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亚胺培南/西司他丁与阿米卡星联合哌拉西林治疗中性粒细胞减少患者感染的前瞻性、随机多中心研究。

Imipenem/cilastatin versus amikacin plus piperacillin in the treatment of infections in neutropenic patients: a prospective, randomized multi-clinic study.

作者信息

Norrby S R, Vandercam B, Louie T, Runde V, Norberg B, Anniko M, Andrien F, Baudrihaye M, Bow E, Burman L A

机构信息

University of Umeå, Sweden.

出版信息

Scand J Infect Dis Suppl. 1987;52:65-78.

PMID:3331044
Abstract

In this open, controlled, randomized multi-clinic trial, monotherapy with imipenem/cilastatin was compared to amikacin plus piperacillin as empiric antibacterial therapy in 210 neutropenic cancer patients. Of patients randomized, 53 (25%) had bacteriologically documented infections and of those 30 had septicemia. A further 80 patients (38%) were evaluable for clinical efficacy but did not have documented infections. Seventy-seven patients (37%) were non-evaluable due to effective antibiotic treatment before the trial, early institution of other antibiotics during the trial, verified non-bacterial infections, no neutropenia or other reasons. There were no significant differences in terms of efficacy between imipenem/cilastatin and amikacin plus piperacillin but a consistent trend towards higher rates of clinical cure or improvement and of elimination of causative pathogens was noted in the imipenem/cilastatin group. In patients who were severely neutropenic (less than 0.1 x 10(9) granulocytes/l), similar cure rates were obtained in the two treatment groups--again with a tendency towards better results in the imipenem/cilastatin group. Among evaluable patients with septicemia, one patient in the imipenem/cilastatin group had persistent Staphylococcus aureus bacteremia during treatment. Five patients in the amikacin plus piperacillin group had persistent bacteremia during treatment; all but one (a Pseudomonas aeruginosa) caused by strains resistant to amikacin or piperacillin. Clinical and laboratory adverse effects were mild in the imipenem/cilastatin group although nausea was significantly more common than in the amikacin plus piperacillin group. Among patients on amikacin plus piperacillin, one died in renal failure, possibly related to treatment. Drug-related serious adverse events were reported in two additional amikacin plus piperacillin patients; one with drug fever and one with hearing loss. Microbiological adverse effects occurred in similar frequencies in the two groups. It is concluded that imipenem/cilastatin is a promising candidate for monotherapy of bacterial infections in neutropenic cancer patients.

摘要

在这项开放性、对照、随机多中心试验中,将亚胺培南/西司他丁单药治疗与阿米卡星加哌拉西林作为经验性抗菌治疗方案,用于210例中性粒细胞减少的癌症患者。在随机分组的患者中,53例(25%)有细菌学证实的感染,其中30例患有败血症。另有80例患者(38%)可评估临床疗效,但未记录感染情况。77例患者(37%)因试验前接受有效抗生素治疗、试验期间早期使用其他抗生素、证实为非细菌感染、无中性粒细胞减少或其他原因而不可评估。亚胺培南/西司他丁与阿米卡星加哌拉西林在疗效方面无显著差异,但亚胺培南/西司他丁组在临床治愈或改善率以及消除致病病原体方面有持续升高的趋势。在严重中性粒细胞减少(粒细胞低于0.1×10⁹/L)的患者中,两个治疗组的治愈率相似——亚胺培南/西司他丁组同样有取得更好结果的趋势。在可评估的败血症患者中,亚胺培南/西司他丁组有1例患者在治疗期间出现持续性金黄色葡萄球菌菌血症。阿米卡星加哌拉西林组有5例患者在治疗期间出现持续性菌血症;除1例(铜绿假单胞菌)外,均由对阿米卡星或哌拉西林耐药的菌株引起。亚胺培南/西司他丁组的临床和实验室不良反应较轻,尽管恶心比阿米卡星加哌拉西林组明显更常见。在使用阿米卡星加哌拉西林的患者中,1例死于肾衰竭,可能与治疗有关。另外2例使用阿米卡星加哌拉西林的患者报告了与药物相关的严重不良事件;1例出现药物热,1例出现听力丧失。两组微生物学不良反应的发生率相似。得出的结论是,亚胺培南/西司他丁是中性粒细胞减少的癌症患者细菌感染单药治疗的一个有前景的候选药物。

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