Local myonecrosis is the main event resulting from snakebite envenomation by the Bothrops genus and, frequently, it is not efficiently neutralized by antivenom administration. Proteases, phospholipases A(2) (PLA(2)) and PLA(2)-like toxins are found in venom related to muscle damage. Functional sites responsible for PLA(2)-like toxins activity have been proposed recently; they consist of a membrane docking-site and a membrane rupture-site. Herein, a combination of functional, biophysical and crystallographic techniques was used to characterize the interaction between suramin and MjTX-I (a PLA(2)-like toxin from Bothrops moojeni venom). Functional in vitro neuromuscular assays were performed to study the biological effects of the protein-ligand interaction, demonstrating that suramin neutralizes the myotoxic effect of MjTX-I. Calorimetric assays showed two different binding events: (i) inhibitor-protein interactions and (ii) toxin oligomerization processes. These hypotheses were also corroborated with dynamic light and small angle X-ray scattering assays. The crystal structure of the MjTX-I/suramin showed a totally different interaction mode compared to other PLA(2)-like/suramin complexes. Thus, we suggested a novel myotoxic mechanism for MjTX-I that may be inhibited by suramin. These results can further contribute to the search for inhibitors that will efficiently counteract local myonecrosis in order to be used as an adjuvant of conventional serum therapy.
Structural and functional characterization of suramin-bound MjTX-I from Bothrops moojeni suggests a particular myotoxic mechanism.
对来自 Bothrops moojeni 的苏拉明结合的 MjTX-I 的结构和功能表征表明了一种特殊的肌毒性机制
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作者:Salvador Guilherme H M, Dreyer Thiago R, Gomes Antoniel A S, Cavalcante Walter L G, Dos Santos Juliana I, Gandin César A, de Oliveira Neto Mário, Gallacci Márcia, Fontes Marcos R M
| 期刊: | Scientific Reports | 影响因子: | 3.900 |
| 时间: | 2018 | 起止号: | 2018 Jul 9; 8(1):10317 |
| doi: | 10.1038/s41598-018-28584-7 | ||
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