PLoS Biology (Dec 2020)

Oligodendrocytes support axonal transport and maintenance via exosome secretion.

  • Carsten Frühbeis,
  • Wen Ping Kuo-Elsner,
  • Christina Müller,
  • Kerstin Barth,
  • Leticia Peris,
  • Stefan Tenzer,
  • Wiebke Möbius,
  • Hauke B Werner,
  • Klaus-Armin Nave,
  • Dominik Fröhlich,
  • Eva-Maria Krämer-Albers

DOI
https://doi.org/10.1371/journal.pbio.3000621
Journal volume & issue
Vol. 18, no. 12
p. e3000621

Abstract

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Neurons extend long axons that require maintenance and are susceptible to degeneration. Long-term integrity of axons depends on intrinsic mechanisms including axonal transport and extrinsic support from adjacent glial cells. The mechanisms of support provided by myelinating oligodendrocytes to underlying axons are only partly understood. Oligodendrocytes release extracellular vesicles (EVs) with properties of exosomes, which upon delivery to neurons improve neuronal viability in vitro. Here, we show that oligodendroglial exosome secretion is impaired in 2 mouse mutants exhibiting secondary axonal degeneration due to oligodendrocyte-specific gene defects. Wild-type oligodendroglial exosomes support neurons by improving the metabolic state and promoting axonal transport in nutrient-deprived neurons. Mutant oligodendrocytes release fewer exosomes, which share a common signature of underrepresented proteins. Notably, mutant exosomes lack the ability to support nutrient-deprived neurons and to promote axonal transport. Together, these findings indicate that glia-to-neuron exosome transfer promotes neuronal long-term maintenance by facilitating axonal transport, providing a novel mechanistic link between myelin diseases and secondary loss of axonal integrity.