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首页> 外文期刊>Current Protein and Peptide Science >Antimicrobial Peptide rBPI_(21): A Translational Overview from Bench to Clinical Studies
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Antimicrobial Peptide rBPI_(21): A Translational Overview from Bench to Clinical Studies

机译:抗菌肽rBPI_(21):从实验到临床研究的概述

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摘要

Gram-negative bacteria infection is sometimes followed by septic shock. This serious health condition is caused by the segregation of the lipopolysaccharide (LPS) from bacterial membrane into the bloodstream. Due to bacterial resistance, new antibiotics are needed. Most of the active antibiotics possess bactericidal effect, but lack LPS neutralization properties to prevent or neutralize septic shock. Antimicrobial peptides are a new class of antibiotics not prone to bacterial resistance, because their main target is the membrane. It is difficult for bacteria to critically change their membrane composition without affecting its molecular processes. rBPI_(21) is a recombinant antimicrobial peptide developed from an antimicrobial protein produced in neutrophils, the bactcricidal/permcability-increasing protein (BPI) that ended phase 111 clinical trials against meningitis with success, reducing serious complications, such as amputations. It interacts preferentially with LPS with high affinity and at the same time has bactericidal effect. Here, we gather evidence that the interaction of the rBPI_(21) with LPS is mainly electrostatic, first, followed by massive LPS aggregation, which is correlated with its clearance from the bloodstream. The molecular mechanism at membrane level includes the peptide interactions with negatively charged phospholipids that promote outer and inner membrane hemi(fusion). This perturbation is followed by membrane permeabilization.
机译:革兰氏阴性细菌感染有时会伴有败血性休克。这种严重的健康状况是由于脂多糖(LPS)从细菌膜向血液的分离所致。由于细菌的耐药性,需要新的抗生素。大多数活性抗生素具有杀菌作用,但缺乏LPS中和特性以防止或中和败血性休克。抗菌肽是一类新型的不易产生细菌耐药性的抗生素,因为它们的主要靶标是膜。细菌很难在不影响其分子过程的情况下严格改变其膜​​组成。 rBPI_(21)是一种重组抗微生物肽,由嗜中性粒细胞中产生的一种抗菌蛋白开发而成,该细菌具有杀细菌/提高渗透性的蛋白(BPI),已成功结束了针对脑膜炎的111期临床试验,减少了截肢等严重并发症。它以高亲和力优先与LPS相互作用,同时具有杀菌作用。在这里,我们收集到的证据表明,rBPI_(21)与LPS的相互作用主要是静电,其次是大量LPS聚集,这与其从血流中清除有关。膜水平的分子机制包括肽与带负电荷的磷脂的相互作用,从而促进外膜和内膜的半融合。该扰动之后是膜透化。

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