4.6 Article

Altered oligodendroglia and astroglia in chronic traumatic encephalopathy

Journal

ACTA NEUROPATHOLOGICA
Volume 142, Issue 2, Pages 295-321

Publisher

SPRINGER
DOI: 10.1007/s00401-021-02322-2

Keywords

Chronic traumatic encephalopathy; Single-nucleus transcriptomics; White matter; Neurodegeneration; Oligodendrocytes; Astrocytes

Funding

  1. Harvard/MIT Joint Research Grants Program in Basic Neuroscience
  2. Concussion Legacy Foundation Young Investigator Fellowship
  3. National Institute on Aging [AG057902, AG06234]
  4. National Institute of Neurological Disorders and Stroke [U54NS115266, U01NS086659]
  5. National Institute of Aging Boston University Alzheimer's Disease Center [P30AG13846]
  6. Concussion Legacy Foundation
  7. Nick and Lynn Buoniconti Foundation

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This study identified specific molecular and cellular differences in oligodendrocytes and astrocytes in CTE patients, showing that oligodendrocytes are most severely affected with altered proportions across subtype clusters, while transcripts associated with neuroinflammation were elevated in astrocytes from CTE patients.
Chronic traumatic encephalopathy (CTE) is a progressive tauopathy found in contact sport athletes, military veterans, and others exposed to repetitive head impacts. White matter rarefaction and axonal loss have been reported in CTE but have not been characterized on a molecular or cellular level. Here, we present RNA sequencing profiles of cell nuclei from postmortem dorsolateral frontal white matter from eight individuals with neuropathologically confirmed CTE and eight age- and sex-matched controls. Analyzing these profiles using unbiased clustering approaches, we identified eighteen transcriptomically distinct cell groups (clusters), reflecting cell types and/or cell states, of which a subset showed differences between CTE and control tissue. Independent in situ methods applied on tissue sections adjacent to that used in the single-nucleus RNA-seq work yielded similar findings. Oligodendrocytes were found to be most severely affected in the CTE white matter samples; they were diminished in number and altered in relative proportions across subtype clusters. Further, the CTE-enriched oligodendrocyte population showed greater abundance of transcripts relevant to iron metabolism and cellular stress response. CTE tissue also demonstrated excessive iron accumulation histologically. In astrocytes, total cell numbers were indistinguishable between CTE and control samples, but transcripts associated with neuroinflammation were elevated in the CTE astrocyte groups compared to controls. These results demonstrate specific molecular and cellular differences in CTE oligodendrocytes and astrocytes and suggest that white matter alterations are a critical aspect of CTE neurodegeneration.

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