Clinical pharmacological study of tazobactam/piperacillin in patients with community-acquired pneumonia

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Vol.58 No.S-1 March 2010

Akira Watanabe¹⁾, Nobuki Aoki²⁾, Yoshihito Niki³⁾, Atsushi Saito⁴⁾, Shigeru Kohno⁵⁾ and Kohya Shiba⁶⁾

¹⁾Research Division for Development of Anti-Infective Agents, Institute of Development, Aging and Cancer, Tohoku University, 4-1 Seiryo, Aoba-ku, Sendai, Miyagi, Japan
²⁾Department of Internal Medicine, Shinrakuen Hospital
³⁾Department of Clinical Infectious Diseases, Showa University School of Medicine
⁴⁾Japanese Red Cross Nagasaki Genbaku Isahaya Hospital
⁵⁾Division of Molecular and Clinical Microbiology, Department of Molecular Microbiology and Immunology, Nagasaki University Graduate School of Biomedical Sciences (Second Department of Internal Medicine)
⁶⁾Jikei University School of Medicine

Abstract

A clinical pharmacological study of tazobactam/piperacillin(TAZ/PIPC), a β-lactamase inhibitor combined with penicillin antibiotic, was conducted on patients with community-acquired pneumonia, together with population pharmacokinetics(PPK) and pharmacokinetics-pharmacodynamics(PK-PD) analysis. Results confirmed TAZ/PIPC dosage propriety for this group of patients.
1. PPK analysis: Patients with pneumonia were compared to healthy adult volunteers for PIPC and TAZ PK parameters. Systemic clearance was lower and the half-life (t_1/2) was longer in those with pneumonia than in healthy volunteers. The steady-state volume of distribution (V) of TAZ in patients with pneumonia was 1.23 times and of PIPC 1.30 times as large as those in healthy adult volunteers. C_max in blood was lower in patients with pneumonia.
2. Clinical effect: Response three days after treatment was 11.6% (5/43 patients) and time to completion/discontinuation of treatment was 86.0% (37/43 patients). Improvement seven days after completion of treatment was 81.4% (35/43 patients).
3. PK-PD analysis: Streptococcus pneumoniae, Haemophilus influenzae, and Moraxella (Branhamella) catarrhalis were detected in 24 patients, and all cases were judged to have "disappeared." Calculated time above MIC (%) was 100% in all cases but one (94.6%). When TAZ/PIPC was administered three times a day (4.5 g×3) or four times a day (4.5 g×4) to patients with pneumonia whose Ccr was 120 mL/min, MIC allowing time above MIC (%) exceeding 30% were 32 μg/mL and 64 μg/mL.
4. Safety: Drug-related adverse events numbering 54 were recognized in 24 patients, i.e., an incidence of 40.0%. Of laboratory test abnormalities, 32 adverse events recognized in 16 patients were regarded as drug-related i.e., an incidence of 26.7%.
Given these results, the appropriate TAZ/PIPC dosage adopted for treatment of community-acquired pneumonia is three times daily at 4.5 g.

Key word

tazobactam/piperacillin, community acquired pneumonia, population pharmacokinetics, PK-PD, clinical trial

Received

June 10, 2009

Accepted

December 8, 2009

Jpn. J. Chemother. 58 (S-1): 11-28, 2010