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A genetically engineered chimeric vaccine against porcine circovirus type 2 (PCV2) is genetically stable in vitro and in vivo.

机译:针对猪圆环病毒2型(PCV2)的基因工程嵌合疫苗在体外和体内均具有遗传稳定性。

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摘要

A vaccine against porcine circovirus type 2 (PCV2), designated PCV1-2 chimera, was recently developed by replacing the capsid gene of the non-pathogenic PCV1 with that of PCV2. The PCV1-2 chimera virus is attenuated in pigs but induces protective immunity against PCV2. In this study, the genetic stability of the PCV1-2 chimera was evaluated for its potential use as a live vaccine. The PCV1-2 chimera virus was serially passaged 11 times in PK-15 cells and 3 times in pigs. The PCV1-2 chimera virus used in this study contained a tracking marker mutation in the capsid gene (F to V at amino acid position 79). Sequence analyses of the PCV1-2 chimera virus after 11 serial passages in PK-15 cells did not reveal any sequence change including the marker mutation. Similarly, there is no change in the genomic sequence of the PCV1-2 chimera virus recovered from pigs during 3 serial in vivo passages. Under in vivo selection pressure, however, the introduced tracking marker mutation in the PCV1-2 chimera quickly mutated (V79F) and restored to its original sequence after one passage in pigs, and remained stable in subsequent 2 passages in pigs. The results indicate that the PCV1-2 chimera virus is genetically stable, and thus should be a good vaccine candidate.
机译:最近开发了一种针对猪圆环病毒2型(PCV2)的疫苗,称为PCV1-2嵌合体,该疫苗通过将非致病性PCV1的衣壳基因替换为PCV2的衣壳基因来开发。猪中的PCV1-2嵌合体病毒减毒,但诱导出针对PCV2的保护性免疫。在这项研究中,评估了PCV1-2嵌合体的遗传稳定性,将其用作活疫苗。 PCV1-2嵌合病毒在PK-15细胞中连续传代11次,在猪中连续传代3次。本研究中使用的PCV1-2嵌合病毒在衣壳基因中包含一个追踪标记突变(第79位氨基酸从F到V)。在PK-15细胞中连续11次传代后,对PCV1-2嵌合病毒的序列分析未发现任何序列变化,包括标记突变。同样,在连续3次体内传代过程中,从猪身上回收的PCV1-2嵌合病毒的基因组序列也没有变化。然而,在体内选择压力下,PCV1-2嵌合体中引入的跟踪标记突变迅速突变(V79F),并在猪中传代一次后恢复到其原始序列,并在随后的猪第二次传代中保持稳定。结果表明,PCV1-2嵌合病毒在遗传上是稳定的,因此应该是一个很好的候选疫苗。

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