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本文引用的文献

1
Antigenicity of partial fragments of recombinant Pasteurella multocida toxin.重组多杀性巴氏杆菌毒素部分片段的抗原性。
J Microbiol Biotechnol. 2010 Dec;20(12):1756-63.
2
Protective potential of an attenuated Pasteurella multocida, which expresses only the N-terminal truncated fragment of P. multocida toxin.仅表达多杀性巴氏杆菌毒素N端截短片段的减毒多杀性巴氏杆菌的保护潜力。
Can J Vet Res. 2010 Jan;74(1):25-9.
3
Expression of 4 truncated fragments of Pasteurella multocida toxin and their immunogenicity.多杀性巴氏杆菌毒素4个截短片段的表达及其免疫原性。
Can J Vet Res. 2009 Jul;73(3):184-9.
4
Pasteurella multocida toxin activation of heterotrimeric G proteins by deamidation.多杀巴斯德菌毒素通过脱酰胺作用激活异源三聚体G蛋白。
Proc Natl Acad Sci U S A. 2009 Apr 28;106(17):7179-84. doi: 10.1073/pnas.0900160106. Epub 2009 Apr 15.
5
Pluronic F127 enhances the effect as an adjuvant of chitosan microspheres in the intranasal delivery of Bordetella bronchiseptica antigens containing dermonecrotoxin.普朗尼克F127增强了壳聚糖微球作为佐剂在鼻内递送含皮肤坏死毒素的支气管败血波氏杆菌抗原中的效果。
Vaccine. 2007 Jun 6;25(23):4602-10. doi: 10.1016/j.vaccine.2007.03.038. Epub 2007 Apr 9.
6
Outer membrane protein H for protective immunity against Pasteurella multocida.用于抵抗多杀性巴氏杆菌的保护性免疫的外膜蛋白H
J Microbiol. 2007 Apr;45(2):179-84.
7
Crystal structures reveal a thiol protease-like catalytic triad in the C-terminal region of Pasteurella multocida toxin.晶体结构揭示了多杀巴斯德氏菌毒素C端区域存在一个类似硫醇蛋白酶的催化三联体。
Proc Natl Acad Sci U S A. 2007 Mar 20;104(12):5139-44. doi: 10.1073/pnas.0608197104. Epub 2007 Mar 14.
8
Pasteurella multocida pathogenesis: 125 years after Pasteur.多杀巴斯德菌的致病机制:巴斯德之后125年
FEMS Microbiol Lett. 2006 Dec;265(1):1-10. doi: 10.1111/j.1574-6968.2006.00442.x.
9
Mucosal inoculation of Lactobacillus expressing hCGbeta induces an anti-hCGbeta antibody response in mice of different strains.表达人绒毛膜促性腺激素β亚基(hCGβ)的乳酸杆菌经黏膜接种可在不同品系小鼠中诱导产生抗hCGβ抗体反应。
Methods. 2006 Feb;38(2):124-32. doi: 10.1016/j.ymeth.2005.09.014.
10
Immunogenicity and efficacy of three recombinant subunit Pasteurella multocida toxin vaccines against progressive atrophic rhinitis in pigs.三种重组亚单位多杀性巴氏杆菌毒素疫苗对猪进行性萎缩性鼻炎的免疫原性和效力
Vaccine. 2006 Jan 9;24(1):27-35. doi: 10.1016/j.vaccine.2005.07.079. Epub 2005 Aug 9.

重组多杀巴斯德氏菌毒素C末端片段赋予的保护性免疫

Protective immunity conferred by the C-terminal fragment of recombinant Pasteurella multocida toxin.

作者信息

Lee Jeongmin, Kang Hae-Eun, Woo Hee-Jong

机构信息

Laboratory of Immunology, College of Veterinary Medicine, Seoul National University, Seoul, Republic of Korea.

出版信息

Clin Vaccine Immunol. 2012 Sep;19(9):1526-31. doi: 10.1128/CVI.00238-12. Epub 2012 Jul 25.

DOI:10.1128/CVI.00238-12
PMID:22837096
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3428383/
Abstract

Pasteurella multocida serogroup D, producing P. multocida toxin (PMT), is a causative pathogen of progressive atrophic rhinitis (PAR) in swine. To evaluate the protective immunity and vaccination efficacy of the truncated form of PMT, a C-terminal form of recombinant PMT (designated PMT2.3; amino acid residues 505 to 1285 of PMT) was expressed in an Escherichia coli expression system, and the humoral and cellular immune responses to PMT2.3 were investigated. PMT2.3 vaccination in mice led to high levels of the anti-PMT antibody with a high neutralizing antibody titer. PMT2.3 also induced a cellular immune response to PMT, as demonstrated by the lymphocyte proliferation assay. Furthermore, strong protection against a homologous challenge with P. multocida was also observed in mice vaccinated with PMT2.3. In PMT2.3 vaccination in swine, high levels of serum antibody titers were observed in offspring from sows vaccinated with PMT2.3. Offspring from sows vaccinated with PMT2.3 or toxoid showed a good growth performance as depicted by mean body weight at the time of sacrifice, as well as in average daily gain in the postweaning period. Low levels of pathological lesions in turbinate atrophy and pneumonia were also observed in these offspring. Therefore, we consider PMT2.3--in the truncated and nontoxic recombinant PMT form--to be an attractive candidate for a subunit vaccine against PAR induced by P. multocida infection.

摘要

产多杀性巴氏杆菌毒素(PMT)的多杀性巴氏杆菌D血清型是猪进行性萎缩性鼻炎(PAR)的致病病原体。为了评估截短形式的PMT的保护性免疫和疫苗接种效果,在大肠杆菌表达系统中表达了重组PMT的C末端形式(命名为PMT2.3;PMT的氨基酸残基505至1285),并研究了对PMT2.3的体液免疫和细胞免疫反应。在小鼠中接种PMT2.3导致产生高滴度中和抗体的高水平抗PMT抗体。淋巴细胞增殖试验表明,PMT2.3还诱导了对PMT的细胞免疫反应。此外,在用PMT2.3接种的小鼠中也观察到对多杀性巴氏杆菌同源攻击的强大保护作用。在猪中接种PMT2.3时,接种PMT2.3的母猪后代血清抗体滴度较高。接种PMT2.3或类毒素的母猪后代在处死时的平均体重以及断奶后时期的平均日增重方面表现出良好的生长性能。在这些后代中还观察到鼻甲萎缩和肺炎的低水平病理损伤。因此,我们认为截短的无毒重组PMT形式的PMT2.3是针对多杀性巴氏杆菌感染诱导的PAR的亚单位疫苗的有吸引力的候选物。