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MSA Glial Pathology

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MSA Glial Pathology

Multiple System Atrophy (MSA) is fundamentally an oligodendrogliopathy — a disease where oligodendrocytes (the myelin-producing cells of the CNS) are the primary pathological target. This distinguishes MSA from Parkinson's disease where neurons are the primary target, and makes glial pathology the central focus for understanding disease mechanisms and developing therapies.

Overview of Glial Pathology in MSA

The glial pathology in MSA encompasses three major cell types:

  • Oligodendrocytes — Primary target, featuring glial cytoplasmic inclusions (GCIs)
  • Astrocytes — Reactive changes in regions with high GCI burden
  • Microglia — Chronic activation creating a neurotoxic inflammatory milieu
  • These three cell types interact in a self-reinforcing cycle of dysfunction that drives progressive neurodegeneration[@jellinger2023].

    Primary: Oligodendrocyte Dysfunction and GCI Formation

    The Oligodendrogliopathy Concept

    Wenning and colleagues proposed in 2009 that MSA is primarily an oligodendrogliopathy — a disease where the primary pathological target is the oligodendrocyte[@wenning2009]. Key evidence:

    • GCI dominance: Glial cytoplasmic inclusions vastly outnumber neuronal cytoplasmic inclusions (10:1 ratio)
    • Temporal precedence: GCIs appear in brain regions before neuronal loss develops
    • Distribution pattern: Oligodendrocyte involvement follows predictable white matter tract patterns
    • Oligodendrocyte death: Severe loss of oligodendrocytes in affected regions

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