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在实验性自身免疫性葡萄膜视网膜炎中,使用腺相关病毒进行四环素诱导的病毒白细胞介素-10眼内基因转移。

Tetracycline-inducible viral interleukin-10 intraocular gene transfer, using adeno-associated virus in experimental autoimmune uveoretinitis.

作者信息

Smith Justine R, Verwaerde Claudie, Rolling Fabienne, Naud Marie-Christine, Delanoye Anne, Thillaye-Goldenberg Brigitte, Apparailly Florence, De Kozak Yvonne

机构信息

INSERM U598, Institut Biomedical des Cordeliers, 75270 Paris, France.

出版信息

Hum Gene Ther. 2005 Sep;16(9):1037-46. doi: 10.1089/hum.2005.16.1037.

Abstract

Members of the adeno-associated virus (AAV) family are good candidates for the treatment of ocular diseases because of their relative lack of pathogenicity. We studied the effect of intraocular injection of AAV2-viral IL-10 (vIL-10) on retinal S-antigen-induced experimental autoimmune uveoretinitis (EAU) in Lewis rats. We demonstrated that AAV2/2-GFP injected into the vitreous body transduced the iris and ciliary body, or anterior uvea, and the retina. We showed that intravitreal injection of the AAV2/2-tetON-vIL-10 construct achieved detectable levels of vIL-10 mRNA and protein within the eye and was effective in protecting the rat retina against destruction. This protection was dependent on the level of vIL-10 present in the aqueous humor/ vitreous body. Intravitreal injection of the same construct encased within an AAV5 shell, AAV2/5-tetONvIL- 10, did not confer any degree of protection. It appeared that the AAV2/5 vectors did not transduce the anterior uvea, the site at which inflammatory cells first localize in EAU, nor the ganglion cell layer; induced low expression of vIL-10 mRNA; and did not achieve detectable levels of transgene expression in the aqueous humor/vitreous body. Local treatment with AAV2/2-tetON-vIL-10 did not dampen the systemic immune response, as determined by S-antigen-specific lymphocyte proliferation. Our results show that local intravitreal injection of AAV2/2 is an effective means by which to deliver immunoregulatory molecules into the eye during uveitis, a chronic human ocular disease.

摘要

腺相关病毒(AAV)家族成员因其相对缺乏致病性,是治疗眼部疾病的良好候选者。我们研究了眼内注射AAV2-病毒白细胞介素-10(vIL-10)对Lewis大鼠视网膜S抗原诱导的实验性自身免疫性葡萄膜视网膜炎(EAU)的影响。我们证明,注入玻璃体的AAV2/2-GFP转导了虹膜、睫状体或前葡萄膜以及视网膜。我们表明,玻璃体内注射AAV2/2-tetON-vIL-10构建体可在眼内实现可检测水平的vIL-10 mRNA和蛋白质,并有效保护大鼠视网膜免受破坏。这种保护取决于房水/玻璃体内vIL-10的水平。玻璃体内注射包裹在AAV5外壳中的相同构建体AAV2/5-tetONvIL-10,未提供任何程度的保护。似乎AAV2/5载体未转导前葡萄膜(EAU中炎症细胞最初定位的部位)和神经节细胞层;诱导vIL-10 mRNA低表达;并且未在房水/玻璃体内实现可检测水平的转基因表达。如通过S抗原特异性淋巴细胞增殖所确定的,用AAV2/2-tetON-vIL-10进行局部治疗并未抑制全身免疫反应。我们的结果表明,在葡萄膜炎(一种慢性人类眼部疾病)期间,玻璃体内局部注射AAV2/2是将免疫调节分子递送至眼内的有效手段。

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