Corrigendum to “Characterization of Zebrafish von Willebrand Factor Reveals Conservation of Domain Structure, Multimerization, and Intracellular Storage”

“…In agreement with this, the PmRab7 gene sequence codes for a deduced polypeptide containing five extremely conserved motifs (G boxes) involved in GTP-binding or GTPase activity and an isoprenylation site (last both C), suggesting that PmRab7 is an active GTPase that is able to cycle between GDP-and GTP bound states [22]. In this study we presented 3D model of PmRab7 for Mg 2+ and GTP binding site analysis, the same model was shown by Arunima et al [23] also, but here first time we are reporting the inactive PmRab7 (GDP) to active PmRab7 (GTP) on the basis of various hydrogen bonding G 18-20, T 46 and K 126 were involved in PmRab7 activation. In the present molecular docking study, CID 1067700 was docked with PmRab7 (Target protein PDB Id: 1VG8) using the docking program GLIDE in the presence of Mg 2+ and GTP.…”

Role of PmRab7 Regulation in WSSV Infection and Functional Validation of Small Molecule as PmRab7 GTPase Inhibitor

“…In agreement with this, the PmRab7 gene sequence codes for a deduced polypeptide containing five extremely conserved motifs (G boxes) involved in GTP-binding or GTPase activity and an isoprenylation site (last both C), suggesting that PmRab7 is an active GTPase that is able to cycle between GDP-and GTP bound states [22]. In this study we presented 3D model of PmRab7 for Mg 2+ and GTP binding site analysis, the same model was shown by Arunima et al [23] also, but here first time we are reporting the inactive PmRab7 (GDP) to active PmRab7 (GTP) on the basis of various hydrogen bonding G 18-20, T 46 and K 126 were involved in PmRab7 activation. In the present molecular docking study, CID 1067700 was docked with PmRab7 (Target protein PDB Id: 1VG8) using the docking program GLIDE in the presence of Mg 2+ and GTP.…”

Role of PmRab7 Regulation in WSSV Infection and Functional Validation of Small Molecule as PmRab7 GTPase Inhibitor