Macro- and Microstructural White Matter Differences in Neurologic Postacute Sequelae of SARS-CoV-2 Infection, 2024, O’Connor et al.

Discussion in 'Long Covid research' started by SNT Gatchaman, Oct 11, 2024.

  1. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    Macro- and Microstructural White Matter Differences in Neurologic Postacute Sequelae of SARS-CoV-2 Infection
    Erin E. O’Connor; Rosangela Salerno-Goncalves; Nikita Rednam; Rory O’Brien; Peter Rock; Andrea R. Levine; Thomas A. Zeffiro

    BACKGROUND AND PURPOSE
    Neuropsychiatric complications of SARS-CoV-2 infection, also known as neurologic postacute sequelae of SARS-CoV-2 infection (NeuroPASC), affect 10%–60% of infected individuals. There is growing evidence that NeuroPASC is a multi system immune dysregulation disease affecting the brain. The behavioral manifestations of NeuroPASC, such as impaired processing speed, executive function, memory retrieval, and sustained attention, suggest widespread WM involvement. Although previous work has documented WM damage following acute SARS-CoV-2 infection, its involvement in NeuroPASC is less clear. We hypothesized that macrostructural and microstructural WM differences in NeuroPASC participants would accompany cognitive and immune system differences.

    MATERIALS AND METHODS
    In a cross-sectional study, we screened a total of 159 potential participants and enrolled 72 participants, with 41 asymptomatic controls (NoCOVID) and 31 NeuroPASC participants matched for age, sex, and education. Exclusion criteria included neurologic disorders unrelated to SARS-CoV-2 infection. Assessments included clinical symptom questionnaires, psychometric tests, brain MRI measures, and peripheral cytokine levels. Statistical modeling included separate multivariable regression analyses of GM/WM/CSF volume, WM microstructure, cognitive, and cytokine concentration between-group differences.

    RESULTS
    NeuroPASC participants had larger cerebral WM volume than NoCOVID controls (β = 0.229; 95% CI: 0.017–0.441; t = 2.16; P = .035). The most pronounced effects were in the prefrontal and anterior temporal WM. NeuroPASC participants also exhibited higher WM mean kurtosis, consistent with ongoing neuroinflammation. NeuroPASC participants had more self-reported symptoms, including headache, and lower performance on measures of attention, concentration, verbal learning, and processing speed. A multivariate profile analysis of the cytokine panel showed different group cytokine profiles (Wald-type-statistic = 44.6, P = .046), with interferon (IFN)-λ1 and IFN-λ2/3 levels higher in the NeuroPASC group.

    CONCLUSIONS
    NeuroPASC participants reported symptoms of lower concentration, higher fatigue, and impaired cognition compatible with WM syndrome. Psychometric testing confirmed these findings. NeuroPASC participants exhibited larger cerebral WM volume and higher WM mean kurtosis than NoCOVID controls. These findings suggest that immune dysregulation could influence WM properties to produce WM volume increases and consequent cognitive effects and headaches. Further work will be needed to establish mechanistic links among these variables.


    Link | PDF (American Journal of Neuroradiology)
     
  2. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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  3. rvallee

    rvallee Senior Member (Voting Rights)

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    They excluded the most common issue found in LC from a LC study?

    But they found it anyway. Damn kids these days.

    ¯\_(ツ)_/¯
     
  4. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    Possibly that meant the exclusion was a pre-existing diagnosis of ME/CFS, ME, CFS, "chronic fatigue" etc. Or they were drawing a distinction between physical and cognitive fatigue.

    It's always confusing when fatigue is so often framed as "neurological".
     
    Peter Trewhitt likes this.

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