首页> 外文期刊>Journal of pediatric hematology/oncology: Official journal of the American Society of Pediatric Hematology/Oncology >Pediatric Febrile Neutropenia: Change in Etiology of Bacteremia, Empiric Choice of Therapy and Clinical Outcomes
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Pediatric Febrile Neutropenia: Change in Etiology of Bacteremia, Empiric Choice of Therapy and Clinical Outcomes

机译:儿科发热中性粒细胞:菌血症病因的变化,疗效选择和临床结果

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Background:The optimal choice of initial antibiotic therapy for patients with high-risk febrile neutropenia (FN) in children is unclear and varies by the institution on the basis of local antibiograms and epidemiology of specific pathogens. The authors evaluated the appropriateness of antibiotics for the empiric treatment of FN in pediatric patients with cancer in our institution on the basis of changes in the epidemiology of organisms isolated from blood cultures (BCx).Methods:The authors conducted a retrospective medical record review of pediatric patients who received any oncology care (including patients with cancer and patients who had stem cell transplant) at University of Chicago Medicine Comer Children's Hospitals (March 2009 to December 2016) with a diagnosis of FN who had at least 1 BCx obtained. They reviewed pathogens isolated from BCx and determined whether they were pathogens or contaminants using the Infectious Diseases Society of America (IDSA) guidelines and the team's decision to treat. They investigated the microbiologic spectrum and susceptibility patterns of pathogens causing bacteremia in pediatric FN and whether the empiric therapy chosen may have affected clinical outcomes.Results:A total of 667 FN episodes were identified in 268 patients. BCx were negative in 497 (74.5%) and were determined to be contaminants in 27 (4%). In 143 episodes (21.5%), the BCx were positive for a pathogenic species. Polymicrobial bacteremia was identified in 25 episodes; a total of 176 pathogens were isolated. The majority of pathogens (95/176, 54%) were Gram-positive (GP), whereas 64 of 162 (36%) were Gram-negative (GN), 5 were fungal, and 4 were mycobacterial. The most common GP pathogens were viridans group streptococci (VGS) (n=34, 19.3%), coagulase-negative staphylococci (n=25, 14%), and methicillin-susceptible Staphylococcus aureus (n=12, 6.8%). Of aerobic GN bacilli, 15 (8.5%) were AmpC producers and 3 (1.7%) carried extended-spectrum beta-lactamases. There was no increase in the prevalence of multidrug-resistant GN isolates during the study period. Patients with VGS and multidrug-resistant GN bacteremia were more likely to be admitted to the pediatric intensive care unit [odds ratio (OR), 3.24; P=0.017; and OR, 2.8; P=0.07, respectively]. There were trends toward a higher prevalence of GP pathogens causing bacteremia and the emergence of VGS with decreased penicillin sensitivity. The prevalence of bacteremia with VGS was higher in acute myelogenous leukemia and neuroblastoma (OR, 2.3; P<0.01) than in patients with other solid tumors.Conclusions:Empiric antibiotic treatment should be tailored to patients' risk for VGS and multidrug-resistant organisms. Individual hospitals should monitor the pathogens causing FN among patients with cancer to guide choice of empiric therapy.
机译:背景:儿童高风险性中性粒细胞率(FN)患者的最佳选择初始抗生素治疗尚不清楚,在机构基于局部抗诊断和特定病原体的流行病学的基础上变化。作者评估了在从血液培养物流行病学(BCX)的有机体流行病学的变化的基础上对癌症患者癌症患者的抗生素的适当性.Methods:作者进行了回顾性的医疗记录审查在芝加哥医学大学(2009年3月至2016年12月)芝加哥医学院(2009年3月至2016年12月,患有癌症和患有干细胞移植患者的癌症和患者)的儿科患者诊断为获得至少1个BCX的FN。他们审查了从BCX中分离的病原体,并确定它们是否是使用美国传染病学会(IDSA)指导方针和团队决定治疗的病原体或污染物。他们调查了导致儿科FN菌血症的病原体的微生物谱和易感性模式以及所选择的透视疗法可能影响临床结果。结果:268例患者共鉴定了667个FN发作。 BCX在497中为阴性(74.5%),并确定为27(4%)的污染物。在143个发作(21.5%)中,BCX对于致病物种呈阳性。在25个发作中鉴定了多发性菌血症;共分离了176条病原体。大多数病原体(95/176,54%)是革兰氏阳性(GP),而162个(36%)的64个(36%)是革兰氏阴性(GN),5例真菌,4例是分枝杆菌。最常见的GP病原体是viridans组链球菌(Vgs)(n = 34,19.3%),凝壳酶阴性葡萄球菌(n = 25,14%)和甲基蛋白敏感的金黄色葡萄球菌(n = 12,6.8%)。有氧gn Bacilli,15(8.5%)是AMPC生产商,3(1.7%)携带的延长光谱β-内酰胺酶。在研究期间,多药抗性GN分离物的患病率没有增加。患有VGS和多药抗性GN菌血症的患者更容易进入儿科重症监护单元[赔率比(或),3.24; P = 0.017;或者,2.8; p = 0.07分别]。 GP病原体患病率较高的趋势导致菌血症和VGS的出现随着青霉素敏感性降低。急性髓性白血病和神经母细胞瘤(或2.3; P <0.01)患者的菌血症患者的患病率高于其他实体肿瘤的患者。结论:经验抗生素治疗应根据患者对VGS和多药物的风险定制。个别医院应监测癌症患者导致FN的病原体,以指导验证疗法选择。

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