Quantitative susceptibility mapping in the brain reflects spatial expression of genes involved in iron homeostasis and myelination

Author:

Cohen Zoe1ORCID,Lau Laurance1,Ahmed Maruf1,Jack Clifford R.2,Liu Chunlei13

Affiliation:

1. Department of Electrical Engineering and Computer Sciences University of California, Berkeley Berkeley California USA

2. Mayo Foundation for Medical Education and Research Rochester Minnesota USA

3. Helen Wills Neuroscience Institute University of California, Berkeley Berkeley California USA

Abstract

AbstractQuantitative susceptibility mapping (QSM) is an MRI modality used to non‐invasively measure iron content in the brain. Iron exhibits a specific anatomically varying pattern of accumulation in the brain across individuals. The highest regions of accumulation are the deep grey nuclei, where iron is stored in paramagnetic molecule ferritin. This form of iron is considered to be what largely contributes to the signal measured by QSM in the deep grey nuclei. It is also known that QSM is affected by diamagnetic myelin contents. Here, we investigate spatial gene expression of iron and myelin related genes, as measured by the Allen Human Brain Atlas, in relation to QSM images of age‐matched subjects. We performed multiple linear regressions between gene expression and the average QSM signal within 34 distinct deep grey nuclei regions. Our results show a positive correlation (p < .05, corrected) between expression of ferritin and the QSM signal in deep grey nuclei regions. We repeated the analysis for other genes that encode proteins thought to be involved in the transport and storage of iron in the brain, as well as myelination. In addition to ferritin, our findings demonstrate a positive correlation (p < .05, corrected) between the expression of ferroportin, transferrin, divalent metal transporter 1, several gene markers of myelinating oligodendrocytes, and the QSM signal in deep grey nuclei regions. Our results suggest that the QSM signal reflects both the storage and active transport of iron in the deep grey nuclei regions of the brain.

Funder

Alzheimer's Drug Discovery Foundation

National Institutes of Health

Publisher

Wiley

Reference108 articles.

1. Allen Human Brain Atlas Technical White Paper: Case Qualification and Donor Profiles. (2013).https://help.brain-map.org/display/humanbrain/Documentation

2. Allen Human Brain Atlas Technical White Paper: Microarray Survey. (2013).https://help.brain-map.org/display/humanbrain/Documentation

3. Allen Institute for Brain Science. (2010).Allen Human Brain Atlas: Microarray [dataset].human.brain-map.org

4. A practical guide to linking brain-wide gene expression and neuroimaging data

5. Ferritin, iron homeostasis, and oxidative damage1,2 1Guest Editor: Mario Comporti 2This article is part of a series of reviews on “Iron and Cellular Redox Status.” The full list of papers may be found on the homepage of the journal.

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