this KID syndrome mutation removed CO2 sensitivity from the Cx26 hemichannel. This is the fourth KID syndrome mutation found to abolish the CO2-sensitivity of the Cx26 hemichannel, and suggests that the altered CO­2-sensitivity could contribute to the pathology of this mutation. Future research on KID syndrome mutations should take care to avoid using a C-terminal tag to track cellular localization and expression or if this is unavoidable, combine this mutation with removal of the 5′ splice site.https://royalsocietypublishing.org/doi/pdf/10.1098/rsos.191128connexinconnexon (hemichannel)mrnaalternative splicingkeratitis ichthyosis deafness syndrome
collection DOAJ
language English
format Article
sources DOAJ
author Jonathan Cook
Elizabeth de Wolf
Nicholas Dale
spellingShingle Jonathan Cook
Elizabeth de Wolf
Nicholas Dale
Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
Royal Society Open Science
connexin
connexon (hemichannel)
mrna
alternative splicing
keratitis ichthyosis deafness syndrome
author_facet Jonathan Cook
Elizabeth de Wolf
Nicholas Dale
author_sort Jonathan Cook
title Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
title_short Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
title_full Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
title_fullStr Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
title_full_unstemmed Cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of Cx26 to prevent expression and cause toxicity in vitro
title_sort cx26 keratitis ichthyosis deafness syndrome mutations trigger alternative splicing of cx26 to prevent expression and cause toxicity in vitro
publisher The Royal Society
series Royal Society Open Science
issn 2054-5703
publishDate 2019-08-01
description The Cx26 mRNA has not been reported to undergo alternative splicing. In expressing a series of human keratitis ichthyosis deafness (KID) syndrome mutations of Cx26 (A88V, N14K and A40V), we found the production of a truncated mRNA product. These mutations, although not creating a cryptic splice site, appeared to activate a pre-existing cryptic splice site. The alternative splicing of the mutant Cx26 mRNA could be prevented by mutating the predicted 3′, 5′ splice sites and the branch point. The presence of a C-terminal fluorescent protein tag (mCherry or Clover) was necessary for this alternative splicing to occur. Strangely, Cx26A88V could cause the alternative splicing of co-expressed WT Cx26—suggesting a trans effect. The alternative splicing of Cx26A88V caused cell death, and this could be prevented by the 3′, 5′ and branch point mutations. Expression of the KID syndrome mutants could be rescued by combining them with removal of the 5′ splice site. We used this strategy to enable expression of Cx26A40V-5′ and demonstrate that this KID syndrome mutation removed CO2 sensitivity from the Cx26 hemichannel. This is the fourth KID syndrome mutation found to abolish the CO2-sensitivity of the Cx26 hemichannel, and suggests that the altered CO­2-sensitivity could contribute to the pathology of this mutation. Future research on KID syndrome mutations should take care to avoid using a C-terminal tag to track cellular localization and expression or if this is unavoidable, combine this mutation with removal of the 5′ splice site.
topic connexin
connexon (hemichannel)
mrna
alternative splicing
keratitis ichthyosis deafness syndrome
url https://royalsocietypublishing.org/doi/pdf/10.1098/rsos.191128
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AT nicholasdale cx26keratitisichthyosisdeafnesssyndromemutationstriggeralternativesplicingofcx26topreventexpressionandcausetoxicityinvitro
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