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Can Inhibitors of Snake Venom Phospholipases A 2 Lead to New Insights into Anti-Inflammatory Therapy in Humans? A Theoretical Study

机译:蛇毒磷脂酶A 2的抑制剂能否为人类抗炎治疗带来新见解?理论研究

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Human phospholipase A 2 ( h PLA 2 ) of the IIA group (HGIIA) catalyzes the hydrolysis of membrane phospholipids, producing arachidonic acid and originating potent inflammatory mediators. Therefore, molecules that can inhibit this enzyme are a source of potential anti-inflammatory drugs, with different action mechanisms of known anti-inflammatory agents. For the study and development of new anti-inflammatory drugs with this action mechanism, snake venom PLA 2 ( sv PLA 2 ) can be employed, since the sv PLA 2 has high similarity with the human PLA 2 HGIIA. Despite the high similarity between these secretory PLA 2 s , it is still not clear if these toxins can really be employed as an experimental model to predict the interactions that occur with the human PLA 2 HGIIA and its inhibitors. Thus, the present study aims to compare and evaluate, by means of theoretical calculations, docking and molecular dynamics simulations, as well as experimental studies, the interactions of human PLA 2 HGIIA and two sv PLA 2 s , Bothrops toxin II and Crotoxin B (BthTX-II and CB, respectively). Our theoretical findings corroborate experimental data and point out that the human PLA 2 HGIIA and sv PLA 2 BthTX-II lead to similar interactions with the studied compounds. From our results, the sv PLA 2 BthTX-II can be used as an experimental model for the development of anti-inflammatory drugs for therapy in humans.
机译:IIA组(HGIIA)的人磷脂酶A 2(h PLA 2)催化膜磷脂的水解,产生花生四烯酸并起有效的炎症介质作用。因此,可以抑制这种酶的分子是潜在的抗炎药的来源,具有已知抗炎剂的不同作用机制。为了研究和开发具有这种作用机制的新型抗炎药,可以使用蛇毒PLA 2(sv PLA 2),因为sv PLA 2与人PLA 2 HGIIA具有高度相似性。尽管这些分泌性PLA 2s之间具有高度相似性,但仍不清楚这些毒素是否真的可以用作预测人PLA 2 HGIIA及其抑制剂发生相互作用的实验模型。因此,本研究旨在通过理论计算,对接和分子动力学模拟以及实验研究来比较和评估人PLA 2 HGIIA与两个sv PLA 2 s,Broprops毒素II和Crotoxin B( BthTX-II和CB)。我们的理论发现证实了实验数据,并指出人PLA 2 HGIIA和sv PLA 2 BthTX-II导致与所研究化合物的相似相互作用。根据我们的结果,sv PLA 2 BthTX-II可用作开发用于人类的抗炎药的实验模型。

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