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Homing Endonucleases: From Microbial Genetic Invaders to Reagents for Targeted DNA Modification

机译:归巢核酸内切酶:从微生物遗传入侵者到靶向DNA修饰的试剂

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摘要

Homing endonucleases are microbial DNA-cleaving enzymes that mobilize their own reading frames by generating double strand breaks at specific genomic invasion sites. These proteins display an economy of size, and yet recognize long DNA sequences (typically 20 to 30 base pairs). They exhibit a wide range of fidelity at individual nucleotide positions in a manner that is strongly influenced by host constraints on the coding sequence of the targeted gene. The activity of these proteins leads to site-specific recombination events that can result in the insertion, deletion, mutation, or correction of DNA sequences. Over the past fifteen years, the crystal structures of representatives from several homing endonuclease families have been solved, and methods have been described to create variants of these enzymes that cleave novel DNA targets. Engineered homing endonucleases proteins are now being used to generate targeted genomic modifications for a variety of biotech and medical applications.
机译:归巢核酸内切酶是微生物DNA裂解酶,通过在特定基因组入侵位点产生双链断裂来动员自己的阅读框架。这些蛋白质显示出大小经济性,但可识别长的DNA序列(通常为20至30个碱基对)。它们以受宿主对靶基因编码序列的限制强烈影响的方式在各个核苷酸位置表现出广泛的保真度。这些蛋白质的活性导致位点特异性重组事件,可导致DNA序列的插入,缺失,突变或校正。在过去的十五年中,已经解决了来自几种归巢核酸内切酶家族的代表的晶体结构,并且描述了创建这些酶的变异体的方法,这些变异体可以裂解新的DNA靶标。现在,工程化的归巢内切核酸酶蛋白被用于生成针对各种生物技术和医学应用的靶向基因组修饰。

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