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Innate immunity in experimental SIV infection and vaccination.

机译:实验性SIV感染和疫苗接种中的先天免疫。

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Innate immunity represents the first line of defence to pathogens besides the physical barrier and seems to play a role in protection against HIV/SIV infection and disease progression. High production of beta-chemokines and CD8+ T cell anti-viral factors in naive as well as in vaccinated macaques has been associated with complete or partial protection against SIV infection indicating that genetic or environmental factors may influence their production. This innate immunity may help in generating HIV/SIV-specific responses upon the first exposure to HIV/SIV. SIV subunit vaccines given by the targeted iliac lymph node route have been shown to induce an increased production of CD8+ T cell suppressor factors and beta-chemokines. Only a few vaccine studies have focused on enhancing the innate immune response against HIV/SIV. The use of unmethylated CpG motifs, HSP and GM-CSF as adjuvants in SIV vaccines has been shown to induce production of HIV/SIV-inhibiting cytokines and beta-chemokines, which seem to beimportant in modulating and steering the adaptive immune responses. HSP has also been shown to induce gammadelta+ T cells, which contribute to the innate immunity. More knowledge about the interplay between the innate and adaptive immune responses is important to develop new HIV/SIV vaccine strategies.
机译:天生的免疫力是除了物理屏障之外对病原体的第一道防线,并且似乎在预防HIV / SIV感染和疾病进展中发挥了作用。在幼稚以及已接种猕猴中,β-趋化因子和CD8 + T细胞抗病毒因子的高产量与完全或部分针对SIV感染的保护有关,表明遗传或环境因素可能影响它们的生产。这种先天免疫力可能有助于在首次接触HIV / SIV时产生针对HIV / SIV的特异性反应。已证明通过靶向淋巴结途径给予的SIV亚单位疫苗可诱导CD8 + T细胞抑制因子和β趋化因子的产生增加。只有少数疫苗研究集中于增强针对HIV / SIV的先天免疫应答。已证明在SIV疫苗中使用未甲基化的CpG基序,HSP和GM-CSF作为佐剂可诱导产生HIV / SIV抑制性细胞因子和β-趋化因子,这在调节和控制适应性免疫应答中似乎很重要。还显示出HSP可以诱导γ+ T细胞,这有助于先天免疫。有关先天性和适应性免疫反应之间相互作用的更多知识对于开发新的HIV / SIV疫苗策略很重要。

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