Principe Luigi, D'Arezzo Silvia, Capone Alessandro, Petrosillo Nicola, Visca Paolo
National Institute for Infectious Diseases Lazzaro Spallanzani, Via Portuense 292, Rome 00149, Italy.
Ann Clin Microbiol Antimicrob. 2009 May 21;8:18. doi: 10.1186/1476-0711-8-18.
Infections sustained by multidrug-resistant (MDR) and pan-resistant Acinetobacter baumannii have become a challenging problem in Intensive Care Units. Tigecycline provided new hope for the treatment of MDR A. baumannii infections, but isolates showing reduced susceptibility have emerged in many countries, further limiting the therapeutic options. Empirical combination therapy has become a common practice to treat patients infected with MDR A. baumannii, in spite of the limited microbiological and clinical evidence supporting its efficacy. Here, the in vitro interaction of tigecycline with seven commonly used anti-Acinetobacter drugs has been assessed.
Twenty-two MDR A. baumannii isolates from Intensive Care Unit (ICU) patients and two reference strains for the European clonal lineages I and II (including 3, 15 and 6 isolates that were resistant, intermediate and susceptible to tigecycline, respectively) were tested. Antimicrobial agents were: tigecycline, levofloxacin, piperacillin-tazobactam, amikacin, imipenem, rifampicin, ampicillin-sulbactam, and colistin. MICs were determined by the broth microdilution method. Antibiotic interactions were determined by chequerboard and time-kill assays. Only antibiotic combinations showing synergism or antagonism in both chequerboard and time-kill assays were accepted as authentic synergistic or antagonistic interactions, respectively.
Considering all antimicrobials in combination with tigecycline, chequerboard analysis showed 5.9% synergy, 85.7% indifference, and 8.3% antagonism. Tigecycline showed synergism with levofloxacin (4 strains; 16.6%), amikacin (2 strains; 8.3%), imipenem (2 strains; 8.3%) and colistin (2 strains; 8.3%). Antagonism was observed for the tigecycline/piperacillin-tazobactam combination (8 strains; 33.3%). Synergism was detected only among tigecycline non-susceptible strains. Time-kill assays confirmed the synergistic interaction between tigecycline and levofloxacin, amikacin, imipenem and colistin for 5 of 7 selected isolates. No antagonism was confirmed by time-kill assays.
This study demonstrates the in vitro synergistic activity of tigecycline in combination with colistin, levofloxacin, amikacin and imipenem against five tigecycline non-susceptible A. baumannii strains, opening the way to a more rationale clinical assessment of novel combination therapies to combat infections caused by MDR and pan-resistant A. baumannii.
耐多药(MDR)和泛耐药鲍曼不动杆菌引起的感染已成为重症监护病房中一个具有挑战性的问题。替加环素为耐多药鲍曼不动杆菌感染的治疗带来了新希望,但在许多国家已出现对其敏感性降低的菌株,进一步限制了治疗选择。尽管支持经验性联合治疗疗效的微生物学和临床证据有限,但它已成为治疗耐多药鲍曼不动杆菌感染患者的常用方法。在此,评估了替加环素与七种常用抗不动杆菌药物的体外相互作用。
测试了来自重症监护病房(ICU)患者的22株耐多药鲍曼不动杆菌分离株以及欧洲克隆谱系I和II的两株参考菌株(分别包括对替加环素耐药、中介和敏感的3株、15株和6株分离株)。抗菌药物包括:替加环素、左氧氟沙星、哌拉西林-他唑巴坦、阿米卡星、亚胺培南、利福平、氨苄西林-舒巴坦和黏菌素。采用肉汤微量稀释法测定最低抑菌浓度(MIC)。通过棋盘法和时间杀菌试验确定抗生素相互作用。只有在棋盘法和时间杀菌试验中均显示协同或拮抗作用的抗生素组合才分别被视为真正的协同或拮抗相互作用。
考虑所有与替加环素联合使用的抗菌药物,棋盘法分析显示协同作用占5.9%,无相互作用占85.7%,拮抗作用占8.3%。替加环素与左氧氟沙星(4株;16.6%)、阿米卡星(2株;8.3%)、亚胺培南(2株;8.3%)和黏菌素(2株;8.3%)显示协同作用。观察到替加环素/哌拉西林-他唑巴坦组合存在拮抗作用(8株;33.3%)。协同作用仅在对替加环素不敏感的菌株中检测到。时间杀菌试验证实了替加环素与左氧氟沙星、阿米卡星、亚胺培南和黏菌素对7株选定分离株中的5株具有协同相互作用。时间杀菌试验未证实存在拮抗作用。
本研究证明了替加环素与黏菌素、左氧氟沙星、阿米卡星和亚胺培南联合对五株对替加环素不敏感的鲍曼不动杆菌菌株具有体外协同活性,为更合理地临床评估用于对抗耐多药和泛耐药鲍曼不动杆菌引起的感染的新型联合疗法开辟了道路。
Zotero 插件