首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Pharmacodynamics of vancomycin alone and in combination with gentamicin at various dosing intervals against methicillin-resistant Staphylococcus aureus-infected fibrin-platelet clots in an in vitro infection model.
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Pharmacodynamics of vancomycin alone and in combination with gentamicin at various dosing intervals against methicillin-resistant Staphylococcus aureus-infected fibrin-platelet clots in an in vitro infection model.

机译:在体外感染模型中单独使用万古霉素和与庆大霉素联用的庆大霉素在不同给药间隔时对耐甲氧西林金黄色葡萄球菌感染的纤维蛋白-血小板凝块的药效学。

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摘要

We compared the pharmacodynamic activities of vancomycin with or without gentamicin in an in vitro infection model with methicilin-resistant Staphylococcus aureus-infected fibrin-platelet clots. Infected fibrin-platelet clots (FPCs) were prepared with human cryoprecipitate, human platelets, thrombin, and the organism (approximately 10[9] CFU of MRSA-494/g) and were suspended with monofilament line in an infection model capable of simulating human pharmacokinetics. Antibiotics were bolused to simulate vancomycin regimens of 2 g every 24 h (q24h), 1 g q12h, 500 mg q6h, and continuous infusion (steady-state concentration of 20 microg/ml) and gentamicin regimens of 1.5 mg/kg of body weight q12h and 5 mg/kg once daily (q.d.). Model experiments were performed in duplicate over 72 h. FPCs were removed from the models in quadruplicate at 0, 8, 24, 32, 48, 72 h, weighed, homogenized, diluted, and plated to determine colony counts. The inoculum density at 72 h was used to compare bactericidal activities between the regimens. All regimens containing vancomycin significantly decreased the bacterial inoculum compared to the growth control (P < 0.001). Vancomycin monotherapy regimens were similar in bacterial kill regardless of dosing frequency. The addition of gentamicin (either q12h or q.d.) significantly improved the bactericidal activity of the vancomycin q6h, q12h, and q24h regimens (P < 0.001). The greatest reduction in bacterial density at 72 h (P < 0.001) and the most rapid rate of kill (time to 99.9% killing) were achieved with the regimen consisting of 2 g of vancomycin q24h plus gentamicin (q.d. or q12h).
机译:我们比较了在有耐甲氧西林的金黄色葡萄球菌感染的纤维蛋白-血小板凝块的体外感染模型中,万古霉素与庆大霉素的药理活性。用人冷沉淀物,人血小板,凝血酶和生物体(MRSA-494 / g的大约10 [9] CFU)制备感染的血纤蛋白血小板凝块(FPC),并用单丝线悬浮在能够模拟人的感染模型中药代动力学。推注抗生素以模拟每24小时(q24h)2 g,1 g q12h,500 mg q6h的万古霉素方案,并连续输注(稳态浓度为20 microg / ml)和庆大霉素方案为1.5 mg / kg体重每天一次(qd)q12h和5 mg / kg。模型实验重复进行72小时。在0、8、24、32、48、72小时一式四份地从模型中取出FPC,称重,匀浆,稀释并铺板以确定菌落计数。 72小时的接种密度用于比较方案之间的杀菌活性。与生长对照相比,所有含有万古霉素的治疗方案均能显着降低细菌接种量(P <0.001)。无论剂量如何,万古霉素单药疗法在细菌杀灭方面均相似。添加庆大霉素(q12h或q.d.)可显着改善万古霉素q6h,q12h和q24h方案的杀菌活性(P <0.001)。由2 g万古霉素q24h加庆大霉素(q.d.或q12h)组成的方案在72 h时细菌密度下降最大(P <0.001),杀灭速度最快(杀灭率达到99.9%)。

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