The endotoxin from gram-negative bacteria consists of a molecule lipopolysaccharide (LPS) which can be shed by bacteria during antimicrobial therapy. A resulting syndrome, endotoxic shock, is a leading cause of death in the developed world. Thus, there is great interest in the development of antimicrobial agents which can reverse rather than promote sepsis, especially given the recent disappointing clinical performance of antiendotoxin therapies. We describe here two small cationic peptides, MBI-27 and MBI-28, which have both antiendotoxic and antibacterial activities in vitro and in vivo in animal models. We had previously demonstrated that these peptides bind to LPS with an affinity equivalent to that of polymyxin B. Consistent with this, the peptides blocked the ability of LPS and intact cells to induce the endotoxic shock mediator, tumor necrosis factor (TNF), upon incubation with the RAW 264.7 murine macrophage cell line. MBI-28 was equivalent to polymyxin B in its ability to block LPS induction of TNF by this cell line, even when added 60 min after the TNF stimulus. Furthermore, MBI-28 offered significant protection in a galactosamine-sensitized mouse model of lethal endotoxic shock. This protection correlated with the ability of MBI-28 to reduce LPS-induced circulating TNF by nearly 90% in this mouse model. Both MBI-27 and MBI-28 demonstrated antibacterial activity against gram-negative bacteria in vitro and in vivo against Pseudomonas aeruginosa infections in neutropenic mice.
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机译:革兰氏阴性细菌的内毒素由分子脂多糖(LPS)组成,在抗菌治疗过程中,细菌可将其排出。内毒素休克所导致的综合症是发达国家的主要死亡原因。因此,人们对开发可以逆转而不是促进败血症的抗微生物剂产生了极大的兴趣,特别是考虑到最近抗内毒素疗法的临床表现令人失望。我们在这里描述了两种小的阳离子肽MBI-27和MBI-28,它们在动物模型中具有体内和体外的抗内毒素和抗菌活性。先前我们已经证明这些肽以与多粘菌素B相同的亲和力与LPS结合。与之相一致的是,这些肽在孵育时阻断了LPS和完整细胞诱导内毒素休克介导物肿瘤坏死因子(TNF)的能力。 RAW 264.7鼠巨噬细胞系。即使在TNF刺激后60分钟添加,MBI-28在阻断LPS诱导该细胞系诱导LPS的能力方面也相当于多粘菌素B。此外,MBI-28在半乳糖胺致敏的致命内毒素性休克小鼠模型中提供了重要的保护。在该小鼠模型中,这种保护与MBI-28将LPS诱导的循环TNF降低近90%的能力相关。 MBI-27和MBI-28均在体外和体内均对革兰氏阴性细菌具有抗中性粒细胞减少的铜绿假单胞菌感染的抗菌活性。
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