Imipenem/funobactam (formerly XNW4107) in vivo pharmacodynamics against serine carbapenemase-producing Gram-negative bacteria: a novel modelling approach for time-dependent killing.

Background Imipenem/funobactam (formerly XNW4107) is a novel β-lactam/β-lactamase inhibitor with activity against MDR Acinetobacter baumannii , Pseudomonas aeruginosa and Enterobacterales strains. Using a neutropenic murine thigh infection model, we aimed to determine the pharmacokinetic/pharmacodynamic (PK/PD) index, relative to funobactam exposure, that correlated most closely with the in vivo efficacy of imipenem/funobactam combination and the magnitude of index required for efficacy against serine carbapenemase-producing clinical strains. Methods Dose-fractionation was conducted against three strains. Imipenem human-simulated regimen (HSR, 500 mg q6h 1 h infusion) efficacy in combination with escalating funobactam exposures against seven A. baumannii , four P. aeruginosa and four Klebsiella pneumoniae (imipenem/funobactam MICs 0.25–16 mg/L) was assessed as 24 h change in log₁₀cfu/thigh. Results Increased funobactam fractionation enhanced efficacy, indicating time-dependent killing. Changes in log₁₀cfu/thigh versus % f T > MIC were poorly predictive of efficacy; bactericidal activity was observed at % f T > MIC = 0%. Across different threshold plasma funobactam concentrations (C _Ts), % f T >  C _{T(1 mg/L)} had the highest correlation with efficacy. Normalizing the % f T >  C _T = 1 mg/L index to the respective isolate imipenem/funobactam MIC ([% f T >  C _T]/MIC) allowed integration of the isolate's susceptibility, which further enhanced the correlation. Median (% f T >  C _{T[1 mg/L]})/MIC values associated with 1-log reductions were 9.82 and 9.90 for A. baumannii and P. aeruginosa, respectively. Median (% f T >  C _{T[1 mg/L]})/MIC associated with stasis was 55.73 for K. pneumoniae. Imipenem/funobactam 500/250 mg q6h 1 h infusion HSR produced >1-log kill against 6/7 A. baumannii , 4/4 P. aeruginosa and stasis against 4/4 K. pneumoniae. Conclusions Imipenem/funobactam showed potent in vivo efficacy against serine carbapenemase-producers. The novel PK/PD index (% f T >  C _T)/MIC appeared to best describe in vivo activity. [ABSTRACT FROM AUTHOR]