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内源性卟啉导致休眠状态的耻垢分枝杆菌的光灭活。

Photoinactivation of dormant Mycobacterium smegmatis due to its endogenous porphyrins.

机构信息

A.N. Bach Institute of Biochemistry, Federal Research Centre 'Fundamentals of Biotechnology' of the Russian Academy of Sciences, Moscow, Russia.

出版信息

Appl Microbiol Biotechnol. 2019 Dec;103(23-24):9687-9695. doi: 10.1007/s00253-019-10197-3. Epub 2019 Nov 12.

DOI:10.1007/s00253-019-10197-3
PMID:31713670
Abstract

Mycobacterium tuberculosis is able to transition into a dormant state, causing a latent state of tuberculosis. Dormant mycobacteria acquire phenotypic resistance to all known antibacterial drugs; they are also able to maintain vitality in the host for decades and become active, causing the active form of the disease. In order to cure latent tuberculosis, new approaches should be developed. Earlier, we discovered accumulation in significant concentrations of porphyrins in dormant Mycobacterium smegmatis, which is a close, fast-growing relative of the causative agent of tuberculosis. In this study, we explore a new possibility to kill dormant mycobacteria by photodynamic inactivation (PDI) using accumulated porphyrins as endogenous photosensitisers. The dormant M. smegmatis were obtained under gradual acidification in Sauton's medium, for 14 days. Cells were exposed to light with different wavelengths emitted by three Spectra X light-emitting diodes (395/25, 470/24, 575/25 nm) and one separated 634-nm LED for 15 min. An increase in the concentration of coproporphyrin in M. smegmatis after 6 days of growth correlated with the beginning of a decrease in metabolic activity and formation of ovoid dormant forms. Dormant bacteria were sensitive to PDI and killed after 15-30 min of illumination, in contrast to active cells. The greatest inactivation of dormant mycobacteria occurred at 395 and 575 nm, which coincides with the main maximum of the absorption spectrum of extracted porphyrins. We, for the first time, demonstrate a successful application of PDI for inactivation of dormant mycobacteria, due to significant accumulation of endogenous photosensitisers-porphyrins.

摘要

结核分枝杆菌能够进入休眠状态,导致潜伏性结核病。休眠分枝杆菌对所有已知的抗菌药物表现出表型耐药性;它们还能够在宿主内存活数十年并变得活跃,引起疾病的活动形式。为了治愈潜伏性结核病,应该开发新的方法。早些时候,我们发现休眠的耻垢分枝杆菌中卟啉积累到显著浓度,耻垢分枝杆菌是结核病病原体的密切、快速生长的近亲。在这项研究中,我们探索了一种新的可能性,即通过光动力失活 (PDI) 使用积累的卟啉作为内源性光敏剂来杀死休眠分枝杆菌。在 Sauton 培养基中逐渐酸化的条件下获得休眠的耻垢分枝杆菌,持续 14 天。将细胞暴露于三种 Spectra X 发光二极管 (395/25、470/24、575/25nm) 和一个单独的 634nm LED 发出的不同波长的光下照射 15 分钟。在生长 6 天后,耻垢分枝杆菌中粪卟啉原的浓度增加与代谢活性下降和形成椭圆形休眠形式的开始相关。休眠细菌对 PDI 敏感,并在 15-30 分钟的光照后被杀死,与活性细胞相反。休眠分枝杆菌的最大失活发生在 395nm 和 575nm,这与提取卟啉的吸收光谱的主要最大值相吻合。我们首次证明了由于内源性光敏剂-卟啉的显著积累,PDI 成功应用于休眠分枝杆菌的失活。

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