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经颅超声辅助基因转染在脑内不同部位的表达比较

Evaluation and optimization of the administration of recombinant adeno-associated viral vectors (serotypes 2/1, 2/2, 2/rh8, 2/9, and 2/rh10) by convection-enhanced delivery to the striatum.

机构信息

Department of Neurosurgery, Frenchay Hospital, Bristol, UK.

出版信息

Hum Gene Ther. 2011 Feb;22(2):237-51. doi: 10.1089/hum.2010.129. Epub 2011 Feb 2.

Abstract

Convection-enhanced delivery (CED) of recombinant adeno-associated virus (rAAV) vectors is a promising approach for delivery of therapeutic transgenes to the brain. In this study we have systematically examined vector dosing in vivo. Infusions of rAAV serotypes 2/1, 2/2, 2/rh8, 2/9, and 2/rh10 expressing an enhanced green fluorescent protein reporter gene were undertaken into the striatum of rats and pigs using CED. Vector distribution, as defined by the volume of distribution and number of transduced cells following each infusion, was determined using stereological methods. Immunohistochemistry was used to determine the transductional tropism of serotypes and to evaluate for the presence of immune cell infiltration into the brain. Vector distribution was highly variable between serotypes. Infusion rate had no significant effect on vector distribution or the occurrence of tissue damage. For serotypes 2/1, 2/2 and 2/rh10, as the vector concentration was increased beyond 10(12) vg/ml, no increase in vector distribution was observed. In contrast, for serotypes 2/rh8 and 2/9, retrograde axonal transport was observed above this threshold concentration. Cell transduction was principally neuronal for all serotypes and was associated with a low-level immune response. In planning clinical trials it is critical that these observations are considered in order to achieve optimal vector dosing.

摘要

经颅超声基因传递(TUS)是一种将治疗性转基因递送到大脑的有前途的方法。在本研究中,我们系统地检查了体内载体剂量。使用 TUS 将表达增强型绿色荧光蛋白报告基因的重组腺相关病毒(rAAV)血清型 2/1、2/2、2/rh8、2/9 和 2/rh10 递送至大鼠和猪的纹状体。使用体视学法确定了每种输注后的分布体积和转导细胞数量来定义载体分布。免疫组织化学用于确定血清型的转导嗜性,并评估免疫细胞是否渗透到大脑中。不同血清型之间的载体分布差异很大。输注率对载体分布或组织损伤的发生没有显著影响。对于血清型 2/1、2/2 和 2/rh10,当载体浓度超过 10(12)vg/ml 时,未观察到载体分布增加。相比之下,对于血清型 2/rh8 和 2/9,在该阈值浓度以上观察到逆行轴突运输。所有血清型的细胞转导主要是神经元,与低水平的免疫反应相关。在规划临床试验时,为了实现最佳载体剂量,必须考虑这些观察结果。

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