首页> 外文期刊>Human Genetics >Identification and characterization of a tissue-specific silencer element in the first intron of the human acid maltase gene.
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Identification and characterization of a tissue-specific silencer element in the first intron of the human acid maltase gene.

机译:人酸性麦芽糖酶基因第一个内含子中组织特异性沉默子元件的鉴定和表征。

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摘要

Deficiency of acid maltase (acid alpha-glucosidase), a lysosomal enzyme that degrades glycogen, results in glycogenosis type II, an autosomal recessive disease whose manifestations and severity largely depend on the level of residual enzyme activity. Previous studies have established that there are transcriptional control elements in the first intron; in particular a silencer responsive to Hes-1 and YY1 has been identified in the human hepatoma line, HepG2. This region functions as an enhancer in human fibroblasts. Here we have localized a silencer active in fibroblasts to a nearby 25-bp element in intron 1. This element repressed thymidine kinase promoter activity by about 50% in both orientations in human fibroblasts. This silencer, as with the previous one, is tissue specific since constructs containing this region are inactive in HepG2 cells. Electrophoretic mobility shift assay revealed three proteins specifically binding to the element in fibroblasts, and site-directed mutagenesis analysis indicated that all the three proteins binding to the element contribute to the silencer function. The data may be helpful for designing therapy to increase the level of enzyme, particularly when, as in most adults with the disease, there is reduced production of structurally normal enzyme.
机译:酸性麦芽糖酶(酸性α-葡萄糖苷酶)的缺乏(一种降解糖原的溶酶体酶)会导致II型糖原症,这是一种常染色体隐性遗传疾病,其表现和严重程度主要取决于残留酶的活性水平。先前的研究已经确定第一内含子中有转录控制元件。特别是已经在人肝癌细胞系HepG2中鉴定出对Hes-1和YY1有反应的沉默子。该区域用作人类成纤维细胞的增强子。在这里,我们已将在成纤维细胞中活跃的沉默子定位到内含子1的附近25 bp元件上。该元件在人类成纤维细胞的两个方向上都将胸苷激酶启动子活性抑制了约50%。与上一个沉默子一样,该沉默子是组织特异性的,因为含有该区域的构建体在HepG2细胞中是无活性的。电泳迁移率变动分析揭示了三种蛋白与成纤维细胞中的元素特异性结合,定点诱变分析表明这三种与元素结合的蛋白均有助于沉默子功能。该数据可能有助于设计提高酶水平的疗法,尤其是在大多数患有该疾病的成年人中,如结构正常的酶的产生减少时。

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