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一种无毒的铜绿假单胞菌外毒素A可诱导针对铜绿假单胞菌外毒素A中毒的主动免疫和被动保护性抗体。

A nontoxic Pseudomonas exotoxin A induces active immunity and passive protective antibody against Pseudomonas exotoxin A intoxication.

作者信息

Chen T Y, Lin C P, Loa C C, Chen T L, Shang H F, Hwang J, Hui C F

机构信息

Institute of Genetics, School of Life Science, National Yang-Ming University, Taipei, Taiwan, ROC.

出版信息

J Biomed Sci. 1999 Sep-Oct;6(5):357-63. doi: 10.1007/BF02253525.

Abstract

Pseudomonas exotoxin A (PE) is one of the most potent cytotoxic agents produced by Pseudomonas aeruginosa. In this study, we examined the possibility of using PE with a deletion of 38 carboxyl-terminal amino acid residues, designated PE(Delta576-613), for active immunization against PE-mediated disease. We first examined the toxic effects of PE and PE(Delta576-613) on 5- and 9-week-old ICR mice. The results show that the subcutaneous administration of PE(Delta576-613) at a dose of 250 microg was still nontoxic to 5- and 9-week-old ICR mice, while native PE was lethal at a dose of 0.5 and 1 microg, respectively. PE(Delta576-613) was then used to immunize ICR mice. The minimum dose of PE(Delta576-613) that could effectively induce anti-PE antibodies in 5- and 9-week-old ICR mice was found to be 250 ng. However, immunization with 250 ng PE(Delta576-613) failed to protect the immunized mice from a lethal dose of PE. The effective immunization dose of PE(Delta576-613) that could protect mice against a 2 microg PE challenge was found to be 15 microg. In addition, sera obtained from PE(Delta576-613)-immunized ICR mice were able to neutralize PE intoxication and effectively protect mice from PE. Thus, PE(Delta576-613) may be used as an alternative route to new PE vaccine development.

摘要

铜绿假单胞菌外毒素A(PE)是铜绿假单胞菌产生的最具细胞毒性的物质之一。在本研究中,我们检测了使用缺失38个羧基末端氨基酸残基的PE(命名为PE(Delta576 - 613))进行主动免疫以预防PE介导疾病的可能性。我们首先检测了PE和PE(Delta576 - 613)对5周龄和9周龄ICR小鼠的毒性作用。结果表明,以250微克的剂量皮下注射PE(Delta576 - 613)对5周龄和9周龄的ICR小鼠仍然无毒,而天然PE分别在0.5微克和1微克的剂量时具有致死性。然后用PE(Delta576 - 613)免疫ICR小鼠。发现在5周龄和9周龄的ICR小鼠中能有效诱导抗PE抗体的PE(Delta576 - 613)的最小剂量为250纳克。然而,用250纳克的PE(Delta576 - 613)免疫未能保护小鼠免受致死剂量PE的攻击。发现能保护小鼠抵抗2微克PE攻击的PE(Delta576 - 613)的有效免疫剂量为15微克。此外,从用PE(Delta576 - 613)免疫的ICR小鼠获得的血清能够中和PE中毒并有效保护小鼠免受PE侵害。因此,PE(Delta576 - 613)可能作为开发新型PE疫苗的一种替代途径。

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