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DNA 疫苗:一种简单的 DNA 传感物质?

DNA vaccines: a simple DNA sensing matter?

机构信息

Laboratory of Malaria Immunology; WPI Immunology Frontier Research Center (IFReC); Osaka University; Osaka, Japan.

Laboratory of Adjuvant Innovation; National Institute of Biomedical Innovation; Osaka, Japan; Laboratory of Vaccine Science; IFReC; Osaka University; Osaka, Japan.

出版信息

Hum Vaccin Immunother. 2013 Oct;9(10):2216-21. doi: 10.4161/hv.25893. Epub 2013 Aug 2.

Abstract

Since the introduction of DNA vaccines two decades ago, this attractive strategy has been hampered by its low immunogenicity in humans. Studies conducted to improve the immunogenicity of DNA vaccines have shown that understanding the mechanism of action of DNA vaccines might be the key to successfully improving their immunogenicity. Our current understanding is that DNA vaccines induce innate and adaptive immune responses in two ways: (1) encoded protein (or polypeptide) antigen(s) by the DNA plasmid can be expressed in stromal cells (i.e., muscle cells) as well as DCs, where these antigens are processed and presented to naïve CD4 or CD8 T cells either by direct or cross presentation, respectively; and (2) the transfected DNA plasmid itself may bind to an un-identified cytosolic DNA sensor and activate the TBK1-STING pathway and the production of type I interferons (IFNs) which function as an adjuvant. Recent studies investigating double-stranded cytosolic DNA sensor(s) have highlighted new mechanisms in which cytosolic DNA may release secondary metabolites, which are in turn recognized by a novel DNA sensing machinery. Here, we discuss these new metabolites and the possibilities of translating this knowledge into improved immunogenicity for DNA vaccines.

摘要

自二十年前 DNA 疫苗问世以来,由于其在人体中的免疫原性较低,这种颇具吸引力的策略一直受到阻碍。为提高 DNA 疫苗的免疫原性而进行的研究表明,了解 DNA 疫苗的作用机制可能是成功提高其免疫原性的关键。我们目前的理解是,DNA 疫苗通过两种方式诱导先天和适应性免疫反应:(1)DNA 质粒编码的蛋白(或多肽)抗原可以在基质细胞(即肌肉细胞)和 DC 中表达,在这些抗原中通过直接或交叉呈递分别被未成熟的 CD4 或 CD8 T 细胞加工和呈递;(2)转染的 DNA 质粒本身可能与未识别的胞质 DNA 传感器结合,并激活 TBK1-STING 途径和 I 型干扰素(IFNs)的产生,IFNs 作为佐剂发挥作用。最近研究双股胞质 DNA 传感器的研究强调了新的机制,其中胞质 DNA 可能释放次生代谢物,而这些次生代谢物反过来又被新型 DNA 感应机制识别。在这里,我们讨论这些新的代谢物,并探讨将这些知识转化为提高 DNA 疫苗免疫原性的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b7fd/3906407/86c85b7b461c/hvi-9-2216-g1.jpg

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