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Regulation of the human T-cell receptor alpha gene enhancer: multiple ubiquitous and T-cell-specific nuclear proteins interact with four hypomethylated enhancer elements.

机译：人类T细胞受体α基因增强子的调节：多种普遍存在的T细胞特异性核蛋白与四个次甲基化增强子元素相互作用。

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摘要

Transcription of human T-cell receptor (TCR) alpha genes is regulated by a T-cell-specific transcriptional enhancer that is located 4.5 kilobases 3' of the C alpha gene segment. Previous studies have demonstrated that this enhancer contains at least five nuclear protein-binding sites called T alpha 1 to T alpha 5. In the studies described in this report, we have determined the molecular requirements for human TCR alpha enhancer function. In vitro mutagenesis and deletion analyses demonstrated that full enhancer activity is retained in a 116-base-pair fragment containing the T alpha 1 and T alpha 2 nuclear protein-binding sites and that both of these sites are required for full enhancer function. Functional enhancer activity requires that the T alpha 1 and T alpha 2 binding sites be separated by more than 15 and fewer than 85 base pairs. However, the sequence of this spacer region and the relative phase of the two binding sites on the DNA helix do not affect enhancer function. Deletion and mutation analyses demonstrated that the T alpha 3 and T alpha 4 nuclear protein-binding sites are not necessary or sufficient for TCR alpha enhancer activity. However, a fragment containing these two sites was able to compensate for T alpha 1 and T alpha 2 mutations that otherwise abolished enhancer activity. Electrophoretic mobility shift analyses of the TCR alpha enhancer binding proteins revealed that the T alpha 1, T alpha 3, and T alpha 4 binding proteins are expressed in a variety of T-cell and non-T-cell tumor cell lines. In contrast, one of the two T alpha 2 binding activities was detected only in T-cell nuclear extracts. The activity of the TCR alpha enhancer does not appear to be regulated solely at the level of DNA methylation on that the enhancer sequences were found to be identically hypomethylated in B and T cells as compared with fibroblasts. Taken together, these results suggest that TCR alpha enhancer activity is regulated by the interaction of multiple T-cell-specific and ubiquitous nuclear proteins with partially redundant cis-acting enhancer elements that are hypomethylated in cells of the lymphoid lineage.

机译：人T细胞受体（TCR）α基因的转录受T细胞特异性转录增强子调控，该增强子位于Cα基因区段3'的4.5碱基处。先前的研究表明，这种增强子包含至少五个称为T alpha 1至T alpha 5的核蛋白结合位点。在本报告中描述的研究中，我们已经确定了人类TCRα增强子功能的分子要求。体外诱变和缺失分析表明，完整的增强子活性保留在含有T alpha 1和T alpha 2核蛋白结合位点的116个碱基对的片段中，而这两个位点都是增强子完全发挥功能所必需的。功能增强子活性要求T alpha 1和T alpha 2结合位点被15个以上且少于85个碱基对分开。但是，该间隔区的序列和DNA螺旋上两个结合位点的相对相位不会影响增强子功能。缺失和突变分析表明，Tα3和Tα4核蛋白结合位点对于TCRα增强子活性不是必需的或不足的。但是，包含这两个位点的片段能够补偿原本就没有增强子活性的T alpha 1和T alpha 2突变。 TCRα增强子结合蛋白的电泳迁移率变动分析表明，Tα1，Tα3和Tα4结合蛋白在多种T细胞和非T细胞肿瘤细胞系中表达。相反，仅在T细胞核提取物中检测到两个T alpha 2结合活性之一。 TCRα增强子的活性似乎并不仅限于DNA甲基化水平，因为发现增强子序列与成纤维细胞相比在B和T细胞中具有相同的低甲基化。综上所述，这些结果表明，TCRα增强子的活性受多种T细胞特异性和普遍存在的核蛋白与部分多余的顺式作用增强子元件（在淋巴谱系的细胞中被甲基化）相互作用的调节。

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期刊名称 Molecular and Cellular Biology
作者
I C Ho; J M Leiden;
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作者单位

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年(卷),期 1982(10),9
年度 1982
页码 4720–4727
总页数 8
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
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专利

1. Regulation of the human T-cell receptor alpha gene enhancer: multiple ubiquitous and T-cell-specific nuclear proteins interact with four hypomethylated enhancer elements. [J] . I C Ho, J M Leiden Molecular and Cellular Biology . 1990,第9期

机译：人类T细胞受体α基因增强子的调节：多种普遍存在的T细胞特异性核蛋白与四个次甲基化增强子元素相互作用。
2. Identification and functional characterization of the human T-cell receptor beta gene transcriptional enhancer: common nuclear proteins interact with the transcriptional regulatory elements of the T-cell receptor alpha and beta genes. [J] . L R Gottschalk, J M Leiden Molecular and Cellular Biology . 1990,第10期

机译：人T细胞受体β基因转录增强子的鉴定和功能表征：普通核蛋白与T细胞受体α和β基因的转录调控元件相互作用。
3. Liver‐enriched HNF‐3α and ubiquitous factors interact with the human transferrin gene enhancer [J] . Augeacute, -Gouillou Corinne, Petropoulos Isabelle, FEBS Letters . 1993,第1a2期

机译：肝脏富集的HNF-3α和泛在因子与人类转铁蛋白基因增强子相互作用
4. Regulation of Genes Involved in Lipid Homeostasis and the Pathogenesis of Atherosclerosis: The Role of Promoters, Enhancers, Hormone Nuclear Receptors and Auxiliary Factors in Apolipoprotein Gene Regulation [C] . Vassilis Zannis, Eleoi Zanni, Dimitris Kardassis NATO Advanced Study Institute on Vascular Endothelium : Mechanisms of Cell Signaling . 1999

机译：调节患有脂质稳态的基因和动脉粥样硬化的发病机制：启动子，增强剂，激素核受体和载脂蛋白基因调控中的辅助因子的作用
5. Biophysical characterization of zinc(II)-binding domains in two systems: Neural zinc finger factor-1 and T-cell co-receptors DC4 and DC8 alpha with T-cell-specific kinase Lck. [D] . Davis, Alisa M. 2007

机译：锌（II）结合域在两个系统中的生物物理特征：神经锌指因子1和T细胞共受体DC4和DC8α与T细胞特异性激酶Lck。
6. Identification and functional characterization of the human T-cell receptor beta gene transcriptional enhancer: common nuclear proteins interact with the transcriptional regulatory elements of the T-cell receptor alpha and beta genes. [O] . L R Gottschalk, J M Leiden 1990

机译：人T细胞受体β基因转录增强子的鉴定和功能表征：普通核蛋白与T细胞受体α和β基因的转录调控元件相互作用。
7. Regulation of the human T-cell receptor alpha gene enhancer: multiple ubiquitous and T-cell-specific nuclear proteins interact with four hypomethylated enhancer elements. [O] . Ho, I C, Leiden, J M 1990

机译：人类T细胞受体α基因增强子的调节：多种普遍存在的T细胞特异性核蛋白与四个次甲基化增强子元素相互作用。

Regulation of the human T-cell receptor alpha gene enhancer: multiple ubiquitous and T-cell-specific nuclear proteins interact with four hypomethylated enhancer elements.

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