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首页> 外文期刊>International journal of molecular medicine >In vitro and in vivo properties of a fully human IgG1 monoclonal antibody that combats multidrug resistant Pseudomonas aeruginosa
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In vitro and in vivo properties of a fully human IgG1 monoclonal antibody that combats multidrug resistant Pseudomonas aeruginosa

机译:对抗多药耐药铜绿假单胞菌的完全人类IgG1单克隆抗体的体外和体内特性

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摘要

The development of an anti-bacterial drug in the form of a monoclonal antibody (mAb) targeting an exposed virulence factor, represents an innovative therapeutic strategy. Consequently, a fully human IgG1 mAb (LST-007) targeting Pseudomonas aeruginosa (PA) flagellin type b was recombinantly expressed and characterized in vitro and in an infection model driven by a multidrug resistant (MDR) PA strain. LST-007 demonstrated a highly specific binding towards whole PA bacteria harboring flagellin type b and its recombinant counterpart, with a K D of 7.4×10 -10 M. In bioactivity assays, LST-007 or titers of Cmax sera derived from pharmacokinetic studies, markedly attenuated PA motility in an equipotent manner. In vivo, parenteral LST-007 (20 mg/kg) given as a single or double-dosing paradigm post-infection, afforded survival (up to 75% at Day 7) in a lethal model of pneumonia driven by the intratracheal (i.t.) instillation of an LD 80 of the MDR PA isolate. This protective effect was markedly superior to that of imipenem (30% survival at Day 7) and totally devoid with an irrelevant, human isotype mAb. These data lay credence that LST-007 may be a valuable adjunct to the limited list of anti-bacterials that can tackle MDR PA strains, thereby warranting its continued development for eventual clinical evaluation.
机译:靶向暴露的毒力因子的单克隆抗体(mAb)形式的抗菌药物的开发代表了一种创新的治疗策略。因此,在体外以及在由多药耐药(MDR)PA菌株驱动的感染模型中,重组表达并靶向了b型铜绿假单胞菌(PA)鞭毛蛋白的人IgG1 mAb(LST-007)。 LST-007表现出对带有b型鞭毛蛋白的整个PA细菌及其重组对应物的高度特异性结合,KD为7.4×10 -10M。在生物活性测定中,LST-007或源自药代动力学研究的Cmax血清效价显着等电位降低PA的运动能力。在体内,以气管内驱动的致死性肺炎模型,以感染后的单次或两次给药方式给予肠胃外LST-007(20 mg / kg),可以存活(在第7天高达75%)。滴加耐多药PA分离株的LD 80。这种保护作用明显优于亚胺培南(在第7天的存活率为30%),并且完全没有无关的人同种型mAb。这些数据证明,LST-007可能是可以解决MDR PA菌株的有限抗菌药物的宝贵辅助,因此有必要对其进行持续开发以用于最终的临床评估。

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