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氟莫西芬用于新生儿感染的临床评估

[Clinical evaluation of flomoxef in neonatal infections].

作者信息

Okura K, Yamakawa M, Kuroki S, Haruta T, Kobayashi Y

机构信息

Department of Pediatrics, Kobe City General Hospital.

出版信息

Jpn J Antibiot. 1991 Nov;44(11):1286-93.

PMID:1784078
Abstract

Serum concentrations, urinary excretion and clinical responses of flomoxef (FMOX) were studied. The results are summarized as follows. 1. Serum concentrations of FMOX were 17.4 micrograms/ml 1-hour after intravenous injection on the average in 5 cases who received approximately 10 mg/kg, 41.8 micrograms/ml in 2 cases given 20 mg/kg, and 69.6 micrograms/ml in 2 cases given 40 mg/kg, indicating that serum concentrations of FMOX changed in a dose-dependent manner in this range. Average serum half-life (T 1/2) in 4 mature babies was 2.48 hours and that in 6 premature babies was 3.17 hours, indicating that elimination rates in premature cases tend to be slower than those in mature cases. Urinary recovery rates averaged 39.2% in the first 6 hours in 5 cases examined. 2. Five newborns or premature babies received FMOX 33.1-80.2 mg/kg (b.i.d. or t.i.d.) via intravenous route for 5 to 8 days. FMOX showed excellent or good clinical effectiveness in the treatment of all patients including 1 case each of sepsis with urinary infection, furunclal otitis, impetigo, uterogenic fetus infection and urinary infection. Bacteriological responses were also studied, and eradication of identified organisms (Escherichia coli 3 strains and Staphylococcus aureus 2 strains) was obtained upon the FMOX treatment, but in 1 strain of S. aureus showed only a decrease. No adverse reactions were observed in any cases, but a slight elevation of eosinophil was noted in 1 patient receiving a dose of 210 mg a day. From the results obtained in these tests, FMOX appears to be very usefull and safe for the treatment of some infectious diseases in neonates.

摘要

研究了氟氧头孢(FMOX)的血清浓度、尿排泄及临床反应。结果总结如下。1. 5例接受约10mg/kg静脉注射的患者,注射后1小时血清中FMOX平均浓度为17.4μg/ml;2例接受20mg/kg的患者为41.8μg/ml;2例接受40mg/kg的患者为69.6μg/ml,表明在此剂量范围内FMOX血清浓度呈剂量依赖性变化。4例足月儿的血清平均半衰期(T1/2)为2.48小时,6例早产儿为3.17小时,表明早产儿的消除率往往比足月儿慢。5例受检者在最初6小时内尿回收率平均为39.2%。2. 5例新生儿或早产儿通过静脉途径接受33.1 - 80.2mg/kg(bid或tid)的FMOX治疗5至8天。FMOX对所有患者的治疗均显示出优异或良好的临床疗效,包括1例合并泌尿系统感染的败血症、1例疖肿性中耳炎、1例脓疱病、1例子宫源性胎儿感染及1例泌尿系统感染。还研究了细菌学反应,FMOX治疗后鉴定出的微生物(3株大肠杆菌和2株金黄色葡萄球菌)被根除,但1株金黄色葡萄球菌仅有所减少。所有病例均未观察到不良反应,但1例每日接受210mg剂量的患者嗜酸性粒细胞略有升高。从这些试验结果来看,FMOX在治疗新生儿某些传染病方面似乎非常有用且安全。

相似文献

1
[Clinical evaluation of flomoxef in neonatal infections].氟莫西芬用于新生儿感染的临床评估
Jpn J Antibiot. 1991 Nov;44(11):1286-93.
2
[Pharmacokinetic and clinical studies on flomoxef in neonates and premature infants].氟氧头孢在新生儿及早产儿中的药代动力学与临床研究
Jpn J Antibiot. 1991 Nov;44(11):1240-9.
3
[Laboratory and clinical evaluations of flomoxef sodium in neonates].
Jpn J Antibiot. 1991 Nov;44(11):1265-85.
4
[Flomoxef in neonates and young infants; clinical efficacy, pharmacokinetic evaluation and effect on the intestinal bacterial flora].
Jpn J Antibiot. 1991 Nov;44(11):1216-27.
5
[Pharmacokinetic and clinical studies on flomoxef in mature and premature infant].氟氧头孢在足月儿和早产儿中的药代动力学及临床研究
Jpn J Antibiot. 1991 Nov;44(11):1294-302.
6
[Pharmacokinetic and clinical evaluations of flomoxef in neonates].氟氧头孢在新生儿中的药代动力学及临床评价
Jpn J Antibiot. 1991 Nov;44(11):1259-64.
7
[Pharmacokinetics and clinical studies on flomoxef in neonates and premature infants. A study of flomoxef in the perinatal collaboration research group].氟氧头孢在新生儿和早产儿中的药代动力学及临床研究。围产期协作研究组关于氟氧头孢的一项研究
Jpn J Antibiot. 1993 Jul;46(7):518-38.
8
[Pharmacokinetics and clinical efficacy of flomoxef in neonates].氟氧头孢在新生儿中的药代动力学及临床疗效
Jpn J Antibiot. 1991 Nov;44(11):1228-39.
9
[Studies of flomoxef in neonates].[氟氧头孢在新生儿中的研究]
Jpn J Antibiot. 1991 Nov;44(11):1250-8.
10
[Bacteriological and clinical studies of flomoxef in the field of pediatrics].
Jpn J Antibiot. 1987 Aug;40(8):1393-406.

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