Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases

BACKGROUND: The neuronal ceroid lipofuscinoses (NCL) are a group of children's inherited neurodegenerative disorders, characterized by blindness, early dementia and pronounced cortical atrophy. The similar pathological and clinical profiles of the different forms of NCL suggest that common dise...

Descripción completa

Detalles Bibliográficos
Autores principales: von Schantz, Carina, Saharinen, Juha, Kopra, Outi, Cooper, Jonathan D, Gentile, Massimiliano, Hovatta, Iiris, Peltonen, Leena, Jalanko, Anu
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2323392/
https://www.ncbi.nlm.nih.gov/pubmed/18371231
http://dx.doi.org/10.1186/1471-2164-9-146
_version_ 1782152647482015744
author von Schantz, Carina
Saharinen, Juha
Kopra, Outi
Cooper, Jonathan D
Gentile, Massimiliano
Hovatta, Iiris
Peltonen, Leena
Jalanko, Anu
author_facet von Schantz, Carina
Saharinen, Juha
Kopra, Outi
Cooper, Jonathan D
Gentile, Massimiliano
Hovatta, Iiris
Peltonen, Leena
Jalanko, Anu
author_sort von Schantz, Carina
collection PubMed
description BACKGROUND: The neuronal ceroid lipofuscinoses (NCL) are a group of children's inherited neurodegenerative disorders, characterized by blindness, early dementia and pronounced cortical atrophy. The similar pathological and clinical profiles of the different forms of NCL suggest that common disease mechanisms may be involved. To explore the NCL-associated disease pathology and molecular pathways, we have previously produced targeted knock-out mice for Cln1 and Cln5. Both mouse-models replicate the NCL phenotype and neuropathology; the Cln1-/- model presents with early onset, severe neurodegenerative disease, whereas the Cln5-/- model produces a milder disease with a later onset. RESULTS: Here we have performed quantitative gene expression profiling of the cortex from 1 and 4 month old Cln1-/- and Cln5-/- mice. Combined microarray datasets from both mouse models exposed a common affected pathway: genes regulating neuronal growth cone stabilization display similar aberrations in both models. We analyzed locus specific gene expression and showed regional clustering of Cln1 and three major genes of this pathway, further supporting a close functional relationship between the corresponding gene products; adenylate cyclase-associated protein 1 (Cap1), protein tyrosine phosphatase receptor type F (Ptprf) and protein tyrosine phosphatase 4a2 (Ptp4a2). The evidence from the gene expression data, indicating changes in the growth cone assembly, was substantiated by the immunofluorescence staining patterns of Cln1-/- and Cln5-/- cortical neurons. These primary neurons displayed abnormalities in cytoskeleton-associated proteins actin and β-tubulin as well as abnormal intracellular distribution of growth cone associated proteins GAP-43, synapsin and Rab3. CONCLUSION: Our data provide the first evidence for a common molecular pathogenesis behind neuronal degeneration in INCL and vLINCL. Since CLN1 and CLN5 code for proteins with distinct functional roles these data may have implications for other forms of NCLs as well.
format Text
id pubmed-2323392
institution National Center for Biotechnology Information
language English
publishDate 2008
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-23233922008-04-21 Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases von Schantz, Carina Saharinen, Juha Kopra, Outi Cooper, Jonathan D Gentile, Massimiliano Hovatta, Iiris Peltonen, Leena Jalanko, Anu BMC Genomics Research Article BACKGROUND: The neuronal ceroid lipofuscinoses (NCL) are a group of children's inherited neurodegenerative disorders, characterized by blindness, early dementia and pronounced cortical atrophy. The similar pathological and clinical profiles of the different forms of NCL suggest that common disease mechanisms may be involved. To explore the NCL-associated disease pathology and molecular pathways, we have previously produced targeted knock-out mice for Cln1 and Cln5. Both mouse-models replicate the NCL phenotype and neuropathology; the Cln1-/- model presents with early onset, severe neurodegenerative disease, whereas the Cln5-/- model produces a milder disease with a later onset. RESULTS: Here we have performed quantitative gene expression profiling of the cortex from 1 and 4 month old Cln1-/- and Cln5-/- mice. Combined microarray datasets from both mouse models exposed a common affected pathway: genes regulating neuronal growth cone stabilization display similar aberrations in both models. We analyzed locus specific gene expression and showed regional clustering of Cln1 and three major genes of this pathway, further supporting a close functional relationship between the corresponding gene products; adenylate cyclase-associated protein 1 (Cap1), protein tyrosine phosphatase receptor type F (Ptprf) and protein tyrosine phosphatase 4a2 (Ptp4a2). The evidence from the gene expression data, indicating changes in the growth cone assembly, was substantiated by the immunofluorescence staining patterns of Cln1-/- and Cln5-/- cortical neurons. These primary neurons displayed abnormalities in cytoskeleton-associated proteins actin and β-tubulin as well as abnormal intracellular distribution of growth cone associated proteins GAP-43, synapsin and Rab3. CONCLUSION: Our data provide the first evidence for a common molecular pathogenesis behind neuronal degeneration in INCL and vLINCL. Since CLN1 and CLN5 code for proteins with distinct functional roles these data may have implications for other forms of NCLs as well. BioMed Central 2008-03-28 /pmc/articles/PMC2323392/ /pubmed/18371231 http://dx.doi.org/10.1186/1471-2164-9-146 Text en Copyright © 2008 von Schantz et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
von Schantz, Carina
Saharinen, Juha
Kopra, Outi
Cooper, Jonathan D
Gentile, Massimiliano
Hovatta, Iiris
Peltonen, Leena
Jalanko, Anu
Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title_full Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title_fullStr Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title_full_unstemmed Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title_short Brain gene expression profiles of Cln1 and Cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in NCL diseases
title_sort brain gene expression profiles of cln1 and cln5 deficient mice unravels common molecular pathways underlying neuronal degeneration in ncl diseases
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2323392/
https://www.ncbi.nlm.nih.gov/pubmed/18371231
http://dx.doi.org/10.1186/1471-2164-9-146
work_keys_str_mv AT vonschantzcarina braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT saharinenjuha braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT kopraouti braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT cooperjonathand braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT gentilemassimiliano braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT hovattaiiris braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT peltonenleena braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases
AT jalankoanu braingeneexpressionprofilesofcln1andcln5deficientmiceunravelscommonmolecularpathwaysunderlyingneuronaldegenerationinncldiseases

Ejemplares similares