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fMRI BOLD Turnover (TBOLD) as a proxy for neuroinflammation.

Created on 22 Jun 2026

Authors

Peka Christova, Lisa M James, Apostolos P Georgopoulos

Published in

Journal of neurophysiology. Jun 21, 2026. Epub Jun 21, 2026.

Abstract

Inflammation is associated with detrimental health outcomes including deleterious effects on the brain. We have recently introduced a new measure of brain function reflecting the moment-to-moment change, or turnover, in the resting state blood oxygen level dependent (BOLD) signal, or TBOLD. In previous studies, increase of TBOLD with age was found to be associated with concomitant decrease in brain volume, whereas both changes were absent in individuals carrying the neuroprotective Human Leukocyte Antigen (HLA) allele DRB1*13:02. Given that TBOLD reflects neurovascular coupling and that neuroinflammation is involved in brain aging, we hypothesized that TBOLD could reflect neuroinflammation. Here, we tested this hypothesis by assessing the association of TBOLD with known inflammatory markers in a large sample of 1390 healthy participants from the Human Connectome Project on Aging/Aging Adult Brain Connectome (AABC). We found a highly significant, positive association between TBOLD and the inflammatory marker C reactive protein (CRP). Furthermore, we found a highly significant association between TBOLD and interleukin 6 (IL-6) in a smaller group of 97 participants for whom IL-6 measurements were available. These findings document significant positive associations of TBOD to systemic inflammatory markers, lending support to hypothesis that TBOLD may serve as a proxy for neuroinflammation.

PMID:
42324453
Bibliographic data and abstract were imported from PubMed on 22 Jun 2026.

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