Antimicrobials, Multiple Drug Resistance & Antibiotics Resistance

Biography

Biography: Ghassan Matar

Abstract

The range of antimicrobial agents that can be used to treat bacterial infections is becoming limited with the constant increase in antimicrobial resistance (AMR). Several genetic factors underlie AMR, including β-lactamase-encoding genes such as bla_CTXM-15 that confers resistance to third-generation cephalosporins, and bla_OXA-48, bla_NDM-1, and bla_KPC-2 that confer resistance to carbapenems. Remaining treatment approaches for such resistant infections include antimicrobial combination therapy and the use of β-lactamase inhibitors. This study assesses the molecular effects of such treatment approaches on antimicrobial resistant Enterobacteriaceae clinical isolates in vitro and in vivo.

Nine clinical Enterobacteriaceae isolates were included in the study. One harboring bla_CTXM-15, one harboring bla_OXA-48, one harboring bla_KPC-2, two harboring bla_NDM-1 and bla_CTXM-15, and four harboring bla_OXA-48 and bla_CTXM-15. Minimal inhibitory concentrations were determined for carbapenems with β-lactamase inhibitors: avibactam, Ca-EDTA, and relebactam. Synergism between antibiotic combinations was determined by double disc diffusion when using colistin with several antibiotics. In vitro and in vivo gene expression levels were done on these combinations with and without inhibitors.

The use of meropenem, imipenem, and ertapenem with the selected β-lactamase inhibitors restored isolate susceptibility in 100%, 87.5%, and 25% of the cases, respectively. Antimicrobial synergism was mostly detected between colistin and meropenem, fosfomycin, or tigecycline. Survival studies revealed the survival of most mice receiving antimicrobial combination therapy with inhibitors as compared to the controls. Overall gene expression levels of resistance genes were variable depending on treatment.

The threat of antibiotic resistant bacterial infections remains viable; however, different approaches to therapy are available.