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单纯疱疹病毒载体与基因向脑内的转移。

Herpes simplex virus vectors and gene transfer to brain.

作者信息

Glorioso J C, Goins W F, Fink D J, DeLuca N A

机构信息

Department of Molecular Genetics & Biochemistry, University of Pittsburgh School of Medicine, PA.

出版信息

Dev Biol Stand. 1994;82:79-87.

PMID:7958486
Abstract

Experiments are in progress to engineer herpes simplex virus type 1 as a gene transfer vector for the nervous system. This virus is well suited for this purpose due to its ability to persist for long periods in a latent state in neurons wherein lytic genes are inactive and a unique viral promoter is capable of inducing transcription from the latent viral genome. The virus can be highly cytotoxic for neurons, however, and thus genes which initiate the lytic cycle must be deleted from the genome in order to force the virus into latency. Candidate genes include the immediately early functions ICP0, ICP27, ICP4 and the virus host shut-off function. The design of a suitable promoter regulator capable of expressing foreign genes during latency must also be developed. Many promoters including strong viral promoters and neuronal-specific cellular promoters have proved to be inadequate due to the transient nature of their activity from the viral vector genome and the viral latency promoter region appears to be weakly active in brain. Current efforts concern the development of auto-regulatable promoters which can remain active even if the viral genome is bound by chromatin.

摘要

将1型单纯疱疹病毒改造为神经系统基因传递载体的实验正在进行中。这种病毒非常适合此目的,因为它能够在神经元中以潜伏状态长期存在,其中裂解基因处于无活性状态,并且一个独特的病毒启动子能够诱导潜伏病毒基因组的转录。然而,该病毒对神经元可能具有高度细胞毒性,因此必须从基因组中删除启动裂解周期的基因,以迫使病毒进入潜伏状态。候选基因包括立即早期功能ICP0、ICP27、ICP4以及病毒宿主关闭功能。还必须开发一种能够在潜伏期间表达外源基因的合适启动子调节因子。由于许多启动子(包括强病毒启动子和神经元特异性细胞启动子)从病毒载体基因组的活性具有短暂性,并且病毒潜伏启动子区域在大脑中似乎活性较弱,已证明它们并不适用。目前的工作集中在开发即使病毒基因组被染色质结合仍能保持活性的自动调节启动子。

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