Literature DB >> 24554667

Boosting functional avidity of CD8+ T cells by vaccinia virus vaccination depends on intrinsic T-cell MyD88 expression but not the inflammatory milieu.

Zhidong Hu1, Jing Wang, Yanmin Wan, Lingyan Zhu, Xiaonan Ren, Sugan Qiu, Yanqin Ren, Songhua Yuan, Xiangqing Ding, Jian Chen, Chenli Qiu, Jun Sun, Xiaoyan Zhang, Jim Xiang, Chao Qiu, Jianqing Xu.   

Abstract

UNLABELLED: T-cell functional avidity is a crucial determinant for efficient pathogen clearance. Although recombinant DNA priming coupled with a vaccinia-vectored vaccine (VACV) boost has been widely used to mount robust CD8+ T-cell responses, how VACV boost shapes the properties of memory CD8+ T cells remains poorly defined. Here, we characterize the memory CD8+ T cells boosted by VACV and demonstrate that the intrinsic expression of MyD88 is critical for their high functional avidity. Independent of selection of clones with high-affinity T-cell receptor (TCR) or of enhanced proximal TCR signaling, the VACV boost significantly increased T-cell functional avidity through a decrease in the activation threshold. VACV-induced inflammatory milieu is not sufficient for this improvement, as simultaneous administration of the DNA vaccine and mock VACV had no effects on the functional avidity of memory CD8+ T cells. Furthermore, reciprocal adoptive transfer models revealed that the intrinsic MyD88 pathway is required for instructing the functional avidity of CD8+ T cells boosted by VACV. Taking these results together, the intrinsic MyD88 pathway is required for the high functional avidity of VACV-boosted CD8+ T cells independent of TCR selection or the VACV infection-induced MyD88-mediated inflammatory milieu. IMPORTANCE: Functional avidity is one of the crucial determinants of T-cell functionality. Interestingly, although it has been demonstrated that a DNA prime-VACV boost regimen elicits high levels of T-cell functional avidity, how VACV changes the low avidity of CD8+ T cells primed by DNA into higher ones in vivo is less defined. Here, we proved that the enhancement of CD8+ T cell avidity induced by VACV boost is mediated by the intrinsic MyD88 pathway but not the MyD88-mediated inflammatory milieu, which might provide prompts in vaccine design.

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Year:  2014        PMID: 24554667      PMCID: PMC4019089          DOI: 10.1128/JVI.03664-13

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  45 in total

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Journal:  Clin Dev Immunol       Date:  2012-04-26
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1.  Low Antigen Dose in Adjuvant-Based Vaccination Selectively Induces CD4 T Cells with Enhanced Functional Avidity and Protective Efficacy.

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3.  Heterologous prime-boost vaccination against tuberculosis with recombinant Sendai virus and DNA vaccines.

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Review 5.  Research Advances for Virus-vectored Tuberculosis Vaccines and Latest Findings on Tuberculosis Vaccine Development.

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Journal:  Front Immunol       Date:  2022-06-23       Impact factor: 8.786

6.  Immune Signature of Enhanced Functional Avidity CD8+ T Cells in vivo Induced by Vaccinia Vectored Vaccine.

Authors:  Zhidong Hu; Lingyan Zhu; Jing Wang; Yanmin Wan; Songhua Yuan; Jian Chen; Xiangqing Ding; Chenli Qiu; Xiaoyan Zhang; Chao Qiu; Jianqing Xu
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7.  The Profile of T Cell Responses in Bacille Calmette-Guérin-Primed Mice Boosted by a Novel Sendai Virus Vectored Anti-Tuberculosis Vaccine.

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8.  Cancer testis antigen Cyclin A1 harbors several HLA-A*02:01-restricted T cell epitopes, which are presented and recognized in vivo.

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Journal:  Cancer Immunol Immunother       Date:  2020-03-10       Impact factor: 6.968

9.  Intrinsic MyD88-Akt1-mTOR Signaling Coordinates Disparate Tc17 and Tc1 Responses during Vaccine Immunity against Fungal Pneumonia.

Authors:  Som Gowda Nanjappa; Nydiaris Hernández-Santos; Kevin Galles; Marcel Wüthrich; M Suresh; Bruce S Klein
Journal:  PLoS Pathog       Date:  2015-09-14       Impact factor: 7.464

  9 in total

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