PROTEIN 3D STRUCTURE COMPARISON
蛋白质 3D 结构比较
基本信息
- 批准号:6290485
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:
- 资助国家:美国
- 起止时间:至
- 项目状态:未结题
- 来源:
- 关键词:
项目摘要
We have developed algorithms for comparison and alignment of protein three dimensional structures. VAST (vector alignment search tool) identifies substructure similarities by comparing the types, connectivity, and relative orientations of SSEs (secondary structure elements). Surprising similarities are identified objectively, by considering the number and scores of superimposable SSE-pairs in the best alignment, and the number of alternative alignments sampled. An optimal residue-by-residue alignments are also identified objectively, as that with the most surprising combination of superposition residual and number of aligned residues. Work this year has focused in three areas. The first is construction of an automated incremental update system, to maintain an all-against-all database of the structure neighbor relationships among domain structures in the public database. The VAST neighbor database now contains nearly 3 million structural superpositions alignments. The second area is construction of an on- the-fly structure neighbor server, which is now in use by structural biologists. This server allows them to transmit confidential coordinate data for VAST comparison against the public structure database, to identify possible remote homologs and to map features from one family member to another. The third area of work this year has been a research project aimed at distinguishing structure neighbors that are related by descent from a common ancestral gene from those that are related by convergence to energetically preferred folding motifs. We have shown that homologs and analogs, as they have been called, may be better distinguished by a test for the HCS (Homologous Core Structure), the substructure conserved among previously identified homologs, than by any measures proposed earlier. Research is in progress to fully automate HCS calculations, and to construct multiple structure alignments of homologous protein domains as clustered by HCS overlap. - protein 3D structure comparison homologous core structure - Neither Human Subjects nor Human Tissues
我们已经开发了比较和比对蛋白质三维结构的算法。Vast(载体比对搜索工具)通过比较SSE(二级结构元素)的类型、连通性和相对取向来确定子结构相似性。通过考虑最佳比对中可重叠的SSE对的数量和分数以及采样的备选比对的数量,客观地识别出惊人的相似之处。还客观地确定了最优的逐个残基的比对,因为具有最令人惊讶的叠加残基和比对残基数量的组合。今年的工作主要集中在三个方面。首先是构建一个自动增量更新系统,以维护公共数据库中域结构之间的结构邻居关系的全盘数据库。庞大的邻居数据库现在包含近300万个结构叠加排列。第二个领域是构建动态结构邻居服务器,结构生物学家现在正在使用该服务器。该服务器允许他们传输机密坐标数据,用于与公共结构数据库进行大量比较,以识别可能的远程同源,并将特征从一个家庭成员映射到另一个家庭成员。今年的第三个工作领域是一个研究项目,旨在区分因共同祖先基因的后裔而相关的结构邻居,以及因趋同于能量偏好的折叠基序而相关的结构邻居。我们已经证明,与先前提出的任何措施相比,通过对HCS(同源核心结构)的测试可能更好地区分同系物和类似物。HCS(同源核心结构)是先前确定的同源物中保守的亚结构。研究正在进行中,以完全自动化的HCS计算,并构建由HCS重叠聚集的同源蛋白质结构域的多个结构比对。-蛋白质3D结构比较同源核心结构-既不是人体受试者也不是人体组织
项目成果
期刊论文数量(0)
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会议论文数量(0)
专利数量(0)
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STEPHEN H. BRYANT其他文献
STEPHEN H. BRYANT的其他文献
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{{ truncateString('STEPHEN H. BRYANT', 18)}}的其他基金
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