Molecular basis for specificity in the druggable kinome: sequence-based analysis

Jianping Chen; Xi Zhang; and Ariel Fernández

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Molecular basis for specificity in the druggable kinome: sequence-based analysis

机译：可药物治疗的基因组特异性的分子基础：基于序列的分析

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Motivation: Rational design of kinase inhibitors remains a challenge partly because there is no clear delineation of the molecular features that direct the pharmacological impact towards clinically relevant targets. Standard factors governing ligand affinity, such as potential for intermolecular hydrophobic interactions or for intermolecular hydrogen bonding do not provide good markers to assess cross reactivity. Thus, a core question in the informatics of drug design is what type of molecular similarity among targets promotes promiscuity and what type of molecular difference governs specificity. This work answers the question for a sizable screened sample of the human pharmacokinome including targets with unreported structure.

机译：动机：激酶抑制剂的合理设计仍然是一个挑战，部分原因是没有明确描述将药理作用导向临床相关靶点的分子特征。控制配体亲和力的标准因子，例如分子间疏水相互作用或分子间氢键结合的潜力，并未提供评估交叉反应性的良好标记。因此，药物设计信息学中的核心问题是靶标之间哪种分子相似性促进混杂，哪种分子差异决定特异性。这项工作回答了人类药代动力学筛查的大量样本问题，其中包括未报告结构的靶标。

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《Bioinformatics》 |2007年第5期|563-572|共10页
作者
Jianping Chen; Xi Zhang; and Ariel Fernández;
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作者单位

Program in Applied Physics and Rice Quantum Institute;

Department of Bioengineering Rice University Houston TX 77005 USA and;

Department of Computer Science The University of Chicago Chicago IL 60637 USA;

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收录信息美国《科学引文索引》(SCI);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
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入库时间 2022-08-18 01:14:18

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1. Molecular basis for specificity in the druggable kinome: sequence-based analysis [J] . Chen JP, Zhang X, Fernandez A Bioinformatics . 2007,第5期

机译：可药物治疗的基因组特异性的分子基础：基于序列的分析
2. Molecular basis for specificity in the druggable kinome: sequence-based analysis [J] . Jianping Chen, Xi Zhang, Ariel Fernandez Bioinformatics . 2007,第5期

机译：可药物治疗的基因组特异性的分子基础：基于序列的分析
3. Computational proteomics of biomolecular interactions in the sequence and structure space of the tyrosine kinome: Deciphering the molecular basis of the kinase inhibitors selectivity. [J] . Verkhivker GM Proteins: Structure, Function, and Genetics . 2007,第4期

机译：酪氨酸激酶组的序列和结构空间中的生物分子相互作用的计算蛋白质组学：解密激酶抑制剂选择性的分子基础。
4. Computational Proteomics of Biomolecular Interactions in Sequence and Structure Space of the Tyrosine Kinome: Evolutionary Constraints and Protein Conformational Selection Determine Binding Signatures of Cancer Drugs [C] . Gennady M. Verkhivker International Workshop on Fuzzy Logic and Applications(WILF 2007); 20070707-10; Camogli(IT) . 2007

机译：酪氨酸激酶组的序列和结构空间中的生物分子相互作用的计算蛋白质组学：进化约束和蛋白质构象选择决定了癌症药物的结合特征。
5. Specificity in the druggable kinome: Molecular basis and its applications. [D] . Zhang, Xi. 2009

机译：在可药物治疗的基因组中的特异性：分子基础及其应用。
6. Molecular basis for specificity in the druggable kinome: sequence-based analysis [O] . Jianping Chen, Xi Zhang, Ariel Fernández -1

机译：可药物治疗的基因组特异性的分子基础：基于序列的分析
7. Molecular basis for specificity in the druggable kinome: sequence-based analysis [O] . Jianping Chen, Xi Zhang, Ariel Fernández 2007

机译：可药物治疗的基因组特异性的分子基础：基于序列的分析

Molecular basis for specificity in the druggable kinome: sequence-based analysis

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