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体内电穿孔显著增强了皮肤转染及对皮内核酸疫苗的免疫反应。

Cutaneous transfection and immune responses to intradermal nucleic acid vaccination are significantly enhanced by in vivo electropermeabilization.

作者信息

Drabick J J, Glasspool-Malone J, King A, Malone R W

机构信息

Hematology-Oncology Service, Walter Reed Army Medical Center, Bethesda, Maryland 20307, USA.

出版信息

Mol Ther. 2001 Feb;3(2):249-55. doi: 10.1006/mthe.2000.0257.

Abstract

Naked DNA injection with electropermeabilization (EP) is a promising method for nucleic acid vaccination (NAV) and in vivo gene therapy. Skin is an ideal target for NAV due to ease of administration and the accessibility of large numbers of antigen-presenting cells within the tissue. This study demonstrates that in vivo skin EP may be used to increase transgene expression up to an average of 83-fold relative to naked DNA injection (50 microg DNA per dose, P < 0.005). Transfected cells were principally located in dermis and included adipocytes, fibroblasts, endothelial cells, and numerous mononuclear cells with dendritic processes in a porcine model. Transfected cells were also observed in lymph nodes draining electropermeabilized sites. A HBV sAg-coding plasmid was used to test skin EP-mediated NAV in a murine model. Analysis of humoral immune responses including immunoglobulin subclass profiles revealed strong enhancement of EP-mediated NAV relative to naked DNA injection, with a Th1-dominant, mixed-response pattern compared to immunization with HBV sAg protein that was exclusively Th2 (P = 0.02). Applications for these findings include NAV-based modulation of immune responses to pathogens, allergens, and tumor-associated antigens and the modification of tolerance.

摘要

采用电穿孔技术的裸DNA注射是一种很有前景的核酸疫苗接种(NAV)和体内基因治疗方法。由于易于给药且组织内存在大量抗原呈递细胞,皮肤是NAV的理想靶点。本研究表明,在猪模型中,相对于裸DNA注射(每剂量50μg DNA,P<0.005),体内皮肤电穿孔可使转基因表达平均提高83倍。转染细胞主要位于真皮层,包括脂肪细胞、成纤维细胞、内皮细胞以及众多具有树突状突起的单核细胞。在电穿孔部位引流的淋巴结中也观察到了转染细胞。在小鼠模型中,使用编码乙肝表面抗原(HBV sAg)的质粒来测试皮肤电穿孔介导的NAV。对体液免疫反应的分析,包括免疫球蛋白亚类谱,显示相对于裸DNA注射,电穿孔介导的NAV有显著增强,与仅为Th2型的HBV sAg蛋白免疫相比,呈现出以Th1为主的混合反应模式(P = 0.02)。这些发现的应用包括基于NAV对病原体、过敏原和肿瘤相关抗原的免疫反应进行调节以及耐受性的改变。

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