, 2008) These

different tissue responses have been inves

, 2008). These

different tissue responses have been investigated under different in vitro and in vivo models in order to understand the local cytotoxicity and the systemic effects of the complex mixture of snake venoms ( Gutierrez et al., 1986; Sanchez et al., 1992; Melo et al., 1993; Melo and Ownby, 1999; Murakami et al., 2005; Teixeira et al., 2009; Escalante et al., 2011). The recommended therapy to snakebite envenomation has been based on the administration of animal-derived antivenom that can ameliorate and stop many of the venom effects (da Silva et al., 2007; Gutierrez et al., 2007, Gutierrez et al., 2011a and Gutierrez et al., 2011b). However, the local response induced by Bothrops snake venoms is described as being only partially neutralized by either the specific or the polyvalent antivenom even if the antivenom IOX1 is locally injected ( Chaves et al., 2003; da Silva et al., 2007; Gutierrez et al., 2007 and Gutierrez et al.,

2011a). The problem is bigger when the therapy is delayed for many different reasons, such as geographical problems or lack of accessibility to the antivenom ( Chippaux, 1998; Pardal et al., 2004; Gutierrez et al., 2007). In many rural areas in Brazil or elsewhere in the world where the antivenom is not easily available, local people use folk medicine such herbal preparations in the snakebite treatment, trying to interrupt the venom effects ( Martz, 1992; Mors et al., 2000; Coe and Anderson, 2005). When it is available, the use of antivenom can still elicit different reactions once they are animal-derived products. The local venom effects are poorly understood, and although many studies have been trying to develop new substances Lumacaftor able to stop or antagonize the powerful local inflammatory response induced by Bothrops venoms, which involves cytokines and white blood cells, it is still a challenge ( Lomonte et al., 1993; Olivo et al., 2007; Gutierrez et al., 2007; Melo et al., 2010). It has been difficult to develop new drugs for snakebite envenoming treatment, either from plants or from new planed synthetic molecules, because they are

not attractive to developed countries nor to big companies once they will not return the investment Parvulin and the endeavor ( Gutierrez et al., 2007; Lomonte et al., 2009). The local myonecrosis and inflammatory response are critical to late disabilities (Gutierrez et al., 1986; Rucavado and Lomonte, 1996; Teixeira et al., 2009), but even the well-known substances used for the treatment of allergic reactions induced by antivenom treatment are not frequently investigated for their anti-inflammatory activities (Chen et al., 2007; Olivo et al., 2007; Thiansookon and Rojnuckarin, 2008; Nascimento et al., 2010). Nascimento et al. (2010) described that dexamethasone decreased the acute inflammatory response induced by Bothrops moojeni in mice, and this observation is ascribed to the ability of dexamethasone to decrease the formation of eicosanoids in the presence of the venom.

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