Crichlow Gregg V, Cheng Kai Fan, Dabideen Darrin, Ochani Mahendar, Aljabari Bayan, Pavlov Valentin A, Miller Edmund J, Lolis Elias, Al-Abed Yousef
Department of Pharmacology, Yale University School of Medicine, New Haven, Connecticut 06520, USA.
J Biol Chem. 2007 Aug 10;282(32):23089-95. doi: 10.1074/jbc.M701825200. Epub 2007 May 25.
Pharmacophores are chemical scaffolds upon which changes in chemical moieties (R-groups) at specific sites are made to identify a combination of R-groups that increases the therapeutic potency of a small molecule inhibitor while minimizing adverse effects. We developed a pharmacophore based on a carbonyloxime (OXIM) scaffold for macrophage migration inhibitory factor (MIF), a protein involved in the pathology of sepsis, to validate that inhibition of a catalytic site could produce therapeutic benefits. We studied the crystal structures of MIF.OXIM-based inhibitors and found two opposite orientations for binding to the active site that were dependent on the chemical structures of an R-group. One orientation was completely unexpected based on previous studies with hydroxyphenylpyruvate and (S,R)-3-(4-hydroxyphenyl)-4,5-dihydro-5-isoxazole acetic acid methyl ester (ISO-1). We further confirmed that the unexpected binding mode targets MIF in cellular studies by showing that one compound, OXIM-11, abolished the counter-regulatory activity of MIF on anti-inflammatory glucocorticoid action. OXIM-11 treatment of mice, initiated 24 h after the onset of cecal ligation and puncture-induced sepsis, significantly improved survival when compared with vehicle-treated controls, confirming that inhibition of the MIF catalytic site could produce therapeutic effects. The crystal structures of the MIF inhibitor complexes provide insight for further structure-based drug design efforts.
药效基团是一种化学骨架,通过在特定位置对化学基团(R基团)进行改变,以确定能提高小分子抑制剂治疗效力同时将副作用降至最低的R基团组合。我们基于羰基肟(OXIM)骨架开发了一种针对巨噬细胞移动抑制因子(MIF)的药效基团,MIF是一种参与脓毒症病理过程的蛋白质,以此来验证抑制催化位点是否能产生治疗效果。我们研究了基于MIF.OXIM的抑制剂的晶体结构,发现与活性位点结合存在两种相反的取向,这取决于R基团的化学结构。基于之前对羟基苯丙酮酸和(S,R)-3-(4-羟基苯基)-4,5-二氢-5-异恶唑乙酸甲酯(ISO-1)的研究,其中一种取向完全出乎意料。我们通过表明一种化合物OXIM-11消除了MIF对抗炎糖皮质激素作用的反调节活性进一步证实,在细胞研究中这种意外结合模式靶向MIF。在盲肠结扎和穿刺诱导的脓毒症发作24小时后开始用OXIM-11治疗小鼠,与用赋形剂处理的对照组相比,显著提高了存活率,证实抑制MIF催化位点可产生治疗效果。MIF抑制剂复合物的晶体结构为进一步基于结构的药物设计努力提供了见解。