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三种类型的人 CpG 基序作为内置佐剂,可差异化调节和增强非病毒和病毒复制子 DNA 疫苗的免疫原性。

Three types of human CpG motifs differentially modulate and augment immunogenicity of nonviral and viral replicon DNA vaccines as built-in adjuvants.

机构信息

Beijing Institute of Biotechnology, Beijing, China.

出版信息

Eur J Immunol. 2013 Jan;43(1):228-39. doi: 10.1002/eji.201242690. Epub 2012 Nov 21.

Abstract

NakedDNA vaccines given by intramuscular injection are efficient in mouse models, but they require improvement for human use. As the immunogenicity of DNA vaccines depends, to a large extent, on the presence of CpG motifs as built-in adjuvants, we addressed this issue by inserting three types of human CpG motifs (A-type, B-type, and C-type) into the backbone of nonviral DNA and viral DNA replicon vectors with distinct immunostimulatory activities on human PBMCs. The adjuvant effects of CpG modifications in DNA vaccines expressing three types of antigens (β-Gal, AHc, or PA4) were then characterized in mice and found to significantly enhance antigen-specific humoral and cell-mediated immune responses. The three types of CpG motifs also differentially affected and modulated immune responses and protective potency against botulinum neurotoxin serotype A and Bacillus anthracis A16R challenge. Taken together, these results demonstrate that insertion of human CpG motifs can differentially modulate the immunogenicity of nonviral DNA vaccines as well as viral DNA replicon vaccines. Our study provides not only a better understanding of the in vivo activities of CpG motif adjuvants but implications for the rational design of such motifs as built-in adjuvants for DNA vectors targeting specific antigens.

摘要

经肌肉注射的裸 DNA 疫苗在小鼠模型中具有高效性,但在人类应用中需要改进。由于 DNA 疫苗的免疫原性在很大程度上取决于作为内置佐剂的 CpG 基序的存在,我们通过将三种类型的人 CpG 基序(A 型、B 型和 C 型)插入非病毒 DNA 和具有不同免疫刺激活性的病毒 DNA 复制子载体的骨架中解决了这个问题在人类 PBMC 上。然后,在表达三种抗原(β-Gal、AHc 或 PA4)的 DNA 疫苗中,CpG 修饰的佐剂作用在小鼠中进行了表征,发现它们显著增强了抗原特异性体液和细胞介导的免疫反应。三种类型的 CpG 基序还以不同的方式影响和调节免疫反应以及对肉毒神经毒素血清型 A 和炭疽杆菌 A16R 挑战的保护效力。总之,这些结果表明,插入人 CpG 基序可以不同程度地调节非病毒 DNA 疫苗和病毒 DNA 复制子疫苗的免疫原性。我们的研究不仅提供了对 CpG 基序佐剂体内活性的更好理解,还为针对特定抗原的 DNA 载体作为内置佐剂设计此类基序提供了启示。

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