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广谱抗病毒化合物ST-669可限制衣原体包涵体的形成和细菌生长,并定位于经处理细胞内的宿主细胞脂滴中。

The broad-spectrum antiviral compound ST-669 restricts chlamydial inclusion development and bacterial growth and localizes to host cell lipid droplets within treated cells.

作者信息

Sandoz Kelsi M, Valiant William G, Eriksen Steven G, Hruby Dennis E, Allen Robert D, Rockey Daniel D

机构信息

Department of Biomedical Sciences, Oregon State University, Corvallis, Oregon, USA.

Siga Technologies, Inc., Corvallis, Oregon, USA.

出版信息

Antimicrob Agents Chemother. 2014 Jul;58(7):3860-6. doi: 10.1128/AAC.02064-13. Epub 2014 Apr 28.

DOI:10.1128/AAC.02064-13
PMID:24777097
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4068599/
Abstract

Novel broad-spectrum antimicrobials are a critical component of a strategy for combating antibiotic-resistant pathogens. In this study, we explored the activity of the broad-spectrum antiviral compound ST-669 for activity against different intracellular bacteria and began a characterization of its mechanism of antimicrobial action. ST-669 inhibits the growth of three different species of chlamydia and the intracellular bacterium Coxiella burnetii in Vero and HeLa cells but not in McCoy (murine) cells. The antichlamydial and anti-C. burnetii activity spectrum was consistent with those observed for tested viruses, suggesting a common mechanism of action. Cycloheximide treatment in the presence of ST-669 abrogated the inhibitory effect, demonstrating that eukaryotic protein synthesis is required for tested activity. Immunofluorescence microscopy demonstrated that different chlamydiae grow atypically in the presence of ST-669, in a manner that suggests the compound affects inclusion formation and organization. Microscopic analysis of cells treated with a fluorescent derivative of ST-669 demonstrated that the compound localized to host cell lipid droplets but not to other organelles or the host cytosol. These results demonstrate that ST-669 affects intracellular growth in a host-cell-dependent manner and interrupts proper development of chlamydial inclusions, possibly through a lipid droplet-dependent process.

摘要

新型广谱抗菌剂是对抗抗生素耐药病原体策略的关键组成部分。在本研究中,我们探究了广谱抗病毒化合物ST-669对不同细胞内细菌的活性,并开始对其抗菌作用机制进行表征。ST-669可抑制三种不同衣原体物种以及细胞内细菌伯纳特立克次体在Vero和HeLa细胞中的生长,但在 McCoy(小鼠)细胞中无此作用。抗衣原体和抗伯纳特立克次体的活性谱与测试病毒所观察到的一致,表明存在共同的作用机制。在ST-669存在的情况下进行环己酰亚胺处理可消除抑制作用,表明真核生物蛋白质合成是测试活性所必需的。免疫荧光显微镜检查表明,在ST-669存在的情况下,不同的衣原体生长异常,其方式表明该化合物会影响包涵体的形成和组织。对用ST-669荧光衍生物处理的细胞进行显微镜分析表明,该化合物定位于宿主细胞脂滴,而非其他细胞器或宿主细胞质。这些结果表明,ST-669以宿主细胞依赖的方式影响细胞内生长,并可能通过脂滴依赖过程干扰衣原体包涵体的正常发育。

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