An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response

PURPOSE: To investigate the clinical features and molecular basis of inherited cataract-microcornea caused by an αA-crystallin gene (CRYAA) mutation in a Chinese family. METHODS: A three-generation Chinese family with members having autosomal dominant cataract and microcornea was recruited. Genomic...

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Autores principales: Zhang, Li-Yun, Yam, Gary Hin-Fai, Tam, Pancy Oi-Sin, Lai, Ricky Yiu-Kwong, Lam, Dennis Shun-Chiu, Pang, Chi-Pui, Fan, Dorothy Shu-Ping
Formato: Texto
Lenguaje:English
Publicado: Molecular Vision 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2690964/
https://www.ncbi.nlm.nih.gov/pubmed/19503744
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author Zhang, Li-Yun
Yam, Gary Hin-Fai
Tam, Pancy Oi-Sin
Lai, Ricky Yiu-Kwong
Lam, Dennis Shun-Chiu
Pang, Chi-Pui
Fan, Dorothy Shu-Ping
author_facet Zhang, Li-Yun
Yam, Gary Hin-Fai
Tam, Pancy Oi-Sin
Lai, Ricky Yiu-Kwong
Lam, Dennis Shun-Chiu
Pang, Chi-Pui
Fan, Dorothy Shu-Ping
author_sort Zhang, Li-Yun
collection PubMed
description PURPOSE: To investigate the clinical features and molecular basis of inherited cataract-microcornea caused by an αA-crystallin gene (CRYAA) mutation in a Chinese family. METHODS: A three-generation Chinese family with members having autosomal dominant cataract and microcornea was recruited. Genomic DNA from peripheral blood or buccal swab samples of five affected and five unaffected members were obtained. Based on 15 genes known to cause autosomal dominant cataract, single nucleotide polymorphisms (SNPs) or microsatellite markers were selected and genotyped for two-point linkage analysis. Direct sequencing was performed to identify the disease-causing mutation. The expression construct coding for recombinant COOH-terminal myc-His-tagged wild type or R12C αA-crystallin protein (CRYAA) was expressed in COS-7 cells. Detergent solubility and subcellular distribution of wild type and R12C CRYAA were examined by western blotting and immunofluorescence, respectively. Heat-shock response was monitored by quantitative polymerase chain reaction (qPCR) of heat-shock proteins 70 and 90α (HSP70 and HSP90α). RESULTS: The five affected family members showed variable lens opacities and microcornea. Clinical features of cataract were asymmetric in two eyes of some affected subjects. A heterozygous missense substitution, c.34C>T, in CRYAA, which is responsible for the R12C amino acid change, segregated with autosomal dominant cataract (ADCC) in this family. This substitution was absent in 103 unrelated controls. When expressed in COS-7 cells, the R12C mutant CRYAA resembled the wild type protein in its solubility when extracted with 0.5% Triton X-100 and with its cytoplasmic localization. However, mutant cells exhibited an altered heat-shock response, evidenced by the delayed expression of HSP70, when compared to cells expressing wild type CRYAA. CONCLUSIONS: The R12C mutation in CRYAA was responsible for a variable type of inherited cataract associated with microcornea in this Chinese family. The altered heat-shock response of mutant cells suggested a change of chaperoning capacity and networking, which could be associated with the pathogenesis of hereditary cataract-microcornea syndrome.
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spelling pubmed-26909642009-06-04 An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response Zhang, Li-Yun Yam, Gary Hin-Fai Tam, Pancy Oi-Sin Lai, Ricky Yiu-Kwong Lam, Dennis Shun-Chiu Pang, Chi-Pui Fan, Dorothy Shu-Ping Mol Vis Research Article PURPOSE: To investigate the clinical features and molecular basis of inherited cataract-microcornea caused by an αA-crystallin gene (CRYAA) mutation in a Chinese family. METHODS: A three-generation Chinese family with members having autosomal dominant cataract and microcornea was recruited. Genomic DNA from peripheral blood or buccal swab samples of five affected and five unaffected members were obtained. Based on 15 genes known to cause autosomal dominant cataract, single nucleotide polymorphisms (SNPs) or microsatellite markers were selected and genotyped for two-point linkage analysis. Direct sequencing was performed to identify the disease-causing mutation. The expression construct coding for recombinant COOH-terminal myc-His-tagged wild type or R12C αA-crystallin protein (CRYAA) was expressed in COS-7 cells. Detergent solubility and subcellular distribution of wild type and R12C CRYAA were examined by western blotting and immunofluorescence, respectively. Heat-shock response was monitored by quantitative polymerase chain reaction (qPCR) of heat-shock proteins 70 and 90α (HSP70 and HSP90α). RESULTS: The five affected family members showed variable lens opacities and microcornea. Clinical features of cataract were asymmetric in two eyes of some affected subjects. A heterozygous missense substitution, c.34C>T, in CRYAA, which is responsible for the R12C amino acid change, segregated with autosomal dominant cataract (ADCC) in this family. This substitution was absent in 103 unrelated controls. When expressed in COS-7 cells, the R12C mutant CRYAA resembled the wild type protein in its solubility when extracted with 0.5% Triton X-100 and with its cytoplasmic localization. However, mutant cells exhibited an altered heat-shock response, evidenced by the delayed expression of HSP70, when compared to cells expressing wild type CRYAA. CONCLUSIONS: The R12C mutation in CRYAA was responsible for a variable type of inherited cataract associated with microcornea in this Chinese family. The altered heat-shock response of mutant cells suggested a change of chaperoning capacity and networking, which could be associated with the pathogenesis of hereditary cataract-microcornea syndrome. Molecular Vision 2009-06-04 /pmc/articles/PMC2690964/ /pubmed/19503744 Text en http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Zhang, Li-Yun
Yam, Gary Hin-Fai
Tam, Pancy Oi-Sin
Lai, Ricky Yiu-Kwong
Lam, Dennis Shun-Chiu
Pang, Chi-Pui
Fan, Dorothy Shu-Ping
An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title_full An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title_fullStr An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title_full_unstemmed An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title_short An αA-crystallin gene mutation, Arg12Cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
title_sort αa-crystallin gene mutation, arg12cys, causing inherited cataract-microcornea exhibits an altered heat-shock response
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2690964/
https://www.ncbi.nlm.nih.gov/pubmed/19503744
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