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多粘菌素B:一首献给内毒素休克古老解药的颂歌。

Polymyxin B: an ode to an old antidote for endotoxic shock.

作者信息

Bhor Vikrant M, Thomas Celestine J, Surolia Namita, Surolia Avadhesha

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bangalore, India.

出版信息

Mol Biosyst. 2005 Sep;1(3):213-22. doi: 10.1039/b500756a. Epub 2005 Jul 29.

Abstract

Endotoxic shock, a syndrome characterized by deranged hemodynamics, coagulation abnormalities, and multiple system organ failure is caused by the release into the circulation of lipopolysaccharide (LPS), the structurally diverse component of Gram-negative bacterial outer membranes, and is responsible for 60% mortality in humans. Polymyxin B (PMB), a cyclic, cationic peptide antibiotic, neutralizes endotoxin but induces severe side effects in the process. The potent endotoxin neutralizing ability of PMB, however, offers possibilities for designing non-toxic therapeutic agents for combating endotoxicosis. Amongst the numerous approaches for combating endotoxic shock, peptide mediated neutralization of LPS seems to be the most attractive one. The precise mode of binding of PMB to LPS and the structural features involved therein have been elucidated only recently using a variety of biophysical approaches. These suggest that efficient neutralization of endotoxin by PMB is not achieved by mere binding to LPS but requires its sequestration from the membrane. Incorporation of this feature into the design of endotoxin neutralizing peptides should lead to the development of effective antidotes for endotoxic shock.

摘要

内毒素休克是一种以血流动力学紊乱、凝血异常和多系统器官功能衰竭为特征的综合征,由革兰氏阴性菌外膜结构多样的成分脂多糖(LPS)释放到循环系统中引起,在人类中导致60%的死亡率。多粘菌素B(PMB)是一种环状阳离子肽抗生素,可中和内毒素,但在此过程中会引发严重的副作用。然而,PMB强大的内毒素中和能力为设计对抗内毒素血症的无毒治疗药物提供了可能性。在对抗内毒素休克的众多方法中,肽介导的LPS中和似乎是最具吸引力的一种。直到最近,才通过各种生物物理方法阐明了PMB与LPS结合的精确模式及其涉及的结构特征。这些表明,PMB对内毒素的有效中和并非仅仅通过与LPS结合来实现,而是需要将其从膜中隔离出来。将这一特性纳入内毒素中和肽的设计中,应该会导致开发出有效的内毒素休克解毒剂。

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