Diffusion MRS tracks distinct trajectories of neuronal development in the cerebellum and thalamus of rat neonates

Author:

Ligneul Clémence1ORCID,Qiu Lily1ORCID,Clarke William T1ORCID,Jbabdi Saad1ORCID,Palombo Marco23ORCID,Lerch Jason P.145

Affiliation:

1. Wellcome Centre for Integrative Neuroimaging, FMRIB, Nuffield Department of Clinical Neurosciences, University of Oxford

2. Cardiff University Brain Research Imaging Centre (CUBRIC), School of Psychology, Cardiff University

3. School of Computer Science and Informatics, Cardiff University

4. Mouse Imaging Centre, The Hospital for Sick Children, Toronto, Ontario, Canada

5. Department of Medical Biophysics, University of Toronto

Abstract

It is currently impossible to non-invasively assess cerebellar cell structure during early development. Here we propose a novel approach to non-invasively and longitudinally track cell-specific development using diffusion-weighted magnetic resonance spectroscopy in combination with microstructural modelling. Tracking metabolite diffusion allows us to probe cell-specific developmental trajectories in the cerebellum and thalamus of healthy rat neonates from post-natal day (P) 5 to P30. Additionally, by comparing different analytical and biophysical microstructural models we can follow the differential contribution of cell bodies and neurites during development. The thalamus serves as a control region to assess the sensitivity of our method to microstructural differences between the regions. We found significant differences between cerebellar and thalamic metabolites diffusion properties. For most metabolites, the signal attenuation is stronger in the thalamus, suggesting less restricted diffusion compared to the cerebellum. There is also a trend for lower signal attenuation and lower ADCs with increasing age, suggesting increasing restriction of metabolite diffusion. This is particularly striking for taurine in the thalamus. We use biophysical modelling to interpret these differences. We report a decreased sphere fraction (or an increased neurite fraction) with age for taurine and total creatine in the cerebellum, marking dendritic growth. Surprisingly, we also report a U-shape trend for segment length (the distance between two embranchments in a dendritic tree) in the cerebellum agreeing with age-matching morphometry of openly available 3D-Purkinje reconstructions. Results demonstrate that diffusion-weighted MRS probes early cerebellar neuronal development non-invasively.

Publisher

eLife Sciences Publications, Ltd

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5. Differential spatiotemporal development of Purkinje cell populations and cerebellum-dependent sensorimotor behaviors;Elife,2021

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