Human superoxide dismutase 1 (hS0D1) maturation through interaction with human copper chaperone for S0D1 (hCCS).

Copper chaperone for superoxide dismutase 1 (SOD1), CCS, is the physiological partner for the complex mechanism of SOD1 maturation. We report an in vitro model for human CCS-dependent SOD1 maturation based on the study of the interactions of human SOD1 (hSODl) with full-length WT human CCS (hCCS), as well as with hCCS mutants and various truncated constructs comprising one or two of the protein's three domains. The synergy between electrospray ionization mass spectrometry (ESI-MS) and NMR is fully exploited. This is an in vitro study of this process at the molecular level. Domain 1 of hCCS is necessary to load hSODl with Cu(l), requiring the heterodimeric complex formation with hSODl fostered by the interaction with domain 2. Domain 3 is responsible for the catalytic formation of the hSODl Cys-57-Cys-146 disulfide bond, which involves both hCCS Cys-244 and Cys-246 via disulfide transfer. [ABSTRACT FROM AUTHOR]