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. 2007 May 15;36(1):64-8.
doi: 10.1016/j.neuroimage.2007.02.039. Epub 2007 Mar 6.

The effects of brain tissue decomposition on diffusion tensor imaging and tractography

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The effects of brain tissue decomposition on diffusion tensor imaging and tractography

Helen D'Arceuil et al. Neuroimage. .

Abstract

There have been numerous high resolution diffusion tensor imaging studies in fixed animal brains, but relatively few studies in human brains. While animal tissues are generally fixed pre-mortem or directly postmortem, this is not possible for human tissue, therefore there is always some delay between death and tissue fixation. The elapsed time between death and tissue fixation, the postmortem interval (PMI), will most likely adversely affect the tissue's diffusion properties. We studied the effects of PMI on the diffusion properties of rodent brain. Eight mice were euthanized and the brains (kept in the skull) were placed in formalin at PMIs of 0, 1, 4 and 14 days. Post fixation they were placed in a solution of GdDTPA and phosphate buffered saline. Brains were scanned with a 3D EPI DTI sequence at 4.7T. DTI data were processed to generate apparent diffusion coefficient (ADC) and fractional anisotropy (FA) maps. DTI tractography was also performed. The temporal changes in regional ADC and FA values were analyzed statistically using a one-way ANOVA, followed by individual Student's T-tests. Regional FA and ADC of gray and white matter decreased significantly with time (p<0.05). DTI tractography showed a decrease in the number and coherence of reconstructed fiber pathways between PMIs 0 and 14. Elapsed time between death and tissue fixation has a major effect upon the brain's diffusion properties and should be born in mind when interpreting fixed brain DTI.

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Figures

Fig. 1
Fig. 1
FA (A) and ADC (B) variation in gray (frontal cortex, basal ganglia and hippocampus) and white matter (corpus callosum genu and fimbria) with increasing postmortem interval (PMI). Eigenvalues (absolute value) in white (C) and gray (D) matter decreased with increasing PMI. Error bars are the standard deviation of the measurement.
Fig. 2
Fig. 2
(A) DTI tractography at PMI 0, shows many fibers originating from all aspects of the corpus callosum in contrast to (B) at PMI 14, which shows severely depleted fiber anatomy in all aspects of the corpus callosum (genu, splenium and body), but in particular the body. (C) shows the change in mean fiber density and length for fibers passing through the corpus callosum: ‘*’ indicates a significant difference from PMI 0.

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