Scientific Reports (Mar 2024)

Experimental and computational evidence that Calpain-10 binds to the carboxy terminus of NaV1.2 and NaV1.6

  • Luis Manuel Arratia,
  • Juan David Bermudes-Contreras,
  • Jorge Armando Juarez-Monroy,
  • Erik Alan Romero-Macías,
  • Julio Cesar Luna-Rojas,
  • Marisol López-Hidalgo,
  • Ana Victoria Vega,
  • Absalom Zamorano-Carrillo

DOI
https://doi.org/10.1038/s41598-024-57117-8
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 12

Abstract

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Abstract Voltage-gated sodium channels (NaV) are pivotal proteins responsible for initiating and transmitting action potentials. Emerging evidence suggests that proteolytic cleavage of sodium channels by calpains is pivotal in diverse physiological scenarios, including ischemia, brain injury, and neuropathic pain associated with diabetes. Despite this significance, the precise mechanism by which calpains recognize sodium channels, especially given the multiple calpain isoforms expressed in neurons, remains elusive. In this work, we show the interaction of Calpain-10 with NaV's C-terminus through a yeast 2-hybrid assay screening of a mouse brain cDNA library and in vitro by GST-pulldown. Later, we also obtained a structural and dynamic hypothesis of this interaction by modeling, docking, and molecular dynamics simulation. These results indicate that Calpain-10 interacts differentially with the C-terminus of NaV1.2 and NaV1.6. Calpain-10 interacts with NaV1.2 through domains III and T in a stable manner. In contrast, its interaction with NaV1.6 involves domains II and III, which could promote proteolysis through the Cys-catalytic site and C2 motifs.