Santos Costa Sofia, Viveiros Miguel, Rosato Adriana E, Melo-Cristino José, Couto Isabel
Global Health and Tropical Medicine, GHTM, Unidade de Microbiologia Médica, Instituto de Higiene e Medicina Tropical, IHMT, Universidade Nova de Lisboa, UNL, Rua da Junqueira, 100, 1349-008, Lisbon, Portugal.
Department of Pathology and Genomic Medicine, Center for Molecular and Translational Human Infectious Diseases Research, Houston Methodist Research Institute, Houston, TX, USA.
BMC Microbiol. 2015 Oct 24;15:232. doi: 10.1186/s12866-015-0572-8.
Efflux has been recognized as a resistance mechanism to antimicrobials in Staphylococcus aureus; however its role on the development of clinically relevant resistance is still poorly characterized. This study aimed to examine the impact of efflux on development of resistance to fluoroquinolones and other antimicrobials in S. aureus strains representing relevant phenotypes in terms of antibiotic susceptibility and efflux activity.
Two closely related methicillin- and ciprofloxacin-resistant Staphylococcus aureus clinical strains, with different efflux capacity and the pan-susceptible strain ATCC25923 were exposed to constant concentrations of the efflux pump (EP) substrates ciprofloxacin, ethidium bromide and cetrimide. Parental and exposed strains were tested regarding their susceptibility towards antibiotics, biocides and ethidium bromide, efflux capacity and levels of EP gene expression. Occurrence of resistance-associated mutations was screened by sequencing.
Multidrug resistance phenotypes emerged upon exposure, independently of the substrate or its concentration, which were correlated with increased efflux capacity of the exposed strains. The temporal pattern of EP gene expression disclosed an early-response with high expression of several genes, followed by a late-response, characterized by overexpression of specific genes. The overall cell response was more pronounced for strains with an initial basal efflux activity. Remarkably, detection of the IS256 element in the promoter regions of mgrA and norA, in some cases associated with increased gene expression, suggests that these genes may be hot spots for IS256 insertion events. The results obtained with exposure of ATCC25923 to ciprofloxacin were particularly striking, revealing a step-wise development of fluoroquinolone resistance, with a first efflux-mediated response, followed by the occurrence of a mutation in grlA that resulted in phenotypic resistance. Additionally, challenge by non-fluoroquinolone agents, particularly cetrimide, promoted cross resistance to fluoroquinolones, revealing the potential role of biocides as selective pressure for the emergence of resistance to these antibiotics.
This study reveals efflux as a significant component of S. aureus resistance to fluoroquinolones and biocides and as a primary mechanism to withstand stress imposed by antimicrobials. This efflux-mediated response can result in the emergence of multidrug resistance in healthcare environments and should be taken into account in the management of this major pathogen.
外排已被认为是金黄色葡萄球菌对抗菌药物的一种耐药机制;然而,其在临床相关耐药性发展中的作用仍未得到充分表征。本研究旨在考察外排在代表抗生素敏感性和外排活性相关表型的金黄色葡萄球菌菌株中对氟喹诺酮类及其他抗菌药物耐药性发展的影响。
将两株密切相关的耐甲氧西林和环丙沙星的金黄色葡萄球菌临床菌株,它们具有不同的外排能力,以及泛敏感菌株ATCC25923暴露于恒定浓度的外排泵(EP)底物环丙沙星、溴化乙锭和十六烷基三甲基溴化铵。对亲本菌株和暴露后的菌株进行抗生素、杀菌剂和溴化乙锭敏感性、外排能力及EP基因表达水平的检测。通过测序筛查耐药相关突变的发生情况。
暴露后出现了多药耐药表型,与底物或其浓度无关,这与暴露后菌株外排能力的增加相关。EP基因表达的时间模式显示为早期反应,多个基因高表达,随后是晚期反应,其特征为特定基因的过表达。对于初始具有基础外排活性的菌株,整体细胞反应更为明显。值得注意的是,在某些情况下,mgrA和norA启动子区域中检测到IS256元件,且与基因表达增加相关,这表明这些基因可能是IS256插入事件的热点。用环丙沙星处理ATCC25923所获得的结果尤为显著,显示出氟喹诺酮耐药性的逐步发展,首先是外排介导的反应,随后grlA发生突变导致表型耐药。此外,非氟喹诺酮类药物,特别是十六烷基三甲基溴化铵的挑战促进了对氟喹诺酮类的交叉耐药,揭示了杀菌剂作为这些抗生素耐药性出现的选择压力的潜在作用。
本研究揭示外排是金黄色葡萄球菌对氟喹诺酮类和杀菌剂耐药性的重要组成部分,也是抵御抗菌药物施加压力的主要机制。这种外排介导的反应可导致医疗环境中多药耐药性的出现,在管理这种主要病原体时应予以考虑。
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