Pharmacokinetics and Adverse Effects of Clofazimine in the Treatment of Pulmonary Non-Tuberculous Mycobacterial Infection
被引:10
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作者:
Watanabe, Fumiya
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Meiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Fukujuji Hosp, Japan AntiTB Assoc, Dept Pharm, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Watanabe, Fumiya
[1
,2
]
Furuuchi, Koji
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Furuuchi, Koji
[3
]
Hanada, Kazuhiko
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机构:
Meiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Hanada, Kazuhiko
[1
]
Fujiwara, Keiji
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Fujiwara, Keiji
[3
]
Uesugi, Fumiko
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Uesugi, Fumiko
[3
]
Hiramatsu, Miyako
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Hiramatsu, Miyako
[3
]
Yoshiyama, Takashi
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Yoshiyama, Takashi
[3
]
Shiraishi, Yuji
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Shiraishi, Yuji
[3
]
Kurashima, Atsuyuki
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机构:
Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Kurashima, Atsuyuki
[3
]
Ohta, Ken
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Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Ohta, Ken
[3
]
Morimoto, Kozo
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Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, Japan
Fukujuji Hosp, Japan AntiTB Assoc, Dept Clin Res, Tokyo, JapanMeiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
Morimoto, Kozo
[3
,4
]
机构:
[1] Meiji Pharmaceut Univ, Dept Pharmacometr & Pharmacokinet, Tokyo, Japan
[2] Fukujuji Hosp, Japan AntiTB Assoc, Dept Pharm, Tokyo, Japan
[3] Fukujuji Hosp, Japan AntiTB Assoc, Resp Dis Ctr, Tokyo, Japan
[4] Fukujuji Hosp, Japan AntiTB Assoc, Dept Clin Res, Tokyo, Japan
Clofazimine (CFZ) is used to treat pulmonary non-tuberculous mycobacterial (NTM) infection; however, its pharmacokinetics remain unexplored in patients with pulmonary NTM, and the relationship between CFZ serum concentration and adverse effects has not been investigated. The objectives of this study were to characterize the pharmacokinetics of CFZ in pulmonary NTM disease treatment and to investigate the relationship between the steady-state CFZ serum concentration and adverse effects. A prospective observational study was conducted on 45 patients with pulmonary NTM treated with CFZ (UMIN000041053). A maximum of five serum samples per patient were taken at the CFZ trough, and serum concentration was measured using high-performance liquid chromatography-mass spectrometry (HPLC-MS). The pharmacokinetics of CFZ were analyzed using a nonlinear mixed effect model. The relationships among steady-state CFZ serum concentration and adverse effects, pigmentation, and heart rate-corrected QT (QTc) interval were investigated. Twenty-six patients had M. avium or M. intracellulare infection and nineteen had M. abscessus infection. The primary CFZ dosage was 50 mg/day. The estimated apparent CFZ clearance, apparent volume of distribution, and half-life were 2.4 L/h, 2,960 L, and 36 days, respectively. The combined use of rifampicin and CFZ significantly reduced CFZ exposure by 22%. Although there was no relationship between CFZ serum concentration and pigmentation intensity, the QTc interval was significantly correlated with CFZ serum concentration. The estimation of accurate pharmacokinetics for CFZ required approximately 5 months of monitoring. The relationship between the serum concentration and specific adverse effects of CFZ confirmed that CFZ serum concentration was not associated with pigmentation but did affect the QTc interval.
机构:
Department of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-TyneDepartment of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-Tyne
Graham J.C.
Tweddle D.A.
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机构:
Department of Child Health, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-TyneDepartment of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-Tyne
Tweddle D.A.
Jenkins D.R.
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机构:
Department of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-TyneDepartment of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-Tyne
Jenkins D.R.
Pollitt C.
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机构:
Department of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-TyneDepartment of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-Tyne
Pollitt C.
Pedler S.J.
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机构:
Department of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-TyneDepartment of Clinical Microbiology, Public Health Laboratory, Royal Victoria Infirmary NHS Trust, Queen Victoria Road, Newcastle-upon-Tyne
Pedler S.J.
European Journal of Clinical Microbiology and Infectious Diseases,
1998,
17
(6):
: 394
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397