Regulation of 4F2 heavy-chain gene expression during normal human T-cell activation can be mediated by multiple distinct molecular mechanisms.

T Lindsten; C H June; C B Thompson; J M Leiden

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Regulation of 4F2 heavy-chain gene expression during normal human T-cell activation can be mediated by multiple distinct molecular mechanisms.

机译：正常人T细胞活化过程中4F2重链基因表达的调节可以通过多种不同的分子机制介导。

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The 4F2 molecule belongs to the set of cell surface antigens which is induced following lectin- or antigen-mediated T-cell activation. The increase in 4F2 cell surface expression following lectin-mediated stimulation has been shown to be accompanied by a parallel increase in the steady-state levels of 4F2 heavy-chain (4F2HC) mRNA. The studies described in this report were designed to further elucidate the molecular mechanisms responsible for induction of 4F2HC gene expression following activation of normal resting human peripheral blood T cells. The low levels of mature 4F2HC mRNA in resting T cells were shown to be the result of a block to transcription elongation within the exon 1-intron 1 region of the 4F2HC gene rather than promoter inactivity. Phorbol myristate acetate stimulation of resting T cells resulted in a 20-fold increase in steady-state 4F2HC mRNA levels which was mediated by removal of this block to transcription elongation. The phorbol myristate acetate-induced increase in 4F2HC gene expression is distinct from previously described AP-1-mediated, phorbol ester-induced gene expression in that it requires new protein synthesis. Treatment of resting T cells with ionomycin plus PMA resulted in a 60-fold increase in 4F2HC mRNA levels. This induction was mediated by both an increase in promoter utilization and removal of the block to transcription elongation. Finally, by increasing the half-life of 4F2HC mRNA, cycloheximide treatment of resting T cells induced an approximately five fold increase in the levels of 4F2HC gene expression, although the physiologic significance of this mechanism remains unclear. These results demonstrate that the level of 4F2HC gene expression in normal peripheral blood T cells can be regulated by at least three distinct molecular pathways: (i) changes in promoter utilization, (ii) modulation of a block to transcription elongation, and (iii) alteration in mRNA stability.

机译：4F2分子属于细胞表面抗原，在凝集素或抗原介导的T细胞活化后被诱导。凝集素介导的刺激后4F2细胞表面表达的增加已显示出4F2重链（4F2HC）mRNA稳态水平的平行增加。本报告中描述的研究旨在进一步阐明激活正常静息人外周血T细胞后诱导4F2HC基因表达的分子机制。静息T细胞中低水平的成熟4F2HC mRNA水平显示是4F2HC基因的外显子1-内含子1区域内转录延长受阻而不是启动子失活的结果。甘草酸肉豆蔻酸乙酸酯刺激静止的T细胞导致稳态4F2HC mRNA水平增加20倍，这是通过去除此阻滞至转录延伸而介导的。佛波肉豆蔻酸酯乙酸盐诱导的4F2HC基因表达增加与先前描述的AP-1介导的佛波酯诱导的基因表达不同，因为它需要新的蛋白质合成。用离子霉素加PMA处理静止的T细胞会导致4F2HC mRNA水平增加60倍。这种诱导是通过启动子利用的增加和转录延长的阻断的去除来介导的。最后，通过延长4F2HC mRNA的半衰期，环己酰亚胺对静止的T细胞的处理诱导4F2HC基因表达水平增加了大约5倍，尽管该机制的生理意义尚不清楚。这些结果表明，正常外周血T细胞中的4F2HC基因表达水平可以通过至少三种不同的分子途径来调节：（i）启动子利用的改变，（ii）调节转录转录延伸的嵌段，和（iii） mRNA稳定性改变。

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《Molecular and Cellular Biology》 |1988年第9期|共7页
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T Lindsten; C H June; C B Thompson; J M Leiden;
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中图分类细胞生物学;
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1. Isolation and structural characterization of the human 4F2 heavy-chain gene, an inducible gene involved in T-lymphocyte activation. [J] . K M Gottesdiener, B A Karpinski, T Lindsten, Molecular and Cellular Biology . 1988,第9期

机译：人4F2重链基因的分离和结构表征，该基因是涉及T淋巴细胞活化的诱导型基因。
2. Rearrangement and expression of T-cell antigen receptor genes in human T-lymphocyte tumor lines and normal human T-cell clones: evidence for allelic exclusion of Ti beta gene expression and preferential use of a J beta 2 gene segment. [J] . J M Leiden, D P Dialynas, A D Duby, Molecular and Cellular Biology . 1986,第9期

机译：人T淋巴细胞肿瘤系和正常人T细胞克隆中T细胞抗原受体基因的重排和表达：等位基因排除Tiβ基因表达并优先使用J beta 2基因区段的证据。
3. The first intron of the 4F2 heavy-chain gene contains a transcriptional enhancer element that binds multiple nuclear proteins. [J] . B A Karpinski, L H Yang, P Cacheris, Molecular and Cellular Biology . 1989,第6期

机译：4F2重链基因的第一个内含子包含与多种核蛋白结合的转录增强子元件。
4. Model-Driven Analysis of Gene Expression Data: Application to Metabolic Re-programming during T-cell Activation [C] . Alyaa M. Abdel-Haleem, Ayman F. Abuelela, Victor Solovyev, International Conference on Bioinformatics and Computational Biology . 2015

机译：基因表达数据模型驱动分析：在T细胞激活过程中应用于代谢重新编程
5. Molecular characterization of signaling pathways critical for mitogen -induced T-cell activation and HTLV -I Tax -mediated pathogenesis [D] . Uhlik, Mark Thomas 2001

机译：对有丝分裂原诱导的T细胞活化和HTLV-I税收介导的发病机制至关重要的信号通路的分子表征
6. Regulation of 4F2 heavy-chain gene expression during normal human T-cell activation can be mediated by multiple distinct molecular mechanisms. [O] . T Lindsten, C H June, C B Thompson, 1988

机译：正常人T细胞活化过程中4F2重链基因表达的调节可以通过多种不同的分子机制介导。
7. Regulation of 4F2 heavy-chain gene expression during normal human T-cell activation can be mediated by multiple distinct molecular mechanisms. [O] . Lindsten, T, June, C H, Thompson, C B, 1988

机译：正常人T细胞活化过程中4F2重链基因表达的调节可以通过多种不同的分子机制介导。
8. Regulation of 4F2 Heavy-Chain Gene Expression during Normal Human T-Cell Activation Can Be Mediated by Multiple Distinct Molecular Mechanisms [R] . Lindsten, T., June, C. H., Thompson, C. B., 1988

机译：正常人T细胞活化过程中4F2重链基因表达的调节可以通过多种不同的分子机制介导

Regulation of 4F2 heavy-chain gene expression during normal human T-cell activation can be mediated by multiple distinct molecular mechanisms.

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