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Priming With Recombinant BCG Expressing Novel HIV-1 Conserved Mosaic Immunogens and Boosting With Recombinant ChAdOx1 Is Safe Stable and Elicits HIV-1-Specific T-Cell Responses in BALB/c Mice

机译:用表达新的HIV-1保守的镶嵌免疫原的重组BCG引发和用重组的ChAdOx1加强免疫是安全稳定并引起BALB / c小鼠HIV-1特异的T细胞反应。

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摘要

BCG is currently the only licensed vaccine against tuberculosis (TB) and confers protection against meningitis and miliary tuberculosis in infants, although pulmonary disease protection in adults is inconsistent. Recently, promising HIV-1 immunogens were developed, such as the T-cell immunogens “tHIVconsvX,” designed using functionally conserved protein regions across group M strains, with mosaic immunogens to improve HIV-1 variant match and response breadth. In this study, we constructed an integrative E. coli-mycobacterial shuttle plasmid, p2auxo.HIVconsvXint, expressing the immunogens HIVconsv1&2. This expression vector used an antibiotic resistance-free mechanism for plasmid selection and maintenance. It was first transformed into a glycine auxotrophic E. coli strain and subsequently transformed into a lysine auxotrophic Mycobacterium bovis BCG strain to generate vaccines BCG.HIVconsv12auxo.int and BCG.HIVconsv22auxo.int. The DNA sequence coding for the HIVconsv1&2 immunogens and protein expression were confirmed and working vaccine stocks were genetically and phenotypically characterized. We demonstrated that BCG.HIVconsv1&22auxo.int in combination with ChAdOx1.tHIVconsv5&6 were well tolerated and induced HIV-1-specific T-cell responses in adult BALB/c mice. In addition, we showed that the BCG.HIVconsv1&22auxo.int vaccine strains were stable in vitro after 35 bacterial generations and in vivo 7 weeks after inoculation. The use of integrative expression vectors and novel HIV-1 immunogens are likely to have improved the mycobacterial vaccine stability and specific immunogenicity and may enable the development of a useful vaccine platform for priming protective responses against HIV-1/TB and other prevalent pediatric pathogens shortly following birth.
机译:卡介苗目前是唯一获得许可的抗结核疫苗,可为婴儿提供针对脑膜炎和粟粒性结核的保护,尽管成人肺部疾病的保护尚不一致。最近,开发了有前途的HIV-1免疫原,例如T细胞免疫原“ tHIVconsvX”,其使用跨M组的功能保守的蛋白质区域设计,并带有镶嵌免疫原以改善HIV-1变体的匹配和反应广度。在这项研究中,我们构建了一个完整的大肠杆菌分枝杆菌穿梭质粒p2auxo.HIVconsvX int ,它表达了免疫原HIVconsv1&2。该表达载体使用无抗生素抗性机制进行质粒选择和维持。首先将其转化为甘氨酸营养缺陷型大肠杆菌菌株,然后转化为赖氨酸营养缺陷型牛分枝杆菌BCG菌株,以生产疫苗BCG.HIVconsv1 2auxo.int 和BCG.HIVconsv2 2auxo.int < / sup>。确认了编码HIVconsv1&2免疫原和蛋白质表达的DNA序列,并对工作中的疫苗储备进行了遗传和表型鉴定。我们证明了BCG.HIVconsv1&2 2auxo.int 与ChAdOx1.tHIVconsv5&6的结合可以很好地耐受并诱导成年BALB / c小鼠的HIV-1特异性T细胞应答。此外,我们证明了BCG.HIVconsv1&2 2auxo.int 疫苗株在35个细菌世代后在体外和在接种后7周在体内都是稳定的。整合表达载体和新型HIV-1免疫原的使用可能会改善分枝杆菌疫苗的稳定性和特异性免疫原性,并可能为不久后引发针对HIV-1 / TB和其他流行儿科病原体的保护性反应开发有用的疫苗平台出生后。

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