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通过短肽段的重复来重建转录激活结构域,揭示了富含谷氨酰胺的激活结构域的模块化组织。

Reconstitution of transcriptional activation domains by reiteration of short peptide segments reveals the modular organization of a glutamine-rich activation domain.

作者信息

Tanaka M, Herr W

机构信息

Cold Spring Harbor Laboratory, New York 11724.

出版信息

Mol Cell Biol. 1994 Sep;14(9):6056-67. doi: 10.1128/mcb.14.9.6056-6067.1994.

Abstract

The POU domain activator Oct-2 contains an N-terminal glutamine-rich transcriptional activation domain. An 18-amino-acid segment (Q18III) from this region reconstituted a fully functional activation domain when tandemly reiterated and fused to either the Oct-2 or GAL4 DNA-binding domain. A minimal transcriptional activation domain likely requires three tandem Q18III segments, because one or two tandem Q18III segments displayed little activity, whereas three to five tandem segments were active and displayed increasing activity with increasing copy number. As with natural Oct-2 activation domains, in our assay a reiterated activation domain required a second homologous or heterologous activation domain to stimulate transcription effectively when fused to the Oct-2 POU domain. These results suggest that there are different levels of synergy within and among activation domains. Analysis of reiterated activation domains containing mutated Q18III segments revealed that leucines and glutamines, but not serines or threonines, are critical for activity in vivo. Curiously, several reiterated activation domains that were inactive in vivo were active in vitro, suggesting that there are significant functional differences in our in vivo and in vitro assays. Reiteration of a second 18-amino-acid segment from the Oct-2 glutamine-rich activation domain (Q18II) was also active, but its activity was DNA-binding domain specific, because it was active when fused to the GAL4 than to the Oct-2 DNA-binding domain. The ability of separate short peptide segments derived from a single transcriptional activation domain to activate transcription after tandem reiteration emphasizes the flexible and modular nature of a transcriptional activation domain.

摘要

POU结构域激活因子Oct-2含有一个富含谷氨酰胺的N端转录激活结构域。当该区域的一个18个氨基酸的片段(Q18III)串联重复并与Oct-2或GAL4 DNA结合结构域融合时,可重构一个功能完全的激活结构域。一个最小的转录激活结构域可能需要三个串联的Q18III片段,因为一个或两个串联的Q18III片段几乎没有活性,而三个到五个串联片段具有活性,且随着拷贝数增加活性增强。与天然的Oct-2激活结构域一样,在我们的检测中,当一个重复的激活结构域与Oct-2 POU结构域融合时,需要第二个同源或异源激活结构域才能有效刺激转录。这些结果表明,激活结构域内部和之间存在不同水平的协同作用。对含有突变Q18III片段的重复激活结构域的分析表明,亮氨酸和谷氨酰胺对体内活性至关重要,而丝氨酸或苏氨酸则不然。奇怪的是,几个在体内无活性的重复激活结构域在体外有活性,这表明我们的体内和体外检测存在显著的功能差异。来自Oct-2富含谷氨酰胺激活结构域的另一个18个氨基酸片段(Q18II)的重复也具有活性,但其活性具有DNA结合结构域特异性,因为它与GAL4 DNA结合结构域融合时比与Oct-2 DNA结合结构域融合时更具活性。来自单个转录激活结构域的单独短肽片段在串联重复后激活转录的能力强调了转录激活结构域的灵活性和模块化性质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/da9c/359132/f97e9d7d7b07/molcellb00009-0455-a.jpg

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