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The Multidrug-Resistant Gram-negative Superbugs Threat Require Intelligent Use of the Last Weapon

机译:耐多药革兰氏阴性超级细菌威胁需要智能使用最后一支武器

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摘要

The global emergence and dissemination of multidrug-resistant Gram-negative superbugs, particularly carbapenem-resistant Acinetobacter baumannii and Klebsiella pneumoniae, lead to the limited effectiveness of antibiotics for treating nosocomial infections. In most cases, polymyxins are the last resort therapy, and these antibiotics must be used intelligently to prolong their efficacy in clinical practice. Polymyxin B and colistin (polymyxin E) were introduced prior to modern drug regulation, and the majority of the ‘old’ drug information is unreliable. Recent pharmacokinetic data do not support the renal dose adjustment of intravenous (IV) polymyxin B as suggested by the manufacturer, and this drug must be scaled by the total body weight. Whereas IV colistin is formulated as an inactive prodrug, colistin methanesulfonate (CMS) has different pharmacokinetic profiles than polymyxin B. To achieve maximum efficacy, CMS should be administered as a loading dose scaled to body weight and a maintenance dose according to the renal profiles. Polymyxin combination therapy is suggested due to a sub-therapeutic plasma concentration in a significant proportion of patients and a high incidence of polymyxin hetero-resistance among Gram-negative superbugs. In conclusion, polymyxins must be reserved as a last resort and should be wisely used when truly indicated.
机译:耐多药的革兰氏阴性超级细菌,特别是耐碳青霉烯的鲍曼不动杆菌和肺炎克雷伯菌的全球出现和传播,导致抗生素治疗医院感染的效果有限。在大多数情况下,多粘菌素是最后的治疗方法,必须明智地使用这些抗生素以延长其在临床实践中的功效。在现代药物监管之前,先引入了多粘菌素B和粘菌素(多粘菌素E),而且大多数“旧”药物信息都不可靠。最近的药代动力学数据不支持制造商建议的调整静脉内(IV)多粘菌素B的肾脏剂量,该药物必须按总体重进行换算。 IV粘菌素被配制为无活性的前药,而粘菌素甲磺酸盐(CMS)与多粘菌素B具有不同的药代动力学特征。为了获得最大功效,CMS应以根据体重定标的负荷剂量和根据肾脏特征确定的维持剂量进行给药。建议使用多粘菌素联合疗法,这是因为在相当大比例的患者中,亚治疗血浆浓度较高,并且革兰氏阴性超级细菌中多粘菌素异抗性的发生率很高。总之,多粘菌素必须保留作为不得已的手段,并且在真正使用时应明智地使用。

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