与多药耐药 HIV-1 蛋白酶变体中抑制剂效力改变相关的构象变化诱导。
Correlating conformational shift induction with altered inhibitor potency in a multidrug resistant HIV-1 protease variant.
机构信息
Department of Chemistry, University of Florida, P.O. Box 117200, Gainesville, Florida 32611, USA.
出版信息
Biochemistry. 2012 Oct 9;51(40):7813-5. doi: 10.1021/bi301010z. Epub 2012 Sep 28.
Abstract
Inhibitor-induced conformational ensemble shifts in a multidrug resistant HIV-1 protease variant, MDR769, are characterized by site-directed spin labeling double electron-electron resonance spectroscopy. For MDR769 compared to the native enzyme, changes in inhibitor IC(50) values are related to a parameter defined as |ΔC|, which is the relative change in the inhibitor-induced shift to the closed state. Specifically, a linear correlation is found between |ΔC| and the magnitude of the change in IC(50), provided that inhibitor binding is not too weak. Moreover, inhibitors that exhibit MDR769 resistance no longer induce a strong shift to a closed conformational ensemble as seen previously in the native enzyme.
摘要
通过定点自旋标记双电子电子共振光谱技术,研究了一种多药耐药 HIV-1 蛋白酶变体 MDR769 中抑制剂诱导的构象整体变化。与天然酶相比,MDR769 中抑制剂 IC50 值的变化与一个被定义为 |ΔC| 的参数相关,该参数是抑制剂诱导的向闭状态转变的相对变化。具体来说,如果抑制剂的结合不是太弱,就会发现 |ΔC| 与 IC50 变化的幅度之间存在线性相关性。此外,与先前在天然酶中观察到的情况相比,表现出 MDR769 耐药性的抑制剂不再诱导强烈的向闭构象整体变化。
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