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在体外,气管支气管上皮细胞中,维生素A在转录水平下调MUC2基因的表达。

Expression of MUC2 gene is down-regulated by vitamin A at the transcriptional level in vitro in tracheobronchial epithelial cells.

作者信息

An G, Luo G, Wu R

机构信息

California Regional Primate Research Center, University of California at Davis 95616.

出版信息

Am J Respir Cell Mol Biol. 1994 May;10(5):546-51. doi: 10.1165/ajrcmb.10.5.8179918.

Abstract

The functional role of airway mucin in the respiratory system is well recognized. The isolation of mucin cDNA clones, MUC genes, introduces new information regarding the structure of the mucin core protein; however, the nature of the authentic core protein of airway mucin is still unresolved. In this communication, the effects of vitamin A on the regulation of MUC2 gene expression in primary tracheobronchial epithelial (TBE) cells of human and nonhuman primates were examined. Vitamin A has been recognized as one of the most important nutrients in the regulation of airway mucous cell differentiation. The expression of the MUC2 gene has been demonstrated in both rat and human tracheal tissues. The monkey cDNA clone MT80 was isolated from a cDNA library derived from vitamin A-depleted cultures of monkey TBE cells using a synthetic oligonucleotide probe corresponding to the 69 nucleotides of a tandemly repeated sequence in human MUC2 cDNA. DNA sequencing revealed a similar tandemly repeated sequence, except that 72 oligonucleotide repeats were observed in the monkey cDNA clone. Using the MT80 cDNA as a probe, the expression of the MUC2 gene was studied in vitro. The corresponding MUC2 message level in primary cultures of monkey TBE cells was down-regulated by vitamin A. This result was consistently demonstrated in primary human and hamster TBE cultures. The down-regulation was both time- and dosage-dependent on vitamin A. A nuclear run-on assay demonstrated a decrease in the transcriptional rate of the MUC2 gene in nuclei isolated from vitamin A-treated cultures. These results suggest that MUC2 gene expression in TBE cells is transcriptionally down-regulated by vitamin A.

摘要

气道黏蛋白在呼吸系统中的功能作用已得到充分认识。黏蛋白cDNA克隆(MUC基因)的分离,为黏蛋白核心蛋白的结构引入了新信息;然而,气道黏蛋白真实核心蛋白的性质仍未明确。在本通讯中,研究了维生素A对人和非人灵长类动物原代气管支气管上皮(TBE)细胞中MUC2基因表达调控的影响。维生素A已被公认为是调节气道黏液细胞分化的最重要营养素之一。MUC2基因在大鼠和人类气管组织中均有表达。猴cDNA克隆MT80是使用与人MUC2 cDNA中串联重复序列的69个核苷酸相对应的合成寡核苷酸探针,从来自维生素A缺乏的猴TBE细胞培养物的cDNA文库中分离得到的。DNA测序显示了一个相似的串联重复序列,只是在猴cDNA克隆中观察到72个寡核苷酸重复。以MT80 cDNA为探针,在体外研究了MUC2基因的表达。维生素A可下调猴TBE细胞原代培养物中相应的MUC2信息水平。这一结果在人及仓鼠TBE细胞原代培养中得到了一致证实。这种下调在时间和剂量上均依赖于维生素A。核转录分析表明,从维生素A处理的培养物中分离的细胞核中,MUC2基因的转录速率降低。这些结果表明,维生素A可在转录水平上下调TBE细胞中MUC2基因的表达。

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