Guideline for the Management of Fever and Neutropenia in Children With Cancer and/or Undergoing Hematopoietic Stem-Cell Transplantation

Lehrnbecher, Thomas; Phillips, Bob; Alexander, Sarah; Alvaro, Frank; Carlesse, Fabianne; Fisher, Brian T.; Hakim, Hana; Santolaya, Marı́a Elena; Castagnola, Elio; Davis, Bonnie L.; Dupuis, L. Lee; Gibson, Faith; Groll, Andreas H.; Gaur, Aditya H.; Gupta, Ajay; Kebudi, Rejin; Petrilli, Sérgio; Steinbach, William J.; Villarroel, Milena; Zaoutis, Theoklis E.; Sung, Lillian

doi:10.1200/jco.2012.42.7161

Cited by 322 publications

(341 citation statements)

References 133 publications

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“…Identification of laboratory markers to efficiently and accurately stratify for patients based on risk of serious infectious complication is badly needed in paediatric oncology [14,32]. Our results for PCT and IL-6 are presented by slightly smaller values of sensitivity and specificity than results of abovementioned meta-analysis published by Philips et al or other single studies [4,6,33].…”

Section: Discussioncontrasting

confidence: 56%

“…In our clinic we start antibiotic therapy in accordance with international 2012 JCO Guideline for management of paediatric febrile neutropenia. We evaluate elements informative for risk stratification included patient-specific factors (including age, malignancy type, and disease status); treatment-specific factors (type and timing of chemotherapy), and episode-specific factors (including height of fever, hypotension, mucositis, blood counts, and available biomarkers -CRP and PCT) [32]. The main criterion for initiating anti-infective therapy remains clinical presentation.…”

Section: Resultsmentioning

confidence: 99%

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The role of CRP, PCT, IL-6 and presepsin in early diagnosis of bacterial infectious complications in paediatric haemato-oncological patients

Plesko¹,

Suvada²,

Makohusová³

et al. 2016

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Bacterial infection is the most common complication in paediatric oncological patients during cancer treatment. A suitable tool for early prediction of unfavourable course of infection is still needed. We performed a prospective longitudinal observational study to evaluate of the role of serum biomarkers (C-reactive protein, procalcitonin, interleukin-6, presepsin) in the early diagnosis of bacteraemia (gram-negative versus gram-positive) in patients with haematological malignancies. We observed 69 febrile episodes in 33 patients (17 male, 16 female; 1.5-18.9 years, mean 7.31 years, median 5 years). Within this sample, there were 22 cases of positive blood cultures, 16 cases of sepsis, 38 cases of fever with no signs or symptoms of sepsis, and two deaths from infectious complications. All markers tested had good negative predictive value (73% -93%). CRP was characterized by good specificity for registration bacteraemia (96%, 95% CI: 85% -99%), but other results were inconclusive. We identified comparably balanced sensitivity (64% -81%) and specificity (61% -88%) for interleukin-6 and procalcitonin, and we proved their quality to predict positive blood culture and clinical signs of sepsis as well. Patients with gram-negative bacteraemia had significantly elevated levels of PCT and IL-6 in comparison with a group of patients with gram-positive bacteraemia (p = 0.04 for PCT and p = 0.005 for IL-6). Presepsin was characterized by poor specificity (27%, 95% CI: 15% -43%) and positive predictive value (24%, 95% CI: 12 -39%) for predicting bacteraemia, and by better sensitivity (84%, 95% CI: 55% -98%) and specificity (58%, 95% CI: 42% -73%) for predicting clinical signs of sepsis. Key words: C-reactive protein, procalcitonin, interleukin-6, presepsin, fever, sepsisBacterial infection is the most common treatment-related complication in patients with haematological malignancies [1]. Documented mortality associated with paediatric febrile neutropenia is 2% [2]. The potential for early diagnosis of bacteraemia through serum biomarkers has been the subject to extensive research [3]. In 2012 Phillips et al published large meta-analysis of 25 studies exploring 14 different biomarkers in 3,585 episodes of febrile neutropenia. CRP, PCT and IL-6 were subject to quantitative meta-analysis. The bivariate estimates of diagnostic precision of these biomarkers and outcomes were done. Data were available for meta-analysis for CRP for microbiologically or clinically documented infection (results: cut off > 50mg/dl, sensitivity 65%, specificity 73%), for PCT assessing microbiologically or clinically documented infection (results: cut off > 0.2 mg/ml, sensitivity 96%, specificity 85%), for IL-6 reporting microbiologically or clinically documented infection (results: cut off > 235 pg/ml, sensitivity 68%, specificity 94%), and gram-negative bacteraemia (results: cut off > 1000 pg/ml, sensitivity 78%, specificity 96%). Huge inconsistencies and heterogeneity in the studies included in this review were the most important limiting factors [...

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Section: Discussioncontrasting

confidence: 56%

Section: Resultsmentioning

confidence: 99%

The role of CRP, PCT, IL-6 and presepsin in early diagnosis of bacterial infectious complications in paediatric haemato-oncological patients

Plesko¹,

Suvada²,

Makohusová³

et al. 2016

neo

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“…Relevant covariate data including demographic features, age, gender, type of malignancy, phase of chemotherapy, clinical features at presentation, duration of symptoms, initial labarotary findings including total white blood cell (WBC) count, absolute neutrophil count (ANC), and platelet count; radiological findings (if applicable) and microbiological results, management and outcomes were also collected. All patients were treated as inpatients following the "International Pediatric Fever and Neutropenia Guideline" [10].…”

Section: Data Collectionmentioning

confidence: 99%

Composite Adverse Event Outcome in Pediatric Cancer Patients with Prolonged Febrile Neutropenia

Matloob¹

2016

Journal of Microbiology and Infectious Diseases

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Objective: Pediatric cancer patients with prolonged febrile neutropenia have increased risk for severe, recurrent or new bacterial and fungal infection. The aim of this study was to identify the risk factors associated with adverse outcomes in this group. Methods:We retrospective analyzed the clinical data of 135 hospitalizations of pediatric cancer patients with prolonged febrile neutropenia from a tertiary health care center of Pakistan. Results:The mean age of the study population was 7.3±4.1 years. There were 98 (72.6%) males and 37 (27.4%) females. Acute leukemia with 88 patients (65.2%) was the most common diagnosis followed by lymphomas 19 patients (14.1%) and solid tumors. Cause of febrile neutropenia was identified in only 58 (43.0%) patients, out of them blood stream infections were found in 22 cases (16.3%), pneumonia in 15 (11.1%), fungal infection in 13 (9.6%), infectious diarrheas in 5 (3.7%) and urinary tract infection (UTI) in 3 (2.2%) of cases. The composite adverse event outcome was observed in 28 (20.7%) of patients, with in-hospital mortality occurring in 7 (5.2%), Pediatric intensive care unit (PICU) admission occurring in 12 (8.9%) and inotropic support was required in 9 (6.7%). On logistic regression analysis AML (Adjusted odds ratio (AOR), 7.6; P<0.001), neutropenia <50/mm 3 (AOR, 10.8; p<0.001), platelets count <50,000/mm 3 (AOR, 5.2; p<0.001), BSI (AOR, 2.3; p 0.05) and fungal infection (AOR, 4.3; p<0.001) were found as independent risk factors for composite adverse event outcome in pediatric cancer patients with prolonged febrile neutropenia.Conclusions: AML, severe myelosuppression, blood stream infections and fungal infection were identifiable risk factors associated with development of adverse event outcome in pediatric cancer patients with prolonged febrile neutropenia. J Microbiol Infect Dis 2016;6(2): 69-73Key words: Febrile neutropenia, pediatric, oncology, adverse outcome Uzamış Febril Nötropeni ile Pediatrik Kanser Hastalarında Karma Olumsuz Durum SonuÖZET Amaç: Uzamış febril nötropeni pediatrik kanserli hastalarında ağır seyirli yeni tanı veya tekrarlayan bakteri ve mantar enfeksiyonu riski artmıştır. Bu çalışmanın amacı, bu grupta olumsuz sonuçlarla ilişkili risk faktörlerini belirlemektir.Yöntemler: Pakistan'ta bir üçüncü basamak sağlık merkezine uzamış febril nötropeni nedeni ile izlenen pediatrik kanser hastalarının 135 hastane yatış epizotu retrospektif olarak analiz edildi. Bulgular: Çalışma grubunun yaş ortalaması 7,3 ± 4,1 yıl idi. Hastaların 98'i (% 72,6) erkek ve 37'si (% 27,4) kadındı. Akut lösemi 88 hastada (% 65,2) ile birinci sırada, lenfoma 19 hasta (% 14,1) ile ikinci sırada idi ve diğer hastalarda solid organ tümörleri en sık görülen tanı olarak saptandı. Febril nötropenin nedeni sadece 58 (% 43,0) hastada tanımlandı. Bu hastalardan 22 olguda (% 16,3) kan akımı enfeksiyonu (KAE), 15 hastada pnömoni (% 11,1), fungal infeksiyon 13 (% 9,6) hastada, ve enfeksiyöz diyare 5 hastada (% 3,7) ve üriner sitem enfeksiyonu 3 (% 2,2) hastada saptandı. Karma olumsu...

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“…A recent systematic review of randomized control trials in pediatric FN [37] concluded that antipseudomonal penicillin and fourth-generation cephalosporin monotherapy were associated with similar failure and mortality rates as aminoglycoside containing combination therapy. The current recommendations also advise monotherapy as initial empirical antibiotic therapy in pediatric FN [3][4][5][6][7][8][9]. Further, Outpatient management and oral antibiotics were found to be safe in low-risk FN with no infection-related mortality observed in any patient and no significant differences in outcomes compared with inpatient management and intravenous therapy.…”

Section: Introductionmentioning

confidence: 99%

“…Indeed an audit of all hospital admission for pediatric FN during the year 2012 in US [8] revealed that 39% of the discharges had a short length of stay (SLOS) of ≤ 3 days; viral infection and upper respiratory infection comprising the majority with 66.4% of them had no identifiable infections. This has led to the risk based approach and use of intravenous or oral antibiotics in 'low risk' patients [9]. Another important paradigm in the management of pediatric FN is use of antibiotic prophylaxis.…”

Section: Introductionmentioning

confidence: 99%

Changing Microbiological Pattern of Pediatric Febrile Neutropenia

Mandal¹,

Singh²

2016

J Antimicrob Agents

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Guideline for the Management of Fever and Neutropenia in Children With Cancer and/or Undergoing Hematopoietic Stem-Cell Transplantation

Abstract: This guideline represents an evidence-based approach to FN specific to children with cancer. Although some recommendations are similar to adult-based guidelines, there are key distinctions in multiple areas. Implementation will require adaptation to the local context.

Cited by 322 publications

References 133 publications

The role of CRP, PCT, IL-6 and presepsin in early diagnosis of bacterial infectious complications in paediatric haemato-oncological patients

The role of CRP, PCT, IL-6 and presepsin in early diagnosis of bacterial infectious complications in paediatric haemato-oncological patients

Composite Adverse Event Outcome in Pediatric Cancer Patients with Prolonged Febrile Neutropenia

Changing Microbiological Pattern of Pediatric Febrile Neutropenia

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