# Pharmacokinetics and safety of fosfomycin and flomoxef administered as part of neonatal sepsis treatment (NeoSep1 Part 1)

**Authors:** Adrie Bekker, Navarat Panjasawatwong, Louise F. Hill, Wolfgang Stohr, A. Sarah Walker, Sally Ellis, Angela Dramowski, Andrew Whitelaw, Christina Obiero, James A. Berkley, Alexander Makazi, Sithembiso Velaphi, Reenu Thomas, Petronella Magagula, Ilhaam Abrahams, Firdose L. Nakwa, Mohammed M. Barday, Alison Van Kwawegen, Kamla Pillay, Silke Gastine, Joseph F. Standing, Peter Skoutari, Francesca Schiavone, Mike Sharland, Seamus O’Brien, Julia A. Bielicki, Tim R. Cressey

PMC · DOI: 10.1128/aac.01126-25 · Antimicrobial Agents and Chemotherapy · 2025-12-29

## TL;DR

This study evaluated the safety and drug levels of fosfomycin and flomoxef in neonates, showing they are safe and effective for treating sepsis.

## Contribution

The study provides new pharmacokinetic data and safety evidence for neonatal use of fosfomycin and flomoxef.

## Key findings

- Fosfomycin and flomoxef achieved 100% target attainment for specific MICs in neonates.
- Adverse events were mostly mild and did not require treatment changes.
- Drug exposures were consistent with published studies, supporting proposed dosing.

## Abstract

Neonatal doses for the off-patent antibiotics fosfomycin and flomoxef, which offer coverage against many extended-spectrum beta-lactamase (ESBL)-producing organisms, are based on limited data. We performed a pharmacokinetic (PK) and safety study of fosfomycin and flomoxef to confirm proposed neonatal dosing before further investigation in a trial (NeoSep1, ISRCTN48721236). Neonates with suspected sepsis, weighing more than 1,000 g, were sequentially enrolled into three antibiotic treatment cohorts: fosfomycin and amikacin (Cohort 1), flomoxef and amikacin (Cohort 2), and flomoxef and fosfomycin (Cohort 3), and followed for 28 days. Plasma samples were taken for PK assessment, with population PK modeling and simulations performed. Sixty-two neonates (48/62 [77%] preterm; 48/62 [77%] ≤7 days postnatal age [PNA]) received at least one dose of study antibiotics. Fosfomycin and flomoxef plasma concentrations were best described by a two-compartment and a one-compartment model, respectively, with postmenstrual age and PNA significantly influencing clearance. The probability of target attainment for fosfomycin was 100% for minimum inhibitory concentrations (MICs) of up to 8 mg/L, and for flomoxef, it was 100% for MICs of up to 0.5 mg/L. Adverse events (AEs) were common in this critically ill cohort. Thirteen (21%) neonates developed 19 trial antibiotic-related AEs (17 with grade ≤2, and 2 of grade 3), none of which required modification or discontinuation of allocated treatment. Seven neonates (11.6%) died. In this predominately preterm population, fosfomycin and flomoxef were safe, with drug exposures similar to published studies supporting the proposed doses for the larger, randomized NeoSep1 trial.

This study is registered with ISRCTN48721236.

## Linked entities

- **Chemicals:** fosfomycin (PubChem CID 441029), flomoxef (PubChem CID 65864), amikacin (PubChem CID 37768)
- **Diseases:** neonatal sepsis (MONDO:0700217)

## Full-text entities

- **Diseases:** sepsis (MESH:D018805), critically ill (MESH:D016638), events (MESH:D002318)
- **Chemicals:** Fosfomycin (MESH:D005578), flomoxef (MESH:C045693), PNA (MESH:D020135), amikacin (MESH:D000583)

## Full text

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## Figures

3 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12888880/full.md

## References

44 references — full list in the complete paper: https://tomesphere.com/paper/PMC12888880/full.md

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Source: https://tomesphere.com/paper/PMC12888880