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Exploiting the porin pathway for polar compound delivery into Gram-negative bacteria

机译:利用孔蛋白途径将极性化合物递送至革兰氏阴性细菌

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Background: In Gram-negative bacteria, the outer-membrane represents an additional barrier for antibiotics to permeate inside pathogens. Our inability to come up with novel effective antibiotics mostly relies upon insufficient understanding of the molecular basis behind outer-membrane penetration. Results: Polar antibiotics can permeate through water-filled porins, such as OmpF and OmpC from Escherichia coli. Through molecular modeling, permeation of imipenem and meropenem was found to be strongly dependent upon capability of drugs to properly align their electric dipole to the internal electric field in the restricted region of the pore. Electrostatics differences between OmpF and OmpC, and modifications along a series of OmpC mutants from E. coli-resistant clinical strains identify a 'preorientation' region, which dramatically affects antibiotic pathway. Conclusion: A novel perspective is presented, suggesting new molecular properties to be included in drug design.
机译:背景:在革兰氏阴性细菌中,外膜代表了抗生素渗透到病原体内部的另一道屏障。我们无法提出新颖有效的抗生素主要是由于对外膜渗透背后的分子基础了解不足。结果:极性抗生素可渗透到充满水的孔蛋白中,例如大肠杆菌中的OmpF和OmpC。通过分子建模,发现亚胺培南和美罗培南的渗透强烈依赖于药物将其电偶极子与孔的受限区域中的内部电场正确对齐的能力。 OmpF和OmpC之间的静电学差异以及对一系列Emp耐药性临床菌株的OmpC突变体的修饰,确定了一个“预定向”区域,该区域会显着影响抗生素途径。结论:提出了一种新颖的观点,表明新的分子特性将被包括在药物设计中。

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