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通过菌株特异性修饰因子控制乙肝病毒转基因的表达和甲基化

Control of expression and methylation of a hepatitis B virus transgene by strain-specific modifiers.

作者信息

Schweizer J, Valenza-Schaerly P, Goret F, Pourcel C

机构信息

UREG Institut Pasteur, Paris, France.

出版信息

DNA Cell Biol. 1998 May;17(5):427-35. doi: 10.1089/dna.1998.17.427.

Abstract

In transgenic animals, genotype-specific modifiers exert a control over transgene methylation and expression that may or may not be position dependent. These factors belong to different classes, some of them possibly related to modifiers of position-effect variegation in Drosophila. The study of hepatitis B virus (HBV) gene expression in transgenic mice has revealed the existence of many factors influencing transcription, including hormones and tissue-specific transcription factors. We now report the effect of genotype-specific modifiers on HBV surface antigen (HBsAg) expression and transgene methylation. Compared with the C57BL/6 background, the DBA/2 and 129sv backgrounds cause enhancement of HBsAg expression, with little or not effect on transgene methylation or transcription. In contrast, a single cross with a BALB/c mouse is responsible for de novo methylation and silencing of the transgene in all offspring. Several modifiers appear to segregate in the progeny of a transgenic E36 male mouse crossed with (C57BL/6 x BALB/c) F1 females, with the emergence of a high-expressor group. Our observations suggest that different modifiers act cooperatively, at both the transcriptional and post-transcriptional levels, as part of a complex system regulating transgene expression. This transgenic model provides a system to genetically map new mouse strain-specific modifiers, some of them involved in epigenetic modification and transcription control.

摘要

在转基因动物中,基因型特异性修饰因子对转基因的甲基化和表达施加控制,这种控制可能依赖于位置,也可能不依赖于位置。这些因子属于不同类别,其中一些可能与果蝇位置效应斑驳的修饰因子有关。对转基因小鼠中乙型肝炎病毒(HBV)基因表达的研究揭示了许多影响转录的因子的存在,包括激素和组织特异性转录因子。我们现在报告基因型特异性修饰因子对HBV表面抗原(HBsAg)表达和转基因甲基化的影响。与C57BL/6背景相比,DBA/2和129sv背景导致HBsAg表达增强,对转基因甲基化或转录几乎没有影响。相反,与BALB/c小鼠的单次杂交导致所有后代中转基因的从头甲基化和沉默。在与(C57BL/6×BALB/c)F1雌性杂交的转基因E36雄性小鼠的后代中,几种修饰因子似乎发生了分离,出现了一个高表达组。我们的观察结果表明,不同的修饰因子在转录和转录后水平协同作用,作为调节转基因表达的复杂系统的一部分。这种转基因模型提供了一个系统,用于对新的小鼠品系特异性修饰因子进行基因定位,其中一些因子参与表观遗传修饰和转录控制。

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