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Current Understanding of Polymyxin B Applications in Bacteraemia/ Sepsis Therapy Prevention: Clinical, Pharmaceutical, Structural and Mechanistic Aspects

机译:目前对多粘菌素B在细菌血症/脓毒症治疗预防中的应用的了解:临床,药物,结构和机制方面

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Polymyxin B (PMB) belongs to a class of antibiotics discovered more than six decades ago. PMB was used for various bacterial infection threatening, in particular to sepsis. Its use, however, was abandoned because of the observation of severe side effects. In the last years this view changed due to the appearance of multi-drug resistant Gram-negative pathogens, which were resistant to most available antibiotics, leading to a re-evaluation of the polymyxin antibiotics (PMB and PME).nnAlthough there is a large market potential for the development of drugs to fight sepsis, the available successful clinical strategies are very limited. The cause for this lies in the clinical failures of a number of drug candidates, which were tested in the last years. This was attributed to some extent to our elementary understanding of the pathophysiology of sepsis, to not optimally designed clinical trials and a lack of appropriate pre-clinical models to establish the proof of concept (POC). At that time there were just humble knowledge about the structural mechanisms involved in the advantageous aspects of PMB-endotoxin interactions to increase the knowledges outcome in sepsis therapy.nnTherefore, the current paper describes the clinical aspects of PMB application in bacteraemia and sepsis therapy. However, the focus of the presented paper lies in the structural and mechanistic aspects of PMB-endotoxin (LPS: lipopolysaccharide) recognition and how this knowledge can be applied for the development or improvement of new clinical drug candidates to support sepsis therapies. Due to chemical similarities between PME and PMB, certain aspects of the use of PME as an antimicrobial agent and in sepsis therapy are considered and compared to PMB.
机译:多粘菌素B(PMB)属于六十多年前发现的一类抗生素。 PMB用于各种威胁细菌感染,尤其是败血症。然而,由于观察到严重的副作用,它的使用被放弃了。在过去的几年中,由于出现了多重耐药的革兰氏阴性病原体,这种观点发生了变化,该病原体对大多数可用的抗生素具有耐药性,从而导致了对多粘菌素抗生素(PMB和PME)的重新评估。对抗败血症药物开发市场潜力巨大,可用的成功临床策略非常有限。其原因在于最近几年对许多候选药物的临床失败进行了测试。这在一定程度上归因于我们对脓毒症的病理生理学的基本了解,未优化设计的临床试验以及缺乏适当的临床前模型来建立概念验证(POC)。那时对PMB-内毒素相互作用的有利方面所涉及的结构机制的了解很少,以增加败血症治疗的知识结局。因此,当前的论文描述了PMB在菌血症和败血症治疗中的临床应用。但是,本文的重点在于PMB-内毒素(LPS:脂多糖)的识别和结构方面,以及如何将该知识用于开发或改善支持败血症治疗的新型临床药物。由于PME和PMB之间的化学相似性,因此考虑将PME用作抗菌剂以及在败血症治疗中使用某些方面,并将其与PMB进行比较。

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