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Liposome-encapsulated-amikacin therapy of Mycobacterium avium complex infection in beige mice.

机译:脂质体包裹的阿米卡星治疗米色小鼠鸟分枝杆菌复合体感染。

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摘要

Efficacy of liposome-encapsulated amikacin and free amikacin against Mycobacterium avium complex was evaluated in the beige mouse (C57BL/6J-bgJ/bgJ) acute infection model. Approximately 10(7) viable M. avium complex serotype 1 cells for which the MIC of amikacin was 8 micrograms/ml were given intravenously. Treatment was started with encapsulated or free amikacin at approximately 110 or 40 mg/kg of body weight 7 or 14 days later. In the former experiment, treatment was given two or three times per week. In the latter experiment, treatment was given daily for 5 days. The animals were sacrificed 5 days after the last dose. Liver, spleen, and lung were homogenized, and viable cell counts were determined on 7H10 agar. An analysis of variance and subsequent Tukey HSD (honestly significant difference) tests indicated that both encapsulated and free amikacin significantly reduced viable cell counts in each of the organs compared with counts in the control group. Compared with free amikacin, encapsulated amikacin significantly reduced viable cell counts in the liver and spleen. Liposome encapsulation of an active agent appears to be a promising therapeutic approach to M. avium complex infection.
机译:在米色小鼠(C57BL / 6J-bgJ / bgJ)急性感染模型中评估了脂质体包裹的丁胺卡那霉素和游离丁胺卡那霉素对鸟分枝杆菌复合物的功效。静脉内给予约10(7)个阿米卡星MIC为8微克/毫升的活的鸟分枝杆菌复杂血清型1细胞。在大约7或14天后,以约110或40 mg / kg体重的胶囊化或游离阿米卡星开始治疗。在以前的实验中,每周接受两次或三次治疗。在后一个实验中,每天进行5天的治疗。最后一剂后5天处死动物。将肝,脾和肺匀浆,并在7H10琼脂上测定活细胞计数。方差分析和随后的Tukey HSD(诚实的显着差异)测试表明,与对照组相比,封装的阿米卡星和游离阿米卡星都显着降低了每个器官中的活细胞计数。与游离阿米卡星相比,封装的阿米卡星显着减少了肝脏和脾脏中的活细胞计数。脂质体包裹活性剂似乎是鸟分枝杆菌复杂感染的有前途的治疗方法。

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