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Legumain Functions as a Transient TrkB Sheddase.

Christoph HolznerKatharina BöttingerConstantin BlöchlChristian G HuberSven O DahmsElfriede DallHans Brandstetter
Published in: International journal of molecular sciences (2023)
While primarily found in endo-lysosomal compartments, the cysteine protease legumain can also translocate to the cell surface if stabilized by the interaction with the RGD-dependent integrin receptor αVβ3. Previously, it has been shown that legumain expression is inversely related to BDNF-TrkB activity. Here we show that legumain can conversely act on TrkB-BDNF by processing the C-terminal linker region of the TrkB ectodomain in vitro. Importantly, when in complex with BDNF, TrkB was not cleaved by legumain. Legumain-processed TrkB was still able to bind BDNF, suggesting a potential scavenger function of soluble TrkB towards BDNF. The work thus presents another mechanistic link explaining the reciprocal TrkB signaling and δ-secretase activity of legumain, with relevance for neurodegeneration.
Keyphrases
  • stress induced
  • cell surface
  • poor prognosis
  • climate change
  • binding protein
  • blood brain barrier