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首页> 外文期刊>Microbial drug resistance: MDR : Mechanisms, epidemiology, and disease >Impacts of Hypervirulence Determinants on Clinical Features and Outcomes of Bacteremia Caused by Extended-Spectrum -Lactamase-Producing Klebsiella pneumoniae
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Impacts of Hypervirulence Determinants on Clinical Features and Outcomes of Bacteremia Caused by Extended-Spectrum -Lactamase-Producing Klebsiella pneumoniae

机译:超高档决定因素对扩展 - 酰胺酶 - 酰胺酶的肺炎肺炎肺炎肺炎肺炎的临床特征和结果的影响

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We investigated the implications of hypervirulence determinants on clinical features of 48 adult patients with bacteremia caused by extended-spectrum -lactamase-producing Klebsiella pneumoniae. Isolates in the hypervirulence group included any of the following virulence determinants: K1/K2 capsule serotypes, hypermucoviscosity phenotype, rmpA gene, or rmpA2 gene. Nonhypervirulence group isolates were negative for all of the above virulence factors. In this study, all isolates used were non-K1/K2 strains. Statistically significant differences were observed in clinical features of patients between the two groups. The hypervirulent isolates (n=19), including 11 isolates with the hypermucoviscosity phenotype, 15 with the rmpA gene, and 16 with the rmpA2 gene, were more commonly recovered from diabetic patients and mainly manifested as secondary bacteremia (such as pneumonia, urinary tract infections, or other localized infections). The nonhypervirulent isolates (n=29) were more commonly recovered from patients after prolonged hospital stays (>30 days) and mostly manifested as primary bacteremia. The overall in-hospital mortality was 56.3%. Hazard ratio (HR) analysis revealed the following positive predictors for mortality: nosocomial infection, stay in an intensive care unit, no removal of the central venous catheter, Charlson comorbidity score, and APACHE II score (15). The negative predictors were initial appropriate antibiotic therapy (HR 0.42) and urinary tract infection (HR 0.19). Charlson score was an independent confounder based on multivariate analysis (HR 1.43, 95% confidence interval 1.04-1.99). In conclusion, hypervirulence determinants played a role in causing secondary infections in diabetic patients; however, the presence of morbidity cofactors could themselves influence mortality, despite the absence of hypervirulence determinants.
机译:我们调查了超高档决定因素对48例成年患者临床特征的影响,由扩展脱水酶产生的Klebsiella肺炎引起的菌血症患者。超级化组中的分离株包括以下任何毒力决定因素:K1 / K2胶囊血清型,高水溶性表型,RMPA基因或RMPA2基因。对于所有上述毒力因子,非吸管基团分离物为阴性。在本研究中,所使用的所有分离物是非K1 / K2菌株。在两组患者的临床特征中观察到统计学上的显着差异。包括11分离物与RMPA基因的高水性致中性表型的高潜力分离物(n = 19),以及具有RMPA2基因的16个分离物,从糖尿病患者中更常见,主要表现为次生菌血症(如肺炎,泌尿道感染或其他局部感染)。在长时间医院停留(> 30天)后,从患者中更常见的患者不起作用的分离物(n = 29),并且主要表现为原发性菌血症。整体院生的死亡率为56.3%。危险比(HR)分析显示以下阳性预测因子用于死亡率:医院感染,留在重症监护手机,不移除中心静脉导管,Charlson合并症评分,Apache II得分(15)。消极预测因子是初始合适的抗生素治疗(HR 0.42)和尿路感染(HR 0.19)。 Charlson得分是基于多变量分析的独立混淆(HR 1.43,95%置信区间1.04-1.99)。总之,过度频率决定簇在导致糖尿病患者中的继发感染方面发挥了作用;然而,尽管没有过度频率决定因素,但发病率辅因子的存在本身可能会影响死亡率。

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