Identification of purinergic system components in the venom of Bothrops mattogrossensis and the inhibitory effect of specioside extracted from Tabebuia aurea.

对马托格罗塞斯矛头蝮蛇毒液中嘌呤能系统成分的鉴定以及从金花风铃木中提取的物种苷的抑制作用

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作者:Dias Dhébora Albuquerque, Souza de Souza Kamylla Fernanda, Moslaves Iluska Senna Bonfá, Buri Marcus Vinicius, Basilio Denise Caroline Luiz Soares, Espinoça Isabelly Teixeira, Parisotto Eduardo Benedetti, Silva-Filho Saulo Euclides, Migliolo Ludovico, Jaques Jeandre Augusto Otsubo, Franco Daniel Guerra, Chudzinski-Tavassi Ana Marisa, Rita Paula Helena Santa, da Silva Denise Brentan, Carollo Carlos Alexandre, Toffoli-Kadri Mônica Cristina, Paredes-Gamero Edgar Julian
Snake bites are a severe problem in the countryside of Brazil and are usually attributed to snakes of the genera Bothrops, Crotalus, and Lachesis. Snake venom can release ectoenzymes and nucleotidases that modulate the purinergic system. In addition to serum therapy against snake poisoning, medicinal plants with anti-inflammatory activities, such as Tabebuia aurea, is empirically applied in accidents that occur in difficult-to-access areas. This study aimed was to verify the presence and activity of nucleotidases in the crude venom of Bothrops mattogrossensis (BmtV) in vitro and characterize the modulation of purinergic components, myeloid differentiation, and inflammatory/oxidative stress markers by BmtV in vivo and in vitro. Moreover, our study assessed the inhibitory activities of specioside, an iridoid isolated from Tabebuia aurea, against the effects of BmtV. Proteomic analysis of venom content and nucleotidase activity confirm the presence of ectonucleotidase-like enzymes in BmtV. In in vivo experiments, BmtV altered purinergic component expression (P2X7 receptor, CD39 and CD73), increased neutrophil numbers in peripheral blood, and elevated oxidative stress/inflammatory parameters such as lipid peroxidation and myeloperoxidase activity. BmtV also decreased viability and increased spreading index and phagocytic activity on macrophages. Specioside inhibited nucleotidase activity, restored neutrophil numbers, and mediate the oxidative/inflammatory effects produced by BmtV. We highlight the effects produced by BmtV in purinergic system components, myeloid differentiation, and inflammatory/oxidative stress parameters, while specioside reduced the main BmtV-dependent effects.

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