Frontiers in Human Neuroscience (Apr 2014)

Use of Diffusion Spectrum imaging in preliminary longitudinal evaluation of Amyotrophic Lateral Sclerosis: development of an imaging biomarker

  • Kumar eAbhinav,
  • Fang-Chang eYeh,
  • Ahmed eEl-Dokla,
  • Lisa M. Ferrando,
  • Yue-Fang eChang,
  • David eLacomis,
  • Robert M. Friedlander,
  • Juan C. Fernandez-Miranda

DOI
https://doi.org/10.3389/fnhum.2014.00270
Journal volume & issue
Vol. 8

Abstract

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Previous diffusion tensor imaging (DTI) studies have shown white matter pathology in ALS, predominantly in the motor pathways. Further these studies have shown that DTI can be used longitudinally to track pathology over time, making white matter pathology a candidate as an outcome measure in future trials. DTI has demonstrated application in group studies, however its derived indices, for example fractional anisotropy, are susceptible to partial volume effects, making its role questionable in examining individual progression. We hypothesize that changes in the white matter are present in ALS beyond the motor tracts, and that the affected pathways and associated pattern of disease progression can be tracked longitudinally using automated diffusion connectometry analysis. Connectometry analysis is based on diffusion spectrum imaging (DSI) and overcomes the limitations of a conventional tractography approach and DTI. The identified affected white matter tracts can then be assessed in a targeted fashion using High definition fiber tractography (a novel white matter MR imaging technique). Changes in quantitative and qualitative markers over time could then be correlated with clinical progression.We illustrate these principles towards developing an imaging biomarker for demonstrating individual progression, by presenting results for five ALS patients, including with longitudinal data in two. Preliminary analysis demonstrated a number of changes bilaterally and asymmetrically in motoric and extramotoric white matter pathways. Further the limbic system was also affected possibly explaining the cognitive symptoms in ALS. In the two longitudinal subjects, the white matter changes were less extensive at baseline, although there was evidence of disease progression in a frontal pattern with a relatively spared postcentral gyrus, consistent with the known pathology in ALS.

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