Characterization of the Protective Cellular Immune Response in Pigs Immunized Intradermally with the Live Attenuated African Swine Fever Virus (ASFV) Lv17/WB/Rie1

被引:4
作者
Pedrera, Miriam [1 ]
Soler, Alejandro [2 ]
Simon, Alicia [2 ]
Casado, Nadia [2 ]
Perez, Covadonga [2 ]
Garcia-Casado, Maria A. [1 ]
Fernandez-Pacheco, Paloma [1 ]
Sanchez-Cordon, Pedro J. [1 ]
Arias, Marisa [2 ]
Gallardo, Carmina [2 ]
机构
[1] CSIC, Inst Nacl Invest & Tecnol Agr & Alimentaria INIA, Ctr Invest San Anim CISA, Madrid 28130, Spain
[2] CSIC, Inst Nacl Invest & Tecnol Agr & Alimentaria INIA, Ctr Invest San Anim CISA, European Union Reference Lab African Swine Fever E, Madrid 28130, Spain
关键词
African swine fever; live-attenuated virus; vaccine; protective cellular response; T-cell; cytokines; domestic pigs; DOMESTIC PIGS; T-LYMPHOCYTES; CYTOTOXIC-T; CHALLENGE; CELLS; EXPRESSION; PHENOTYPE;
D O I
10.3390/vaccines12040443
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Candidate vaccines against African swine fever virus (ASFV) based on naturally attenuated or genetically modified viruses have the potential to generate protective immune responses, although there is no consensus on what defines a protective immune response against ASFV. Studies, especially in sensitive host species and focused on unravelling protective mechanisms, will contribute to the development of safer and more effective vaccines. The present study provides a detailed analysis of phenotypic and functional data on cellular responses induced by intradermal immunization and subsequent boosting of domestic pigs with the naturally attenuated field strain Lv17/WB/Rie1, as well as the mechanisms underlying protection against intramuscular challenge with the virulent genotype II Armenia/07 strain. The transient increase in IL-8 and IL-10 in serum observed after immunization might be correlated with survival. Protection was also associated with a robust ASFV-specific polyfunctional memory T-cell response, where CD4CD8 and CD8 T cells were identified as the main cellular sources of virus-specific IFN gamma and TNF alpha. In parallel with the cytokine response, these T-cell subsets also showed specific cytotoxic activity as evidenced by the increased expression of the CD107a degranulation marker. Along with virus-specific multifunctional CD4CD8 and CD8 T-cell responses, the increased levels of antigen experienced in cytotoxic CD4 T cells observed after the challenge in immunized pigs might also contribute to controlling virulent infection by killing mechanisms targeting infected antigen-presenting cells. Future studies should elucidate whether the memory T-cell responses evidenced in the present study persist and provide long-term protection against further ASFV infections.
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