4.7 Article

Myelin and iron concentration in the human brain: A quantitative study of MRI contrast

Journal

NEUROIMAGE
Volume 93, Issue -, Pages 95-106

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.neuroimage.2014.02.026

Keywords

PIXE; Phosphorus; Magnetic susceptibility; Simulations

Funding

  1. COST Action [BM1001]
  2. Alzheimer Forschungsinitiative e.V. (AFI) [11861]
  3. European Union
  4. Free State of Saxony [EU-ESF 100154907]
  5. German Research Foundation (DFG) [MO 2249/2-1, PP 1608, GRK 1097]

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During the last five years ultra-high-field magnetic resonance imaging (MRI) has enabled an unprecedented view of living human brain. Brain tissue contrast in most MRI sequences is known to reflect mainly the spatial distributions of myelin and iron. These distributions have been shown to overlap significantly in many brain regions, especially in the cortex. It is of increasing interest to distinguish and identify cortical areas by their appearance in MRI, which has been shown to be feasible in vivo. Parcellation can benefit greatly from quantification of the independent contributions of iron and myelin to MRI contrast. Recent studies using susceptibility mapping claim to allow such a separation of the effects of myelin and iron in MRI. We show, using post-mortem human brain tissue, that this goal can be achieved. After MRI scanning of the block with appropriate T-1 mapping and T-2* weighted sequences, we section the block and apply a novel technique, proton induced X-ray emission (PIXE), to spatially map iron, phosphorus and sulfur elemental concentrations, simultaneously with 1 mu m spatial resolution. Because most brain phosphorus is located in myelin phospholipids, a calibration step utilizing element maps of sulfur enables semi-quantitative ex vivo mapping of myelin concentration. Combining results for iron and myelin concentration in a linear model, we have accurately modeled MRI tissue contrasts. Conversely, iron and myelin concentrations can now be estimated from appropriate MRI measurements in post-mortem brain samples. (C) 2014 Elsevier Inc. All rights reserved.

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