Accelerated brain aging in chronic low back pain

Accelerated brain aging in chronic low back pain

•Chronic low back pain was associated with greater brain age over chronological age.•Discrepancies between groups for brain age were greatest at older ages.•Individuals with chronic low back pain had lower cerebellar gray matter density.•Higher brain age was linked with a widespread pattern of lower...

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Veröffentlicht in:Brain research 2021-03, Vol.1755, p.147263-147263, Article 147263
Hauptverfasser: Yu, Gary Z., Ly, Maria, Karim, Helmet T., Muppidi, Nishita, Aizenstein, Howard J., Ibinson, James W.
Format: Artikel
Sprache:eng
Schlagworte:
Aging
Aging - physiology
Cerebral Cortex - physiopathology
Chronic low back pain
Chronic Pain - physiopathology
Cognition - physiology
Gray Matter - physiopathology
Humans
Life Sciences & Biomedicine
Low Back Pain - physiopathology
Machine learning
Magnetic Resonance Imaging - methods
Neurosciences
Neurosciences & Neurology
Pain Measurement
Science & Technology
Structural neuroimaging
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Zusammenfassung:•Chronic low back pain was associated with greater brain age over chronological age.•Discrepancies between groups for brain age were greatest at older ages.•Individuals with chronic low back pain had lower cerebellar gray matter density.•Higher brain age was linked with a widespread pattern of lower gray matter density.•Brain age may serve as an aggregate measure of holistic gray matter changes. Chronic low back pain (CLBP) is a leading cause of disability and is associated with neurodegenerative changes in brain structure. These changes lead to impairments in cognitive function and are consistent with those seen in aging, suggesting an accelerated aging pattern. In this study we assessed this using machine-learning estimated brain age (BA) as a holistic metric of morphometric changes associated with aging. Structural imaging data from 31 non-depressed CLBP patients and 32 healthy controls from the Pain and Interoception Imaging Network were included. Using our previously developed algorithm, we estimated BA per individual based on grey matter density. We then conducted multivariable linear modeling for effects of group, chronological age, and their interaction on BA. We also performed two voxel-wise analyses comparing grey matter density between CLBP and control individuals and the association between gray matter density and BA. There was an interaction between CLBP and greater chronological age on BA such that the discrepancy in BA between healthy and CLBP individuals was greater for older individuals. In CLBP individuals, BA was not associated with sex, current level of pain, duration of CLBP, or mild to moderate depressive symptoms. CLBP individuals had lower cerebellar grey matter density compared to healthy individuals. Brain age was associated with lower gray matter density in numerous brain regions. CLBP was associated with greater BA, which was more profound in later life. BA as a holistic metric was sensitive to differences in gray matter density in numerous regions which eluded direct comparison between groups.
ISSN:0006-8993
1872-6240
DOI:10.1016/j.brainres.2020.147263