评估多组分重组疫苗对胸膜肺炎放线杆菌的小鼠保护作用。

Evaluation of multicomponent recombinant vaccines against Actinobacillus pleuropneumoniae in mice.

机构信息

Division of Bacterial Diseases, National Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Harbin, China.

出版信息

Acta Vet Scand. 2010 Sep 11;52(1):52. doi: 10.1186/1751-0147-52-52.

DOI:10.1186/1751-0147-52-52

PMID:20831818

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2944310/

Abstract

BACKGROUND

Porcine contagious pleuropneumonia (PCP) is a highly contagious disease that is caused by Actinobacillus pleuropneumoniae (APP) and characterized by severe fibrinous necrotizing hemorrhagic pleuropneumonia, which is a severe threat to the swine industry. In addition to APP RTX-toxins I (ApxI), APP RTX-toxin II (ApxII), APP RTX-toxin III (ApxIII) and Outer membrane protein (OMP), there may be other useful antigens that can contribute to protection. In the development of an efficacious vaccine against APP, the immunogenicities of multicomponent recombinant subunit vaccines were evaluated.

METHODS

Six major virulent factor genes of APP, i.e., apxI, apxII, apxIII, APP RTX-toxins IV (apxIV), omp and type 4 fimbrial structural (apfa) were expressed. BALB/c mice were immunized with recombinant ApxI ( rApxI), recombinant ApxII (rApxII), recombinant ApxIII (rApxIII) and recombinant OMP (rOMP) (Group I); rApxI, rApxII, rApxIII, recombinant ApxIV (rApxIV), recombinant Apfa (rApfa) and rOMP (Group II); APP serotype 1 (APP1) inactivated vaccine (Group III); or phosphate-buffered saline (PBS) (Control group), respectively. After the first immunization, mice were subjected to two booster immunizations at 2-week intervals, followed by challenge with APP1 Shope 4074 and APP2 S1536.

RESULTS

The efficacy of the multicomponent recombinant subunit vaccines was evaluated on the basis of antibody titers, survival rates, lung lesions and indirect immunofluorescence (IIF) detection of APP. The antibody level of Group I was significantly higher than those of the other three groups (P < 0.05). The survival rate of Group I was higher than that of Groups II and III (P < 0.05) and the control (P < 0.01). Compared with the other three groups, the lungs of Group I did not exhibit obvious hemorrhage or necrosis, and only showed weak and scattered fluorescent dots by IIF detection.

CONCLUSION

The result indicates that the multicomponent recombinant subunit vaccine composed of rApxI, rApxII, rApxIII and rOMP can provide effective cross-protection against homologous and heterologous APP challenge.

摘要

背景

猪传染性胸膜肺炎（PCP）是一种高度传染性疾病，由胸膜肺炎放线杆菌（APP）引起，其特征为严重的纤维素性坏死性出血性胸膜肺炎，这对养猪业构成了严重威胁。除 APP RTX-毒素 I（ApxI）、APP RTX-毒素 II（ApxII）、APP RTX-毒素 III（ApxIII）和外膜蛋白（OMP）外，可能还有其他有用的抗原有助于保护。在开发针对 APP 的有效疫苗时，评估了多组分重组亚单位疫苗的免疫原性。

方法

表达 APP 的 6 种主要毒力因子基因，即 apxI、apxII、apxIII、APP RTX-毒素 IV（apxIV）、omp 和 4 型菌毛结构（apfa）。BALB/c 小鼠用重组 ApxI（rApxI）、重组 ApxII（rApxII）、重组 ApxIII（rApxIII）和重组 OMP（rOMP）（第 I 组）；rApxI、rApxII、rApxIII、重组 ApxIV（rApxIV）、重组 Apfa（rApfa）和 rOMP（第 II 组）；APP 血清型 1（APP1）灭活疫苗（第 III 组）；或磷酸盐缓冲盐水（PBS）（对照组）分别免疫。第一次免疫后，每隔 2 周进行两次加强免疫，然后用 APP1 Shope 4074 和 APP2 S1536 进行攻毒。

结果

根据抗体滴度、存活率、肺病变和 APP 的间接免疫荧光（IIF）检测，评估了多组分重组亚单位疫苗的效果。第 I 组的抗体水平明显高于其他三组（P<0.05）。第 I 组的存活率高于第 II 组和第 III 组（P<0.05）和对照组（P<0.01）。与其他三组相比，第 I 组的肺脏没有明显的出血或坏死，仅通过 IIF 检测显示出微弱且分散的荧光点。

结论

结果表明，由 rApxI、rApxII、rApxIII 和 rOMP 组成的多组分重组亚单位疫苗可对同源和异源 APP 攻毒提供有效保护。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/70ee/2944310/fa2a2393551a/1751-0147-52-52-1.jpg

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评估多组分重组疫苗对胸膜肺炎放线杆菌的小鼠保护作用。

Evaluation of multicomponent recombinant vaccines against Actinobacillus pleuropneumoniae in mice.

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSION

背景

方法

结果

结论

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