Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease

Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease

Abstract The maintenance of genomic integrity is essential for normal cellular functions. However, it is difficult to maintain over a lifetime in postmitotic cells such as neurons, in which DNA damage increases with age and is exacerbated by multiple neurological disorders, including Alzheimer’s dis...

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Main Authors: Niraj M. Shanbhag, Mark D. Evans, Wenjie Mao, Alissa L. Nana, William W. Seeley, Anthony Adame, Robert A. Rissman, Eliezer Masliah, Lennart Mucke
Format: Article
Language:English
Published: BMC 2019-05-01
Series:Acta Neuropathologica Communications
Subjects:
Alzheimer’s disease
Astrocytes
DNA damage
53BP1
γH2AX
Neurons
Online Access:http://link.springer.com/article/10.1186/s40478-019-0723-5
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spelling doaj-33b1ec13cbdc43688c297b151953f6c32020-11-25T02:26:54ZengBMCActa Neuropathologica Communications2051-59602019-05-017111810.1186/s40478-019-0723-5Early neuronal accumulation of DNA double strand breaks in Alzheimer’s diseaseNiraj M. Shanbhag0Mark D. Evans1Wenjie Mao2Alissa L. Nana3William W. Seeley4Anthony Adame5Robert A. Rissman6Eliezer Masliah7Lennart Mucke8Gladstone Institute of Neurological DiseaseGladstone Institute of Neurological DiseaseGladstone Institute of Neurological DiseaseMemory and Aging Center, Department of Neurology, University of California San FranciscoMemory and Aging Center, Department of Neurology, University of California San FranciscoDepartment of Neurosciences, University of California at San DiegoDepartment of Neurosciences, University of California at San DiegoDepartment of Neurosciences, University of California at San DiegoGladstone Institute of Neurological DiseaseAbstract The maintenance of genomic integrity is essential for normal cellular functions. However, it is difficult to maintain over a lifetime in postmitotic cells such as neurons, in which DNA damage increases with age and is exacerbated by multiple neurological disorders, including Alzheimer’s disease (AD). Here we used immunohistochemical staining to detect DNA double strand breaks (DSBs), the most severe form of DNA damage, in postmortem brain tissues from patients with mild cognitive impairment (MCI) or AD and from cognitively unimpaired controls. Immunostaining for γH2AX—a post-translational histone modification that is widely used as a marker of DSBs—revealed increased proportions of γH2AX-labeled neurons and astrocytes in the hippocampus and frontal cortex of MCI and AD patients, as compared to age-matched controls. In contrast to the focal pattern associated with DSBs, some neurons and glia in humans and mice showed diffuse pan-nuclear patterns of γH2AX immunoreactivity. In mouse brains and primary neuronal cultures, such pan-nuclear γH2AX labeling could be elicited by increasing neuronal activity. To assess whether pan-nuclear γH2AX represents DSBs, we used a recently developed technology, DNA damage in situ ligation followed by proximity ligation assay, to detect close associations between γH2AX sites and free DSB ends. This assay revealed no evidence of DSBs in neurons or astrocytes with prominent pan-nuclear γH2AX labeling. These findings suggest that focal, but not pan-nuclear, increases in γH2AX immunoreactivity are associated with DSBs in brain tissue and that these distinct patterns of γH2AX formation may have different causes and consequences. We conclude that AD is associated with an accumulation of DSBs in vulnerable neuronal and glial cell populations from early stages onward. Because of the severe adverse effects this type of DNA damage can have on gene expression, chromatin stability and cellular functions, DSBs could be an important causal driver of neurodegeneration and cognitive decline in this disease.http://link.springer.com/article/10.1186/s40478-019-0723-5Alzheimer’s diseaseAstrocytesDNA damage53BP1γH2AXNeurons
collection DOAJ
language English
format Article
sources DOAJ
author Niraj M. Shanbhag
Mark D. Evans
Wenjie Mao
Alissa L. Nana
William W. Seeley
Anthony Adame
Robert A. Rissman
Eliezer Masliah
Lennart Mucke
spellingShingle Niraj M. Shanbhag
Mark D. Evans
Wenjie Mao
Alissa L. Nana
William W. Seeley
Anthony Adame
Robert A. Rissman
Eliezer Masliah
Lennart Mucke
Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
Acta Neuropathologica Communications
Alzheimer’s disease
Astrocytes
DNA damage
53BP1
γH2AX
Neurons
author_facet Niraj M. Shanbhag
Mark D. Evans
Wenjie Mao
Alissa L. Nana
William W. Seeley
Anthony Adame
Robert A. Rissman
Eliezer Masliah
Lennart Mucke
author_sort Niraj M. Shanbhag
title Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
title_short Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
title_full Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
title_fullStr Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
title_full_unstemmed Early neuronal accumulation of DNA double strand breaks in Alzheimer’s disease
title_sort early neuronal accumulation of dna double strand breaks in alzheimer’s disease
publisher BMC
series Acta Neuropathologica Communications
issn 2051-5960
publishDate 2019-05-01
description Abstract The maintenance of genomic integrity is essential for normal cellular functions. However, it is difficult to maintain over a lifetime in postmitotic cells such as neurons, in which DNA damage increases with age and is exacerbated by multiple neurological disorders, including Alzheimer’s disease (AD). Here we used immunohistochemical staining to detect DNA double strand breaks (DSBs), the most severe form of DNA damage, in postmortem brain tissues from patients with mild cognitive impairment (MCI) or AD and from cognitively unimpaired controls. Immunostaining for γH2AX—a post-translational histone modification that is widely used as a marker of DSBs—revealed increased proportions of γH2AX-labeled neurons and astrocytes in the hippocampus and frontal cortex of MCI and AD patients, as compared to age-matched controls. In contrast to the focal pattern associated with DSBs, some neurons and glia in humans and mice showed diffuse pan-nuclear patterns of γH2AX immunoreactivity. In mouse brains and primary neuronal cultures, such pan-nuclear γH2AX labeling could be elicited by increasing neuronal activity. To assess whether pan-nuclear γH2AX represents DSBs, we used a recently developed technology, DNA damage in situ ligation followed by proximity ligation assay, to detect close associations between γH2AX sites and free DSB ends. This assay revealed no evidence of DSBs in neurons or astrocytes with prominent pan-nuclear γH2AX labeling. These findings suggest that focal, but not pan-nuclear, increases in γH2AX immunoreactivity are associated with DSBs in brain tissue and that these distinct patterns of γH2AX formation may have different causes and consequences. We conclude that AD is associated with an accumulation of DSBs in vulnerable neuronal and glial cell populations from early stages onward. Because of the severe adverse effects this type of DNA damage can have on gene expression, chromatin stability and cellular functions, DSBs could be an important causal driver of neurodegeneration and cognitive decline in this disease.
topic Alzheimer’s disease
Astrocytes
DNA damage
53BP1
γH2AX
Neurons
url http://link.springer.com/article/10.1186/s40478-019-0723-5
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