Decreased Vector Gene Expression from E2b Gene-Deleted Adenovirus Serotype 5 Vaccines Intensifies Proinflammatory Immune Responses.

Q2 Biochemistry, Genetics and Molecular Biology Clinical and Vaccine Immunology Pub Date : 2017-06-05 Print Date: 2017-06-01 DOI:10.1128/CVI.00061-17
Dionisia Quiroga, Yasser A Aldhamen, Sarah Godbehere, Laura Harding, Andrea Amalfitano
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引用次数: 2

Abstract

Recombinant adenovirus serotype 5 (Ad5) vectors are promising vaccine candidates due to their intrinsic immunogenicity and potent transgene expression; however, widespread preexisting Ad5 immunity has been considered a developmental impediment to the use of traditional, or conventional, E1 and E3 gene-deleted Ad5 (Ad5[E1-]) vaccines. Even in the presence of anti-Ad5 immunity, recent murine and human studies have confirmed E2b gene-deleted Ad5 (Ad5[E1-,E2b-]) vaccines to be highly efficacious inducers of transgene-specific memory responses and significantly less toxic options than Ad5[E1-] vaccines. While these findings have been substantially confirmed, the molecular mechanisms underlying the different reactions to these vaccine platforms are unknown. Using cultures of human peripheral blood mononuclear cells (hPBMCs) derived from multiple human donors, we found that Ad5[E1-,E2b-] vaccines trigger higher levels of hPBMC proinflammatory cytokine secretion than Ad5[E1-] vaccines. Interestingly, these responses were generated regardless of the donors' preexisting anti-Ad5 humoral and cell-mediated immune response status. In vitro hPBMC infection with the Ad5[E1-,E2b-] vaccine also provoked greater Th1-dominant gene responses yet smaller amounts of Ad-derived gene expression than Ad5[E1-] vaccines. These results suggest that Ad5[E1-,E2b-] vaccines, in contrast to Ad5[E1-] vaccines, do not promote activities that suppress innate immune signaling, thereby allowing for improved vaccine efficacy and a superior safety profile independently of previous Ad5 immunity.

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E2b基因缺失腺病毒血清5型疫苗载体基因表达降低增强促炎免疫反应
重组腺病毒血清型5 (Ad5)载体由于其固有的免疫原性和有效的转基因表达而成为有希望的候选疫苗;然而,广泛存在的预先存在的Ad5免疫被认为是使用传统或常规E1和E3基因缺失的Ad5 (Ad5[E1-])疫苗的发育障碍。即使存在抗Ad5免疫,最近的小鼠和人类研究已经证实,E2b基因缺失的Ad5 (Ad5[E1-,E2b-])疫苗是转基因特异性记忆反应的高效诱导剂,并且毒性明显低于Ad5[E1-]疫苗。虽然这些发现已基本得到证实,但对这些疫苗平台的不同反应背后的分子机制尚不清楚。使用来自多个人类供体的人外周血单核细胞(hPBMCs)培养物,我们发现Ad5[E1-,E2b-]疫苗比Ad5[E1-]疫苗触发更高水平的hpbbmc促炎细胞因子分泌。有趣的是,这些反应的产生与供体先前存在的抗ad5体液和细胞介导的免疫反应状态无关。与Ad5[E1-,E2b-]疫苗相比,Ad5[E1-]疫苗在体外感染hPBMC时也引起了更大的th1显性基因反应,但ad源性基因的表达量较少。这些结果表明,与Ad5[E1-,E2b-]疫苗相比,Ad5[E1-]疫苗不促进抑制先天免疫信号的活动,从而提高了疫苗效力,并具有独立于先前Ad5免疫的优越安全性。
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来源期刊
Clinical and Vaccine Immunology
Clinical and Vaccine Immunology 医学-传染病学
CiteScore
2.88
自引率
0.00%
发文量
0
审稿时长
1.5 months
期刊介绍: Cessation. First launched as Clinical and Diagnostic Laboratory Immunology (CDLI) in 1994, CVI published articles that enhanced the understanding of the immune response in health and disease and after vaccination by showcasing discoveries in clinical, laboratory, and vaccine immunology. CVI was committed to advancing all aspects of vaccine research and immunization, including discovery of new vaccine antigens and vaccine design, development and evaluation of vaccines in animal models and in humans, characterization of immune responses and mechanisms of vaccine action, controlled challenge studies to assess vaccine efficacy, study of vaccine vectors, adjuvants, and immunomodulators, immune correlates of protection, and clinical trials.
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