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Potent Antipneumococcal Activity of Gemifloxacin Is Associated with Dual Targeting of Gyrase and Topoisomerase IV an In Vivo Target Preference for Gyrase and Enhanced Stabilization of Cleavable Complexes In Vitro

机译：吉米沙星的有效抗肺炎球菌活性与回旋酶和拓扑异构酶IV的双重靶向回旋酶的体内靶标相关并增强了可裂解复合物的体外稳定性

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We investigated the roles of DNA gyrase and topoisomerase IV in determining the susceptibility of Streptococcus pneumoniae to gemifloxacin, a novel fluoroquinolone which is under development as an antipneumococcal drug. Gemifloxacin displayed potent activity against S. pneumoniae 7785 (MIC, 0.06 μg/ml) compared with ciprofloxacin (MIC, 1 to 2 μg/ml). Complementary genetic and biochemical approaches revealed the following. (i) The gemifloxacin MICs for isogenic 7785 mutants bearing either parC or gyrA quinolone resistance mutations were marginally higher than wild type at 0.12 to 0.25 μg/ml, whereas the presence of both mutations increased the MIC to 0.5 to 1 μg/ml. These data suggest that both gyrase and topoisomerase IV contribute significantly as gemifloxacin targets in vivo. (ii) Gemifloxacin selected first-step gyrA mutants of S. pneumoniae 7785 (gemifloxacin MICs, 0.25 μg/ml) encoding Ser-81 to Phe or Tyr, or Glu-85 to Lys mutations. These mutants were cross resistant to sparfloxacin (which targets gyrase) but not to ciprofloxacin (which targets topoisomerase IV). Second-step mutants (gemifloxacin MICs, 1 μg/ml) exhibited an alteration in parC resulting in changes of ParC hot spot Ser-79 to Phe or Tyr. Thus, gyrase appears to be the preferential in vivo target. (iii) Gemifloxacin was at least 10- to 20-fold more effective than ciprofloxacin in stabilizing a cleavable complex (the cytotoxic lesion) with either S. pneumoniae gyrase or topoisomerase IV enzyme in vitro. These data suggest that gemifloxacin is an enhanced affinity fluoroquinolone that acts against gyrase and topoisomerase IV in S. pneumoniae, with gyrase the preferred in vivo target. The marked potency of gemifloxacin against wild type and quinolone-resistant mutants may accrue from greater stabilization of cleavable complexes with the target enzymes.

机译：我们研究了DNA促旋酶和拓扑异构酶IV在确定肺炎链球菌对吉非沙星（一种正在开发为抗肺炎球菌药物的新型氟喹诺酮）的敏感性中的作用。与环丙沙星（MIC，1至2μg/ ml）相比，吉米沙星对肺炎链球菌7785（MIC，0.06μg/ ml）表现出强效活性。互补的遗传和生化方法揭示了以下内容。（i）带有parC或gyrA喹诺酮耐药性突变的等基因7785个突变体的吉非沙星MIC略高于野生型，为0.12至0.25μg/ ml，而两种突变的存在均将MIC提高至0.5至1μg/ ml。这些数据表明，回旋酶和拓扑异构酶IV均作为吉非沙星在体内的靶标。（ii）吉米沙星选择了肺炎链球菌7785的第一步gyrA突变体（吉米沙星MIC，0.25μg/ ml），其Ser-81编码为Phe或Tyr，Glu-85编码为Lys突变。这些突变体对sparfloxacin（靶向促旋酶）有交叉耐药性，但对环丙沙星（靶向拓扑异构酶IV）却没有交叉耐药性。第二步突变体（吉米沙星MIC，1μg/ ml）显示parC发生变化，导致ParC热点Ser-79变为Phe或Tyr。因此，回旋酶似乎是优先的体内靶标。（iii）在体外用肺炎链球菌回旋酶或拓扑异构酶IV酶稳定可裂解复合物（细胞毒性病变）方面，吉米沙星比环丙沙星至少有效10到20倍。这些数据表明吉非沙星是一种增强的亲和力氟喹诺酮，可对抗肺炎链球菌中的回旋酶和拓扑异构酶IV，回旋酶是优选的体内靶标。吉非沙星对野生型和喹诺酮耐药突变体的显着效力可能来自与目标酶的可裂解复合物的更大稳定性。

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期刊名称 Antimicrobial Agents and Chemotherapy
作者
Victoria J. Heaton; Jane E. Ambler; L. Mark Fisher;
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年(卷),期 2000(44),11
年度 2000
页码 3112–3117
总页数 6
原文格式 PDF
正文语种
中图分类药学;微生物学;
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专利

1. Potent antipneumococcal activity of gemifloxacin is associated with dual targeting of gyrase and topoisomerase IV, an in vivo target preference for gyrase, and enhanced stabilization of cleavable complexes in vitro. [J] . Heaton VJ, Ambler JE, Fisher LM Antimicrobial agents and chemotherapy. . 2000,第11期

机译：吉非沙星的有效抗肺炎球菌活性与回旋酶和拓扑异构酶IV的双重靶向作用，对回旋酶的体内靶标偏爱以及增强的可裂解复合物的体外稳定性有关。
2. Novel dual-targeting benzimidazole urea inhibitors of DNA gyrase and topoisomerase IV possessing potent antibacterial activity: Intelligent design and evolution through the judicious use of structure-guided design and stucture-activity relationships [J] . Charifson PS, Grillot AL, Grossman TH, Journal of Medicinal Chemistry . 2008,第17期

机译：具有强力抗菌活性的新型DNA促旋酶和拓扑异构酶IV双靶标苯并咪唑脲抑制剂：通过明智地使用结构指导的设计和结构与活性的关系，智能设计和开发
3. Pyrrolopyrimidine inhibitors of DNA gyrase B (GyrB) and topoisomerase IV (ParE). Part I: Structure guided discovery and optimization of dual targeting agents with potent, broad-spectrum enzymatic activity [J] . TariL.W., TrzossM., BensenD.C., Bioorganic and Medicinal Chemistry Letters . 2013,第5期

机译：DNA旋转酶B（GyrB）和拓扑异构酶IV（PARE）的吡咯哒嘧啶抑制剂。第一部分：结构引导和优化双靶向剂，具有效率，广谱酶活性
4. Design, Synthesis, Biophysical and Structure-Activity Properties of a Novel Dual MDM2 and MDMX Targeting Stapled α-Helical Peptide: ATSP-7041 Exhibits Potent In Vitro and In Vivo Efficacy in Xenograft Models of Human Cancer [C] . V. Guerlavais, K. Darlak, B. Graves American Peptide Symposium . 2013

机译：新型双MDM2和MDMX靶向吻合α-螺旋肽的设计，合成，生物物理和结构 - 活性特性：ATSP-7041在体外表现出效率和体内人类癌症的模型
5. Targeting of DNA gyrase in Streptococcus pneumoniae by sparfloxacin: selective targeting of gyrase or topoisomerase IV by quinolones. [O] . X S Pan, L M Fisher 1997

机译：司帕沙星靶向肺炎链球菌中的DNA促旋酶：喹诺酮类药物选择性靶向促旋酶或拓扑异构酶IV。
6. Potent Antipneumococcal Activity of Gemifloxacin Is Associated with Dual Targeting of Gyrase and Topoisomerase IV, an In Vivo Target Preference for Gyrase, and Enhanced Stabilization of Cleavable Complexes In Vitro [O] . Heaton, Victoria J., Ambler, Jane E., Fisher, L. Mark 2000

机译：吉米沙星的有效抗肺炎球菌活性与回旋酶和拓扑异构酶IV的双重靶向，回旋酶的体内靶标相关，并增强了可裂解复合物的体外稳定性

Potent Antipneumococcal Activity of Gemifloxacin Is Associated with Dual Targeting of Gyrase and Topoisomerase IV an In Vivo Target Preference for Gyrase and Enhanced Stabilization of Cleavable Complexes In Vitro

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