1. A Screen of the Conserved Kinome for Negative Regulators of LIN-12 Negative Regulatory Region ('NRR')-Missense Activity in
- Author
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Yuting, Deng, Katherine Leisan, Luo, Daniel D, Shaye, and Iva, Greenwald
- Subjects
wnk-1 ,mig-15 ,Notch ,Receptors, Notch ,hpo-11 ,kinase ,Mutation, Missense ,Mutant Screen Report ,Cell Cycle Proteins ,Protein Serine-Threonine Kinases ,Regulatory Sequences, Nucleic Acid ,kin-3 ,Vulva ,LIN-12 ,C. elegans ,Animals ,Female ,RNA Interference ,Caenorhabditis elegans ,Caenorhabditis elegans Proteins ,negative regulator ,RNA, Double-Stranded ,Signal Transduction ,Transcription Factors - Abstract
Genetic analysis of LIN-12/Notch signaling in C. elegans has provided many insights into human biology. Activating missense mutations in the Negative Regulatory Region (NRR) of the ectodomain of LIN-12/Notch were first described in C. elegans, and similar mutations in human Notch were later found to cause T-cell acute lymphoblastic leukemia (T-ALL). The ubiquitin ligase sel-10/Fbw7 is the prototype of a conserved negative regulator of lin-12/Notch that was first defined by loss-of-function mutations that enhance lin-12 NRR-missense activity in C. elegans, and then demonstrated to regulate Notch activity in mammalian cells and to be a bona fide tumor suppressor in T-ALL. Here, we report the results of an RNAi screen of 248 C. elegans protein kinase-encoding genes with human orthologs for enhancement of a weakly activating NRR-missense mutation of lin-12 in the Vulval Precursor Cells. We identified, and validated, thirteen kinase genes whose loss led to increase lin-12 activity; eleven of these genes have never been implicated previously in regulating Notch activity in any system. Depleting the activity of five kinase genes (cdk-8, wnk-1, kin-3, hpo-11, and mig-15) also significantly enhanced the activity of a transgene in which heterologous sequences drive expression of the untethered intracellular domain of LIN-12, suggesting that they increase the activity or stability of the signal-transducing form of LIN-12/Notch. Precedents set by other regulators of lin-12/Notch defined through genetic interactions in C. elegans suggest that this new set of genes may include negative regulators that are functionally relevant to mammalian development and cancer.
- Published
- 2019