Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.

Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.

The mammalian eye lens expresses a high concentration of crystallins (α, β and γ-crystallins) to maintain the refractive index essential for lens transparency. Crystallins are long-lived proteins that do not turnover throughout life. The structural destabilization of crystallins by UV exposure, glyc...

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Main Authors: Usha P Andley, Eric Tycksen, Brittney N McGlasson-Naumann, Paul D Hamilton
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0190817
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spelling doaj-5fab3fb3577a4ec7b1ec4b52d0640cdd2021-03-03T19:45:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01131e019081710.1371/journal.pone.0190817Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.Usha P AndleyEric TycksenBrittney N McGlasson-NaumannPaul D HamiltonThe mammalian eye lens expresses a high concentration of crystallins (α, β and γ-crystallins) to maintain the refractive index essential for lens transparency. Crystallins are long-lived proteins that do not turnover throughout life. The structural destabilization of crystallins by UV exposure, glycation, oxidative stress and mutations in crystallin genes leads to protein aggregation and development of cataracts. Several destabilizing mutations in crystallin genes are linked with human autosomal dominant hereditary cataracts. To investigate the mechanism by which the α-crystallin mutations Cryaa-R49C and Cryab-R120G lead to cataract formation, we determined whether these mutations cause an altered expression of specific transcripts in the lens at an early postnatal age by RNA-seq analysis. Using knock-in mouse models previously generated in our laboratory, in the present work, we identified genes that exhibited altered abundance in the mutant lenses, including decreased transcripts for Clic5, an intracellular water channel in Cryaa-R49C heterozygous mutant lenses, and increased transcripts for Eno1b in Cryab-R120G heterozygous mutant lenses. In addition, RNA-seq analysis revealed increased histones H2B, H2A, and H4 gene expression in Cryaa-R49C mutant lenses, suggesting that the αA-crystallin mutation regulates histone expression via a transcriptional mechanism. Additionally, these studies confirmed the increased expression of histones H2B, H2A, and H4 by proteomic analysis of Cryaa-R49C knock-in and Cryaa;Cryab gene knockout lenses reported previously. Taken together, these findings offer additional insight into the early transcriptional changes caused by Cryaa and Cryab mutations associated with autosomal dominant human cataracts, and indicate that the transcript levels of certain genes are affected by the expression of mutant α-crystallin in vivo.https://doi.org/10.1371/journal.pone.0190817
collection DOAJ
language English
format Article
sources DOAJ
author Usha P Andley
Eric Tycksen
Brittney N McGlasson-Naumann
Paul D Hamilton
spellingShingle Usha P Andley
Eric Tycksen
Brittney N McGlasson-Naumann
Paul D Hamilton
Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
PLoS ONE
author_facet Usha P Andley
Eric Tycksen
Brittney N McGlasson-Naumann
Paul D Hamilton
author_sort Usha P Andley
title Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
title_short Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
title_full Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
title_fullStr Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
title_full_unstemmed Probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
title_sort probing the changes in gene expression due to α-crystallin mutations in mouse models of hereditary human cataract.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description The mammalian eye lens expresses a high concentration of crystallins (α, β and γ-crystallins) to maintain the refractive index essential for lens transparency. Crystallins are long-lived proteins that do not turnover throughout life. The structural destabilization of crystallins by UV exposure, glycation, oxidative stress and mutations in crystallin genes leads to protein aggregation and development of cataracts. Several destabilizing mutations in crystallin genes are linked with human autosomal dominant hereditary cataracts. To investigate the mechanism by which the α-crystallin mutations Cryaa-R49C and Cryab-R120G lead to cataract formation, we determined whether these mutations cause an altered expression of specific transcripts in the lens at an early postnatal age by RNA-seq analysis. Using knock-in mouse models previously generated in our laboratory, in the present work, we identified genes that exhibited altered abundance in the mutant lenses, including decreased transcripts for Clic5, an intracellular water channel in Cryaa-R49C heterozygous mutant lenses, and increased transcripts for Eno1b in Cryab-R120G heterozygous mutant lenses. In addition, RNA-seq analysis revealed increased histones H2B, H2A, and H4 gene expression in Cryaa-R49C mutant lenses, suggesting that the αA-crystallin mutation regulates histone expression via a transcriptional mechanism. Additionally, these studies confirmed the increased expression of histones H2B, H2A, and H4 by proteomic analysis of Cryaa-R49C knock-in and Cryaa;Cryab gene knockout lenses reported previously. Taken together, these findings offer additional insight into the early transcriptional changes caused by Cryaa and Cryab mutations associated with autosomal dominant human cataracts, and indicate that the transcript levels of certain genes are affected by the expression of mutant α-crystallin in vivo.
url https://doi.org/10.1371/journal.pone.0190817
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AT pauldhamilton probingthechangesingeneexpressionduetoacrystallinmutationsinmousemodelsofhereditaryhumancataract
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