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首页> 外文期刊>Journal of Medicinal Chemistry >Fast Small Molecule Similarity Searching with Multiple Alignment Profiles of Molecules Represented in One-Dimension
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Fast Small Molecule Similarity Searching with Multiple Alignment Profiles of Molecules Represented in One-Dimension

机译:一维表示的分子的多个排列轮廓的快速小分子相似性搜索

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Multiple sequence alignment has proven to be a powerful method for creating protein and DNA sequence alignment profiles.These profiles of protein families are useful tools for identifying conserved motifs,such as the catalytic triad of the serine protease family or the seven transmembrane helices of the G-protein coupled receptor family.Ultimately,the understanding of the critical motifs within a family is useful for identifying new members of the family.Due to the complexity of protein-ligand recognition,no universally accepted method exists for clustering small molecules into families with the same or similar biological activity.A combination of the concept of multiple sequence alignment and the 1-dimensional molecular representation described earlier offers a new method for profiling sets of small molecules with the same biological activity.These small molecule profiles can isolate key commonalties within the set of bioactive compounds much like a multiple sequence alignment can isolate critical motifs within a protein family.The small molecule profiles then make useful tools for searching small molecule databases for new compounds with the same biological activity.The technique is demonstrated here using the human ether-a-go-go potassium channel and the kinase SRC.
机译:事实证明,多序列比对是创建蛋白质和DNA序列比对谱的有效方法。这些蛋白家族谱可用于识别保守的基序,例如丝氨酸蛋白酶家族的催化三联体或G的七个跨膜螺旋。 -蛋白偶联受体家族。最终,了解一个家族中的关键基序可用于识别该家族的新成员。由于蛋白-配体识别的复杂性,目前尚无普遍接受的方法将小分子与相同或相似的生物活性。多序列比对的概念和较早描述的一维分子表示的结合提供了一种新的方法,可对具有相同生物活性的小分子进行分析,这些小分子图谱可以隔离关键的共同点。一组生物活性化合物,就像多序列比对可以蛋白质家族中的关键关键基序。小分子图谱随后成为有用的工具,可在小分子数据库中搜索具有相同生物活性的新化合物。该技术在此通过人类以太钾通道和激酶进行了证明SRC。

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