头孢托罗在小鼠大腿和肺部感染模型中对多种细菌病原体的体内药效学研究。
In vivo pharmacodynamics of ceftobiprole against multiple bacterial pathogens in murine thigh and lung infection models.
作者信息
Craig W A, Andes D R
机构信息
Department of Medicine, Section of Infectious Diseases, University of Wisconsin School of Medicine and Public Health, Madison, WI, USA.
出版信息
Antimicrob Agents Chemother. 2008 Oct;52(10):3492-6. doi: 10.1128/AAC.01273-07. Epub 2008 Aug 1.
Ceftobiprole medocaril is the parenteral prodrug of ceftobiprole, a novel pyrrolidinone broad-spectrum cephalosporin with in vitro and in vivo bactericidal activities against methicillin-resistant Staphylococcus aureus (MRSA) and penicillin-resistant Streptococcus pneumoniae (PRSP). We have used murine thigh and lung infection models in neutropenic and normal mice to characterize the in vivo pharmacokinetic (PK)-pharmacodynamic (PD) activities of ceftobiprole against multiple strains of S. aureus (including MRSA), S. pneumoniae (including PRSP), and gram-negative bacilli. Serum levels of ceftobiprole following the administration of multiple doses were determined by a microbiological assay. In vivo bactericidal activities and postantibiotic effects (PAEs) of ceftobiprole against MRSA and PRSP strains were determined from serial CFU/thigh values following single doses of ceftobiprole (40 and 160 mg/kg of body weight). Dose fractionation studies were used to determine which PK-PD index correlated best with activity. Magnitudes of the PK-PD indices were calculated from MICs and PK parameters. A sigmoid dose-response model was used to estimate the dose (mg/kg/24 h) required to achieve a static and 2-log(10) kill effects over 24 h. PK results showed area under the concentration-time curve/dose values of 1.8 to 2.8 and half-lives of 0.29 to 0.51 h. MICs ranged from 0.015 to 2 microg/ml. Ceftobiprole demonstrated time-dependent killing; its in vivo PAEs varied from 3.8 h to 4.8 h for MRSA and from 0 to 0.8 h for PRSP. The time above MIC (T > MIC) correlated best with efficacy for both MRSA and PRSP. The T > MIC values required for the static doses were significantly longer (P < 0.001) for Enterobacteriaceae (36 to 45%) than for S. aureus (14 to 28%) and S. pneumoniae (15 to 22%). The drug showed activities in the lung model similar to those in the thigh model. The presence of neutrophils significantly enhanced the activity of ceftobiprole against S. pneumoniae but only slightly against Klebsiella pneumoniae. Based on its PD profile, ceftobiprole is a promising new beta-lactam agent with activity against gram-negative and gram-positive organisms including MRSA and PRSP.
头孢比普甲磺酸盐是头孢比普的肠外前体药物,头孢比普是一种新型吡咯烷酮类广谱头孢菌素,对耐甲氧西林金黄色葡萄球菌(MRSA)和耐青霉素肺炎链球菌(PRSP)具有体外和体内杀菌活性。我们使用了中性粒细胞减少和正常小鼠的鼠大腿和肺部感染模型,以表征头孢比普对多株金黄色葡萄球菌(包括MRSA)、肺炎链球菌(包括PRSP)和革兰氏阴性杆菌的体内药代动力学(PK)-药效学(PD)活性。多次给药后头孢比普的血清水平通过微生物测定法确定。头孢比普对MRSA和PRSP菌株的体内杀菌活性和抗生素后效应(PAE)由单次剂量头孢比普(40和160mg/kg体重)后的连续CFU/大腿值确定。剂量分割研究用于确定哪个PK-PD指数与活性相关性最佳。PK-PD指数的大小由MIC和PK参数计算得出。使用S形剂量反应模型估计在24小时内实现静态和2-log(10)杀灭效果所需的剂量(mg/kg/24小时)。PK结果显示浓度-时间曲线下面积/剂量值为1.8至2.8,半衰期为0.29至0.51小时。MIC范围为0.015至2μg/ml。头孢比普表现出时间依赖性杀菌作用;其对MRSA的体内PAE为3.8小时至4.8小时,对PRSP为0至0.8小时。高于MIC的时间(T>MIC)与MRSA和PRSP的疗效相关性最佳。肠杆菌科细菌达到静态剂量所需的T>MIC值(36%至45%)显著长于金黄色葡萄球菌(14%至28%)和肺炎链球菌(15%至22%)(P<0.001)。该药物在肺部模型中的活性与在大腿模型中的活性相似。中性粒细胞的存在显著增强了头孢比普对肺炎链球菌的活性,但对肺炎克雷伯菌的活性仅略有增强。基于其PD特征,头孢比普是一种有前景的新型β-内酰胺类药物,对包括MRSA和PRSP在内的革兰氏阴性和革兰氏阳性菌具有活性。
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