White matter damage due to vascular, tau, and TDP-43 pathologies and its relevance to cognition

Sheelakumari Raghavan,David T Jones,Robert I Reid,Hugo Botha,Mary M Machulda,Val J Lowe,Ronald C Petersen,Clifford R Jack,Melissa E Murray,Jonathan Graff‐Radford ,Jennifer L Whitwell,Scott A Przybelski,R Ross Reichard,Billie J Matchett,Michelle M Mielke,Kejal Kantarci,David S Knopman,Keith A Josephs,Timothy G Lesnick,Vijay K Ramanan,Prashanthi Vemuri

doi:10.1186/s40478-022-01319-6

Sheelakumari Raghavan, David T Jones + Show 19 more

Open Access

https://doi.org/10.1186/s40478-022-01319-6

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Abstract

Multi-compartment modelling of white matter microstructure using Neurite Orientation Dispersion and Density Imaging (NODDI) can provide information on white matter health through neurite density index and free water measures. We hypothesized that cerebrovascular disease, Alzheimer’s disease, and TDP-43 proteinopathy would be associated with distinct NODDI readouts of white matter damage which would be informative for identifying the substrate for cognitive impairment. We identified two independent cohorts with multi-shell diffusion MRI, amyloid and tau PET, and cognitive assessments: specifically, a population-based cohort of 347 elderly randomly sampled from the Olmsted county, Minnesota, population and a clinical research-based cohort of 61 amyloid positive Alzheimer’s dementia participants. We observed an increase in free water and decrease in neurite density using NODDI measures in the genu of the corpus callosum associated with vascular risk factors, which we refer to as the vascular white matter component. Tau PET signal reflective of 3R/4R tau deposition was associated with worsening neurite density index in the temporal white matter where we measured parahippocampal cingulum and inferior temporal white matter bundles. Worsening temporal white matter neurite density was associated with (antemortem confirmed) FDG TDP-43 signature. Post-mortem neuropathologic data on a small subset of this sample lend support to our findings. In the community-dwelling cohort where vascular disease was more prevalent, the NODDI vascular white matter component explained variability in global cognition (partial R2 of free water and neurite density = 8.3%) and MMSE performance (8.2%) which was comparable to amyloid PET (7.4% for global cognition and 6.6% for memory). In the AD dementia cohort, tau deposition was the greatest contributor to cognitive performance (9.6%), but there was also a non-trivial contribution of the temporal white matter component (8.5%) to cognitive performance. The differences observed between the two cohorts were reflective of their distinct clinical composition. White matter microstructural damage assessed using advanced diffusion models may add significant value for distinguishing the underlying substrate (whether cerebrovascular disease versus neurodegenerative disease caused by tau deposition or TDP-43 pathology) for cognitive impairment in older adults.Graphical abstract

Highlights

The prevalence of neurodegenerative pathologies and cerebrovascular disease (CVD) increases with age [1]
Alzheimer’s disease (AD) and CVD are the major contributors of cognitive decline in the elderly and are widely studied, evidence suggests the co-occurrence of medial temporal lobe (MTL) changes are caused by the TAR DNA binding protein of 43 kDa (TDP-43) [2,3,4], recently referred to as limbic-predominant agerelated TDP-43 encephalopathy (LATE) [5]
Neurite Orientation Dispersion and Density Imaging (NODDI) measurements were associated with vascular risk factors, amyloid, tau, and TDP‐43 As explained in the introduction, the present study confirmed the relevance of Genu white matter (WM) changes to cerebrovascular health

Summary

Introduction

The prevalence of neurodegenerative pathologies and cerebrovascular disease (CVD) increases with age [1]. Alzheimer’s disease (AD) and CVD are the major contributors of cognitive decline in the elderly and are widely studied, evidence suggests the co-occurrence of medial temporal lobe (MTL) changes are caused by the TAR DNA binding protein of 43 kDa (TDP-43) [2,3,4], recently referred to as limbic-predominant agerelated TDP-43 encephalopathy (LATE) [5]. Our studies have shown that frontal fibers are more vulnerable to age-related and CVD related changes [6, 10] and that the measurement of diffusion properties in the genu of the corpus callosum (we refer to this tract as “Genu”) captures WM damage primarily characterized by aging and CVD. The inferior temporal lobe tau which is affected in Braak stages III-IV; has high tau burden along the AD continuum [17]

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