4.4 Article

Identification and molecular characterization of five putative toxins from the venom gland of the snake Philodryas chamissonis (Serpentes: Dipsadidae)

Journal

TOXICON
Volume 108, Issue -, Pages 19-31

Publisher

PERGAMON-ELSEVIER SCIENCE LTD
DOI: 10.1016/j.toxicon.2015.09.032

Keywords

Rear-fanged snakes; Cloning; Snake venom metalloproteases; Serine proteases; CRISP; Gene expression

Funding

  1. FONDECYT [1120254, 1120181, 3130742, 3110129]
  2. CONICYT

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Philodryas chamissonis is a rear-fanged snake endemic to Chile. Its bite produces mild to moderate symptoms with proteolytic and anti-coagulant effects. Presently, the composition of the venom, as well as, the biochemical and structural characteristics of its toxins, remains unknown. In this study, we cloned and reported the first full-length sequences of five toxin-encoding genes from the venom gland of this species: Type III snake venom metalloprotease (SVMP), snake venom serine protease (SVSP), Cysteine-rich secretory protein (CRISP), alpha and beta subunits of C-type lectin-like protein (CLP) and C-type natriuretic peptide (NP). These genes are highly expressed in the venom gland and their sequences exhibited a putative signal peptide, suggesting that these are components of the venom. These putative toxins had different evolutionary relationships with those reported for some front-fanged snakes, being SVMP, SVSP and CRISP of P. chamissonis closely related to the toxins present in Elapidae species, while NP was more related to those of Viperidae species. In addition, analyses suggest that the alpha and beta subunits of CLP of P. chamissonis might have a alpha-subunit scaffold in common with Viperidae species, whose highly variable C-terminal region might have allowed the diversification in a and (I subunits. Our results provide the first molecular description of the toxins possibly implicated in the envenomation of prey and humans by the bite of P. chamissonis. (C) 2015 Elsevier Ltd. All rights reserved.

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