抗菌细胞分裂抑制剂 PC190723 是一种 FtsZ 聚合稳定剂,可诱导丝状体组装和浓缩。
The antibacterial cell division inhibitor PC190723 is an FtsZ polymer-stabilizing agent that induces filament assembly and condensation.
机构信息
Centro de Investigaciones Biológicas, Consejo Superior de Investigaciones Cientificas, Ramiro de Maeztu 9, Spain.
出版信息
J Biol Chem. 2010 May 7;285(19):14239-46. doi: 10.1074/jbc.M109.094722. Epub 2010 Mar 8.
Cell division protein FtsZ can form single-stranded filaments with a cooperative behavior by self-switching assembly. Subsequent condensation and bending of FtsZ filaments are important for the formation and constriction of the cytokinetic ring. PC190723 is an effective bactericidal cell division inhibitor that targets FtsZ in the pathogen Staphylococcus aureus and Bacillus subtilis and does not affect Escherichia coli cells, which apparently binds to a zone equivalent to the binding site of the antitumor drug taxol in tubulin (Haydon, D. J., Stokes, N. R., Ure, R., Galbraith, G., Bennett, J. M., Brown, D. R., Baker, P. J., Barynin, V. V., Rice, D. W., Sedelnikova, S. E., Heal, J. R., Sheridan, J. M., Aiwale, S. T., Chauhan, P. K., Srivastava, A., Taneja, A., Collins, I., Errington, J., and Czaplewski, L. G. (2008) Science 312, 1673-1675). We have found that the benzamide derivative PC190723 is an FtsZ polymer-stabilizing agent. PC190723 induced nucleated assembly of Bs-FtsZ into single-stranded coiled protofilaments and polymorphic condensates, including bundles, coils, and toroids, whose formation could be modulated with different solution conditions. Under conditions for reversible assembly of Bs-FtsZ, PC190723 binding reduced the GTPase activity and induced the formation of straight bundles and ribbons, which was also observed with Sa-FtsZ but not with nonsusceptible Ec-FtsZ. The fragment 2,6-difluoro-3-methoxybenzamide also induced Bs-FtsZ bundling. We propose that polymer stabilization by PC190723 suppresses in vivo FtsZ polymer dynamics and bacterial division. The biochemical action of PC190723 on FtsZ parallels that of the microtubule-stabilizing agent taxol on the eukaryotic structural homologue tubulin. Both taxol and PC190723 stabilize polymers against disassembly by preferential binding to each assembled protein. It is yet to be investigated whether both ligands target structurally related assembly switches.
细胞分裂蛋白 FtsZ 可以通过自身开关组装形成具有协同行为的单链丝状纤维。随后 FtsZ 丝的浓缩和弯曲对于细胞分裂环的形成和收缩很重要。PC190723 是一种有效的杀菌细胞分裂抑制剂,它以金黄色葡萄球菌和枯草芽孢杆菌中的 FtsZ 为靶点,而不影响大肠杆菌细胞,显然它与微管中抗肿瘤药物紫杉醇的结合位点等效(Haydon,DJ,Stokes,NR,Ure,R.,Galbraith,G.,Bennett,JM,Brown,DR,Baker,PJ,Barynin,VV,Rice,DW,Sedelnikova,SE,Heal,JR,Sheridan,JM,Aiwale,ST,Chauhan,PK,Srivastava,A.,Taneja,A.,Collins,I.,Errington,J.,和 Czaplewski,LG.(2008)科学 312,1673-1675)。我们发现苯甲酰胺衍生物 PC190723 是一种 FtsZ 聚合物稳定剂。PC190723 诱导 Bs-FtsZ 成核组装成单链螺旋原丝和多态凝聚物,包括束、线圈和环,其形成可以通过不同的溶液条件进行调节。在 Bs-FtsZ 可逆组装的条件下,PC190723 结合降低了 GTPase 活性并诱导了直束和带状物的形成,这也观察到了 Sa-FtsZ 但不是非易感 Ec-FtsZ。片段 2,6-二氟-3-甲氧基苯甲酰胺也诱导了 Bs-FtsZ 束。我们提出,PC190723 通过聚合物稳定抑制了体内 FtsZ 聚合物动力学和细菌分裂。PC190723 对 FtsZ 的生化作用类似于微管稳定剂紫杉醇对真核结构同源物微管蛋白的作用。紫杉醇和 PC190723 通过优先结合每个组装蛋白来稳定聚合物防止解组装。尚待研究这两种配体是否都针对结构相关的组装开关。
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