首页> 外文期刊>Bioorganic and Medicinal Chemistry Letters >Inhibitors of the acetyltransferase domain of N-acetylglucosamine-1- phosphate-uridylyltransferase/glucosamine-1-phosphate-acetyltransferase (GlmU). Part 2: Optimization of physical properties leading to antibacterial aryl sulfonamides
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Inhibitors of the acetyltransferase domain of N-acetylglucosamine-1- phosphate-uridylyltransferase/glucosamine-1-phosphate-acetyltransferase (GlmU). Part 2: Optimization of physical properties leading to antibacterial aryl sulfonamides

机译:N-乙酰基氨基葡萄糖-1-磷酸-尿苷基转移酶/氨基葡萄糖-1-磷酸-乙酰基转移酶(GlmU)的乙酰基转移酶结构域的抑制剂。第2部分:优化物理性质,从而产生抗菌性芳基磺酰胺

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摘要

A previously described aryl sulfonamide series, originally found through HTS, targets GlmU, a bifunctional essential enzyme involved in bacterial cell wall synthesis. Using structure-guided design, the potency of enzyme inhibition was increased in multiple isozymes from different bacterial species. Unsuitable physical properties (low Log D and high molecular weight) of those compounds prevented them from entering the cytoplasm of bacteria and inhibiting cell growth. Further modifications described herein led to compounds that possessed antibacterial activity, which was shown to occur through inhibition of GlmU. The left-hand side amide and the right-hand side sulfonamides were modified such that enzyme inhibitory activity was maintained (IC50 0.1 μM against GlmU isozymes from Gram-negative organisms), and the lipophilicity was increased giving compounds with Log D -1 to 3. Antibacterial activity in an efflux-pump deficient mutant of Haemophilus influenzae resulted for compounds such as 13.
机译:最初通过HTS找到的先前描述的芳基磺酰胺系列靶向GlmU,GlmU是参与细菌细胞壁合成的一种双功能必需酶。使用结构指导的设计,来自不同细菌物种的多种同工酶的酶抑制能力得到了提高。这些化合物的不合适的物理性质(低Log D和高分子量)阻止它们进入细菌的细胞质并抑制细胞生长。本文所述的进一步修饰导致具有抗菌活性的化合物,该化合物显示出通过抑制GlmU而发生。修饰左侧酰胺和右侧磺酰胺,以保持酶抑制活性(对革兰氏阴性生物的GlmU同工酶的IC50 <0.1μM),并且增加了亲脂性,得到具有Log D -1的化合物3.对诸如13的化合物产生了流感嗜血杆菌外排泵缺陷型突变体的抗菌活性。

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