Effectiveness of cefmetazole versus meropenem for invasive urinary tract infections caused by extended-spectrum β-lactamase-producing Escherichia coli

Author:

Hayakawa Kayoko1ORCID,Matsumura Yasufumi2ORCID,Uemura Kohei3,Tsuzuki Shinya14,Sakurai Aki5,Tanizaki Ryutaro6,Shinohara Koh2ORCID,Hashimoto Takehiro7,Hase Ryota8,Matono Takashi9,Kato Hideaki10ORCID,Mawatari Momoko11,Hara Hiroshi12,Hamada Yukihiro13,Saito Sho1,Ohmagari Norio1,Doi Yohei514

Affiliation:

1. Disease Control and Prevention Center, National Center for Global Health and Medicine , Tokyo, Japan

2. Department of Clinical Laboratory Medicine, Kyoto University Graduate School of Medicine , Kyoto, Japan

3. Interfaculty Initiative in Information Studies, The University of Tokyo , Tokyo, Japan

4. Faculty of Medicine and Health Sciences, University of Antwerp , Antwerp, Belgium

5. Departments of Microbiology and Infectious Diseases, Fujita Health University School of Medicine , Aichi, Japan

6. Department of Internal Medicine and General Medicine, Ise Municipal General Hospital , Mie, Japan

7. Infection Control Center, Oita University Hospital , Oita, Japan

8. Department of Infectious Diseases, Japanese Red Cross Narita Hospital , Chiba, Japan

9. Department of Infectious Diseases, Aso Iizuka Hospital , Fukuoka, Japan

10. Infection Prevention and Control Department, Yokohama City University Hospital , Kanagawa, Japan

11. Department of Infectious Diseases, Japanese Red Cross Medical Center , Tokyo, Japan

12. Department of pharmacy, Yokohama Brain and Spine Center , Kanagawa, Japan

13. Department of pharmacy, Tokyo Women’s Medical University Hospital , Tokyo, Japan

14. Division of Infectious Diseases, University of Pittsburgh School of Medicine , Pittsburgh, Pennsylvania, USA

Abstract

ABSTRACT Cefmetazole is active against extended-spectrum β-lactamase-producing Escherichia coli (ESBLEC) and is a potential candidate for carbapenem-sparing therapy. This multicenter, observational study included patients hospitalized for invasive urinary tract infection due to ESBLEC between March 2020 and November 2021 at 10 facilities in Japan, for whom either cefmetazole or meropenem was initiated as a definitive therapy within 96 h of culture collection and continued for at least 3 d. Outcomes included clinical and microbiological effectiveness, recurrence within 28 d, and all-cause mortality (14 d, 30 d, in-hospital). Outcomes were adjusted for the inverse probability of propensity scores for receiving cefmetazole or meropenem. Eighty-one and forty-six patients were included in the cefmetazole and meropenem groups, respectively. Bacteremia accounted for 43% of the cefmetazole group, and 59% of the meropenem group. The crude clinical effectiveness, 14 d, 30 d, and in-hospital mortality for patients in the cefmetazole and meropenem groups were 96.1% vs 90.9%, 0% vs 2.3%, 0% vs 12.5%, and 2.6% vs 13.3%, respectively. After propensity score adjustment, clinical effectiveness, the risk of in-hospital mortality, and the risk of recurrence were similar between the two groups ( P = 0.54, P = 0.10, and P = 0.79, respectively). In all cases with available data (cefmetazole : n = 61, meropenem : n = 22), both drugs were microbiologically effective. In all isolates, bla CTX-M was detected as the extended-spectrum β-lactamase gene. The predominant CTX-M subtype was CTX-M-27 (47.6%). Cefmetazole showed clinical and bacteriological effectiveness comparable to meropenem against invasive urinary tract infection due to ESBLECs.

Funder

Grant-in Aid for Scientific Research

MHLW

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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