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Structural characterization of PPTI, a kunitz-type protein from the venom of Pseudocerastes persicus

机译:PPTI的结构特征,PPTI是伪蛇梨毒液中的kunitz型蛋白

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摘要

The main purpose of this report is to investigate the structural property and new potential function of PPTI (Pseudocerastes Persicus Trypsin Inhibitor), a kunitz-type protein with inhibitory effect against trypsin proteolytic activity. Besides kunitz-type serine protease inhibitors, PPTI shows clear-cut similarities with dendrotoxins (DTXs), the other kunitz-type protein subfamily. The most important reason is the presence of functionally important residues of DTXs at correspondingly the same positions in PPTI. As such, we proposed the new ability of PPTI for inhibiting voltage-gated potassium channels and consequently its dual functionality. At first, we determined the solution structure of PPTI via Nuclear Magnetic Resonance (NMR) spectroscopy. Then by homology modeling, we constructed the model structure of trypsin-PPTI complex to confirm the same interaction pattern as trypsin-BPTI at complex interface. Finally, by Brownian dynamics (BD) simulations of PPTI NMR derived ensemble structure as ligand against homology model of human Kv1.1 potassium channel as receptor, we evaluated the potential DTX-like activity of PPTI. The results of our study support the proposed dual functionality of PPTI.
机译:这份报告的主要目的是研究PPTI(假瓷膏Persicus胰蛋白酶抑制剂)的结构特性和新的潜在功能,PPTI是一种对胰蛋白酶蛋白水解活性具有抑制作用的kunitz型蛋白。除kunitz型丝氨酸蛋白酶抑制剂外,PPTI与其他kunitz型蛋白亚家族树突毒素(DTX)表现出明显的相似性。最重要的原因是DTX的功能重要残基存在于PPTI中相应的相同位置。因此,我们提出了PPTI抑制电压门控钾通道并因此具有双重功能的新功能。首先,我们通过核磁共振(NMR)光谱确定了PPTI的溶液结构。然后通过同源性建模,构建了胰蛋白酶-PPTI复合物的模型结构,以确认在复杂界面上与胰蛋白酶-BPTI相同的相互作用模式。最后,通过针对人类Kv1.1钾离子通道作为受体的同源性模型对PPTI NMR衍生的集合结构作为配体的布朗动力学(BD)模拟,我们评估了PPTI潜在的DTX样活性。我们的研究结果支持了PPTI的双重功能。

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