Abstract Background Antimicrobial resistance among GN pathogens is a serious global public health issue, affecting adult and pediatric populations. New treatment options for carbapenem-resistant or ESBL-producing pathogens are needed. Methods This study was a Phase 2/3, open-label, randomized, active-controlled, multinational clinical study enrolling children (birth to 18 years old) with confirmed or suspected hospital-acquired/ventilator-associated bacterial pneumonia, complicated intra-abdominal infection, or complicated urinary tract infection including pyelonephritis. Participants required hospitalization and intravenous antibacterial therapy and were randomized 3:1 to IMI/REL or active control. Bacterial pathogens isolated from primary infection sites were sent to a central laboratory (IHMA; Schaumburg, IL, USA) for testing by broth microdilution of IMI/REL using CLSI guidelines. Molecular mechanisms of resistance to IMI and/or IMI/REL were characterized; PFGE typing was used to determine relatedness of isolates. Susceptibility and molecular characterization of isolates were compared to surveillance data from SMART, a global surveillance study monitoring pathogen prevalence and resistance of GN bacteria. Results Of 115 participants randomized, 90 were in the microbiological modified intent-to-treat population (mMITT) population. MIC distributions from clinical trial and surveillance isolates were similar (Fig 1-4). IMI nonsusceptible (NS) baseline pathogens (7 Enterobacterales (non-Morganellaceae) (N=4) and P. aerguinosa (N=3)) from the mMITT population were evaluated for resistance determinants against β-lactams using PCR and sequencing. Of the 4 IMI NS Enterobacterales isolates evaluated, 3 were susceptible (S) to IMI/REL, (the isolates carrying KPC, AmpC, or no acquired β-lactamase were S), the isolate carrying NDM-1 was NS. Of the 3 IMI NS Psa isolates evaluated, 1 was S to IMI/REL, with 1 isolate carrying PDC-374 being S, and the isolate carrying the VEB-9 ESBL and 1 of the isolates carrying PDC-374 being NS. Conclusion Isolates from this clinical trial were generally susceptible to IMI/REL with low MICs and representative of pediatric surveillance isolates. Disclosures Katherine Young, M.S., Merck & Co., Inc.: Stocks/Bonds (Public Company) David W. Hilbert, PhD, Merck & Co., Inc.: Stocks/Bonds (Public Company) Carmelle Norice, MD, Merck & Co., Inc.: Stocks/Bonds (Public Company) Prachi Nair, BS, Merck & Co., Inc.: Stocks/Bonds (Private Company) Christopher Bruno, MD, Merck & Co., Inc.: Stocks/Bonds (Public Company)
Young et al. (Thu,) studied this question.