Efficient targeting of a SCID gene by an engineered single-chain homing endonuclease

被引:117
作者
Grizot, Sylvestre [1 ]
Smith, Julianne [2 ]
Daboussi, Fayza [1 ]
Prieto, Jesus [3 ]
Redondo, Pilar [3 ]
Merino, Nekane [4 ]
Villate, Maider [4 ]
Thomas, Severine [1 ]
Lemaire, Laetitia [2 ]
Montoya, Guillermo [3 ]
Blanco, Francisco J. [4 ]
Paques, Frederic [1 ,2 ]
Duchateau, Philippe [1 ]
机构
[1] Cellectis SA, F-93235 Romainville, France
[2] Cellectis Genome Surg, F-93235 Romainville, France
[3] Spanish Natl Canc Ctr CNIO, Macromol Crystallog Grp, Struct Biol & Biocomp Program, Madrid 28029, Spain
[4] CIC BioGUNE, Struct Biol Unit, Derio 48160, Spain
关键词
ZINC-FINGER NUCLEASES; I-CREI; CRYSTAL-STRUCTURE; HOMOLOGOUS RECOMBINATION; SITE RECOGNITION; MAMMALIAN-CELLS; DNA RECOGNITION; ARCHAEAL INTRON; GENOME; MEGANUCLEASES;
D O I
10.1093/nar/gkp548
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Sequence-specific endonucleases recognizing long target sequences are emerging as powerful tools for genome engineering. These endonucleases could be used to correct deleterious mutations or to inactivate viruses, in a new approach to molecular medicine. However, such applications are highly demanding in terms of safety. Mutations in the human RAG1 gene cause severe combined immunodeficiency (SCID). Using the I-CreI dimeric LAGLIDADG meganuclease as a scaffold, we describe here the engineering of a series of endonucleases cleaving the human RAG1 gene, including obligate heterodimers and single-chain molecules. We show that a novel single-chain design, in which two different monomers are linked to form a single molecule, can induce high levels of recombination while safeguarding more effectively against potential genotoxicity. We provide here the first demonstration that an engineered meganuclease can induce targeted recombination at an endogenous locus in up to 6% of transfected human cells. These properties rank this new generation of endonucleases among the best molecular scissors available for genome surgery strategies, potentially avoiding the deleterious effects of previous gene therapy approaches.
引用
收藏
页码:5405 / 5419
页数:15
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