Bi-directional and shared epigenomic signatures following proton and 56Fe irradiation

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作者
Soren Impey
Timothy Jopson
Carl Pelz
Amanuel Tafessu
Fatema Fareh
Damian Zuloaga
Tessa Marzulla
Lara-Kirstie Riparip
Blair Stewart
Susanna Rosi
Mitchell S. Turker
Jacob Raber
机构
[1] Oregon Health and Science University,Oregon Stem Cell Center and Department of Pediatrics
[2] Oregon Health and Science University,Department of Cell and Developmental Biology
[3] Departments of Neurological Surgery and Physical Therapy and Rehabilitation Science,Brain and Spinal Injury Center
[4] University of California,Department of Behavioral Neuroscience
[5] San Francisco,Oregon Institute of Occupational Health Sciences and Department of Molecular and Medical Genetics
[6] Oregon Health and Science University,Departments of Neurology and Radiation Medicine
[7] Oregon Health and Science University,undefined
[8] Division of Neuroscience ONPRC,undefined
[9] Oregon Health and Science University,undefined
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摘要
The brain’s response to radiation exposure is an important concern for patients undergoing cancer therapy and astronauts on long missions in deep space. We assessed whether this response is specific and prolonged and is linked to epigenetic mechanisms. We focused on the response of the hippocampus at early (2-weeks) and late (20-week) time points following whole body proton irradiation. We examined two forms of DNA methylation, cytosine methylation (5mC) and hydroxymethylation (5hmC). Impairments in object recognition, spatial memory retention, and network stability following proton irradiation were observed at the two-week time point and correlated with altered gene expression and 5hmC profiles that mapped to specific gene ontology pathways. Significant overlap was observed between DNA methylation changes at the 2 and 20-week time points demonstrating specificity and retention of changes in response to radiation. Moreover, a novel class of DNA methylation change was observed following an environmental challenge (i.e. space irradiation), characterized by both increased and decreased 5hmC levels along the entire gene body. These changes were mapped to genes encoding neuronal functions including postsynaptic gene ontology categories. Thus, the brain’s response to proton irradiation is both specific and prolonged and involves novel remodeling of non-random regions of the epigenome.
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