Literature DB >> 23263697

Alterations in brain structure and function in breast cancer survivors: effect of post-chemotherapy interval and relation to oxidative DNA damage.

Susan K Conroy1, Brenna C McDonald, Dori J Smith, Lyndsi R Moser, John D West, Lisa M Kamendulis, James E Klaunig, Victoria L Champion, Frederick W Unverzagt, Andrew J Saykin.   

Abstract

Neuroimaging studies have begun to uncover the neural substrates of cancer and treatment-related cognitive dysfunction, but the time course of these changes in the years following chemotherapy is unclear. This study analyzed multimodality 3T MRI scans to examine the structural and functional effects of chemotherapy and post-chemotherapy interval (PCI) in a cohort of breast cancer survivors (BCS; n = 24; PCI mean 6, range 3-10 y) relative to age- and education-matched healthy controls (HC; n = 23). Assessments included voxel-based morphometry for gray matter density (GMD) and fMRI for activation profile during a 3-back working memory task. The relationships between brain regions associated with PCI and neuropsychological performance, self-reported cognition, and oxidative and direct DNA damage as measured in peripheral lymphocytes were assessed in secondary analyses. PCI was positively associated with GMD and activation on fMRI in the right anterior frontal region (Brodmann Areas 9 and 10) independent of participant age. GMD in this region was also positively correlated with global neuropsychological function. Memory dysfunction, cognitive complaints, and oxidative DNA damages were increased in BCS compared with HC. Imaging results indicated lower fMRI activation in several regions in the BCS group. BCS also had lower GMD than HC in several regions, and in these regions, GMD was inversely related to oxidative DNA damage and learning and memory neuropsychological domain scores. This is the first study to show structural and functional effects of PCI and to relate oxidative DNA damage to brain alterations in BCS. The relationship between neuroimaging and cognitive function indicates the potential clinical relevance of these findings. The relationship with oxidative DNA damage provides a mechanistic clue warranting further investigation.

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Year:  2012        PMID: 23263697      PMCID: PMC3543695          DOI: 10.1007/s10549-012-2385-x

Source DB:  PubMed          Journal:  Breast Cancer Res Treat        ISSN: 0167-6806            Impact factor:   4.872


  44 in total

1.  Alterations in brain activation during working memory processing associated with breast cancer and treatment: a prospective functional magnetic resonance imaging study.

Authors:  Brenna C McDonald; Susan K Conroy; Tim A Ahles; John D West; Andrew J Saykin
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2.  A metaanalysis of studies of the effects of cancer chemotherapy on various domains of cognitive function.

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Review 7.  Meta-analysis of cognitive functioning in breast cancer survivors previously treated with standard-dose chemotherapy.

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8.  Acrylonitrile-induced oxidative stress and oxidative DNA damage in male Sprague-Dawley rats.

Authors:  Xinzhu Pu; Lisa M Kamendulis; James E Klaunig
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  64 in total

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Review 2.  Cognitive effects of cancer systemic therapy: implications for the care of older patients and survivors.

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Review 3.  Default mode network as a potential biomarker of chemotherapy-related brain injury.

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6.  Peroxisomes contribute to oxidative stress in neurons during doxorubicin-based chemotherapy.

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7.  Neuroimaging biomarkers and cognitive function in non-CNS cancer and its treatment: current status and recommendations for future research.

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8.  Systematic review of self-reported cognitive function in cancer patients following chemotherapy treatment.

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Review 9.  Clinical characteristics, pathophysiology, and management of noncentral nervous system cancer-related cognitive impairment in adults.

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Review 10.  The 2013 SFRBM discovery award: selected discoveries from the butterfield laboratory of oxidative stress and its sequela in brain in cognitive disorders exemplified by Alzheimer disease and chemotherapy induced cognitive impairment.

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Journal:  Free Radic Biol Med       Date:  2014-07-01       Impact factor: 7.376

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