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Polymyxin Acute Kidney Injury: Dosing and Other Strategies to Reduce Toxicity

机译:多粘菌素急性肾损伤:剂量和其他减少毒性的策略

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Polymyxins are valuable antimicrobials for the management of multidrug-resistant Gram-negative bacteria; however, nephrotoxicity associated with these drugs is a very common side effect that occurs during treatment. This article briefly reviews nephrotoxic mechanisms and risk factors for polymyxin-associated acute kidney injury (AKI) and discusses dosing strategies that may mitigate kidney damage without compromising antimicrobial activity. Polymyxins have a very narrow therapeutic window and patients requiring treatment with these drugs are frequently severely ill and have multiple comorbidities, which increases the risk of AKI. Notably, there is a significant overlap between therapeutic and toxic plasma polymyxin concentrations that substantially complicates dose selection. Recent dosing protocols for both colistin and polymyxin B have been developed and may help fine tune dose adjustment of these antibiotics. Minimizing exposure to modifiable risk factors, such as other nephrotoxic agents, is strongly recommended. The dose should be carefully selected, particularly in high-risk patients. The administration of oxidative stress-reducing drugs is a promising strategy to ameliorate polymyxin-associated AKI, but still requires support from clinical studies.
机译:多粘菌素是管理多重耐药性革兰氏阴性细菌的有价值的抗菌剂。然而,与这些药物有关的肾毒性是在治疗期间发生的非常常见的副作用。本文简要回顾了与多粘菌素相关的急性肾损伤(AKI)的肾毒性机制和危险因素,并讨论了可减轻肾脏损害而不损害抗菌活性的给药策略。多粘菌素的治疗窗口非常狭窄,需要用这些药物治疗的患者经常病重,并有多种合并症,这增加了AKI的风险。值得注意的是,在治疗性和毒性血浆多粘菌素浓度之间存在明显的重叠,这使剂量选择复杂化。已开发出针对大肠菌素和多粘菌素B的最新给药方案,这些方案可能有助于微调这些抗生素的剂量。强烈建议将暴露于可改变的风险因素(例如其他肾毒性药物)的风险降至最低。应谨慎选择剂量,尤其是在高危患者中。减轻氧化应激的药物的给药是改善多粘菌素相关性AKI的有前途的策略,但仍需要临床研究的支持。

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