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在假定蛋白质中鉴定新型限制性内切核酸酶样折叠家族。

Identification of novel restriction endonuclease-like fold families among hypothetical proteins.

作者信息

Kinch Lisa N, Ginalski Krzysztof, Rychlewski Leszek, Grishin Nick V

机构信息

Department of Biochemistry, Howard Hughes Medical Institute, University of Texas Southwestern Medical Center, 5323 Harry Hines Boulevard, Dallas, TX 75390-9050, USA.

出版信息

Nucleic Acids Res. 2005 Jun 22;33(11):3598-605. doi: 10.1093/nar/gki676. Print 2005.

Abstract

Restriction endonucleases and other nucleic acid cleaving enzymes form a large and extremely diverse superfamily that display little sequence similarity despite retaining a common core fold responsible for cleavage. The lack of significant sequence similarity between protein families makes homology inference a challenging task and hinders new family identification with traditional sequence-based approaches. Using the consensus fold recognition method Meta-BASIC that combines sequence profiles with predicted protein secondary structure, we identify nine new restriction endonuclease-like fold families among previously uncharacterized proteins and predict these proteins to cleave nucleic acid substrates. Application of transitive searches combined with gene neighborhood analysis allow us to confidently link these unknown families to a number of known restriction endonuclease-like structures and thus assign folds to the uncharacterized proteins. Finally, our method identifies a novel restriction endonuclease-like domain in the C-terminus of RecC that is not detected with structure-based searches of the existing PDB database.

摘要

限制性核酸内切酶和其他核酸切割酶构成了一个庞大且极其多样的超家族,尽管保留了负责切割的共同核心折叠,但它们之间几乎没有序列相似性。蛋白质家族之间缺乏显著的序列相似性使得同源性推断成为一项具有挑战性的任务,并阻碍了用传统的基于序列的方法识别新家族。使用将序列谱与预测的蛋白质二级结构相结合的一致性折叠识别方法Meta-BASIC,我们在先前未表征的蛋白质中鉴定出九个新的限制性核酸内切酶样折叠家族,并预测这些蛋白质可切割核酸底物。传递搜索与基因邻域分析相结合的应用使我们能够自信地将这些未知家族与许多已知的限制性核酸内切酶样结构联系起来,从而为未表征的蛋白质指定折叠。最后,我们的方法在RecC的C末端鉴定出一个新的限制性核酸内切酶样结构域,而现有的PDB数据库基于结构的搜索未检测到该结构域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d501/1157100/5442e2c08f16/gki676f1.jpg

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