Clinical and microbiological evaluation of extended-spectrum β-lactamase producing <i>Escherichia coli</i> bacteremia

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Vol.57 No.6 November 2009

Clinical and microbiological evaluation of extended-spectrum β-lactamase producing Escherichia coli bacteremia

Yukihiro Yamaguchi¹⁾, Tetsuro Muratani^2,3), Kohei Okubo⁴⁾ and Tetsuro Matsumoto²⁾

¹⁾Departments of Internal Medicine, Infectious Diseases, Kenwakai Otemachi Hospital, 15-1 Otemachi, Kokura-Kita, Fukuoka, Japan
²⁾Department of Urology, University of Occupational and Environmental Health
³⁾Department of Clinical Laboratory, Kyurin Corporation
⁴⁾Department of Clinical Laboratory, Kenwakai Otemachi Hospital

Abstract

Subjects were 10 consecutive patients with bacteremia caused by extended-spectrum β-lactamase(ESBL)-producing Escherichia coli seen from March to November 2009 and evaluated for microbiology data, clinical course, and clinical outcome. Their mean age was 82.3 years (59-103 years). Hospital acquired infection cases numbered 4, cases of admission from nursing homes 5, and strictly community-acquired infection cases 1. All strains were susceptible to meropenem, imipenem/cilastatin, piperacillin/tazobactam, flomoxef, and amikacin, followed by fosfomycin, faropenem, gentamicin, and trimethoprim/sulfamethoxazole. All strains were highly resistant to levofloxacin. Clinical presentation involved 3 cases of septic shock, 4 of severe sepsis, 2 of sepsis, and 1 of non-sepsis. Infection sources numbered 6 of urinary tract infections, 3 of primary sepsis, and 1 of cholangitis. ESBL strains numbered 4 of CTX-M-14 and 2 each of CTX-M14+CTX-M-2 and CTX-M3. In one case in which the isolated strain was not retained, polymerase chain reaction(PCR) was not done. Result of pulsed-field gel electrophoresis(PFGE) after cutting by Not I for eight strains, excluding case 2 and case 3, showed two pairs of identical patterns, but other strains differed. No outbreak from a single strain was seen. Crude mortality was 40% and 14-day mortality in the flomoxef group was 16.7%, not inferior to mortality in the imipenem/cilastatin group (50%). Flomoxef may therefore be a good choice for deescalation of ESBL producing E. coli bacteremia, although its narrow spectrum is not feasible for empiric therapy in hospital-acquired bacteremia. To reduce carbapenem consumption and prevent further resistance, it is important to evaluate flomoxef efficacy in treating ESBL-producing organisms.

Key word

Escherichia coli, Extended-spectrum β-lactamase, bacteremia, flomoxef

Received

May 25, 2009

Accepted

September 17, 2009

Jpn. J. Chemother. 57 (6): 502-507, 2009