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腺病毒DNA中的序列基序可阻断刺激性CpG基序引发的免疫激活。

Sequence motifs in adenoviral DNA block immune activation by stimulatory CpG motifs.

作者信息

Krieg A M, Wu T, Weeratna R, Efler S M, Love-Homan L, Yang L, Yi A K, Short D, Davis H L

机构信息

Interdisciplinary Immunology Program and Department of Internal Medicine, University of Iowa College of Medicine, Iowa City, IA 52242, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Oct 13;95(21):12631-6. doi: 10.1073/pnas.95.21.12631.

Abstract

Unmethylated CpG dinucleotides in particular base contexts (CpG-S motifs) are relatively common in bacterial DNA but are rare in vertebrate DNA. B cells and monocytes have the ability to detect such CpG-S motifs that trigger innate immune defenses with production of Th1-like cytokines. Despite comparable levels of unmethylated CpG dinucleotides, DNA from serotype 12 adenovirus is immune-stimulatory, but serotype 2 is nonstimulatory and can even inhibit activation by bacterial DNA. In type 12 genomes, the distribution of CpG-flanking bases is similar to that predicted by chance. However, in type 2 adenoviral DNA the immune stimulatory CpG-S motifs are outnumbered by a 15- to 30-fold excess of CpG dinucleotides in clusters of direct repeats or with a C on the 5' side or a G on the 3' side. Synthetic oligodeoxynucleotides containing these putative neutralizing (CpG-N) motifs block immune activation by CpG-S motifs in vitro and in vivo. Eliminating 52 of the 134 CpG-N motifs present in a DNA vaccine markedly enhanced its Th1-like function in vivo, which was increased further by the addition of CpG-S motifs. Thus, depending on the CpG motif, prokaryotic DNA can be either immune-stimulatory or neutralizing. These results have important implications for understanding microbial pathogenesis and molecular evolution and for the clinical development of DNA vaccines and gene therapy vectors.

摘要

特定碱基环境中的未甲基化CpG二核苷酸(CpG-S基序)在细菌DNA中相对常见,但在脊椎动物DNA中却很少见。B细胞和单核细胞能够检测到此类CpG-S基序,这些基序通过产生Th1样细胞因子触发先天性免疫防御。尽管未甲基化的CpG二核苷酸水平相当,但12型腺病毒的DNA具有免疫刺激作用,而2型腺病毒的DNA则无刺激作用,甚至可以抑制细菌DNA的激活作用。在12型基因组中,CpG侧翼碱基的分布与随机预测的分布相似。然而,在2型腺病毒DNA中,免疫刺激的CpG-S基序数量比直接重复序列簇中或5'端为C或3'端为G的CpG二核苷酸多出15至30倍。含有这些推定的中和(CpG-N)基序的合成寡脱氧核苷酸在体外和体内均可阻断CpG-S基序的免疫激活。去除DNA疫苗中存在的134个CpG-N基序中的52个,可显著增强其在体内的Th1样功能,添加CpG-S基序可进一步增强该功能。因此,根据CpG基序的不同,原核DNA既可以具有免疫刺激作用,也可以具有中和作用。这些结果对于理解微生物发病机制和分子进化以及DNA疫苗和基因治疗载体的临床开发具有重要意义。

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