Introduction
The occurrence of febrile neutropenia in cancer patients should lead to cautious severity assessment in order to provide appropriate management and therefore improve prognosis [
1]. Despite specific recommendations, febrile neutropenia is still associated with high morbidity and mortality [
2] and elevated health-related costs. The underlying conditions associated with febrile neutropenia make patients more vulnerable. Cancer itself compromises survival [
3], impairs innate and adaptative immunity, and patients have a higher chance of developing a nosocomial infection [
4]. Therefore, severe infections are common in this population. To help physicians safely decide the site of care for patients with febrile neutropenia, criteria have been determined [
5], and sensitive scoring systems have been validated to limit patients' misclassification [
6]. In this setting, Multinational Association for Supportive Care in Cancer (MASCC) criteria were developed to help physicians make decisions about the site of care and overall management of patients with febrile neutropenia. This score mainly relies on subjective criteria such as the evaluation of clinical symptoms and hydration state.
Sepsis, severe sepsis and septic shock were defined 15 years ago as a continuum of increasing severity of the host response to the pathogen [
3] closely related to predisposition, organ failure and systemic response, and to the microorganism and site of infection [
7]. Management of septic patients has significantly improved over the past decade as a result of consensus guidelines published by 11 scientific societies [
8‐
10]. These recommendations have been widely disseminated, but detecting patients at risk remains a daily challenge in emergency medicine.
The presence of cancer may impair the prognosis of acute patients [
8], including septic patients [
11] visiting the emergency department (ED) [
12]. Reports on the management of febrile neutropenia in EDs are scarce, retrospective and mainly single centre studies. Interestingly, a French survey based on declarative questionnaires reported that 1 out of 31 cancer teams involved emergency physicians in their organizational strategy to manage patients with febrile neutropenia [
13]. As the incidence of sepsis has increased in the general population [
14], more patients visit the ED for this reason [
15] and this had led to a dramatic increase in number of cancer patients in this setting [
16].
This study was carried out to describe the management of patients with febrile neutropenia in EDs and to determine how management complies with recommendations. The secondary objective was to determine the factors associated with adequate management.
Materials and methods
Study design and ethics
This was a prospective multicentre study carried out in 47 French EDs over a six-month period (4 February to 4 August, 2008). The inform consent from patients was required for this study. The study protocol and patient information procedures were approved by the institutional review board for the protection of human subjects of the Cochin Port-Royal (Paris, France).
Recruitment of patients
Patients were included if they were adults (>18 years old) who presented at a participating ED with febrile neutropenia after myelotoxic treatment for cancer. Delay between last cytotoxic treatment and occurrence of febrile neutropenia was not pre-specified to enter the study. Definition of febrile neutropenia consisted of a white blood cell count less than 1,000/μL (or neutrophils <500/μL), with a core temperature above 8.3°C (or >38°C on two consecutive occasions). Patients who presented with febrile neutropenia in another setting or who refused to participate were not included in the study.
Procedure and data collection
An investigator (SA) contacted by phone the team leader of each participating centre to describe the study and explain criteria for eligibility. Each team leader gave the information about this study to the ED team. The physician on duty invited eligible patients to participate and implemented the electronic form. As this was an observation study, data were collected on the basis of usual practices.
The characteristics of each participating centre were recorded, with special reference to the management of febrile neutropenia. Data collected for each patient included demographic characteristics, physical data and medical history focusing on cancer and outcome (discharge, admission, admission to an ICU, death).
Study objectives
The primary objective was to describe the management of patients with febrile neutropenia in EDs and to determine whether management complies with recommendations. The secondary objective was to determine the factors associated with adequate management.
Evaluation criteria in the guidelines were identified to accurately assess the primary end points. Patients with febrile neutropenia were divided into two groups: those with and those without severe sepsis or septic shock (SS/SSh).
Patients with SS/SSh were selected according to the following criteria [
9,
17]: blood lactate more than 4 mmol/L, or low blood pressure before fluid challenge (systolic blood pressure <90 mmHg or 40 mmHg below usual systolic blood pressure), or at least one organ dysfunction (pulse oxymetry [SpO
2] <95% with fraction of inspired oxygen >0.5, blood creatinine >176 μmol/L or oliguria, international normalised ratio >2, bilirubinemia >78 μmol/L, Glasgow Coma Scale <15). Thrombopenia was excluded from the criteria because of the potential effect of chemotherapy on platelet counts. Patients without SS/SSh were identified as high risk or low risk according to the MASCC classification [
6] (Table
1). Of note, data that allowed determination of MASCC and presence of SS/SSh were collected at the bedside by attending physicians. Implementation of the database was not intended to help physicians detecting the severity of a patient's condition.
Table 1
Classification according to the Multinational Association for Supportive Care in Cancer(MASCC) [
6]
Burden of illness | |
Age < 60 years | 2 |
Outpatient status | 3 |
No chronic obstructive pulmonary disease | 4 |
No previous fungal infection | 4 |
Clinical state at admission | |
No or mild symptoms | 5 |
Moderate symptoms | 3 |
Systolic blood pressure <90 mmHg | 5 |
No dehydration needing perfusion | 3 |
Implementation of the following guidelines was assessed. Management of patients with SS/SSh required for the 90 first minutes [
9,
10]: (i) a dose regimen of adequate (broad-spectrum) intravenous antimicrobial therapy; (ii) fluid challenge (500 mL) if mean arterial blood pressure was less than 65 mmHg; (iii) lactate measurement; (iv) at least one blood culture; and (v) hospitalization. Management of patients without SS/SSh who were high risk according to MASCC criteria required [
18‐
20]: (i) adequate intravenous antimicrobial agent (broad-spectrum beta-lactam with or without an aminoglycoside); (ii) no initiation of granulocyte-cell stimulating factor (G-CSF); and (iii) hospitalization. Management of patients without SS/SSh who were low-risk according to MASCC criteria required [
18‐
20]: (i) adequate oral antimicrobial agent (quinolone or amoxicillin/clavulanate or cephalosporin); (ii) no initiation of G-CSF; and (iii) hospital discharge.
Patients were divided into two groups; those managed according to recommendations and those who were not, irrespective of initial severity. The two populations were compared to determine the factors associated with adequate management.
Statistical analysis
Quantitative variables are described as the mean ± standard deviation or median (range) and quantitative variables as number and percent. The adequacy of management according to recommendations was determined for the two sub-groups using Pearson's chi-squared test or Fisher's exact test for qualitative variables and the Student's t test or Wilcoxon rank sum test for quantitative variables. All tests were two-sided. A P value of less than 5% were considered statistically significant. All statistical analyses were carried out using R software (Vienna University of Economics and Business, 1090 Vienna, Austria).
Discussion
The results of this study suggest that cancer patients with febrile neutropenia visiting the ED are likely to present with SS/SSh, and their management does not comply with current guidelines especially in those with more severe infections.
The 47 participating centres were distributed across France and presented heterogeneous characteristics. This was representative of French EDs overall. As only 60% of hospitals had a dedicated cancer unit, it was assumed that cancer patients with febrile neutropenia visited community hospitals with this acute adverse event. This suggests that procedures to treat these patients should be available in every ED. However, only 40% of participating centres reported a written protocol for the management of febrile neutropenia. A total of 198 consecutive patients with febrile neutropenia were included in the study. The demographic characteristics of these patients corresponded to epidemiologic data published by the French Institute Survey for cancer [
16].
EDs are first dedicated to the management of patients with severe disorders including severe infections. A recent study reported that SS/SSh accounted for more than 500,000 visits annually in US EDs [
21]. In addition, the incidence of severe sepsis is increasing [
22], cancer is a predisposing factor for sepsis, and the number of cancer patients will almost double within one decade [
23]. Optimising prevention of febrile neutropenia is therefore an important part of the management. Forty-seven (24%) patients were treated with G-CSF to prevent febrile neutropenia, whereas 174 (88%) had one or more risk factors that should have prompted the prophylactic use of G-CSF [
24]. In our sample, there was an under-use of G-CSF in patients at risk of febrile neutropenia. The under-use of G-CSF in oncology practice was also reported previously by Hayes [
25]. We therefore believe that emergency physicians will have increasing chances to treat febrile neutropenia.
In their series used to derive and validate the Mortality in Emergency Department Sepsis (MEDS) score, Shapiro and colleagues reported that 35.5% and 2.5% of patients visiting the ED with infection had severe sepsis and septic shock, respectively [
12]. Here we reported that 89 (45%) patients with febrile neutropenia presented with SS/SSh. This underscores that chemotherapy-related neutropenia in cancer patients is a risk factor for developing severe infection. In our series, very few patients that developed severe infections were treated according to current guidelines. Indeed, adequate management was initiated in only six patients. This may suggest that detecting severe infections is challenging for emergency physicians. Initial severity assessment is sometimes falsely reassuring and patients may worsen during their stay in the ED [
26]. A study conducted in Brazil [
14] reported that ED physicians were able to detect severe infection in 15.8% of cases. Implementation of the Surviving Sepsis Campaign guidelines improved detection of severe infections but 61.5% of patients remained under-treated because of inadequate assessment. Measuring lactate concentration has been recommended to help physicians detect [
26] and manage severe infections [
27]. We observed that lactate was infrequently measured in the present series. Therefore, procedures to optimise detection of severe infection were partially applied in our patients that did not seem to be perceived as severely ill.
A burden of evidence supports the paramount role of early recognition and prompt management of severe infection, and admission to the ICU when applicable [
27]. The prognosis of patients with severe infection actually depends on their initial management; that is, treatment received in the ED for half of patients [
28]. We observed that few patients received adequate antimicrobial therapy or fluid challenge in an appropriate time-span. We therefore conclude that patients with severe infection were under-treated. Similar findings were reported in a large Spanish study [
29], as an incredibly low rate of patients admitted with SS/SSh received process-of-care according to bundles, even after an educational program involving physicians and nurses of the ED and ICU. An inadequate initial assessment may result from difficulties to correctly implement guidelines in a busy ED. First, equipment and physicians' skills to provide complex technical procedures to patients vary betwen hospitals [
30]. Barriers can also be related to time consumption of procedures necessary to implement procedures for severe infections. In addition, all team leaders are not fully confident in guidelines to treat severe infections [
31]. However, we checked fluid loading and delay to first antimicrobial agent that do not require specific skills or organisation. We observed that these basic treatments were not correctly delivered. In a series of sepsis with hypotension, the delay to antimicrobial agents was over six hours in more than half of patients because infection was not recognised. We believe that most patients were not treated according to guidelines because initial assessment failed to detect the severity of disease.
Despite the efforts in the past decade to produce and distribute specific guidelines for treating severe infection, difficulties persist to detect SS/SSh even in typically at-risk patients such as those with febrile neutropenia.
Delay to first antimicrobial agent has an impact on prognosis in patients presenting infection with severity criteria [
32]. Guidelines to treat patients with SS/SSh endorse that first dose of antibiotics should be given in a timespan shorter than 90 minutes [
9]. Whereas it can be assumed that earlier antimicrobial agents would improve prognosis in febrile neutropenia, no evidence can currently lead to any recommendations about delay. Consequently, guidelines to treating patients with febrile neutropenia are not clear regarding delays to treatment; therefore, objectives are easier to obtain. This may partly explain why management of patients without SS/SSh frequently reached goals.
A puzzling result is that supportive care was not modified by the intervention of the oncologist or haematologist: the presence of a medical unit dedicated to cancer in the same hospital, the existence of written procedures about febrile neutropenia, or the oncologist's advice did not improve the quality of care. Despite recent validation studies, the relevance of MASCC to guide site of care can be limited because several cornerstone items are missing from this evaluation tool [
18]. This supports the fact that the assessment of severity of infection in a short time-span appears to be particularly challenging in onco-haematological patients [
33].
The study has several limitations. Whereas simplicity of the study design presumably improved acceptability and feasibility, we cannot rule out that patients could be missed because making clinical research around the clock is sometimes difficult in busy EDs. Our study did not follow up the patients. It was decided to carry out a descriptive study and patients' outcomes were not recorded. Thus, it is unknown whether the prognosis of the patients with febrile neutropenia would have changed if recommendations had been implemented. In addition, the study was proposed to 350 French hospitals, but only 47 took part. Therefore, results could have been biased because EDs that participated were possibly more involved in the management of patients with sepsis and/or cancer. However, these centres were geographically distributed across France and were representative of French EDs because they were mostly set in general hospitals. In addition, only 19 Eds had a written procedure for febrile neutropenia. The convenience series was also limited because no patient waived the invitation to participate in this prospective study. Another limitation was the use of MASCC criteria to decide on the site of care and antimicrobial therapy because this score has never been validated in the ED setting. Stratification of patients using the MASCC scoring system is debatable as consensus meetings suggest that it is not superior to expert advice. However, the MASCC classification has been regularly used as a gold standard to stratify patients with febrile neutropenia. In addition MASCC calculation depends on the burden of the onco-haematological disorder. However, it is usually accepted that patients with advanced cancer under-estimate the severity of the disorder [
34,
35]. As emergency physicians usually obtain past medical history from patients' interviews, they may misclassify severity of febrile neutropenia when assessed by MASCC level. Finally, we found that patients with more severe and mild febrile neutropenia were inadequately treated according to a univariate analysis. We were unable to identify risk factors for inadequate management by a multivariate analysis, partly because of the size of the sample.
Acknowledgements
This study was supported by Amgen France. The funding source did not participate in the study design, data collection, analysis, interpretation of data, writing of the manuscript or the decision to submit the manuscript for publication.
We are indebted to Dr Eric Leuteneger and ABR Pharma for their valuable technical and logistical support. The study was approved by the French Society of Emergency Medicine (Société Française de Médecine d'Urgence, SFMU).
We are very grateful to all local investigators who participated in the recruitment of patients: (01) Ain: CH Bourg-en-Bresse, Dr Eskandinian; (03) Allier: CH Vichy, Dr Limoges; (06) Alpes Maritimes: CHU Nice, Dr Burgos; (07) Ardèche: CH Annonay, Dr Gauclere; (07) Ardèche: CH Aubenas, Dr Barjon; (09) Ariège: CH Val d'Ariège, Dr Mimoun; (13) Bouches-du-Rhône: CH Martigues, Dr Durand; (15) Cantal: CH Aurillac, Dr Dejou; (15) Cantal: CH Mauriac, Dr Lamalle; (17) Charente-Maritime: CH La Rochelle, Dr Tabary; (17) Charente-Maritime: CH Rochefort sur Mer, Dr Fazilleau; (19) Corrèze: CH Tulles, Dr Beaujean; (22) Côtes d'Armor: CH Saint Brieuc, Dr Floch; (24) Dordogne: CH Périgueux, Dr Ely; (26) Drôme: CH Valence, Dr Abou Abbas; (28) Eure et Loire: CH Chartres, Dr Maisonnier; (35) Ile et Vilaine: CH Saint Malo, Dr Verley; (36) Indre: CH Le Blanc, Dr Sylvestre; (37) Indre et Loire: CH Chinon, Dr Gerard; (37) Indre et Loire: CHU Tours, Pr Lanotte; (38) Isère: CHU Grenoble, Dr Ara Somohano; (40) Landes: CH Mont de Marsan, Dr Harambat; (42) Loire: CHU Saint Etienne, Dr Viallon; (44) Loire Atlantique: CH Châteaubriant, Dr Hourdin; (45) Loiret: CH Montargis, Dr Klein; (45) Loiret: CH Orléans, Dr Martin; (47) Lot et Garonne: CH Agen, Dr De Bortoli; (49) Maine et Loire: CHU Angers, Dr Pattier; (54) Meurthe et Moselle: CH Lunéville, Dr Rosa; (59) Nord: CH Dunkerque, Dr Delangue; (62) Pas de Calais: CH Saint Omer, Dr Capelle; (63) Puy de Dôme: CH Thiers, Dr Poitrineau; (63) Puy de Dôme: CHU Clermont Ferrand, Dr Peyrat; (64) Pyrénées Atlantiques: CH Bayonne, Dr Sevilla; (64) Pyrénées Atlantiques: CH Pau, Dr Mangon; (71) Saône et Loire: CH Mâcon, Dr Delbrassine; (72) Sarthe: CH Le Mans, Dr Coroller-Bec; (75) Paris: CHU Cochin, Dr André; (75) Paris: CHU Hôtel Dieu, Dr Kierzek; (75) Paris: CHU Pitié-Salpétrière, Dr Delerme; (75) Paris: CHU Saint Antoine, Dr Chaille; (75) Paris: CHU Saint Louis, Dr Taboulet; (75) Paris: CHU Tenon, Dr Cassy; (79) Deux Sèvres: CH Niort, Dr Delaunoy; (81) Tarn: CH Albi, Dr Depierre; (91) Essonne: CH Longjumeau, Dr Andrianjafy; (94) Créteil: CHU Henri Mondor, Dr Santin.
Competing interests
Yann-Erick Claessens received fees from Amgen France. All other authors declare that they have no competing interests.
Authors' contributions
SA contributed to the conception, design, and drafting of the manuscript. PT contributed to collection of the data. CE contributed to interpretation and analysis of data and drafting the manuscript. NM contributed to the critical revision of the manuscript. MN contributed to the management of the study. GK contributed to collection of the data. MB contributed to collection of the data. FP contributed to collection of the data. SC contributed to collection of the data. HC contributed to collection of the data. JLP contributed to the critical revision of the manuscript. YEC contributed to the conception, design, interpretation and analysis of data and drafting the manuscript.