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IV 型菌毛亚基蛋白 ApfA 有助于抵抗猪传染性胸膜肺炎。

Type IV fimbrial subunit protein ApfA contributes to protection against porcine pleuropneumonia.

机构信息

Institute of Microbiology of the Academy of Sciences of the Czech Republic, v,v,i,, Videnska 1083, CZ-142 20 Prague, Czech Republic.

出版信息

Vet Res. 2012 Jan 12;43(1):2. doi: 10.1186/1297-9716-43-2.

Abstract

Porcine pleuropneumonia caused by Actinobacillus pleuropneumoniae accounts for serious economic losses in the pig farming industry worldwide. We examined here the immunogenicity and protective efficacy of the recombinant type IV fimbrial subunit protein ApfA as a single antigen vaccine against pleuropneumonia, or as a component of a multi-antigen preparation comprising five other recombinant antigens derived from key virulence factors of A. pleuropneumoniae (ApxIA, ApxIIA, ApxIIIA, ApxIVA and TbpB). Immunization of pigs with recombinant ApfA alone induced high levels of specific serum antibodies and provided partial protection against challenge with the heterologous A. pleuropneumoniae serotype 9 strain. This protection was higher than that engendered by vaccination with rApxIVA or rTbpB alone and similar to that observed after immunization with the tri-antigen combination of rApxIA, rApxIIA and rApxIIIA. In addition, rApfA improved the vaccination potential of the penta-antigen mixture of rApxIA, rApxIIA, rApxIIIA, rApxIVA and rTbpB proteins, where the hexa-antigen vaccine containing rApfA conferred a high level of protection on pigs against the disease. Moreover, when rApfA was used for vaccination alone or in combination with other antigens, such immunization reduced the number of pigs colonized with the challenge strain. These results indicate that ApfA could be a valuable component of an efficient subunit vaccine for the prevention of porcine pleuropneumonia.

摘要

猪传染性胸膜肺炎由胸膜肺炎放线杆菌引起,给全球养猪业造成了严重的经济损失。在此,我们研究了重组 IV 型菌毛亚单位蛋白 ApfA 作为单一抗原疫苗对胸膜肺炎的免疫原性和保护效力,或作为包含源自胸膜肺炎放线杆菌 5 种关键毒力因子的 5 种其他重组抗原(ApxIA、ApxIIA、ApxIIIA、ApxIVA 和 TbpB)的多抗原制剂的组成部分的效力。单独用重组 ApfA 免疫猪可诱导高水平的特异性血清抗体,并对异源血清型 9 菌株的攻毒提供部分保护。这种保护作用高于单独用 rApxIVA 或 rTbpB 接种产生的保护作用,与用 rApxIA、rApxIIA 和 rApxIIIA 三联抗原免疫产生的保护作用相似。此外,rApfA 提高了 rApxIA、rApxIIA、rApxIIIA、rApxIVA 和 rTbpB 蛋白五抗原混合物的疫苗接种潜力,其中含有 rApfA 的六抗原疫苗对猪的疾病提供了高水平的保护。此外,当 rApfA 单独或与其他抗原一起用于免疫接种时,这种免疫接种减少了攻毒菌株定植的猪的数量。这些结果表明,ApfA 可能是预防猪传染性胸膜肺炎的有效亚单位疫苗的有价值成分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a3d/3276438/779af1859e7c/1297-9716-43-2-1.jpg

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