Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology

Neuronal degeneration is a hallmark of many DNA repair syndromes. Yet, how DNA damage causes neuronal degeneration and whether defects in different repair systems affect the brain differently is largely unknown. Here, we performed a systematic detailed analysis of neurodegenerative changes in mouse...

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Autores principales: Jaarsma, Dick, van der Pluijm, Ingrid, de Waard, Monique C., Haasdijk, Elize D., Brandt, Renata, Vermeij, Marcel, Rijksen, Yvonne, Maas, Alex, van Steeg, Harry, Hoeijmakers, Jan H. J., van der Horst, Gijsbertus T. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3234220/
https://www.ncbi.nlm.nih.gov/pubmed/22174697
http://dx.doi.org/10.1371/journal.pgen.1002405
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author Jaarsma, Dick
van der Pluijm, Ingrid
de Waard, Monique C.
Haasdijk, Elize D.
Brandt, Renata
Vermeij, Marcel
Rijksen, Yvonne
Maas, Alex
van Steeg, Harry
Hoeijmakers, Jan H. J.
van der Horst, Gijsbertus T. J.
author_facet Jaarsma, Dick
van der Pluijm, Ingrid
de Waard, Monique C.
Haasdijk, Elize D.
Brandt, Renata
Vermeij, Marcel
Rijksen, Yvonne
Maas, Alex
van Steeg, Harry
Hoeijmakers, Jan H. J.
van der Horst, Gijsbertus T. J.
author_sort Jaarsma, Dick
collection PubMed
description Neuronal degeneration is a hallmark of many DNA repair syndromes. Yet, how DNA damage causes neuronal degeneration and whether defects in different repair systems affect the brain differently is largely unknown. Here, we performed a systematic detailed analysis of neurodegenerative changes in mouse models deficient in nucleotide excision repair (NER) and transcription-coupled repair (TCR), two partially overlapping DNA repair systems that remove helix-distorting and transcription-blocking lesions, respectively, and that are associated with the UV-sensitive syndromes xeroderma pigmentosum (XP) and Cockayne syndrome (CS). TCR–deficient Csa(−/−) and Csb(−/−) CS mice showed activated microglia cells surrounding oligodendrocytes in regions with myelinated axons throughout the nervous system. This white matter microglia activation was not observed in NER–deficient Xpa(−/−) and Xpc(−/−) XP mice, but also occurred in Xpd(XPCS) mice carrying a point mutation (G602D) in the Xpd gene that is associated with a combined XPCS disorder and causes a partial NER and TCR defect. The white matter abnormalities in TCR–deficient mice are compatible with focal dysmyelination in CS patients. Both TCR–deficient and NER–deficient mice showed no evidence for neuronal degeneration apart from p53 activation in sporadic (Csa(−/−), Csb(−/−)) or highly sporadic (Xpa(−/−), Xpc(−/−)) neurons and astrocytes. To examine to what extent overlap occurs between both repair systems, we generated TCR–deficient mice with selective inactivation of NER in postnatal neurons. These mice develop dramatic age-related cumulative neuronal loss indicating DNA damage substrate overlap and synergism between TCR and NER pathways in neurons, and they uncover the occurrence of spontaneous DNA injury that may trigger neuronal degeneration. We propose that, while Csa(−/−) and Csb(−/−) TCR–deficient mice represent powerful animal models to study the mechanisms underlying myelin abnormalities in CS, neuron-specific inactivation of NER in TCR–deficient mice represents a valuable model for the role of NER in neuronal maintenance and survival.
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spelling pubmed-32342202011-12-15 Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology Jaarsma, Dick van der Pluijm, Ingrid de Waard, Monique C. Haasdijk, Elize D. Brandt, Renata Vermeij, Marcel Rijksen, Yvonne Maas, Alex van Steeg, Harry Hoeijmakers, Jan H. J. van der Horst, Gijsbertus T. J. PLoS Genet Research Article Neuronal degeneration is a hallmark of many DNA repair syndromes. Yet, how DNA damage causes neuronal degeneration and whether defects in different repair systems affect the brain differently is largely unknown. Here, we performed a systematic detailed analysis of neurodegenerative changes in mouse models deficient in nucleotide excision repair (NER) and transcription-coupled repair (TCR), two partially overlapping DNA repair systems that remove helix-distorting and transcription-blocking lesions, respectively, and that are associated with the UV-sensitive syndromes xeroderma pigmentosum (XP) and Cockayne syndrome (CS). TCR–deficient Csa(−/−) and Csb(−/−) CS mice showed activated microglia cells surrounding oligodendrocytes in regions with myelinated axons throughout the nervous system. This white matter microglia activation was not observed in NER–deficient Xpa(−/−) and Xpc(−/−) XP mice, but also occurred in Xpd(XPCS) mice carrying a point mutation (G602D) in the Xpd gene that is associated with a combined XPCS disorder and causes a partial NER and TCR defect. The white matter abnormalities in TCR–deficient mice are compatible with focal dysmyelination in CS patients. Both TCR–deficient and NER–deficient mice showed no evidence for neuronal degeneration apart from p53 activation in sporadic (Csa(−/−), Csb(−/−)) or highly sporadic (Xpa(−/−), Xpc(−/−)) neurons and astrocytes. To examine to what extent overlap occurs between both repair systems, we generated TCR–deficient mice with selective inactivation of NER in postnatal neurons. These mice develop dramatic age-related cumulative neuronal loss indicating DNA damage substrate overlap and synergism between TCR and NER pathways in neurons, and they uncover the occurrence of spontaneous DNA injury that may trigger neuronal degeneration. We propose that, while Csa(−/−) and Csb(−/−) TCR–deficient mice represent powerful animal models to study the mechanisms underlying myelin abnormalities in CS, neuron-specific inactivation of NER in TCR–deficient mice represents a valuable model for the role of NER in neuronal maintenance and survival. Public Library of Science 2011-12-08 /pmc/articles/PMC3234220/ /pubmed/22174697 http://dx.doi.org/10.1371/journal.pgen.1002405 Text en Jaarsma et al. http://creativecommons.org/licenses/by/4.0/ 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 author and source are properly credited.
spellingShingle Research Article
Jaarsma, Dick
van der Pluijm, Ingrid
de Waard, Monique C.
Haasdijk, Elize D.
Brandt, Renata
Vermeij, Marcel
Rijksen, Yvonne
Maas, Alex
van Steeg, Harry
Hoeijmakers, Jan H. J.
van der Horst, Gijsbertus T. J.
Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title_full Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title_fullStr Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title_full_unstemmed Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title_short Age-Related Neuronal Degeneration: Complementary Roles of Nucleotide Excision Repair and Transcription-Coupled Repair in Preventing Neuropathology
title_sort age-related neuronal degeneration: complementary roles of nucleotide excision repair and transcription-coupled repair in preventing neuropathology
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3234220/
https://www.ncbi.nlm.nih.gov/pubmed/22174697
http://dx.doi.org/10.1371/journal.pgen.1002405
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