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Treating cachexia using soluble ACVR2B improves survival, alters mTOR localization, and attenuates liver and spleen responses.

Tuuli A NissinenJaakko HentiläFabio PennaAnita LampinenJuulia H LautaojaVasco FachadaTanja HolopainenOlli RitvosRiikka KiveläJuha J Hulmi
Published in: Journal of cachexia, sarcopenia and muscle (2018)
The prolonged survival with continued ACVR2 ligand blocking could potentially be attributed in part to the maintenance of limb and respiratory muscle mass, but many observed non-muscle effects suggest that the effect may be more complex than previously thought. Our novel finding showing decreased mTOR localization in skeletal muscle with lysosomes/late-endosomes in cancer opens up new research questions and possible treatment options for cachexia.
Keyphrases
  • skeletal muscle
  • cell proliferation
  • papillary thyroid
  • insulin resistance
  • free survival
  • squamous cell
  • metabolic syndrome
  • young adults