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Different cis-acting DNA elements control expression of the human apolipoprotein AI gene in different cell types.

机译:不同的顺式作用DNA元件控制人载脂蛋白AI基因在不同细胞类型中的表达。

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摘要

In mammals, the gene coding for apolipoprotein AI (apoAI), a protein of the plasma lipid transport system, is expressed only in the liver and the intestine. A series of plasmids containing various lengths of sequences flanking the 5' end of the human apoAI gene were constructed and assayed for transient expression after introduction into cultured human hepatoma (HepG2), colon carcinoma (Caco-2), and epithelial (HeLa) cells. The results showed that while most of these constructs are expressed in HepG2 and Caco-2 cells, none of them is expressed in HeLa cells. In addition, the results indicated that a DNA segment located between nucleotides -256 and -41 upstream from the transcription start site of this gene is necessary and sufficient for maximal levels of expression in HepG2 but not in Caco-2 cells, while a DNA segment located between nucleotides -2052 and -192 is required for maximal levels of expression in Caco-2 cells. Moreover, it was shown that the -256 to -41 DNA segment functions as a hepatoma cell-specific transcriptional enhancer with both homologous and heterologous promoters. These results indicate that different cis- and possibly trans-acting factors are involved in the establishment and subsequent regulation of expression of the apoAI gene in the mammalian liver and intestine.
机译:在哺乳动物中,编码载脂蛋白AI(apoAI)(血浆脂质转运系统的蛋白)的基因仅在肝脏和肠中表达。构建了一系列包含不同长度长度的人类apoAI基因5'侧翼序列的质粒,并将其引入培养的人肝癌(HepG2),结肠癌(Caco-2)和上皮(HeLa)细胞后进行瞬时表达分析。结果显示,尽管这些构建体中的大多数在HepG2和Caco-2细胞中表达,但它们都不在HeLa细胞中表达。另外,结果表明,该基因的转录起始位点上游的核苷酸-256和-41之间的DNA片段对于在HepG2中而不是在Caco-2细胞中达到最大表达水平是必要且充分的,而在DNA片段中Caco-2细胞中的最大表达水平需要位于核苷酸-2052和-192之间的分子。此外,已经表明,-256至-41DNA片段作为具有同源和异源启动子的肝癌细胞特异性转录增强子。这些结果表明,在哺乳动物的肝和肠中apoAI基因表达的建立和随后的调节中涉及不同的顺式和可能的反式作用因子。

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