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Insight towards the conserved water mediated recognition of catalytic and structural Zn+2 ions in human Matrix Metalloproteinase-8 enzyme: A study by MD-simulation methods

机译:保守水介导的人类基质金属蛋白酶8酶催化和结构中Zn + 2离子识别的见解:MD模拟方法研究

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摘要

Human matrix metalloproteinase-8 (hMMP-8) plays a important role in the progression of colorectal cancer, metastasis, multiple sclerosis and rheumetoid arthritis. Extensive MD-simulation of the PDB and solvated structures of hMMP-8 has revealed the presence of few conserved water molecules around the catalytic and structural zinc (ZnC and ZnS) ions. The coordination of two conserved water molecules (W and WS) to ZnS and the H-bonding interaction of WS to S151 have indicated the plausible involvement of that metal ion in the catalytic process. Beside this the coupling of ZnC and ZnS metal ions (ZnC – WH (W1)…..W2 ….H162 - ZnS) through two conserved hydrophilic centers (occupied by water molecules) may also provide some rational on the recognition of two zinc ions which were separated by ~13 Å in their X-ray structures. This unique recognition of both the Zn+2 ions in the enzyme through conserved water molecules may be implemented/ exploited for the design of antiproteolytic agent using water mimic drug design protocol.
机译:人基质金属蛋白酶8(hMMP-8)在结直肠癌,转移,多发性硬化和类风湿关节炎的进展中起重要作用。广泛的MD模拟的hMMP-8的PDB和溶剂化结构表明,在催化和结构化锌离子(ZnC和ZnS)周围几乎没有保守的水分子。两种保守的水分子(W和WS)与ZnS的配位以及WS与S151的H键相互作用表明,该金属离子可能参与了催化过程。除此之外,通过两个保守的亲水中心(被水分子占据)的ZnC和ZnS金属离子(ZnC – WH(W1)….W2….H162-ZnS)的偶联还可以为识别两个锌离子提供一些合理的方法。在X射线结构中被〜13Å隔开。通过保守水分子对酶中Zn +2 离子的这种独特识别可以使用水模拟药物设计方案进行/开发,用于抗蛋白水解剂的设计。

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