Identification of a novel NAMPT inhibitor by CRISPR/Cas9 chemogenomic profiling in mammalian cells

David Estoppey; Jeffrey W. Hewett; Chantale T. Guy; Edmund Harrington; Jason R. Thomas; Markus Schirle; Rachel Cuttat; Annick Waldt; Bertran Gerrits; Zinger Yang; Sven Schuierer; Xuewen Pan; Kevin Xie; Walter Carbone; Judith Knehr; Alicia Lindeman; Carsten Russ; Elizabeth Frias; Gregory R. Hoffman; Malini Varadarajan; Nadire Ramadan; John S. Reece-Hoyes; Qiong Wang; Xin Chen; Gregory McAllister; Guglielmo Roma; Tewis Bouwmeester; Dominic Hoepfner

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Identification of a novel NAMPT inhibitor by CRISPR/Cas9 chemogenomic profiling in mammalian cells

机译：哺乳动物细胞中CRISPR / CAS9化学组分鉴定新的命名抑制剂

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Chemogenomic profiling is a powerful and unbiased approach to elucidate pharmacological targets and the mechanism of bioactive compounds. Until recently, genome-wide, high-resolution experiments of this nature have been limited to fungal systems due to lack of mammalian genome-wide deletion collections. With the example of a novel nicotinamide phosphoribosyltransferase (NAMPT) inhibitor, we demonstrate that the CRISPR/Cas9 system enables the generation of transient homo- and heterozygous deletion libraries and allows for the identification of efficacy targets and pathways mediating hypersensitivity and resistance relevant to the compound mechanism of action.

机译：化学因子分析是一种强大而无偏的方法来阐明药理学靶标和生物活性化合物的机制。直到最近，由于缺乏哺乳动物基因组缺失收集，这种性质的基因组的高分辨率实验仅限于真菌系统。通过新型烟酰胺磷酰基转移酶（Nampt）抑制剂的实例，我们证明了CRISPR / CAS9系统能够产生瞬时均匀和杂合的缺失文库，并允许鉴定介质介导对化合物相关的过敏和抗性和抗性的疗效靶标和途径行动机制。

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《Scientific reports.》 |2017年第1期|共6页
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David Estoppey; Jeffrey W. Hewett; Chantale T. Guy; Edmund Harrington; Jason R. Thomas; Markus Schirle; Rachel Cuttat; Annick Waldt; Bertran Gerrits; Zinger Yang; Sven Schuierer; Xuewen Pan; Kevin Xie; Walter Carbone; Judith Knehr; Alicia Lindeman; Carsten Russ; Elizabeth Frias; Gregory R. Hoffman; Malini Varadarajan; Nadire Ramadan; John S. Reece-Hoyes; Qiong Wang; Xin Chen; Gregory McAllister; Guglielmo Roma; Tewis Bouwmeester; Dominic Hoepfner;
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1. Identification of novel mammalian proprioceptive receptor using proprioceptor-specific CRISPR/Cas9 genome editing [J] . Eujung Kim, Han Kyoung Choe IBRO Reports . 2019,第3期

机译：使用本体感受器特异的CRISPR / Cas9基因组编辑识别新型哺乳动物本体感受器
2. Generating Single Cell-Derived Knockout Clones in Mammalian Cells with CRISPR/Cas9 [J] . Christopher J. Giuliano Current Protocols in Molecular Biology . 2019,第期

机译：在哺乳动物细胞中生成单细胞衍生的敲除克隆，用CRISPR / CAS9
3. Characterization of genomic deletion efficiency mediated by clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 nuclease system in mammalian cells. [J] . Matthew C. Canver, Daniel E. Bauer, Abhishek Dass, The Journal of biological chemistry . 2017,第6期

机译：哺乳动物细胞中簇状规则间隔的短回文重复序列（CRISPR）/ Cas9核酸酶系统介导的基因组删除效率的表征。
4. CRISPR/CAS9 TARGETING MICRORNA-24 IN CHINESE HAMSTER OVARY CELLS INCREASES GROWTH AND BOOSTS PRODUCTIVITY [C] . Niamh Keogh, Kevin Kellner, Nga T Lao, Cell culture engineering conference . 2018

机译：CRISPR / CAS9靶向MICRORNA-24在中国仓鼠卵巢细胞中提高生长和生产力
5. Using the CRISPR/Cas9 Technology to Generate a Mammalian Cell Line Knock out for Armcx Genes [D] . Ghimire, Sushma 2019

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6. Identification of a novel NAMPT inhibitor by CRISPR/Cas9 chemogenomic profiling in mammalian cells [O] . David Estoppey, Jeffrey W. Hewett, Chantale T. Guy, -1

机译：通过CRISPR / Cas9化学基因组分析在哺乳动物细胞中鉴定新型NAMPT抑制剂
7. Cell-cell contact-induced gene editing/activation in mammalian cells using a synNotch-CRISPR/Cas9 system [O] . Hongxin Huang, Xin Zhang, Jie Lv, 2020

机译：使用Synnotch-Crispr / Cas9系统，细胞 - 细胞接触诱导的基因编辑/活化在哺乳动物细胞中

Identification of a novel NAMPT inhibitor by CRISPR/Cas9 chemogenomic profiling in mammalian cells

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