Department of Clinical Microbiology, Hippokration General Hospital, and Infectious Diseases Unit, Third Department of Paediatrics, Aristotle University, Thessaloniki, Greece.
Euro Surveill. 2012 Feb 16;17(7):20088.
We report 570 carbapenemase-producing Klebsiella pneumoniae (CPKP) clinical isolates in a 1,040-bed Greek tertiary hospital during 2004 to 2010. The first CPKP (VIM-producing) was isolated in September 2004. Despite initial containment, VIM producers have become endemic since 2006. KPC-producing K. pneumoniae was first isolated in August 2007 from a patient who came from Israel, spread rapidly, and outcompeted VIM. Overall, 267 (47%) VIM-producing and 301 (53%) KPC-producing strains were isolated, including 141 (24.7%) from patients with bacteraemia. Two isolates carrying both VIM and KPC were isolated in two consecutive months in 2009, but not since. The prevalence of CPKP increased from 0% in 2003 to 38.3% in 2010 (p<0.0001). All genotyped KPC producers harboured blaKPC-2 and belonged to two clones, among which the hyperepidemic Greek clone, related to those from the United States and Israel, predominated. Most metallo-beta-lactamase (MBL) producers carried the blaVIM-1 gene and belonged to several clones, whereas all but one isolate with blaVIM-12 were clustered within a five-month period, arising from one clone. Resistance to non-beta-lactam antibiotics was also increased among CPKP. They were almost invariably resistant to ciprofloxacin and trimethoprim-sulfamethoxazole. Resistance to colistin increased from 3.5% (4/115) in 2008 to 20.8% (25/120) in 2010, and resistance to tigecycline also increased. Following reinforcement of infection control measures, prevalence of CPKP (mainly KPC) has been reduced since mid-2009 (from 46% in 2009 to 38.3% in 2010). In view of the exhaustion of available therapies, investment in infection control resources and optimal antibiotic use is urgently required.
我们报告了 2004 年至 2010 年期间在一家拥有 1040 张床位的希腊三级医院中 570 株产碳青霉烯酶肺炎克雷伯菌(CPKP)的临床分离株。第一株产碳青霉烯酶肺炎克雷伯菌(VIM 型)于 2004 年 9 月分离。尽管最初得到了控制,但自 2006 年以来,VIM 产酶株已成为地方性菌株。2007 年 8 月,从一名来自以色列的患者中首次分离出产 KPC 的肺炎克雷伯菌,该菌迅速传播并取代了 VIM。总的来说,共分离到 267 株(47%)产 VIM 和 301 株(53%)产 KPC 的菌株,其中 141 株(24.7%)来自菌血症患者。2009 年连续两个月从两名患者中分离到同时携带 VIM 和 KPC 的两种菌株,但此后未再分离到。2010 年,CPKP 的流行率从 2003 年的 0%增加到 38.3%(p<0.0001)。所有基因分型的 KPC 产酶株均携带 blaKPC-2 基因,属于两个克隆株,其中流行的希腊克隆株与来自美国和以色列的克隆株相关,占主导地位。大多数金属β-内酰胺酶(MBL)产酶株携带 blaVIM-1 基因,属于几个克隆株,而除一株 blaVIM-12 之外的所有菌株均在 5 个月内聚集在一起,来自一个克隆株。CPKP 对非β-内酰胺类抗生素的耐药性也增加了。它们几乎对环丙沙星和复方磺胺甲噁唑具有耐药性。多粘菌素耐药性从 2008 年的 3.5%(4/115)增加到 2010 年的 20.8%(25/120),而替加环素的耐药性也增加了。加强感染控制措施后,自 2009 年中旬以来(从 2009 年的 46%降至 2010 年的 38.3%),CPKP(主要是 KPC)的流行率有所下降。鉴于现有治疗方法的局限性,迫切需要投资于感染控制资源和优化抗生素的使用。
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