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Solving nucleic acid structures by molecular replacement: examples from group II intron studies

机译:通过分子置换解决核酸结构:II组内含子研究的实例

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摘要

Structured RNA molecules are key players in ensuring cellular viability. It is now emerging that, like proteins, the functions of many nucleic acids are dictated by their tertiary folds. At the same time, the number of known crystal structures of nucleic acids is also increasing rapidly. In this context, molecular replacement will become an increasingly useful technique for phasing nucleic acid crystallographic data in the near future. Here, strategies to select, create and refine molecular-replacement search models for nucleic acids are discussed. Using examples taken primarily from research on group II introns, it is shown that nucleic acids are amenable to different and potentially more flexible and sophisticated molecular-replacement searches than proteins. These observations specifically aim to encourage future crystallographic studies on the newly discovered repertoire of noncoding transcripts.
机译:结构化RNA分子是确保细胞活力的关键因素。现在正在出现的是,与蛋白质一样,许多核酸的功能也取决于其三级折叠。同时,核酸的已知晶体结构的数量也在迅速增加。在这种情况下,在不久的将来,分子置换将成为用于定相核酸晶体学数据的越来越有用的技术。在此,讨论了选择,创建和完善核酸分子替换搜索模型的策略。使用主要来自对II组内含子的研究的例子,表明核酸比蛋白质更适合于不同的并且可能更灵活和复杂的分子置换搜索。这些观察特别旨在鼓励将来对新发现的非编码转录本库进行晶体学研究。

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