| Literature DB >> 27563734 |
Daniele Chaves-Moreira1, Fábio Rogério de Moraes2, Ícaro Putinhon Caruso2, Olga Meiri Chaim1, Andrea Senff-Ribeiro1, Anwar Ullah2,3, Luciane Sussuchi da Silva2, Jorge Chahine2, Raghuvir K Arni2, Silvio Sanches Veiga1.
Abstract
Loxoscelism refers to the clinical symptoms that develop after brown spider bites. Brown spider venoms contain several phospholipase-D isoforms, which are the main toxins responsible for both the cutaneous and systemic effects of loxoscelism. Understanding of the phospholipase-D catalytic mechanism is crucial for the development of specific treatment that could reverse the toxic effects caused by the spider bite. Based on enzymatic, biological, structural, and thermodynamic tests, we show some features suitable for designing drugs against loxoscelism. Firstly, through molecular docking and molecular dynamics predictions, we found three different molecules (Suramin, Vu0155056, and Vu0359595) that were able to bind the enzyme's catalytic site and interact with catalytically important residues (His12 or His47) and with the Mg2+ co-factor. The binding promoted a decrease in the recombinant brown spider venom phospholipase-D (LiRecDT1) enzymatic activity. Furthermore, the presence of the inhibitors reduced the hemolytic, dermonecrotic, and inflammatory activities of the venom toxin in biological assays. Altogether, these results indicate the mode of action of three different LiRecDT1 inhibitors, which were able to prevent the venom toxic effects. This strengthen the idea of the importance of designing a specific drug to treat the serious clinical symptoms caused by the brown spider bite, a public health problem in several parts of the world, and until now without specific treatment. J. Cell. Biochem. 118: 726-738, 2017.Entities:
Keywords: BROWN SPIDER; INHIBITOR; LOXOSCELES INTERMEDIA; RECOMBINANT TOXIN; VENOM PHOSPHOLIPASE-D
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Year: 2016 PMID: 27563734 DOI: 10.1002/jcb.25678
Source DB: PubMed Journal: J Cell Biochem ISSN: 0730-2312 Impact factor: 4.429