Molecular Pharmacology and Chemistry Program and Tri-Institutional Research Program, Memorial Sloan-Kettering Cancer Center, New York, NY 10065, USA.
Chembiochem. 2012 Jan 2;13(1):129-36. doi: 10.1002/cbic.201100585. Epub 2011 Nov 23.
MenE, the o-succinylbenzoate (OSB)-CoA synthetase from bacterial menaquinone biosynthesis, is a promising new antibacterial target. Sulfonyladenosine analogues of the cognate reaction intermediate, OSB-AMP, have been developed as inhibitors of the MenE enzymes from Mycobacterium tuberculosis (mtMenE), Staphylococcus aureus (saMenE) and Escherichia coli (ecMenE). Both a free carboxylate and a ketone moiety on the OSB side chain are required for potent inhibitory activity. OSB-AMS (4) is a competitive inhibitor of mtMenE with respect to ATP (K(i) =5.4±0.1 nM) and a noncompetitive inhibitor with respect to OSB (K(i) =11.2±0.9 nM). These data are consistent with a Bi Uni Uni Bi Ping-Pong kinetic mechanism for these enzymes. In addition, OSB-AMS inhibits saMenE with K(i)(app) =22±8 nM and ecMenE with K(i)(OSB) =128±5 nM. Putative active-site residues, Arg222, which may interact with the OSB aromatic carboxylate, and Ser302, which may bind the OSB ketone oxygen, have been identified through computational docking of OSB-AMP with the unliganded crystal structure of saMenE. A pH-dependent interconversion of the free keto acid and lactol forms of the inhibitors is also described, along with implications for inhibitor design.
MenE 是细菌甲萘醌生物合成中的 o-琥珀酰苯甲酸(OSB)-CoA 合成酶,是一种很有前途的新型抗菌靶标。作为 MenE 酶(结核分枝杆菌 mtMenE、金黄色葡萄球菌 saMenE 和大肠杆菌 ecMenE)的同源反应中间体 OSB-AMP 的磺酰腺苷类似物已被开发为抑制剂。OSB 侧链上的游离羧酸盐和酮部分对于有效的抑制活性都是必需的。OSB-AMS(4)是 mtMenE 相对于 ATP(K(i) =5.4±0.1 nM)的竞争性抑制剂,相对于 OSB(K(i) =11.2±0.9 nM)是非竞争性抑制剂。这些数据与这些酶的双 Uni Uni Bi Ping-Pong 动力学机制一致。此外,OSB-AMS 抑制 saMenE 的 K(i)(app) =22±8 nM,抑制 ecMenE 的 K(i)(OSB) =128±5 nM。通过对 saMenE 未配体晶体结构进行 OSB-AMP 的计算对接,确定了可能与 OSB 芳基羧酸盐相互作用的推定活性位点残基 Arg222 和可能与 OSB 酮氧结合的 Ser302。还描述了抑制剂的游离酮酸和内醇形式之间的 pH 依赖性互变,以及对抑制剂设计的影响。
