Cell Reports (Nov 2018)

Secretion of Tau via an Unconventional Non-vesicular Mechanism

  • Maria Merezhko,
  • Cecilia A. Brunello,
  • Xu Yan,
  • Helena Vihinen,
  • Eija Jokitalo,
  • Riikka-Liisa Uronen,
  • Henri J. Huttunen

Journal volume & issue
Vol. 25, no. 8
pp. 2027 – 2035.e4

Abstract

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Summary: Tauopathies are characterized by cerebral accumulation of Tau protein aggregates that appear to spread throughout the brain via a cell-to-cell transmission process that includes secretion and uptake of pathological Tau, followed by templated misfolding of normal Tau in recipient cells. Here, we show that phosphorylated, oligomeric Tau clusters at the plasma membrane in N2A cells and is secreted in vesicle-free form in an unconventional process sensitive to changes in membrane properties, particularly cholesterol and sphingomyelin content. Cell surface heparan sulfate proteoglycans support Tau secretion, possibly by facilitating its release after membrane penetration. Notably, secretion of endogenous Tau from primary cortical neurons is mediated, at least partially, by a similar mechanism. We suggest that Tau is released from cells by an unconventional secretory mechanism that involves its phosphorylation and oligomerization and that membrane interaction may help Tau to acquire properties that allow its escape from cells directly through the plasma membrane. : Merezhko et al. show that Tau protein is released from cells by an unconventional secretory mechanism that can be manipulated by changing plasma membrane properties. Phosphorylated oligomeric Tau clusters at the plasma membrane, allowing its escape from cells directly through the plasma membrane. Keywords: Alzheimer’s disease, tauopathy, neurodegeneration, disease mechanism, transcellular propagation, unconventional protein secretion, lipid raft, exocytosis, oligomerization, aggregation