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中型细胞外囊泡对神经元和原代星形胶质细胞培养物中腺相关病毒转导效率的影响。

Impact of Medium-Sized Extracellular Vesicles on the Transduction Efficiency of Adeno-Associated Viruses in Neuronal and Primary Astrocyte Cell Cultures.

机构信息

Department of Genetics, Cell- and Immunobiology, Semmelweis University, Nagyvárad tér 4, 1089 Budapest, Hungary.

Department of Physiology, Semmelweis University, Tűzoltó street 37-47, 1094 Budapest, Hungary.

出版信息

Int J Mol Sci. 2021 Apr 19;22(8):4221. doi: 10.3390/ijms22084221.

Abstract

(1) Adeno-associated viruses (AAV) are safe and efficient gene therapy vectors with promising results in the treatment of several diseases. Extracellular vesicles (EV) are phospholipid bilayer-surrounded structures carrying several types of lipids, proteins, and nucleic acids with the ability to cross biological barriers. EV-associated AAVs might serve as new and efficient gene therapy vectors considering that they carry the benefits of both AAVs and EVs. (2) We tested vesicle-associated AAVs and vesicles mixed with AAVs on two major cell types of the central nervous system: a neural cell line (N2A) and primary astrocyte cells. (3) In contrast to previously published in vivo observations, the extracellular vesicle packaging did not improve but, in the case of primary astrocyte cells, even inhibited the infection capacity of the AAV particles. The observed effect was not due to the inhibitory effects of the vesicles themselves, since mixing the AAVs with extracellular vesicles did not change the effectiveness. (4) Our results suggest that improvement of the in vivo efficacy of the EV-associated AAV particles is not due to the enhanced interaction between the AAV and the target cells, but most likely to the improved delivery of the AAVs through tissue barriers and to the shielding of AAVs from neutralizing antibodies.

摘要

(1) 腺相关病毒(AAV)是一种安全且高效的基因治疗载体,在治疗多种疾病方面取得了有前景的成果。细胞外囊泡(EV)是一种磷脂双层包围的结构,携带多种类型的脂质、蛋白质和核酸,具有穿过生物屏障的能力。考虑到它们兼具 AAV 和 EV 的优点,EV 相关的 AAV 可能成为新的高效基因治疗载体。

(2) 我们在中枢神经系统的两种主要细胞类型上测试了囊泡相关的 AAV 和与 AAV 混合的囊泡:神经细胞系(N2A)和原代星形胶质细胞。

(3) 与先前发表的体内观察结果相反,细胞外囊泡的包装并没有提高,而是在原代星形胶质细胞中,甚至抑制了 AAV 颗粒的感染能力。观察到的效果不是由于囊泡本身的抑制作用,因为将 AAV 与细胞外囊泡混合并没有改变其有效性。

(4) 我们的结果表明,EV 相关的 AAV 颗粒在体内疗效的提高不是由于 AAV 与靶细胞之间的相互作用增强,而是很可能由于 AAV 通过组织屏障的递呈得到改善,以及 AAV 免受中和抗体的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dd82/8073863/8cac6748ba13/ijms-22-04221-g001.jpg

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