Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation

Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation

In the present study, we prepared a SCA3 animal model by generating transgenic mice expressing polyglutamine-expanded ataxin-3-Q79. Ataxin-3-Q79 was expressed in brain areas implicated in SCA3 neurodegeneration, including cerebellum, pontine nucleus and substantia nigra. Ataxin-3-Q79 transgenic mice...

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Main Authors: An-Hsun Chou, Tu-Hsueh Yeh, Pin Ouyang, Ying-Ling Chen, Si-Ying Chen, Hung-Li Wang
Format: Article
Language:English
Published: Elsevier 2008-07-01
Series:Neurobiology of Disease
Subjects:
Spinocerebellar ataxia type 3
Ataxin-3
Polyglutamine-expanded ataxin-3
SCA3 transgenic mice
Cerebellum
Microarray analysis
Online Access:http://www.sciencedirect.com/science/article/pii/S0969996108000673
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spelling doaj-147b561a68324264a53797da6300a29c2021-03-20T04:55:44ZengElsevierNeurobiology of Disease1095-953X2008-07-0131189101Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulationAn-Hsun Chou0Tu-Hsueh Yeh1Pin Ouyang2Ying-Ling Chen3Si-Ying Chen4Hung-Li Wang5Department of Anesthesiology, Chang Gung Memorial Hospital, Kwei-San, Tao-Yuan, Taiwan, ROC; Graduate Institute of Clinical Medical Science, Chang Gung University School of Medicine, Kwei-San, Tao-Yuan, Taiwan, ROCDepartment of Neurology, Chang Gung Memorial Hospital, Kwei-San, Tao-Yuan, Taiwan, ROCDepartment of Anatomy, Chang Gung University School of Medicine, Kwei-San, Tao-Yuan, Taiwan, ROCDepartment of Physiology, Chang Gung University School of Medicine, Kwei-San, Tao-Yuan, Taiwan, ROC; Chang Gung Institute of Technology, Kwei-San, Tao-Yuan, Taiwan, ROCDepartment of Physiology, Chang Gung University School of Medicine, Kwei-San, Tao-Yuan, Taiwan, ROCDepartment of Physiology, Chang Gung University School of Medicine, Kwei-San, Tao-Yuan, Taiwan, ROC; Corresponding author.In the present study, we prepared a SCA3 animal model by generating transgenic mice expressing polyglutamine-expanded ataxin-3-Q79. Ataxin-3-Q79 was expressed in brain areas implicated in SCA3 neurodegeneration, including cerebellum, pontine nucleus and substantia nigra. Ataxin-3-Q79 transgenic mice displayed motor dysfunction with an onset age of 5–6 months, and neurological symptoms deteriorated in the following months. A prominent neuronal loss was not found in the cerebellum of 10 to 11-month-old ataxin-3-Q79 mice displaying pronounced ataxic symptoms, suggesting that instead of neuronal demise, ataxin-3-Q79 causes neuronal dysfunction of the cerebellum and resulting ataxia. To test the involvement of transcriptional dysregulation in ataxin-3-Q79-induced cerebellar malfunction, microarray analysis and real-time RT-PCR assays were performed to identify altered cerebellar mRNA expressions of ataxin-3-Q79 mice. Compared to non-transgenic mice or mice expressing wild-type ataxin-3-Q22, 10 to 11-month-old ataxin-3-Q79 mice exhibited downregulated mRNA expressions of proteins involved in glutamatergic neurotransmission, intracellular calcium signaling/mobilization or MAP kinase pathways, GABAA/B receptor subunits, heat shock proteins and transcription factor regulating neuronal survival and differentiation. Upregulated expressions of Bax, cyclin D1 and CDK5-p39, which may mediate neuronal death, were also observed in ataxin-3-Q79 transgenic mice. The involvement of transcriptional abnormality in initiating the pathological process of SCA3 was indicated by the finding that 4 to 5-month-old ataxin-3-Q79 mice, which did not display neurological phenotype, exhibited downregulated mRNA levels of genes involved in glutamatergic signaling and signal transduction. Our study suggests that polyglutamine-expanded ataxin-3 causes cerebellar dysfunction and ataxia by disrupting the normal pattern of gene transcriptions.http://www.sciencedirect.com/science/article/pii/S0969996108000673Spinocerebellar ataxia type 3Ataxin-3Polyglutamine-expanded ataxin-3SCA3 transgenic miceCerebellumMicroarray analysis
collection DOAJ
language English
format Article
sources DOAJ
author An-Hsun Chou
Tu-Hsueh Yeh
Pin Ouyang
Ying-Ling Chen
Si-Ying Chen
Hung-Li Wang
spellingShingle An-Hsun Chou
Tu-Hsueh Yeh
Pin Ouyang
Ying-Ling Chen
Si-Ying Chen
Hung-Li Wang
Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
Neurobiology of Disease
Spinocerebellar ataxia type 3
Ataxin-3
Polyglutamine-expanded ataxin-3
SCA3 transgenic mice
Cerebellum
Microarray analysis
author_facet An-Hsun Chou
Tu-Hsueh Yeh
Pin Ouyang
Ying-Ling Chen
Si-Ying Chen
Hung-Li Wang
author_sort An-Hsun Chou
title Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
title_short Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
title_full Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
title_fullStr Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
title_full_unstemmed Polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of SCA3 transgenic mice by inducing transcriptional dysregulation
title_sort polyglutamine-expanded ataxin-3 causes cerebellar dysfunction of sca3 transgenic mice by inducing transcriptional dysregulation
publisher Elsevier
series Neurobiology of Disease
issn 1095-953X
publishDate 2008-07-01
description In the present study, we prepared a SCA3 animal model by generating transgenic mice expressing polyglutamine-expanded ataxin-3-Q79. Ataxin-3-Q79 was expressed in brain areas implicated in SCA3 neurodegeneration, including cerebellum, pontine nucleus and substantia nigra. Ataxin-3-Q79 transgenic mice displayed motor dysfunction with an onset age of 5–6 months, and neurological symptoms deteriorated in the following months. A prominent neuronal loss was not found in the cerebellum of 10 to 11-month-old ataxin-3-Q79 mice displaying pronounced ataxic symptoms, suggesting that instead of neuronal demise, ataxin-3-Q79 causes neuronal dysfunction of the cerebellum and resulting ataxia. To test the involvement of transcriptional dysregulation in ataxin-3-Q79-induced cerebellar malfunction, microarray analysis and real-time RT-PCR assays were performed to identify altered cerebellar mRNA expressions of ataxin-3-Q79 mice. Compared to non-transgenic mice or mice expressing wild-type ataxin-3-Q22, 10 to 11-month-old ataxin-3-Q79 mice exhibited downregulated mRNA expressions of proteins involved in glutamatergic neurotransmission, intracellular calcium signaling/mobilization or MAP kinase pathways, GABAA/B receptor subunits, heat shock proteins and transcription factor regulating neuronal survival and differentiation. Upregulated expressions of Bax, cyclin D1 and CDK5-p39, which may mediate neuronal death, were also observed in ataxin-3-Q79 transgenic mice. The involvement of transcriptional abnormality in initiating the pathological process of SCA3 was indicated by the finding that 4 to 5-month-old ataxin-3-Q79 mice, which did not display neurological phenotype, exhibited downregulated mRNA levels of genes involved in glutamatergic signaling and signal transduction. Our study suggests that polyglutamine-expanded ataxin-3 causes cerebellar dysfunction and ataxia by disrupting the normal pattern of gene transcriptions.
topic Spinocerebellar ataxia type 3
Ataxin-3
Polyglutamine-expanded ataxin-3
SCA3 transgenic mice
Cerebellum
Microarray analysis
url http://www.sciencedirect.com/science/article/pii/S0969996108000673
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