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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Role of RNA splicing in mediating lineage-specific expression of the von Willebrand factor gene in the endothelium.
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Role of RNA splicing in mediating lineage-specific expression of the von Willebrand factor gene in the endothelium.

机译:RNA拼接在内皮中von Willebrand因子基因的谱系特异性表达中的作用。

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摘要

We previously demonstrated that the first intron of the human von Willebrand factor (vWF) is required for gene expression in the endothelium of transgenic mice. Based on this finding, we hypothesized that RNA splicing plays a role in mediating vWF expression in the vasculature. To address this question, we used transient transfection assays in human endothelial cells and megakaryocytes with intron-containing and intronless human vWF promoter-luciferase constructs. Next, we generated knockin mice in which LacZ was targeted to the endogenous mouse vWF locus in the absence or presence of the native first intron or heterologous introns from the human β-globin, mouse Down syndrome critical region 1, or hagfish coagulation factor X genes. In both the in vitro assays and the knockin mice, the loss of the first intron of vWF resulted in a significant reduction of reporter gene expression in endothelial cells but not megakaryocytes. This effect was rescued to varying degrees by the introduction of a heterologous intron. Intron-mediated enhancement of expression was mediated at a posttranscriptional level. Together, these findings implicate a role for intronic splicing in mediating lineage-specific expression of vWF in the endothelium.
机译:我们之前证明了在转基因小鼠的内皮中的基因表达需要人von Willebrand因子(VWF)的第一个内含子。基于这一发现,我们假设RNA剪接在介导脉管系统中的vwf表达中发挥作用。为了解决这个问题,我们使用人类内皮细胞和巨核细胞的瞬时转染测定与内含子和无内部人的VWF启动子 - 荧光素酶构建体。接下来,我们产生的基因小鼠,其中LacZ在从人β-珠蛋白,小鼠羽绒综合征临界区域1或Hagfish凝血因子X基因的情况下在没有或存在的原生第一内含子或异源内含子的情况下靶向内源小鼠VWF基因座。在体外测定和基本小鼠的两种情况下,VWF的第一个内含子的损失导致内皮细胞中报告基因表达的显着减少,而不是巨核细胞。通过引入异源内含子来救出这种效果以不同程度的效果。内含子介导的表达增强在预幕前水平介导。这些发现在一起致力于在内皮中介导VWF的谱系特异性表达中的内部内部表达的作用。

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