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对新型抗衣原体化合物的耐药性是通过沙眼衣原体 secY 中的突变介导的。

Resistance to a novel antichlamydial compound is mediated through mutations in Chlamydia trachomatis secY.

机构信息

Molecular and Cellular Biology Program, Oregon State University, Corvallis, Oregon, USA.

出版信息

Antimicrob Agents Chemother. 2012 Aug;56(8):4296-302. doi: 10.1128/AAC.00356-12. Epub 2012 May 29.

DOI:10.1128/AAC.00356-12
PMID:22644029
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3421553/
Abstract

A novel and quantitative high-throughput screening approach was explored as a tool for the identification of novel compounds that inhibit chlamydial growth in mammalian cells. The assay is based on accumulation of a fluorescent marker by intracellular chlamydiae. Its utility was demonstrated by screening 42,000 chemically defined compounds against Chlamydia caviae GPIC. This analysis led to the identification of 40 primary-hit compounds. Five of these compounds were nontoxic to host cells and had similar activities against both C. caviae GPIC and Chlamydia trachomatis. The inhibitory activity of one of the compounds, (3-methoxyphenyl)-(4,4,7-trimethyl-4,5-dihydro-1H-[1,2]dithiolo[3,4-C]quinolin-1-ylidene)amine (MDQA), was chlamydia specific and was selected for further study. Selection for resistance to MDQA led to the generation of three independent resistant clones of C. trachomatis. Amino acid changes in SecY, a protein involved in Sec-dependent secretion in Gram-negative bacteria, were associated with the resistance phenotype. The amino acids changed in each of the resistant mutants are located in the predicted central channel of a SecY crystal structure, based on the known structure of Thermus thermophilus SecY. These experiments model a process that can be used for the discovery of antichlamydial, anti-intracellular, or antibacterial compounds and has led to the identification of compounds that may have utility in both antibiotic discovery and furthering our understanding of chlamydial biology.

摘要

一种新颖的高通量筛选方法被探索出来,作为鉴定抑制哺乳动物细胞中衣原体生长的新型化合物的工具。该测定法基于细胞内衣原体积累荧光标记物。通过筛选 42000 种化学定义的化合物对衣原体 GPIC 进行了验证,证明了其有效性。该分析导致鉴定出 40 种主要命中化合物。其中 5 种化合物对宿主细胞无毒,对衣原体 GPIC 和沙眼衣原体均具有相似的活性。其中一种化合物,(3-甲氧基苯基)-(4,4,7-三甲基-4,5-二氢-1H-[1,2]二噻咯[3,4-C]喹啉-1-亚基)胺(MDQA)的抑制活性具有衣原体特异性,并被选为进一步研究。选择对 MDQA 的抗性导致产生了三种独立的沙眼衣原体抗性克隆。与耐药表型相关的是,SecY 蛋白(一种参与革兰氏阴性细菌 Sec 依赖性分泌的蛋白质)中的氨基酸发生了变化。每个抗性突变体中发生变化的氨基酸都位于 SecY 晶体结构的预测中央通道中,该结构基于耐热栖热菌 SecY 的已知结构。这些实验模拟了一个可以用于发现抗衣原体、抗细胞内或抗细菌化合物的过程,并鉴定出可能在抗生素发现和进一步了解衣原体生物学方面具有用途的化合物。

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本文引用的文献

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The SecY complex: conducting the orchestra of protein translocation.SecY 复合物:指挥蛋白易位的管弦乐队。
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Specific chlamydial inclusion membrane proteins associate with active Src family kinases in microdomains that interact with the host microtubule network.特定的衣原体包涵体膜蛋白与小窝内的活性Src 家族激酶相关,这些激酶与宿主微管网络相互作用。
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Impact of azithromycin resistance mutations on the virulence and fitness of Chlamydia caviae in guinea pigs.阿奇霉素耐药突变对豚鼠鹦鹉热衣原体毒力和适应性的影响。
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The chlamydial functional homolog of KsgA confers kasugamycin sensitivity to Chlamydia trachomatis and impacts bacterial fitness.沙眼衣原体 KsgA 的功能同源物赋予了杀霉素敏感性,并影响了细菌的适应性。
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Protein structure prediction on the Web: a case study using the Phyre server.网络上的蛋白质结构预测:使用Phyre服务器的案例研究
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Rifalazil retains activity against rifampin-resistant mutants of Chlamydia pneumoniae.利福拉齐对肺炎衣原体耐利福平突变株仍具有活性。
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