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抗绿脓杆菌外毒素V F(ab')(2)在铜绿假单胞菌相关性脓毒症中的治疗应用。

Therapeutic administration of anti-PcrV F(ab')(2) in sepsis associated with Pseudomonas aeruginosa.

作者信息

Shime N, Sawa T, Fujimoto J, Faure K, Allmond L R, Karaca T, Swanson B L, Spack E G, Wiener-Kronish J P

机构信息

Department of Anesthesia and Perioperative Care, University of California, San Francisco, CA 94143, USA.

出版信息

J Immunol. 2001 Nov 15;167(10):5880-6. doi: 10.4049/jimmunol.167.10.5880.

Abstract

The effects of rabbit-derived polyclonal Ab against PcrV, a protein involved in the translocation of type III secreted toxins of Pseudomonas aeruginosa, was investigated in two animal models of P. aeruginosa sepsis. In a mouse survival study, the i.v. administration of anti-PcrV IgG after the airspace instillation of a lethal dose of P. aeruginosa resulted in the complete survival of the animals. In a rabbit model of septic shock associated with Pseudomonas-induced lung injury, animals treated with anti-PcrV IgG intratracheally or i.v. had significant decreases in lung injury, bacteremia, and plasma TNF-alpha and significant improvement in the hemodynamic parameters associated with shock compared with animals treated in a similar manner with nonspecific control IgG. The administration of anti-PcrV F(ab')(2) showed protective effects comparable to those of whole anti-PcrV IgG. These results document that the therapeutic administration of anti-PcrV IgG blocks the type III secretion system-mediated virulence of P. aeruginosa and prevents septic shock and death, and that these protective effects are largely Fc independent. We conclude that Ab therapy neutralizing the type III secretion system has significant potential against lethal P. aeruginosa infections.

摘要

在两种铜绿假单胞菌败血症动物模型中,研究了兔源抗PcrV多克隆抗体(PcrV是一种参与铜绿假单胞菌III型分泌毒素转运的蛋白质)的作用。在一项小鼠存活研究中,在向气腔注入致死剂量的铜绿假单胞菌后静脉注射抗PcrV IgG,结果动物全部存活。在与铜绿假单胞菌诱导的肺损伤相关的败血性休克兔模型中,与用非特异性对照IgG以类似方式治疗的动物相比,经气管内或静脉注射抗PcrV IgG治疗的动物肺损伤、菌血症和血浆肿瘤坏死因子-α显著降低,与休克相关的血流动力学参数有显著改善。给予抗PcrV F(ab')(2)显示出与整个抗PcrV IgG相当的保护作用。这些结果证明,抗PcrV IgG的治疗性给药可阻断铜绿假单胞菌III型分泌系统介导的毒力,预防败血性休克和死亡,且这些保护作用在很大程度上不依赖Fc。我们得出结论,中和III型分泌系统的抗体疗法对致死性铜绿假单胞菌感染具有显著潜力。

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