Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells

Kleinstiver Benjamin P.; Tsai Shengdar Q.; Prew Michelle S.; Nguyen Nhu T.; Welch Moira M.; Lopez Jose M.; McCaw Zachary R.; Aryee Martin J.; Joung J. Keith

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Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells

机译：人类细胞中CRISPR-Cas Cpf1核酸酶的全基因组特异性

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The activities and genome-wide specificities of CRISPR-Cas Cpf1 nucleases(1) are not well defined. We show that two Cpf1 nucleases from Acidaminococcus sp. BV3L6 and Lachnospiraceae bacterium ND2006 (AsCpf1 and LbCpf1, respectively) have on-target efficiencies in human cells comparable with those of the widely used Streptococcus pyogenes Cas9 (SpCas9)(2-5). We also report that four to six bases at the 3' end of the short CRISPR RNA (crRNA) used to program Cpf1 nucleases are insensitive to single base mismatches, but that many of the other bases in this region of the crRNA are highly sensitive to single or double substitutions. Using GUIDE-seq and targeted deep sequencing analyses performed with both Cpf1 nucleases, we were unable to detect off-target cleavage for more than half of 20 different crRNAs. Our results suggest that AsCpf1 and LbCpf1 are highly specific in human cells.

机译：CRISPR-Cas Cpf1核酸酶的活性和全基因组特异性（1）尚不明确。我们显示了从Acidaminococcus sp两个Cpf1核酸酶。 BV3L6和Lachnospiraceae细菌ND2006（分别为AsCpf1和LbCpf1）在人细胞中的靶上效率可与广泛使用的化脓性链球菌Cas9（SpCas9）（2-5）相媲美。我们还报告说，用于编程Cpf1核酸酶的短CRISPR RNA（crRNA）3'末端有4至6个碱基对单碱基错配不敏感，但是crRNA这个区域中的许多其他碱基对单或双取代。使用两种Cpf1核酸酶进行的GUIDE-seq和靶向深度测序分析，我们无法检测到超过20种不同crRNA中一半以上的脱靶切割。我们的结果表明，AsCpf1和LbCpf1在人类细胞中具有高度特异性。

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《Nature biotechnology》 |2016年第8期|共7页
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Kleinstiver Benjamin P.; Tsai Shengdar Q.; Prew Michelle S.; Nguyen Nhu T.; Welch Moira M.; Lopez Jose M.; McCaw Zachary R.; Aryee Martin J.; Joung J. Keith;
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1. Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells [J] . Kleinstiver Benjamin P., Tsai Shengdar Q., Prew Michelle S., Nature biotechnology . 2016,第8期

机译：人类细胞中CRISPR-Cas Cpf1核酸酶的全基因组特异性
2. Genome-wide analysis reveals specificities of Cpf1 endonucleases in human cells (vol 34, pg 863, 2016) [J] . Kim Daesik, Kim Jungeun, Hur Junho K., Nature biotechnology . 2016,第8期

机译：全基因组分析揭示了Cpf1核酸内切酶在人类细胞中的特异性（第34卷，第863页，2016年）
3. Genome-wide analysis reveals specificities of Cpf1 endonucleases in human cells [J] . Kim Daesik, Kim Jungeun, Hur Junho K., Nature biotechnology . 2016,第8期

机译：全基因组分析揭示了人类细胞中Cpf1核酸内切酶的特异性
4. ALTERING, IMPROVING, AND DEFINING THE SPECIFICITIES OF CRISPR-CAS NUCLEASES [C] . Benjamin P. Kleinstiver, Michelle S. Prew, Vikram Pattanayak, Scale-up and manufacturing of cell-based therapies V . 2017

机译：改变，改善和定义CRISPR-CAS核糖核酸的特异性
5. ANALYSIS OF THE STRUCTURE AND CELL-SPECIFIC TRANSCRIPTION OF THE BOVINE PARATHYROID HORMONE GENE (MICROCOCCAL NUCLEASE). [D] . WEAVER, CHRISTINE ALSTON. 1986

机译：牛副甲状旁腺激素基因（微球菌核酸酶）的结构和细胞特异性转录分析。
6. Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells [O] . Benjamin P. Kleinstiver, Shengdar Q. Tsai, Michelle S. Prew, -1

机译：人类细胞中CRISPR-Cas Cpf1核酸酶的全基因组特异性
7. Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells [O] . Benjamin P Kleinstiver, Shengdar Q Tsai, Michelle S Prew, 2016

机译：CARPR-CAS CPF1在人细胞中的基因组特异性

Genome-wide specificities of CRISPR-Cas Cpf1 nucleases in human cells

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