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Monitoring Tuberculosis Drug Activity in Live Animals by Using Near-Infrared Fluorescence Imaging

机译:通过使用近红外荧光成像监测活血中的结核病药物活性

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摘要

Worldwide, tuberculosis (TB) is the leading cause of death due to infection with a single pathogenic agent, Mycobacterium tuberculosis. In the absence of an effective vaccine, new, more powerful antibiotics are required to halt the growing spread of multidrug-resistant strains and to shorten the duration of TB treatment. However, assessing drug efficacy at the preclinical stage remains a long and fastidious procedure that delays the progression of drugs down the pipeline and towards the clinic. In this investigation, we report the construction, optimization, and characterization of genetically engineered near-infrared (NIR) fluorescent reporter strains of the pathogens Mycobacterium marinum and Mycobacterium tuberculosis that enable the direct visualization of bacteria in infected zebrafish and mice, respectively. Fluorescence could be measured precisely in infected immunodeficient mice, while its intensity appeared to be below the limit of detection in immunocompetent mice, probably because of the lower bacterial load obtained in these animals. Furthermore, we show that the fluorescence level accurately reflects the bacterial load, as determined by CFU enumeration, thus enabling the efficacy of antibiotic treatment to be assessed in live animals in real time. The NIR fluorescent imaging system disclosed here is a valuable resource for TB research and can serve to accelerate drug development.
机译:在全球范围内,结核病(TB)是由于具有单一致病剂,结核分枝杆菌的感染导致死亡原因。在没有有效的疫苗的情况下,需要新的更强大的抗生素来停止多药抗性菌株的越来越多的蔓延,并缩短结核病治疗的持续时间。然而,评估临床前阶段的药物效果仍然是一种长而尖锐的程序,延迟了管道和诊所的药物进展。在这项调查中,我们报告了基因工程近红外(NIR)荧光报道菌株的施工,优化和表征分枝杆菌和结核分枝杆菌分枝杆菌的荧光报道菌株分别能够分别直接可视化受感染的斑马鱼和小鼠的细菌。荧光可以精确测量在感染的免疫缺陷小鼠中,而其强度似乎低于免疫活性小鼠的检测极限,可能是因为这些动物中获得的细菌载量降低。此外,我们表明荧光水平精确地反映了由CFU枚举确定的细菌载荷,从而使抗生素治疗能够实时在活体动物中进行评估。这里公开的NIR荧光成像系统是TB研究的有价值的资源,并且可以用于加速药物发育。

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