Summary of randomized controlled trials comparing cefepime with other antibiotics in empirical therapy of febrile neutropenia, published between 2015 and March 2020

Summary of randomized controlled trials comparing cefoperazone/sulbactam with other antibiotics in empirical therapy of febrile neutropenia, published between 2010 and March 2020

Our current practice is to use cefepime as first-line EAT in both adults and pediatric high risk FN requiring intravenous therapy with an average positive response of 60%–65%. We recommend that institutes follow their local antibiotic sensitivity pattern in choosing their first-line therapy and cefepime is a valid option that can provide benefit of monotherapy.

Status of Early Discontinuation of Empirical Antibiotics in Fever of Unknown Origin (Fuo)

The traditional approach since advent of EAT for FN had been to continue antibiotics till resolution of fever and till recovery of counts. However, recent reports especially in pediatric FN found that discontinuation of antibiotics before marrow recovery did not increase fatality due to bacterial infections.[23],[24] ECIL recommends that in select patients with FUO who have been hemodynamically stable since presentation and have been afebrile for ≥48 h, EAT can be discontinued within 72 h irrespective of neutrophil recovery, however, these patients should be kept under close observation.[3] Evidence for this discontinuation approach comes from limited studies, recent ones are summarized in [Table 3].

Summary of studies evaluating early discontinuation of empirical antibiotic therapy in febrile neutropenia of unknown origin, published between 2015 and March 2020

In an open-label, randomized, controlled phase 4-trial on optimization of EAT in patients with hematological malignancies including transplant recipients with FN without etiological diagnosis, it was found safe to discontinue antibiotics after 72 h of apyrexia and clinical recovery irrespective of neutrophil count, without increasing the frequency of recurrent fever (recurrence rate 14%), secondary infections, or mortality.[26] In the prospective observational ANTIBIOSTOP study (2018), feasibility and safety of short-term antibiotic treatment in patients exhibiting FUO irrespective of their neutrophil count was evaluated and found to be safe with a response rate of 57%–59% in the two groups studied.[27] In a meta-analysis by Stern et al., on early discontinuation of antibiotics for FN, 8 RCTs comprising a total of 662 distinct FUO episodes in both adults and children were included.[28] Studies had variable designs and criteria for discontinuation of antibiotics. No significant difference was seen between the short-antibiotic therapy arm and the long-antibiotic therapy arm for all-cause mortality, clinical failure rates, and other secondary outcomes. However, the author's concluded that the existing evidence have low certainty to make strong recommendation on the safety of antibiotic discontinuation before neutropenia resolution and well-designed, adequately powered RCTs are required to address this issue in the era of rising antibiotic resistance.

In our study, discontinuation of antibiotics was successful in 60% FUO episodes, and we continue to practice this approach in select cases of FUO to minimize antibiotic use and its associated collateral damage of augmenting antibiotic resistance.

Challenges: Then and Now

One of the most important challenges at our center and in other resource limited settings from developing countries is the high prevalence of multidrug-resistant gram-negative infections both in the community and in hospital acquired settings. In our study, MDI was 34% of total episodes of FN, with a significantly high incidence of MDR GNB at 51% of total MDI. Our latest antibiogram in 2019 shows that various Gram-negative bacilli have 43%–85% sensitivity to cefoperazone-sulbactam, 45% to 95% sensitivity to amikacin, 40%–80% to cefepime, and 30%–76% for piperacillin-tazobactam. Resistance to carbapenems was seen in 5%–15% of Pseudomonas and Burkholderia species, while resistance rate was up to 55% for Klebsiella, Acinetobacter, and Escherichia coli. As there is growing resistance worldwide, newer antimicrobial agents especially against MDR GNB are very limited and pipeline of drug development is also very slow and parched, rational use of available antibiotics becomes essential for short-term patient-related outcomes and for long-term outcomes of containment of resistance.

Sending blood cultures and timely initiation of EAT at the onset of fever is essential for optimal outcome, however, full and consistent compliance to FN protocol is variable in different settings. Delayed presentation to health-care facility after onset of fever which can lead to a complicated clinical course is an added challenge in resource limited settings.

Most of the guidelines define use of empirical first line antibiotic and outline pathways for antibiotic modification at 48–72 h depending on the microbiological results and clinical course of patients. They also describe indications for the use of antifungals and antivirals. Nevertheless, the management of complicated FN beyond empirical treatment requires more of clinical experience and expertise and intensive supportive care.

Another challenge faced mostly in resource limited settings is implementation of infection control practices for both health-care workers (HCW), patients and their care-givers because of lack of alertness and incentive among HCW and poor personal hygiene, lack of resources and awareness among patients and care-givers belonging to low socioeconomic background. Regular and systematic educational sessions for all cadres of HCW as well as for patients and care-givers and methods for the assessment of compliance are imperative to improve infection control.

Way Forward

The management of FN is a collective effort, requires collaboration with Departments of Microbiology, Pharmacology, Hospital Infection Control Committee, besides the treating clinical departments of Medical Oncology, Medicine, and Pediatrics. It needs continuous monitoring of infection control practices, institute's antibiotic sensitivity patterns over time, regular audits of clinical outcomes and revision of antibiotic policies if needed, and a robust antibiotic stewardship program. Finally, institutional policies for using appropriate antibiotics has to be tailored to (i) local sensitivity data, (ii) patient's risk factor for resistant infection, and (iii) patient's risk factors for a complicated clinical course.[3] Early discontinuation of EAT is a promising approach in select cases of FUO.

FN is generally stratified as low or high risk in majority of guidelines and the standard approach in stable presentation is escalation. However, the subset of patients with prolonged and profound neutropenia as in AML induction and during salvage induction for relapsed leukemia should be considered as very high risk and may benefit from a de-escalation approach, though this indication and approach is not very clearly and separately defined in the literature. Furthermore, as stated in the ECIL guidelines, escalation and de-escalation approach with relevant indications can be a more appropriate method in the setting of high prevalence of MDR GNB.[3] This will help in reducing high infection related mortality by avoiding initial inadequate EAT and by timely initiation of appropriate antibiotic covering resistant pathogen. However, physicians frequently hesitate to de-escalate appropriately and change a regimen that has already achieved clinical improvement; this has to be overcome by a good stewardship program. Novel biomarkers for early identification of resistant pathogens like rapid molecular diagnostic tests for sepsis using nucleic acid amplification techniques or host targeted technologies may guide the way forward.[29],[30]

At our center, we have initiated a study evaluating role of sepsis bundle (with tailored antibiotic de-escalation approach based on clinical biomarkers) at the onset of very high risk FN during AML and relapsed leukemia induction. The application of sepsis bundle in FN has not been studied prospectively so far and we expect our results to be available by mid of 2021.

Conflict of Interest

There are no conflicts of interest.

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Publication History

Received: 17 May 2020

Accepted: 03 July 2020

Article published online:
17 May 2021

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