头孢洛普南在儿科领域的药代动力学和临床研究。头孢洛普南儿科研究组
[Pharmacokinetic and clinical studies with cefluprenam in the pediatric field. Pediatric Study Group of Gefluprenam].
作者信息
Fujii R, Abe T, Tajima T, Kobayashi M, Terashima I, Meguro H, Sunakawa K, Yokota T, Akita H, Kusumoto Y, Iwata S, Satoh Y, Toyonaga Y, Ishihara T, Nakamura H, Iwai N, Nakamura H, Kuno K, Katoh T, Ogawa A, Itomi K, Okumura A, Hayakawa F, Takahashi H, Etoh M
机构信息
Department of Pediatrics, School of Medicine, Teikyo University.
出版信息
Jpn J Antibiot. 1997 Jul;50(7):597-621.
Evaluation of efficacy and safety of cefluprenam (code number: E1077, abbreviation: CFLP), a newly developed injectable cephem antibiotics was conducted on adult patients with various infections, and followed by the study group organized from 39 institutions in pediatric field, as the drug showed no toxicity problems in suckling animals. Informed consents from legal representatives were obtained prior to the study. 1. Clinical efficacy. Two-hundred eighty one cases were included for analysis of clinical efficacy after 40 cases of exclusion or drop-out were subtracted from a total of 321 cases. However, the cumulative number of cases evaluable for analysis was considered to be 289, because 8 cases that had 2 different diseases at the same time were counted in each category of disease. In the cases in which causative organisms were identified (group A), 148 of 154 cases were rated as good or excellent, with an efficacy rate of 96.1%. As for clinical efficacies by disease, efficacy rates were 6/6 for purulent meningitis, 4/5 for sepsis, 95.7% (62/65) for pneumonia, 100.0% (29/29) for urinary tract infections, and 94.1% (16/17) for skin and soft tissue infections. The rate of excellent responses among excellent and good responses was 73.6% (109/148), showing a higher value than any of recent injectable beta-lactams. On 32 cases with S. pneumoniae infection, the efficacy rate of CFLP was 100.0%. In the cases where causative organisms were not identified (group B), 128 of 135 cases were rated as good or excellent, with an efficacy rate of 94.8%. In the all cases including both the group A and the group B, the efficacy rate was 95.2% (276/289) and the rate of excellent responses among excellent and good response was 70.7% (195/276). Against severe infections, CFLP exhibited excellent clinical efficacy, showing an efficacy rate of 8/8 for meningitis, 3/5 for sepsis and 100.0% (22/22) for severe pneumonia. As for bacteriological responses, eradication rates were 95.2% (177/186) in total. Against Gram-positive cocci, the eradication rate was 92.7% (76/82), with eradication rates of 94.3% (33/35) for Staphylococcus aureus, and 93.3% (28/30) for Streptococcus pneumoniae. Against Gram-negative rods, the eradication rate was 97.1% (101/104), and eradication rates were 100.0% (22/22) for Escherichia coli, 97.5% (39/40) for Haemophilus influenzae and 100.0% (19/19) for Molaxella catarrhalis. In cases in which more than 3 days of treatment with previous chemotherapy resulted in no response, the efficacy rate of CFLP was 94.2% (98/104), rated excellent in 68 cases and good in 30 cases. In these cases, the eradication rate was 98.1% (52/53). 2. Pharmacokinetics. CFLP was intravenously administerrd to 12 subjects at doses of 20 to 40 mg (potency)/kg. In 9 subjects aged more than 12 months, maximum serum levels (Cmax), T 1/2 beta and AUC of CFLP were 155.3 +/- 9.8 micrograms/ml, 1.43 +/- 0.18 hours and 111.7 +/- 15.0 micrograms.hr/ml, respectively, when a dose of 20 mg (potency)/kg was used. In 2 subjects aged not more than 12 months, the mean Cmax, T 1/2 beta and AUC were 153 micrograms/ml, 1.6 hour and 81 micrograms.hr/ml, respectively, at a dose of 20 mg(potency)/kg. The mean Cmax, T 1/2 beta and AUC were 332 micrograms/ml, 0.93 hours and 157.3 micrograms.hr/ml, respectively, in 1 subject at a dose of 40 mg (potency)/kg. In 10 subjects dosed 20 mg (potency)/kg, urinary levels were 2413 +/- 512, 1471 +/- 524, and 470 +/- 115 micrograms/ml in 0-2, 2-4, and 4-6 hours after dosing, respectively, showing a cumulative urinary excretion rate of 61.4 +/- 6.3%. In 1 subject dosed 40 mg (potency)/kg, urinary levels were 5700 and 4770 micrograms/ml in 0-2 p3d 2-4 hours after dosing, respectively, showing a cumulative urinary excretion rate of 42.1%. Cerebrospinal fluid concentrations of CFLP, on 10 subjects with purulent meningitis dosed 40-103 mg (potency)/kg were 3.2-32.9 micrograms/ml at 0.5-2 hours after administration within 4 days after the onset of
对新开发的注射用头孢烯类抗生素头孢洛奈(代号:E1077,缩写:CFLP)在患有各种感染的成年患者中进行了疗效和安全性评估,并在儿科领域由39个机构组成的研究组中进行了后续研究,因为该药物在哺乳类动物中未显示出毒性问题。在研究前获得了法定代表人的知情同意书。1. 临床疗效。从总共321例患者中排除或剔除40例后,纳入281例患者进行临床疗效分析。然而,可评估分析的累积病例数被认为是289例,因为8例同时患有两种不同疾病的患者在每种疾病类别中都被计算在内。在确定了病原体的病例(A组)中,154例中的148例被评为良好或优秀,有效率为96.1%。按疾病划分的临床疗效方面,化脓性脑膜炎的有效率为6/6,败血症为4/5,肺炎为95.7%(62/65),尿路感染为100.0%(29/29),皮肤和软组织感染为94.1%(16/17)。在良好和优秀反应中,优秀反应率为73.6%(109/148),高于近期任何一种注射用β-内酰胺类药物。在32例肺炎链球菌感染病例中,CFLP的有效率为100.0%。在未确定病原体的病例(B组)中,135例中的128例被评为良好或优秀,有效率为94.8%。在包括A组和B组的所有病例中,有效率为95.2%(276/289),在良好和优秀反应中优秀反应率为70.7%(195/276)。针对严重感染,CFLP表现出优异的临床疗效,脑膜炎的有效率为8/8,败血症为3/5,重症肺炎为100.0%(22/22)。在细菌学反应方面,总体根除率为95.2%(177/186)。针对革兰氏阳性球菌,根除率为92.7%(76/82),金黄色葡萄球菌的根除率为94.3%(33/35),肺炎链球菌的根除率为93.3%(28/30)。针对革兰氏阴性杆菌,根除率为97.1%(101/104),大肠杆菌的根除率为100.0%(22/22),流感嗜血杆菌的根除率为97.5%(39/40),卡他莫拉菌的根除率为100.0%(19/19)。在先前化疗治疗3天以上无反应的病例中,CFLP的有效率为94.2%(98/104),其中68例评为优秀,30例评为良好。在这些病例中,根除率为98.1%(52/53)。2. 药代动力学。以20至40mg(效价)/kg的剂量对12名受试者静脉注射CFLP。在9名年龄超过12个月的受试者中,当使用20mg(效价)/kg的剂量时,CFLP的血清最高浓度(Cmax)、半衰期(T 1/2β)和药时曲线下面积(AUC)分别为155.3±9.8μg/ml、1.43±0.18小时和111.7±15.0μg·hr/ml。在2名年龄不超过12个月的受试者中,当使用20mg(效价)/kg的剂量时,平均Cmax、T 1/2β和AUC分别为153μg/ml、1.6小时和81μg·hr/ml。在1名受试者中,当使用40mg(效价)/kg的剂量时,平均Cmax、T 1/2β和AUC分别为332μg/ml、0.93小时和157.3μg·hr/ml。在10名给予20mg(效价)/kg剂量的受试者中,给药后0至2小时、2至4小时和4至6小时的尿药浓度分别为2413±512、1471±524和470±115μg/ml,累积尿排泄率为61.4±6.3%。在1名给予40mg(效价)/kg剂量的受试者中,给药后0至2小时和2至4小时的尿药浓度分别为5700和4770μg/ml,累积尿排泄率为42.1%。在10名患有化脓性脑膜炎、给予40 - 103mg(效价)/kg剂量的受试者中,给药后0.5至2小时脑脊液中CFLP的浓度在发病后4天内为3.2 - 32.9μg/ml 。
Zotero 插件