Alves-Silva Marcus Vinícius, Nico Dirlei, Morrot Alexandre, Palatnik Marcos, Palatnik-de-Sousa Clarisa B
Laboratório de Biologia e Bioquímica de Leishmania, Departamento de Microbiologia Geral, Instituto de Microbiologia Paulo de Góes, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Rio de Janeiro, Brazil; Programa de Pós-Graduação em Biotecnologia Vegetal e Bioprocessos, Centro de Ciências da Saúde, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Rio de Janeiro, Brazil.
Laboratório de Biologia e Bioquímica de Leishmania, Departamento de Microbiologia Geral, Instituto de Microbiologia Paulo de Góes, Universidade Federal do Rio de Janeiro , Rio de Janeiro, Rio de Janeiro , Brazil.
Front Immunol. 2017 Feb 23;8:100. doi: 10.3389/fimmu.2017.00100. eCollection 2017.
The nucleoside hydrolase (NH36) and NH A34480 of share 93% of sequence identity. In mice, the NH36 induced protection against visceral leishmaniasis is mediated by a CD4+ T cell response against its C-terminal domain (F3). Besides this CD4+ Th1 response, prevention and cure of infection require also additional CD8+ and regulatory T-cell responses to the NH36 N-terminal (F1 domain). We investigated if mice vaccination with F1 and F3 domains cloned in tandem, in a recombinant chimera, with saponin, optimizes the vaccine efficacy against infection above the levels promoted by the two admixed domains or by each domain independently. The chimera induced the highest IgA, IgG, and IgG2a anti-NH36 antibody, IDR, IFN-γ, and IL-10 responses, while TNF-α was more secreted by mice vaccinated with F3 or all F3-contaning vaccines. Additionally, the chimera and the F1 vaccine also induced the highest proportions of CD4+ and CD8+ T cells secreting IL-2, TNF-α, or IFN-γ alone, TNF-α in combination with IL-2 or IFN-γ, and of CD4+ multifunctional cells secreting IL-2, TNF-α, and IFN-γ. Correlating with the immunological results, the strongest reductions of skin lesions sizes were determined by the admixed domains (80%) and by the chimera (84%), which also promoted the most pronounced and significant reduction of the parasite load (99.8%). Thus, the epitope presentation in a recombinant chimera optimizes immunogenicity and efficacy above the levels induced by the independent or admixed F1 and F3 domains. The multiparameter analysis disclosed that the Th1-CD4+ T helper response induced by the chimera is mainly directed against its FRYPRPKHCHTQVA epitope. Additionally, the YPPEFKTKL epitope of F1 induced the second most important CD4+ T cell response, and, followed by the DVAGIVGVPVAAGCT, FMLQILDFYTKVYE, and ELLAITTVVGNQ sequences, also the most potent CD8+ T cell responses and IL-10 secretion. Remarkably, the YPPEFKTKL epitope shows high amino acid identity with a multipotent PADRE sequence and stimulates simultaneously the CD4+, CD8+ T cell, and a probable T regulatory response. With this approach, we advanced in the design of a NH36 polytope vaccine capable of inducing cross-protection to cutaneous leishmaniasis.
核苷水解酶(NH36)与的NH A34480序列一致性达93%。在小鼠中,NH36诱导的针对内脏利什曼病的保护作用由针对其C端结构域(F3)的CD4 + T细胞应答介导。除了这种CD4 + Th1应答外,感染的预防和治愈还需要对NH36 N端(F1结构域)产生额外的CD8 +和调节性T细胞应答。我们研究了用重组嵌合体中串联克隆的F1和F3结构域与皂苷一起对小鼠进行疫苗接种,是否能使针对感染的疫苗效力比两个混合结构域或每个结构域单独诱导的水平更高。该嵌合体诱导了最高的IgA、IgG和IgG2a抗NH36抗体、IDR、IFN -γ和IL - 10应答,而接种F3或所有含F3疫苗的小鼠分泌的TNF -α更多。此外,嵌合体和F1疫苗还诱导了单独分泌IL - 2、TNF -α或IFN -γ、TNF -α与IL - 2或IFN -γ组合的CD4 +和CD8 + T细胞以及分泌IL - 2、TNF -α和IFN -γ的CD4 +多功能细胞的最高比例。与免疫结果相关的是,混合结构域(80%)和嵌合体(84%)使皮肤病变大小减少最为显著,它们还使寄生虫负荷显著降低(99.8%)。因此,重组嵌合体中的表位呈递使免疫原性和效力比独立或混合的F1和F3结构域诱导的水平更高。多参数分析表明,嵌合体诱导的Th1 - CD4 +辅助性T细胞应答主要针对其FRYPRPKHCHTQVA表位。此外,F1的YPPEFKTKL表位诱导了第二重要的CD4 + T细胞应答,其次是DVAGIVGVPVAAGCT、FMLQILDFYTKVYE和ELLAITTVVGNQ序列,也诱导了最有效的CD8 + T细胞应答和IL - 10分泌。值得注意的是,YPPEFKTKL表位与多能PADRE序列具有高度氨基酸一致性,并同时刺激CD4 +、CD8 + T细胞以及可能的调节性T细胞应答。通过这种方法,我们在设计一种能够诱导对皮肤利什曼病产生交叉保护的NH36多表位疫苗方面取得了进展。
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