Flomoxef and fosfomycin in combination for the treatment of neonatal sepsis in the setting of highly prevalent antimicrobial resistance

Author:

Darlow Christopher A.1ORCID,Farrington Nicola1,Johnson Adam1,McEntee Laura1,Unsworth Jennifer1,Jimenez-Valverde Ana1,Kolamunnage-Dona Ruwanthi2,Da Costa Renata M A3,Ellis Sally3,Franceschi François3,Sharland Mike4,Neely Michael5,Piddock Laura J. V.3ORCID,Das Shampa1ORCID,Hope William1

Affiliation:

1. Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool Health Partners, UK

2. Department of Health Data Science, University of Liverpool, Liverpool Health Partners, UK

3. Global Antibiotic Research and Development Partnership, 15 Chemin Camille-Vidart, 1202 Geneva, Switzerland

4. Paediatric Infectious Diseases Research Group, St George’s, University of London, UK

5. Children’s Hospital Los Angeles and the Keck School of Medicine, University of Southern California, Los Angeles, CA, USA

Abstract

Abstract Background Neonatal sepsis is a serious bacterial infection of neonates, globally killing up to 680 000 babies annually. It is frequently complicated by antimicrobial resistance, particularly in low- and middle-income country (LMIC) settings with widespread resistance to the WHO’s recommended empirical regimen of ampicillin and gentamicin. Objectives We assessed the utility of flomoxef and fosfomycin as a potential alternative empirical regimen for neonatal sepsis in these settings. Methods We studied the combination in a 16-arm dose-ranged hollow-fibre infection model (HFIM) experiment and chequerboard assays. We further assessed the combination using clinically relevant regimens in the HFIM with six Enterobacterales strains with a range of flomoxef/fosfomycin MICs. Results Pharmacokinetic/pharmacodynamic modelling of the HFIM experimental output, along with data from chequerboard assays, indicated synergy of this regimen in terms of bacterial killing and prevention of emergence of fosfomycin resistance. Flomoxef monotherapy was sufficient to kill 3/3 strains with flomoxef MICs ≤0.5 mg/L to sterility. Three of three strains with flomoxef MICs ≥8 mg/L were not killed by fosfomycin or flomoxef monotherapy; 2/3 of these were killed with the combination of the two agents. Conclusions These data suggest that flomoxef/fosfomycin could be an efficacious and synergistic regimen for the empirical treatment of neonatal sepsis in LMIC settings with prevalent antimicrobial resistance. Our HFIM results warrant further assessment of the flomoxef/fosfomycin combination in clinical trials.

Funder

GARDP

German Federal Ministry of Education and Research

German Federal Ministry of Health

Médecins Sans Frontières

Netherlands Ministry of Health, Welfare and Sport

United Kingdom Department for International Development

United Kingdom National Institute of Health Research

North West England Medical Research Council Fellowship Scheme in Clinical Pharmacology and Therapeutics

Medical Research Council

University of Liverpool

University of Manchester

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology,Microbiology (medical)

Reference47 articles.

1. Neonatal sepsis;Shane;Lancet,2017

2. Neonatal cause-of-death estimates for the early and late neonatal periods for 194 countries: 2000-2013;Oza;Bull World Health Organ,2015

3. Estimates of possible severe bacterial infection in neonates in sub-Saharan Africa, south Asia, and Latin America for 2012: a systematic review and meta-analysis;Seale;Lancet Infect Dis,2014

4. Antibiotic use for sepsis in neonates and children: 2016 evidence update;Fuchs;WHO-Reviews,2016

5. Pocket book of hospital care for children;WHO,2013

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