Communications Biology (Oct 2024)

Stepwise release of Activin-A from its inhibitory prodomain is modulated by cysteines and requires furin coexpression to promote melanoma growth

  • Katarina Pinjusic,
  • Manon Bulliard,
  • Benjamin Rothé,
  • Saeid Ansaryan,
  • Yeng-Cheng Liu,
  • Pierpaolo Ginefra,
  • Céline Schmuziger,
  • Hatice Altug,
  • Daniel B. Constam

DOI
https://doi.org/10.1038/s42003-024-07053-0
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 18

Abstract

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Abstract The Activin-A precursor dimer can be cleaved by furin, but how this proteolytic maturation is regulated in vivo and how it facilitates access to signaling receptors is unclear. Here, analysis in a syngeneic melanoma grafting model shows that without furin coexpression, Activin-A failed to accelerate tumor growth, correlating with failure of one or both subunits to undergo cleavage in signal-sending cells, even though compensatory processing by host cells nonetheless sustained elevated circulating Activin-A levels. In reporter assays, furin-independent cleavage of one subunit enabled juxtacrine Activin-A signaling, whereas completion of proteolytic maturation by coexpressed furin or by recipient cells stimulated contact-independent activity, crosstalk with BMP receptors, and signal inhibition by follistatin. Mechanistically, Activin-A processing was modulated by allosteric disulfide bonds flanking the furin site. Disruption of these disulfide linkages with the prodomain enabled Activin-A binding to cognate type II receptors independently of proteolytic maturation. Stepwise proteolytic maturation is a novel mechanism to control Activin-A protein interactions and signaling.