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Dissection of Genetic Mechanisms Governing the Expression of Serum Retroviral gp70 Implicated in Murine Lupus Nephritis

机译:剖析影响鼠狼疮肾炎的血清逆转录病毒gp70表达的遗传机制。

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The endogenous retroviral envelope glycoprotein, gp70, implicated in murine lupus nephritis is secreted by hepatocytes as an acute phase protein, and it has been thought to be a product of an endogenous xenotropic virus, NZB-X1. However, since endogenous polytropic (PT) and modified polytropic (mPT) viruses encode gp70s that are closely related to xenotropic gp70, these viruses can be additional sources of serum gp70. To better understand the genetic basis of the expression of serum gp70, we analyzed the abundance of xenotropic, PT, or mPT gp70 RNAs in livers and the genomic composition of corresponding proviruses in various strains of mice, including two different Sgp (serum gp70 production) congenic mice. Our results demonstrated that the expression of different viral gp70 RNAs was remarkably heterogeneous among various mouse strains and that the level of serum gp70 production was regulated by multiple structural and regulatory genes. Additionally, a significant contribution of PT and mPT gp70s to serum gp70 was revealed by the detection of PT and mPT, but not xenotropic transcripts in 129 mice, and by a closer correlation of serum levels of gp70 with the abundance of PT and mPT gp70 RNAs than with that of xenotropic gp70 RNA in Sgp3 congenic mice. Furthermore, the injection of lipopolysaccharides selectively up-regulated the expression of xenotropic and mPT gp70 RNAs, but not PT gp70 RNA. Our data indicate that the genetic origin of serum gp70 is more heterogeneous than previously thought, and that distinct retroviral gp70s are differentially regulated in physiological vs inflammatory conditions.
机译:肝细胞分泌与急性狼疮性肾炎有关的内源性逆转录病毒包膜糖蛋白gp70,它是急性期蛋白,被认为是内源性异种病毒NZB-X1的产物。但是,由于内源性多变(PT)和修饰的多变(mPT)病毒编码与异源gp70密切相关的gp70,因此这些病毒可能是血清gp70的其他来源。为了更好地了解血清gp70表达的遗传基础,我们分析了肝脏中异种,PT或mPT gp70 RNA的丰度以及各种小鼠品系中相应原病毒的基因组组成,其中包括两种不同的Sgp(血清gp70产生)同系小鼠。我们的结果表明,不同的病毒gp70 RNA的表达在各种小鼠品系中明显异质,并且血清gp70的产生水平受多种结构和调控基因的调控。此外,通过检测129小鼠中的PT和mPT,但检测到非亲和性转录本,以及血清gp70水平与PT和mPT gp70 RNA的丰度紧密相关,揭示了PT和mPT gp70s对血清gp70的显着贡献。与Sgp3同系小鼠异种gp70 RNA相比。此外,注射脂多糖可选择性上调异种和mPT gp70 RNA的表达,但不上调PT gp70 RNA的表达。我们的数据表明,血清gp70的遗传起源比以前认为的更加异质,并且在生理条件与炎症条件下,不同的逆转录病毒gp70s受到差异调节。

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