4.4 Article

Developmental and regional dependence of macromolecular proton fraction and fractional anisotropy in fixed brain tissue

Journal

NMR IN BIOMEDICINE
Volume 36, Issue 7, Pages -

Publisher

WILEY
DOI: 10.1002/nbm.4915

Keywords

formalin fixation; fractional anisotropy; macromolecular proton fraction; myelin

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Imaging fixed tissue offers improved signal-to-noise ratio and resolution, however, the accuracy of quantitative MRI parameters in fixed brain tissue needs validation. This study compares MR-derived markers of brain development, MPF and FA, between in vivo and fixed tissue measures. The results suggest that MPF can be used as a proxy for in vivo measurements, but its bias needs to be corrected.
An important advantage of imaging fixed tissue is a gain in signal-to-noise ratio and in resolution due to unlimited scan time. However, the fidelity of quantitative MRI parameters in fixed brain tissue, particularly in developmental settings, requires validation. Macromolecular proton fraction (MPF) and fractional anisotropy (FA) indices are quantitative markers of myelination and axonal integrity relevant to preclinical and clinical research. The goal of this study was to assert the correspondence of MR-derived markers of brain development MPF and FA between in vivo and fixed tissue measures. MPF and FA were compared in several white and gray matter structures of the normal mouse brain at 2, 4, and 12 weeks of age. At each developmental stage, in vivo imaging was performed, followed by paraformaldehyde fixation and a second imaging session. MPF maps were acquired from three source images (magnetization transfer weighted, proton density weighted, and T-1 weighted), and FA was obtained from diffusion tensor imaging. The MPF and FA values, measured in the cortex, striatum, and major fiber tracts, were compared before and after fixation using Bland-Altman plots, regression analysis, and analysis of variance. MPF values of the fixed tissue were consistently greater than those from in vivo measurements. Importantly, this bias varied significantly with brain region and the developmental stage of the tissue. At the same time, FA values were preserved after fixation, across tissue types and developmental stages. The results of this study suggest that MPF and FA in fixed brain tissue can be used as a proxy for in vivo measurements, but additional considerations should be made to correct for the bias in MPF.

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