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Myung, Kyungjae
Center for Genomic Integrity
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Large-scale generation and phenotypic characterization of zebrafish CRISPR mutants of DNA repair genes

Author(s)
Shin, UnbeomNakhro, KhriezhanuoOh, Chang-KyuCarrington, BlakeSong, HeaInVarshney, Gaurav K.Kim, YeongjaeSong, HyeminJeon, SangeunRobbins, GabrielleKim, SanginYoon, SuhyeonChoi, Yong JunKim, Yoo JungBurgess, ShawnKang, SukhyunSood, RamanLee, YoonsungMyung, Kyungjae
Issued Date
2021-11
DOI
10.1016/j.dnarep.2021.103173
URI
https://scholarworks.unist.ac.kr/handle/201301/55343
Fulltext
https://www.sciencedirect.com/science/article/pii/S1568786421001294?via%3Dihub
Citation
DNA REPAIR, v.107, pp.103173
Abstract
A systematic knowledge of the roles of DNA repair genes at the level of the organism has been limited due to the lack of appropriate experimental approaches using animal model systems. Zebrafish has become a powerful vertebrate genetic model system with availability due to the ease of genome editing and large-scale phenotype screening. Here, we generated zebrafish mutants for 32 DNA repair and replication genes through multiplexed CRISPR/Cas9-mediated mutagenesis. Large-scale phenotypic characterization of our mutant collection revealed that three genes (atad5a, ddb1, pcna) are essential for proper embryonic development and hematopoiesis; seven genes (apex1, atrip, ino80, mre11a, shfm1, telo2, wrn) are required for growth and development during juvenile stage and six genes (blm, brca2, fanci, rad51, rad54l, rtel1) play critical roles in sex development. Furthermore, mutation in six genes (atad5a, brca2, polk, rad51, shfm1, xrcc1) displayed hypersensitivity to DNA damage agents. Our zebrafish mutant collection provides a unique resource for understanding of the roles of DNA repair genes at the organismal level.
Publisher
ELSEVIER
ISSN
1568-7864
Keyword (Author)
ZebrafishDNA repairCRIPSRCas9Multiplex mutagenesisSex developmentHematopoiesisDNA damage sensitivity
Keyword
EMBRYONIC-DEVELOPMENTBLOOMS-SYNDROMEIN-VITRODAMAGEPROTEINMICEATMMUTATIONSMETHYLBRCA2

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