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吩噻嗪鎓类抗菌光敏剂是细菌多药耐药泵的底物。

Phenothiazinium antimicrobial photosensitizers are substrates of bacterial multidrug resistance pumps.

作者信息

Tegos George P, Hamblin Michael R

机构信息

BAR414, Wellman Center for Photomedicine, Massachusetts General Hospital, 40 Blossom Street, Boston, Massachusetts 02114, USA.

出版信息

Antimicrob Agents Chemother. 2006 Jan;50(1):196-203. doi: 10.1128/AAC.50.1.196-203.2006.

Abstract

Antimicrobial photodynamic therapy (PDT) combines a nontoxic photoactivatable dye, or photosensitizer (PS), with harmless visible light to generate singlet oxygen and free radicals that kill microbial cells. Although the light can be focused on the diseased area, the best selectivity is achieved by choosing a PS that binds and penetrates microbial cells. Cationic phenothiazinium dyes, such as methylene blue and toluidine blue O, have been studied for many years and are the only PSs used clinically for antimicrobial PDT. Multidrug resistance pumps (MDRs) are membrane-localized proteins that pump drugs out of cells and have been identified for a wide range of organisms. We asked whether phenothiazinium salts with structures that are amphipathic cations could potentially be substrates of MDRs. We used MDR-deficient mutants of Staphylococcus aureus (NorA), Escherichia coli (TolC), and Pseudomonas aeruginosa (MexAB) and found 2 to 4 logs more killing than seen with wild-type strains by use of three different phenothiazinium PSs and red light. Mutants that overexpress MDRs were protected from killing compared to the wild type. Effective antimicrobial PSs of different chemical structures showed no difference in light-mediated killing depending on MDR phenotype. Differences in uptake of phenothiazinium PS by the cells depending on level of MDR expression were found. We propose that specific MDR inhibitors could be used in combination with phenothiazinium salts to enhance their photodestructive efficiency.

摘要

抗菌光动力疗法(PDT)将无毒的光可激活染料或光敏剂(PS)与无害的可见光相结合,以产生单线态氧和自由基来杀死微生物细胞。尽管光可以聚焦在患病区域,但通过选择能够结合并穿透微生物细胞的PS可实现最佳的选择性。阳离子吩噻嗪染料,如亚甲蓝和甲苯胺蓝O,已被研究多年,并且是临床上唯一用于抗菌PDT的PS。多药耐药泵(MDR)是位于细胞膜上的蛋白质,可将药物泵出细胞,并且已在多种生物体中得到鉴定。我们研究了具有两亲性阳离子结构的吩噻嗪盐是否可能是MDR的底物。我们使用了金黄色葡萄球菌(NorA)、大肠杆菌(TolC)和铜绿假单胞菌(MexAB)的MDR缺陷型突变体,发现使用三种不同的吩噻嗪PS和红光时,其杀灭效果比野生型菌株高出2至4个对数。与野生型相比,过表达MDR的突变体受到保护而不被杀死。不同化学结构的有效抗菌PS在光介导的杀灭效果上,根据MDR表型没有差异。发现细胞对吩噻嗪PS的摄取因MDR表达水平而异。我们建议特定的MDR抑制剂可与吩噻嗪盐联合使用,以提高其光破坏效率。

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