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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Meropenem-Vaborbactam Tested against Contemporary Gram-Negative Isolates Collected Worldwide during 2014, Including Carbapenem-Resistant, KPC-Producing, Multidrug-Resistant, and Extensively Drug-Resistant Enterobacteriaceae
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Meropenem-Vaborbactam Tested against Contemporary Gram-Negative Isolates Collected Worldwide during 2014, Including Carbapenem-Resistant, KPC-Producing, Multidrug-Resistant, and Extensively Drug-Resistant Enterobacteriaceae

机译:Meropenem-VaborbAdtam测试了2014年全球收集的当代革兰阴性分离物,包括耐鲤鱼,生产KPC,抗性,抗毒性抗药性肠杆菌薄膜

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We evaluated the activity of meropenem-vaborbactam against contemporary non-fastidious gram-negative clinical isolates, including resistant phenotypes and carbapenemase genotypes of Enterobacteriaceae. Meropenem-vaborbactam (inhibitor at 8 mu g/ml) and comparators were susceptibility tested using reference broth microdilution methods against 14,304 gram-negative clinical isolates collected worldwide during 2014. Carbapenemase encoding genes were screened by PCR/sequencing. Meropenem-vaborbactam (MIC50/90, <= 0.015/0.06 mu g/ml) inhibited 99.1 and 99.3% of the 10,426 Enterobacteriaceae isolates tested at < 1 and <2 mu g/ml, respectively. Meropenem inhibited 97.3 and 97.7% of these isolates at the same concentrations. Against Enterobacteriaceae displaying carbapenem resistance (CRE) (n=265), multidrug (MDR) (n=1,210) or extensively drug (XDR) (n=161) resistant phenotypes, meropenem-vaborbactam displayed MIC50/90 values at 0.5/32, 0.03/1 and 0.5/32 mu g/ml, respectively, whereas meropenem activity was 16/> 32, 0.06/32 and 0.5/32 mu g/ml, respectively. Among all geographic regions, the highest meropenem-vaborbactam activity was observed for CRE and MDR isolates from the U.S. (MIC50/90, 0.03/1 and 0.03/0.12 mu g/ml, respectively). Meropenem- vaborbactam was very active against 135 KPC-producers, and all isolates were inhibited by <= 8 mug/ml (133 isolates at <= 2 mu g/ml). This combination had limited activity against isolates producing metallo-beta-lactamases (including 25 NDM-1 and 16 VIM-producers) and/or oxacillinases (27 OXA-48/-163) that were detected mainly in Asia-Pacific and some European countries. The activity of meropenem-vaborbactam was similar to that of meropenem alone against Pseudomonas aeruginosa, Acinetobacter spp. and Stenotrophomonas maltophilia. Meropenem-vaborbactam was active against contemporary Enterobacteriaceae collected worldwide, and this combination demonstrated enhanced activity when compared to meropenem and most comparator agents against CRE and KPC-producers that are often MDR.
机译:我们评估了Meropenem-vaborbActam对当代非缩小革兰阴性临床分离株的活动,包括肠癌的抗性表型和碳癌酶基因型。 Meropenem-Vabbordam(抑制剂在8μg/ ml)和比较器中使用参考肉汤微量稀释方法对全世界收集的14,304克阴性临床分离株进行测试,通过PCR /测序筛选碳丙二碱酶编码基因。 Meropenem-vabbordam(MIC50 / 90,<= 0.015 /0.06μg/ ml)抑制了99.1和99.3%的10,426肠杆菌的分离物分别在<1和<2μg/ ml处测试。梅洛宁以相同浓度抑制97.3和97.7%的这些分离物。针对肠杆菌区显示碳酸杆菌(CRE)(N = 265),多药(MDR)(n = 1,210)或广泛的药物(XDR)(n = 161)抗性表型,Meropenem-vabbordam显示MIC50 / 90值0.5 / 32,分别0.03 / 1和0.5 /32μg,而Meropenem活性分别为16 /> 32,0.06 / 32和0.5 /32μg/ ml。在所有地理区域中,从U.S的CRE和MDR分离物中观察到最高的梅洛芬-VabbordAdaM活性。(MIC50 / 90,0.03 / 1和0.03 /0.12μg/ ml)。 Meropenem- vabbordActam对135kpc-生产者非常活跃,并且通过<= 8麦克约/ ml(133分离物为<=2μg/ ml)抑制所有分离株。这种组合对产生金属β-内酰胺酶(包括25ndm-1和16个Vim-生产者)和/或氧化酶(27只Oxa-48 / -163)的分离物的活性有限,主要在亚太地区和一些欧洲国家检测到。 Meropenem-VabbordActam的活性与单独的梅洛涅伦姆的活性相似,针对假单胞菌铜绿假单胞菌,术语。和斯滕科莫洛尼亚野生疗法。 Meropenem-VabbordActam活跃于全球收集的当代肠杆菌,并且与梅罗普伦姆和普通MDR的KPC制作人的大多数比较剂相比,这种组合表现出增强的活动。

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