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首页> 外文期刊>Organic & biomolecular chemistry >Synthesis and evaluation of inhibitors of E. coli PgaB, a polysaccharide de-N-acetylase involved in biotilm formation
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Synthesis and evaluation of inhibitors of E. coli PgaB, a polysaccharide de-N-acetylase involved in biotilm formation

机译:E. coli PgaB抑制剂的合成和评估,E。coli PgaB是一种参与生物菌体形成的多糖脱N-乙酰酶

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摘要

Many medically important biofilm forming bacteria produce similar polysaccharide intercellular adhesins (PIA) consisting of partially de-Af-acetylated β-(1→ 6)-N-acetylglucosamme polymers (dPNAG). In Escherichia coli, de-N-acetylation of the β-(1→ 6)-7V-acetylglucosamine polymer (PNAG) is catalysed by the carbohydrate esterase family 4 deacetylase PgaB. The de-N-acetylation of PNAG is essential for productive PNAG-dependent biofilm formation. Here, we describe the development of a fluorogenic assay to monitor PgaB activity in vitro and the synthesis of a series of PgaB inhibitors. The synthesized inhibitors consist of a metal chelating functional group on a glucosamine scaffold to target the active site metal ion of PgaB. Optimal inhibition was observed with N-thioglycolyl amide (K_i = 480 μM) and N-methyl-Nglycolyl amide (K_i= 320 μM) glucosamine derivatives. A chemoenzymatic synthesis of an N-thioglycolyl amide PNAG pentasaccharide led to an inhibitor with an improved K_i; of 280μm.
机译:许多医学上重要的生物膜形成细菌会产生类似的多糖细胞间粘附素(PIA),由部分去Af-乙酰化的β-(1→6)-N-乙酰氨基葡萄糖聚合物(dPNAG)组成。在大肠杆菌中,碳水化合物酯酶家族4脱乙酰基酶PgaB催化β-(1→6)-7V-乙酰基葡糖胺聚合物(PNAG)的脱N-乙酰化。 PNAG的脱N-乙酰化对于生产性PNAG依赖的生物膜形成至关重要。在这里,我们描述了检测体外PgaB活性的荧光检测方法的开发以及一系列PgaB抑制剂的合成。合成的抑制剂由葡糖胺支架上的金属螯合官能团组成,以靶向PgaB的活性位点金属离子。用N-硫代糖基酰胺(K_i = 480μM)和N-甲基-N-糖基酰胺(K_i = 320μM)葡糖胺衍生物观察到最佳抑制作用。化学合成N-硫代乙醇酰基酰胺PNAG五糖导致抑制剂的K_i值提高; 280μm

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  • 来源
    《Organic & biomolecular chemistry》 |2012年第35期|p.7103-7107|共5页
  • 作者单位

    Department of Chemistry, University of Toronto, Toronto, Ontario M5S 3H6, Canada;

    Department of Chemistry, University of Toronto, Toronto, Ontario M5S 3H6, Canada;

    Program in Molecular Structure and Function, The Hospital of Sick Children and Department of Biochemistry, University of Toronto, Ontario M5G 1X8, Canada;

    Program in Molecular Structure and Function, The Hospital of Sick Children and Department of Biochemistry, University of Toronto, Ontario M5G 1X8, Canada;

    Department of Chemistry, University of Toronto, Toronto, Ontario M5S 3H6, Canada;

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