锌指核酸酶
斑马鱼
锌指
生物
生殖系
基因组编辑
胚胎干细胞
基因
遗传学
细胞生物学
转录激活物样效应核酸酶
清脆的
计算生物学
转录因子
作者
Xiangdong Meng,Marcus B. Noyes,Lihua Julie Zhu,Nathan D. Lawson,Scot A. Wolfe
摘要
Direct genomic manipulation at a specific locus is still not feasible in most vertebrate model organisms. In vertebrate cell lines, genomic lesions at a specific site have been introduced using zinc-finger nucleases (ZFNs)1,2,3. Here we adapt this technology to create targeted mutations in the zebrafish germ line. ZFNs were engineered that recognize sequences in the zebrafish ortholog of the vascular endothelial growth factor-2 receptor, kdr (also known as kdra). Co-injection of mRNAs encoding these ZFNs into one-cell-stage zebrafish embryos led to mutagenic lesions at the target site that were transmitted through the germ line with high frequency. The use of engineered ZFNs to introduce heritable mutations into a genome obviates the need for embryonic stem cell lines and should be applicable to most animal species for which early-stage embryos are easily accessible.
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