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通过设计 Notch 受体无规则卷曲区域的电荷模式来控制转录活性。

Control of transcriptional activity by design of charge patterning in the intrinsically disordered RAM region of the Notch receptor.

机构信息

T. C. Jenkins Department of Biophysics, Johns Hopkins University, Baltimore, MD 21218.

Department of Biomedical Engineering, Washington University in St. Louis, St. Louis, MO 63130.

出版信息

Proc Natl Acad Sci U S A. 2017 Oct 31;114(44):E9243-E9252. doi: 10.1073/pnas.1706083114. Epub 2017 Oct 12.

Abstract

Intrinsically disordered regions (IDRs) play important roles in proteins that regulate gene expression. A prominent example is the intracellular domain of the Notch receptor (NICD), which regulates the transcription of Notch-responsive genes. The NICD sequence includes an intrinsically disordered RAM region and a conserved ankyrin (ANK) domain. The 111-residue RAM region mediates bivalent interactions of NICD with the transcription factor CSL. Although the sequence of RAM is poorly conserved, the linear patterning of oppositely charged residues shows minimal variation. The conformational properties of polyampholytic IDRs are governed as much by linear charge patterning as by overall charge content. Here, we used sequence design to assess how changing the charge patterning within RAM affects its conformational properties, the affinity of NICD to CSL, and Notch transcriptional activity. Increased segregation of oppositely charged residues leads to linear decreases in the global dimensions of RAM and decreases the affinity of a construct including a C-terminal ANK domain (RAMANK) for CSL. Increasing charge segregation from WT RAM sharply decreases transcriptional activation for all permutants. Activation also decreases for some, but not all, permutants with low charge segregation, although there is considerable variation. Our results suggest that the RAM linker is more than a passive tether, contributing local and/or long-range sequence features that modulate interactions within NICD and with downstream components of the Notch pathway. We propose that sequence features within IDRs have evolved to ensure an optimal balance of sequence-encoded conformational properties, interaction strengths, and cellular activities.

摘要

无规则区域(IDR)在调控基因表达的蛋白质中发挥着重要作用。一个突出的例子是 Notch 受体(NICD)的细胞内结构域,它调控 Notch 反应基因的转录。NICD 序列包括一个无规则的 RAM 区域和一个保守的锚蛋白重复(ANK)结构域。由 111 个残基组成的 RAM 区域介导 NICD 与转录因子 CSL 的二价相互作用。尽管 RAM 的序列没有很好的保守性,但带相反电荷的残基的线性排列显示出最小的变化。多价两性离子 IDR 的构象特性不仅受总电荷含量的影响,还受线性电荷模式的影响。在这里,我们使用序列设计来评估在 RAM 中改变电荷模式如何影响其构象特性、NICD 与 CSL 的亲和力以及 Notch 转录活性。增加带相反电荷的残基的分离会导致 RAM 的整体尺寸线性减小,并降低包括 C 端 ANK 结构域(RAMANK)的结构域与 CSL 的亲和力。与 WT RAM 相比,增加电荷分离会导致所有突变体的转录激活急剧降低。对于一些但不是所有电荷分离低的突变体,激活也会降低,尽管存在相当大的差异。我们的结果表明,RAM 接头不仅仅是一个被动的系绳,它还贡献了局部和/或远程序列特征,调节了 NICD 内部以及与 Notch 途径下游成分的相互作用。我们提出,IDR 中的序列特征已经进化到确保序列编码的构象特性、相互作用强度和细胞活性之间的最佳平衡。

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