Neonatal SEPSIS Clinical Trial
Official title:
Intravenous and Oral Fosfomycin in Hospitalised Neonates With Clinical Sepsis: an Open-label Safety and Pharmacokinetics Study (neoFosfo)
Neonatal sepsis has a high risk of morbidity and mortality. The current WHO and national guidelines recommend antibiotics to which resistance is reported in neonatal populations, although the available data is limited. Research on alternative empirical regimens for neonatal sepsis which are affordable, safe and cost-effective, with a step-down oral option, is needed. AMR is an issue of global public health concern and is one of the WHO's global health priority areas. Understanding the benefits, risks, MIC capacity and PK of fosfomycin will influence global policy on the case management of neonates with sepsis in Kenya and international settings.
Antimicrobial resistance (AMR) has become a major issue in global health. Despite progress in
the reduction of under 5 mortality rates in recent decades, the proportion of neonatal deaths
occurring within this age group has increased, with almost one quarter of all neonatal deaths
occurring due to serious bacterial infection. Common bacteria causing neonatal sepsis are now
exhibiting widespread resistance to several classes of antibiotics. There is an urgent need
to discover new, effective treatments and re-evaluate existing therapeutic agents to treat
infections potentially caused by multi-drug resistant (MDR) pathogens. Gram-negative bacteria
(GNB) predominate as the cause of neonatal sepsis, and are increasingly associated with high
rates of resistance to the currently recommended WHO empirical therapy regimen of
ampicillin/penicillin and gentamicin. There is therefore a need to develop an updated empiric
regimen with improved efficacy in the context of increasing MDR sepsis in neonates. New
antimicrobials under development will be expensive once licensed, and there are currently
virtually no planned trials to assess their efficacy in neonates in low- and middle-income
countries (LMICs).
One potential strategy is utilising an existing off-patent (and therefore affordable)
antibiotic available in intravenous and oral formulations - fosfomycin. Fosfomycin has a wide
spectrum of activity against Gram-positive and Gram-negative bacteria causing neonatal
sepsis. It is mainly used for resistant urinary tract infections in adults, but has licenced
neonatal and paediatric doses in Europe (though dosing regimens vary between countries). Both
oral and IV formulations are available. A large clinical trial to assess the efficacy of a
fosfomycin plus an aminoglycoside combination (compared to the current WHO recommended
ampicillin and gentamicin) is anticipated, including sites in Kenya. The ultimate aim is for
fosfomycin to be included in the WHO Essential Medicines List for children (EMLc) and be
available for use in developing countries, where rates of resistance to ampicillin and
gentamicin have been estimated at over 40%. The first steps before this trial are to clarify
the pharmacokinetics (PK) and safety profile of fosfomycin in neonates, as well as generating
further information regarding local patterns of bacterial susceptibility to fosfomycin. The
aim of this study is to fulfil both these steps. Fosfomycin (IV and oral) PK will be
investigated among 60 babies admitted to hospital and being treated for presumed sepsis;
administered alongside the standard antibiotics. Another 60 babies receiving standard
treatment only (without PK sampling) will be monitored in the same way to compare adverse
events. In the laboratory at CGMR-C, previously archived bacterial isolates will be tested
for their sensitivity to fosfomycin.
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