Rocha Kenneth, Magallon Jesus, Reeves Craig, Phan Kimberly, Vu Peter, Oakley-Havens Crista L, Kwan Stella, Ramirez Maria Soledad, LaVoi Travis, Donow Haley, Chapagain Prem, Santos Radleigh, Pinilla Clemencia, Giulianotti Marc A, Tolmasky Marcelo E
Center for Applied Biotechnology Studies, Department of Biological Science, College of Natural Sciences and Mathematics, California State University Fullerton, Fullerton, CA 92831, USA.
Center for Translational Science, Florida International University, Port St. Lucie, FL 34987, USA.
Biomedicines. 2021 Sep 14;9(9):1218. doi: 10.3390/biomedicines9091218.
The aminoglycoside 6'--acetyltransferase type Ib (AAC(6')-Ib) is a common cause of resistance to amikacin and other aminoglycosides in Gram-negatives. Utilization of mixture-based combinatorial libraries and application of the positional scanning strategy identified an inhibitor of AAC(6')-Ib. This inhibitor's chemical structure consists of a pyrrolidine pentamine scaffold substituted at four locations (R1, R3, R4, and R5). The substituents are two -phenyl groups (R1 and R4), an -hydroxymethyl group (R3), and a 3-phenylbutyl group (R5). Another location, R2, does not have a substitution, but it is named because its stereochemistry was modified in some compounds utilized in this study. Structure-activity relationship (SAR) analysis using derivatives with different functionalities, modified stereochemistry, and truncations was carried out by assessing the effect of the addition of each compound at 8 µM to 16 µg/mL amikacin-containing media and performing checkerboard assays varying the concentrations of the inhibitor analogs and the antibiotic. The results show that: (1) the aromatic functionalities at R1 and R4 are essential, but the stereochemistry is essential only at R4; (2) the stereochemical conformation at R2 is critical; (3) the hydroxyl moiety at R3 as well as stereoconformation are required for full inhibitory activity; (4) the phenyl functionality at R5 is not essential and can be replaced by aliphatic groups; (5) the location of the phenyl group on the butyl carbon chain at R5 is not essential; (6) the length of the aliphatic chain at R5 is not critical; and (7) all truncations of the scaffold resulted in inactive compounds. Molecular docking revealed that all compounds preferentially bind to the kanamycin C binding cavity, and binding affinity correlates with the experimental data for most of the compounds evaluated. The SAR results in this study will serve as the basis for the design of new analogs in an effort to improve their ability to induce phenotypic conversion to susceptibility in amikacin-resistant pathogens.
氨基糖苷类6'-乙酰基转移酶Ib型(AAC(6')-Ib)是革兰氏阴性菌对阿米卡星和其他氨基糖苷类药物耐药的常见原因。利用基于混合物的组合文库并应用位置扫描策略鉴定出了一种AAC(6')-Ib抑制剂。该抑制剂的化学结构由一个在四个位置(R1、R3、R4和R5)被取代的吡咯烷五胺支架组成。取代基为两个苯基(R1和R4)、一个羟甲基(R3)和一个3-苯基丁基(R5)。另一个位置R2没有取代基,但因其立体化学在本研究中使用的一些化合物中被修饰而得名。通过评估在含8 μM至16 μg/mL阿米卡星的培养基中添加每种化合物的效果,并进行棋盘法实验来改变抑制剂类似物和抗生素的浓度,使用具有不同官能团、修饰的立体化学和截短的衍生物进行了构效关系(SAR)分析。结果表明:(1)R1和R4处的芳香官能团是必需的,但立体化学仅在R4处是必需的;(2)R2处的立体化学构象至关重要;(3)R3处的羟基部分以及立体构象对于完全抑制活性是必需的;(4)R5处的苯基官能团不是必需的,可以被脂肪族基团取代;(5)R5处丁基碳链上苯基的位置不是必需的;(6)R5处脂肪族链的长度不关键;(7)支架的所有截短都导致化合物无活性。分子对接显示所有化合物优先结合到卡那霉素C结合腔,并且结合亲和力与大多数评估化合物的实验数据相关。本研究中的SAR结果将作为设计新类似物的基础,以努力提高它们在耐阿米卡星病原体中诱导表型转化为敏感性的能力。
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