Characterization of selectivity and pharmacophores of type 1 sea anemone toxins by screening seven Na-v sodium channel isoforms

During their evolution, animals have developed a set of cysteine-rich peptides capable of binding various extracellular sites of voltage-gated sodium channels (VGSC). Sea anemone toxins that target VGSCs delay their inactivation process, but little is known about their selectivities. Here we report the investigation of three native type 1 toxins (CGTX-II, delta-AITX-Bcg1a and delta-AITX-Bcg1b) purified from the venom of Bunodosoma cangicum. Both delta-AITX-Bcg1a and delta-AITX-Bcg1b toxins were fully sequenced. The three peptides were evaluated by patch-clamp technique among Nav1.1-1.7 isoforms expressed in mammalian cell lines, and their preferential targets are Na(v)1.5 > 1.6 > 1.1. We also evaluated the role of some supposedly critical residues in the toxins which would interact with the channels, and observed that some substitutions are not critical as expected. In addition, CGTX-II and delta-AITX-Bcg1a evoke different shifts in activation/inactivation Boltzmann curves in Nav1.1 and 1.6. Moreover, our results suggest that the interaction region between toxins and VGSCs is not restricted to the supposed site 3 (S3-54 linker of domain IV), and this may be a consequence of distinct surface of contact of each peptide vs. targeted channel. Our data suggest that the contact surfaces of each peptide may be related to their surface charges, as CGTX-II is more positive than delta-AITX-Bcg1a and delta-AITX-Bcg1b. (C) 2011 Elsevier Inc. All rights reserved.

Italian Ministero dellUniversita e della Ricerca Scientifica e Tecnologica

Italian Ministero dell'Universita e della Ricerca Scientifica e Tecnologica [MIUR-PRIN2003-2005-2001055320, 2003052919, MIUR-FIRB2001-RBNE01XMP4-002, MIUR-FISR2001 0300179]

Universita di MilanoBicocca

Universita di Milano-Bicocca [MIUR-PRIN2003-2005]

Conselho Nacional de Desenvolvimento Cientifico e Tecnologico [CNPq]

Conselho Nacional de Desenvolvimento Cientifico e Tecnologico

FAPESP

FAPESP [Brazilian Government] [07/56525-3, 06/02892-2]