AAV 病毒的先天免疫感应

IF 3.9 3区 医学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Human gene therapy Pub Date : 2024-07-01 Epub Date: 2024-07-05 DOI:10.1089/hum.2024.040
Di Cao, Barry J Byrne, Ype P de Jong, Cox Terhorst, Dongsheng Duan, Roland W Herzog, Sandeep R P Kumar
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引用次数: 0

摘要

基于腺相关病毒(AAV)的病毒载体被广泛应用于人类基因疗法,并成为多种遗传疾病获批治疗方法的基础。然而,对载体和转基因产品的免疫反应使这些应用在临床实践中变得非常复杂。AAV 载体的先天性免疫识别作用最初并不明确,因为在动物模型(包括 NHP 研究)中,载体给药后早期的炎症反应通常很轻微。然而,最近的研究不断发现先天性免疫通路由 AAV 载体触发,为抗原递呈细胞提供激活信号,并启动适应性免疫反应。内体 DNA 受体收费样受体 9(TLR9)对 AAV 基因组的感应促进了早期炎症反应和干扰素的表达。因此,浆细胞树突状细胞(pDCs)中 TLR9>MyD88 通路的激活会通过 I 型干扰素(IFN I)调节抗原交叉呈递 DCs,并最终激活 CD8+ T 细胞。另外,pDC 也可能通过产生 IL-1 细胞因子,从而激活 IL-1R1>MyD88 信号通路,以不依赖 TLR9 的方式促进 CD8+ T 细胞应答。AAV 可诱导单核细胞衍生的 DC 中细胞因子的表达,进而增加抗体的形成。AAV 包囊与补体成分结合可能会进一步提高 B 细胞的活化。在人体全身使用高剂量载体的情况下,AAV 载体可引发补体激活,其中包括传统途径和替代途径,从而导致严重中毒。最后,有证据表明,AAV 载体的囊壳会激活 TLR2,并激活核酸的其他先天受体。这些观察结果表明,AAV 载体可以启动多种先天性免疫途径,而且很可能是冗余的,从而导致夸张的适应性免疫反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Innate Immune Sensing of Adeno-Associated Virus Vectors.

Adeno-associated virus (AAV) based viral vectors are widely used in human gene therapy and form the basis of approved treatments for several genetic diseases. Immune responses to vector and transgene products, however, substantially complicate these applications in clinical practice. The role of innate immune recognition of AAV vectors was initially unclear, given that inflammatory responses early after vector administration were typically mild in animal models. However, more recent research continues to identify innate immune pathways that are triggered by AAV vectors and that serve to provide activation signals for antigen-presenting cells and initiation of adaptive immune responses. Sensing of the AAV genome by the endosomal DNA receptor toll-like receptor 9 (TLR9) promotes early inflammatory response and interferon expression. Thus, activation of the TLR9>MyD88 pathway in plasmacytoid dendritic cells (pDCs) leads to the conditioning of antigen cross-presenting DCs through type I interferon (IFN-I) and ultimately CD8+ T cell activation. Alternatively, pDCs may also promote CD8+ T cell responses in a TLR9-independent manner by the production of IL-1 cytokines, thereby activating the IL-1R1>MyD88 signaling pathway. AAV can induce cytokine expression in monocyte-derived DCs, which in turn increases antibody formation. Binding of AAV capsid to complement components likely further elevates B cell activation. At high systemic vector doses in humans and in non-human primates, AAV vectors can trigger complement activation, with contributions by classical and alternative pathways, leading to severe toxicities. Finally, evidence for activation of TLR2 by the capsid and of additional innate receptors for nucleic acids has been presented. These observations show that AAV vectors can initiate several and likely redundant innate immune pathways resulting in an exaggerated adaptive immune response.

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来源期刊
Human gene therapy
Human gene therapy 医学-生物工程与应用微生物
CiteScore
6.50
自引率
4.80%
发文量
131
审稿时长
4-8 weeks
期刊介绍: Human Gene Therapy is the premier, multidisciplinary journal covering all aspects of gene therapy. The Journal publishes in-depth coverage of DNA, RNA, and cell therapies by delivering the latest breakthroughs in research and technologies. Human Gene Therapy provides a central forum for scientific and clinical information, including ethical, legal, regulatory, social, and commercial issues, which enables the advancement and progress of therapeutic procedures leading to improved patient outcomes, and ultimately, to curing diseases.
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