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Multiple structural clustering of bromodomains of the bromo and extra terminal (BET) proteins highlights subtle differences in their structural dynamics and acetylated leucine binding pocket

机译：溴和额外末端的溴莫蛋白的多种结构聚类（BET）蛋白质突出了其结构动力学和乙酰化亮氨酸粘合口袋的微妙差异

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BET proteins are epigenetic readers whose deregulation results in cancer and inflammation. We show that BET proteins (BRD2, BRD3, BRD4 and BRDT) are globally similar with subtle differences in the sequences and structures of their N-terminal bromodomain. Principal component analysis and nonnegative matrix factorization reveal distinct structural clusters associated with specific BET family members, experimental methods, and source organisms. Subtle variations in structural dynamics are evident in the acetylated lysine (Kac) binding pocket of BET bromodomains. Using multiple structural clustering methods, we have also identified representative structures of BET proteins, which are potentially useful for developing potential therapeutic agents.

机译：BET蛋白是表观遗传读者，其放松导致癌症和炎症。我们表明BET蛋白（BRD2，BRD3，BRD4和BRDT）在全球类似于其N末端溴琼瘤的序列和结构的微妙差异。主成分分析和非负矩阵分解揭示了与特定赌注家族成员，实验方法和源生物相关的不同结构簇。结构动态的微妙变化在乙酰化赖氨酸（KAC）结合口袋中是明显的，下注溴染色瘤。使用多种结构聚类方法，我们还确定了BET蛋白的代表性结构，这可能对开发潜在的治疗剂有用。

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《International Conference on Computational Science》|2015年|744 p. :|共13页
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作者
Suryani Lukman; Zeyar Aung; Kelvin Sim;
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中图分类 TP301.5-532;
关键词
epigenetic; bromodomain; structural analysis; clustering; non-negative matrix factorization;

机译：表观遗传;溴琼瘤;结构分析;聚类;非负矩阵分解;

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专利

1. Multiple Structural Clustering of Bromodomains of the Bromo and Extra Terminal (BET) Proteins Highlights Subtle Differences in Their Structural Dynamics and Acetylated Leucine Binding Pocket [J] . Suryani Lukman, Zeyar Aung, Kelvin Sim Procedia Computer Science . 2015,第1期

机译：溴和额外末端（BET）蛋白的溴结构域的多个结构聚类突出显示它们的结构动力学和乙酰化的亮氨酸结合口袋的细微差别
2. GSK789: A Selective Inhibitor of the First Bromodomains (BD1) of the Bromo and Extra Terminal Domain (BET) Proteins [J] . Watson Robert J., Bamborough Paul, Barnett Heather, Journal of Medicinal Chemistry . 2020,第17期

机译：GSK789：溴和额外末端域（BET）蛋白的第一溴瘤（BD1）的选择性抑制剂
3. The Optimization of a Novel, Weak Bromo and Extra Terminal Domain (BET) Bromodomain Fragment Ligand to a Potent and Selective Second Bromodomain (BD2) Inhibitor [J] . Seal Jonathan T., Atkinson Stephen J., Aylott Helen, Journal of Medicinal Chemistry . 2020,第17期

机译：新颖，弱溴和额外末端域（BET）溴域片段配体的优化至有效和选择性的第二溴琼瓜（BD2）抑制剂
4. Multiple structural clustering of bromodomains of the bromo and extra terminal (BET) proteins highlights subtle differences in their structural dynamics and acetylated leucine binding pocket [C] . Suryani Lukman, Zeyar Aung, Kelvin Sim International Conference on Computational Science . 2015

机译：溴和额外末端的溴莫蛋白的多种结构聚类（BET）蛋白质突出了其结构动力学和乙酰化亮氨酸粘合口袋的微妙差异
5. Structure and dynamics of ribonucleoproteins by X-ray crystallography and NMR: Structural basis of Piwi PAZ domain binding preference for 2'-O-methylated 3' terminal ssRNAs. [D] . Tjhen, Richard June. 2010

机译：通过X射线晶体学和NMR分析核糖核蛋白的结构和动力学：Piwi PAZ域对2'-O-甲基化3'端ssRNA的结合偏好的结构基础。
6. Structural Basis and Specificity of Acetylated Transcription Factor GATA1 Recognition by BET Family Bromodomain Protein Brd3 [O] . Roland Gamsjaeger, Sarah R. Webb, Janine M. Lamonica, 2011

机译：BET家族溴结构域蛋白Brd3识别乙酰化转录因子GATA1的结构基础和特异性
7. Multiple Structural Clustering of Bromodomains of the Bromo and Extra Terminal (BET) Proteins Highlights Subtle Differences in Their Structural Dynamics and Acetylated Leucine Binding Pocket [O] . Lukman Suryani, Aung Zeyar, Sim Kelvin 2015

机译：溴和额外末端（BET）蛋白的溴结构域的多个结构聚类突出显示它们的结构动力学和乙酰化的亮氨酸结合口袋的细微差别

Multiple structural clustering of bromodomains of the bromo and extra terminal (BET) proteins highlights subtle differences in their structural dynamics and acetylated leucine binding pocket

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