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Optimization of HIV-1 Envelope DNA Vaccine Candidates within Three Different Animal Models, Guinea Pigs, Rabbits and Cynomolgus Macaques

机译:三种不同动物模型(豚鼠,兔和食蟹猕猴)中HIV-1信封DNA疫苗候选物的优化

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HIV-1 DNA vaccines have many advantageous features. Evaluation of HIV-1 vaccine candidates often starts in small animal models before macaque and human trials. Here, we selected and optimized DNA vaccine candidates through systematic testing in rabbits for the induction of broadly neutralizing antibodies (bNAb). We compared three different animal models: guinea pigs, rabbits and cynomolgus macaques. Envelope genes from the prototype isolate HIV-1 Bx08 and two elite neutralizers were included. Codon-optimized genes, encoded secreted gp140 or membrane bound gp150, were modified for expression of stabilized soluble trimer gene products, and delivered individually or mixed. Specific IgG after repeated i.d. inoculations with electroporation confirmed in vivo expression and immunogenicity. Evaluations of rabbits and guinea pigs displayed similar results. The superior DNA construct in rabbits was a trivalent mix of non-modified codon-optimized gp140 envelope genes. Despite NAb responses with some potency and breadth in guinea pigs and rabbits, the DNA vaccinated macaques displayed less bNAb activity. It was concluded that a trivalent mix of non-modified gp140 genes from rationally selected clinical isolates was, in this study, the best option to induce high and broad NAb in the rabbit model, but this optimization does not directly translate into similar responses in cynomolgus macaques.
机译:HIV-1 DNA疫苗具有许多优势。通常在小型动物模型中进行猕猴和人体试验之前,对候选HIV-1疫苗进行评估。在这里,我们通过在兔子中广泛诱导中和抗体(bNAb)的系统测试选择和优化了DNA疫苗候选物。我们比较了三种不同的动物模型:豚鼠,兔子和食蟹猕猴。来自原型分离株HIV-1 Bx08的包膜基因和两个精英中和剂被包括在内。对密码子优化的基因(编码的分泌型gp140或膜结合型gp150)进行了修饰,以表达稳定的可溶性三聚体基因产物,并单独或混合输送。重复i.d.电穿孔接种证实了其体内表达和免疫原性。对兔子和豚鼠的评估显示了相似的结果。兔中优良的DNA构建体是未经修饰的密码子优化的gp140包膜基因的三价混合物。尽管在豚鼠和兔子中NAb反应具有一定的效力和广度,但接种过DNA的猕猴的bNAb活性较低。结论是,在本研究中,来自合理选择的临床分离株的未修饰gp140基因的三价混合物是诱导高和宽NAb在兔模型中的最佳选择,但这种优化不能直接转化为食蟹猴的类似反应猕猴。

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