The purpose of this study was to critically evaluate the impact of an institutional blood culture notification protocol called RAIDS (rapid administration of antimicrobials by an infectious diseases specialist) on t...The purpose of this study was to critically evaluate the impact of an institutional blood culture notification protocol called RAIDS (rapid administration of antimicrobials by an infectious diseases specialist) on time to optimization of antimicrobial therapy in hospitalized patients with gram-negative bacteremia. Time to antibiotic optimization was compared in patients with gram-negative bacilli isolated from blood cultures obtained from March-May 2011 (pre-RAIDS) versus March-May 2013 (post-RAIDS). The results show that patients in the pre-RAIDS study group had a significantly longer time to antibiotic optimization when compared to the post-RAIDS group (median (IQR), 27.6 (10.8-75.8) h vs. 3.1 (0.8-34.3) h, p = 0.03). The RAIDS protocol resulted in quicker time to antibiotic de-escalation (pre- vs. post-RAIDS; median (IQR), 27.6 (10.8-134.5) h vs. 4.3 (1.4-32.6) h, p = 0.03). There were no differences in clinical outcomes such as clinical cure, microbiological cure, and 30-day mortality between pre-RAIDS and post-RAIDS study groups. Patients in the post-RAIDS arm were more likely to receive appropriate empiric and definitive treatment. Implementation of the RAIDS protocol, which was an ASP (antimicrobial stewardship program) initiative, resulted in quicker time to antibiotic de-escalation and overall treatment optimization. RAIDS reduced the unnecessary use of broad-spectrum antimicrobial in this study population.展开更多
文摘The purpose of this study was to critically evaluate the impact of an institutional blood culture notification protocol called RAIDS (rapid administration of antimicrobials by an infectious diseases specialist) on time to optimization of antimicrobial therapy in hospitalized patients with gram-negative bacteremia. Time to antibiotic optimization was compared in patients with gram-negative bacilli isolated from blood cultures obtained from March-May 2011 (pre-RAIDS) versus March-May 2013 (post-RAIDS). The results show that patients in the pre-RAIDS study group had a significantly longer time to antibiotic optimization when compared to the post-RAIDS group (median (IQR), 27.6 (10.8-75.8) h vs. 3.1 (0.8-34.3) h, p = 0.03). The RAIDS protocol resulted in quicker time to antibiotic de-escalation (pre- vs. post-RAIDS; median (IQR), 27.6 (10.8-134.5) h vs. 4.3 (1.4-32.6) h, p = 0.03). There were no differences in clinical outcomes such as clinical cure, microbiological cure, and 30-day mortality between pre-RAIDS and post-RAIDS study groups. Patients in the post-RAIDS arm were more likely to receive appropriate empiric and definitive treatment. Implementation of the RAIDS protocol, which was an ASP (antimicrobial stewardship program) initiative, resulted in quicker time to antibiotic de-escalation and overall treatment optimization. RAIDS reduced the unnecessary use of broad-spectrum antimicrobial in this study population.
