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Enhancement of suicidal DNA vaccine potency by delaying suicidal DNA-induced cell death.

机译:通过延迟自杀性DNA诱导的细胞死亡来增强自杀性DNA疫苗的效力。

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DNA-based alphaviral RNA replicon vectors, also called suicidal DNA vectors, alleviate the concerns of integration or transformation related to conventional DNA vectors since suicidal DNA vectors eventually cause apoptosis of transfected cells. However, the expression of inserted genes in these vectors is transient and the potency of suicidal DNA vaccines may be compromised because of apoptotic cell death. Therefore, to enhance the immune response to the human papillomavirus type 16 (HPV-16) E7 antigen, we generated a DNA-based Semliki Forest virus vector, pSCA1, encoding E7 fused with BCL-xL, an antiapoptotic member of the BCL-2 family. Our results indicated that pSCA1 encoding E7/BCL-xL fusion protein delayed cell death in the pSCA1-transfected dendritic cell line and generated significantly higher E7-specific CD8(+) T-cell-mediated immune responses and better antitumor effects than pSCA1 encoding wild-type E7 gene in vaccinated mice. The antiapoptotic function of BCL-xL is important for the enhancement of antigen-specific CD8(+) T-cell responses in vaccinated mice, because a point mutant of BCL-xL lacking antiapoptotic function was ineffective. These results suggest that strategies to delay suicidal DNA-induced cell death using antiapoptotic proteins may greatly enhance the potency of suicidal DNA.
机译:基于DNA的α病毒RNA复制子载体,也称为自杀DNA载体,减轻了与常规DNA载体相关的整合或转化的担忧,因为自杀DNA载体最终导致转染细胞的凋亡。但是,插入的基因在这些载体中的表达是瞬时的,自杀性DNA疫苗的效力可能由于凋亡的细胞死亡而受到损害。因此,为了增强对人乳头瘤病毒16型(HPV-16)E7抗原的免疫应答,我们生成了基于DNA的Semliki Forest病毒载体pSCA1,其编码与BCL-2的抗凋亡成员BCL-xL融合的E7。家庭。我们的结果表明,编码E7 / BCL-xL融合蛋白的pSCA1延迟了pSCA1转染的树突状细胞系中的细胞死亡,并且比编码野生型pSCA1的E7特异性CD8(+)T细胞介导的免疫反应产生了更高的抗肿瘤作用,并具有更好的抗肿瘤作用接种小鼠中的E型E7基因。 BCL-xL的抗凋亡功能对于增强疫苗接种小鼠中的抗原特异性CD8(+)T细胞应答非常重要,因为缺乏抗凋亡功能的BCL-xL的点突变体无效。这些结果表明,使用抗凋亡蛋白来延迟自杀性DNA诱导的细胞死亡的策略可能会大大增强自杀性DNA的效力。

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