C-terminal frameshift mutations generate viable knockout mutants with developmental defects for three essential protein kinases

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摘要 Loss-of-function mutants are fundamental resources for gene function studies.However,it is difficult to generate viable and heritable knockout mutants for essential genes.Here,we show that targeted editing of the C-terminal sequence of the embryo lethal gene MITOGEN-ACTIVATED PROTEIN KINASES 1(OsMPK1)results in weak mutants.This C-terminal-edited osmpk1 mutants displayed severe developmental defects and altered disease resistance but generated tens of viable seeds that inherited the mutations.Using the same C-terminal editing approach,we also obtained viable mutants for a wallassociated protein kinase(Os07g0493200)and a leucine-rich repeat receptor-like protein kinase(Os01g0239700),while the null mutations of these genes were lethal.These data suggest that protein kinase activity could be reduced by introducing frameshift mutations adjacent to the C-terminus,which could generate valuable resources for gene function studies and tune protein kinase activity for signaling pathway engineering.

作者 Yun Zhang Miao-Miao Cui Run-Nan Ke Yue-Dan Chen Kabin Xie

机构地区 National Key Laboratory of Crop Genetic Improvement Hubei Key Laboratory of Plant Pathology

出处《aBIOTECH》 EI CAS CSCD 2024年第2期219-224,共6页 生物技术通报（英文版）

基金 supported by the National Natural Science Foundation of China(32293243) Fundamental Research Funds for the Central Universities(2021ZKPY002,2662023PY006) supported by Hainan Yazhou Bay Seed Laboratory and the China National Seed Group(project B23YQ1516).

关键词 CRISPR/Cas9 Lethal mutant Protein kinases Genome editing C-TERMINUS

分类号 Q51 [生物学—生物化学]

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C-terminal frameshift mutations generate viable knockout mutants with developmental defects for three essential protein kinases

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