Population pharmacokinetics of doxapram in low-birth-weight Japanese infants with apnea

被引:0
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作者
Yuki Ogawa
Mitsuru Irikura
Yuka Kobaru
Mayu Tomiyasu
Yoshie Kochiyama
Mamiko Uriu
Yoichi Ishitsuka
Yuki Kondo
Eiji Yukawa
Noboru Kamada
Hitoshi Ohno
Toshio Yamazaki
Tetsumi Irie
机构
[1] Kumamoto University,Department of Clinical Chemistry and Informatics, Graduate School of Pharmaceutical Sciences
[2] Daiichi University,Laboratory of Evidence
[3] Kissei Pharmaceutical Co.,Based Pharmacotherapy, College of Pharmaceutical Sciences
[4] Ltd.,Pharmacokinetics Research
[5] Fujita Health University,Department of Pediatrics, School of Medicine
[6] Kumamoto University,Center for Clinical Pharmaceutical Sciences
来源
European Journal of Pediatrics | 2015年 / 174卷
关键词
Apnea; NONMEM; Population pharmacokinetics; Premature infants; Doxapram;
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学科分类号
摘要
This study aimed to determine the population pharmacokinetics of doxapram in low-birth-weight (LBW) infants. A total of 92 serum concentration measurements that were obtained from 34 Japanese neonates were analyzed using nonlinear mixed-effect modeling (NONMEM). Estimates generated by NONMEM indicated that clearance of doxapram (CL; L/kg/h) was affected by postmenstrual age (PMA; weeks), body weight (BW; g), and aspartate aminotransferase (AST; IU/L). In addition, the volume of distribution (Vd; L/kg) was affected by gestational age (GA; weeks). The final pharmacokinetic model was as follows: CL = BW / PMA × 0.0453 × serum AST−0.373; Vd = 2.54 (if GA >28 weeks) and Vd = 2.54 × 2.11 (if GA ≤28 weeks). The interindividual variabilities in CL and Vd were 39.9 and 83.0 %, respectively, and the residual variability was 20.9 %. To clarify the reasons for large interindividual variations, the enzymes involved in the metabolic pathway of doxapram were also determined. We found that doxapram was metabolized by CYP3A4/5.
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页码:509 / 518
页数:9
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