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Novel adeno-associated viral vectors for retinal gene therapy

机译:用于视网膜基因治疗的新型腺相关病毒载体

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Vectors derived from adeno-associated virus (AAV) are currently the most promising vehicles for therapeutic gene delivery to the retina. Recently, subretinal administration of AAV2 has been demonstrated to be safe and effective in patients with a rare form of inherited childhood blindness, suggesting that AAV-mediated retinal gene therapy may be successfully extended to other blinding conditions. This is further supported by the great versatility of AAV as a vector platform as there are a large number of AAV variants and many of these have unique transduction characteristics useful for targeting different cell types in the retina including glia, epithelium and many types of neurons. Naturally occurring, rationally designed or in vitro evolved AAV vectors are currently being utilized to transduce several different cell types in the retina and to treat a variety of animal models of retinal disease. The continuous and creative development of AAV vectors provides opportunities to overcome existing challenges in retinal gene therapy such as efficient transfer of genes exceeding AAV's cargo capacity, or the targeting of specific cells within the retina or transduction of photoreceptors following routinely used intravitreal injections. Such developments should ultimately advance the treatment of a wide range of blinding retinal conditions.
机译:衍生自腺相关病毒(AAV)的载体是目前最有希望的将治疗性基因传递至视网膜的载体。最近,已证明在患有罕见形式的遗传性儿童期盲症的患者中,视网膜下给药AAV2是安全有效的,这表明AAV介导的视网膜基因治疗可能会成功地扩展到其他致盲条件。 AAV作为载体平台的多功能性进一步支持了这一点,因为存在大量的AAV变体,其中许多具有独特的转导特性,可用于靶向视网膜中的不同细胞类型,包括神经胶质,上皮和许多类型的神经元。天然存在的,合理设计的或体外进化的AAV载体目前正被用于转导视网膜中几种不同的细胞类型并治疗多种视网膜疾病的动物模型。 AAV载体的不断创新开发为克服视网膜基因治疗中的现有挑战提供了机会,例如有效转移超过AAV载货量的基因,或在常规使用玻璃体内注射后靶向视网膜内的特定细胞或感光细胞的转导。这样的发展最终将促进各种盲目的视网膜疾病的治疗。

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