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A Score of the Ability of a Three-Dimensional Protein Model to Retrieve Its Own Sequence as a Quantitative Measure of Its Quality and Appropriateness

机译:三维蛋白质模型检索其自身序列的能力得分以此作为对其质量和适当性的定量度量

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摘要

BackgroundDespite the remarkable progress of bioinformatics, how the primary structure of a protein leads to a three-dimensional fold, and in turn determines its function remains an elusive question. Alignments of sequences with known function can be used to identify proteins with the same or similar function with high success. However, identification of function-related and structure-related amino acid positions is only possible after a detailed study of every protein. Folding pattern diversity seems to be much narrower than sequence diversity, and the amino acid sequences of natural proteins have evolved under a selective pressure comprising structural and functional requirements acting in parallel.
机译:背景技术尽管生物信息学取得了显着进展,但蛋白质的一级结构如何导致三维折叠,进而确定其功能仍然是一个难以捉摸的问题。具有已知功能的序列比对可用于成功鉴定具有相同或相似功能的蛋白质。但是,只有在对每种蛋白质进行了详细研究之后,才能鉴定出功能相关和结构相关的氨基酸位置。折叠模式的多样性似乎比序列多样性要窄得多,天然蛋白质的氨基酸序列是在选择性压力下进化的,该压力包括并行作用的结构和功能要求。

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