Division of Hepatology and Gene Therapy, Center for Applied Medical Research, Pamplona, Spain.
PLoS One. 2013 Jul 2;8(7):e67748. doi: 10.1371/journal.pone.0067748. Print 2013.
Recombinant adenoassociated viral vectors (rAAV) have proven to be excellent candidates for gene therapy clinical applications. Recent results showed that cellular immunity to AAV represents a major challenge facing the clinical use of systemic administration of these vectors. Interestingly, no preclinical animal model has previously fully reproduced the clinical findings. The aim of the present work was to enhance the T cell immune response against AAV capsid in mice by the administration of a rAAV expressing the immunostimulatory cytokine IL-12. Our results indicate that although IL-12 expression enhanced the AAV capsid-specific immune response it failed to eliminate transduced hepatocytes and long-term expression was achieved. We found that AAV-mediated transgene expression is altered by IL-12-induced liver inflammation. However, IL-12 expression has no effect over preexisting AAV-mediated transgene expression. IL-12 down-regulates AAV mediated transgene expression via induction of IFN-γ production by NK and T cells, but without altering the transduction efficiency measured by viral genomes. Our results indicate that liver inflammation affects the formation of transcriptionally active AAV vector genomes through an unknown mechanism that can be avoided by the use of DNA-demethylating or anti-inflammatory agents.
重组腺相关病毒载体(rAAV)已被证明是基因治疗临床应用的优秀候选者。最近的研究结果表明,细胞免疫对 AAV 是这些载体系统给药临床应用面临的主要挑战。有趣的是,以前没有任何临床前动物模型完全重现临床发现。本研究的目的是通过给予表达免疫刺激细胞因子 IL-12 的 rAAV 来增强小鼠对 AAV 衣壳的 T 细胞免疫反应。我们的结果表明,尽管 IL-12 的表达增强了 AAV 衣壳的特异性免疫反应,但未能消除转导的肝细胞并实现了长期表达。我们发现,IL-12 诱导的肝炎症改变了 AAV 介导的转基因表达。然而,IL-12 的表达对预先存在的 AAV 介导的转基因表达没有影响。IL-12 通过诱导 NK 和 T 细胞产生 IFN-γ 下调 AAV 介导的转基因表达,但不改变通过病毒基因组测量的转导效率。我们的结果表明,肝炎症通过未知机制影响转录活性 AAV 载体基因组的形成,可通过使用 DNA 去甲基化或抗炎剂来避免。
