| Literature DB >> 35996692 |
KangBo Ng1,2, Tom Bland1,2, Nisha Hirani1, Nathan W Goehring1,2.
Abstract
Engineered analog sensitive kinases provide a highly effective method for acute, controllable, and highly selective inhibition of kinase activity. Here we describe the design and characterization of an analog sensitive allele of the polarity kinase, PKC-3. This allele supports normal function as measured by its ability to exclude PAR-2 from the anterior membrane of zygotes, and is rapidly and reversibly inhibited in a dose-dependent manner by the ATP analog 1NA-PP1. This allele provides a new tool to explore the role of PKC-3 in diverse contexts within C. elegans , particularly those in which acute and reversible control of PKC-3 kinase activity may be desired. Copyright:Entities:
Year: 2022 PMID: 35996692 PMCID: PMC9391946 DOI: 10.17912/micropub.biology.000610
Source DB: PubMed Journal: MicroPubl Biol ISSN: 2578-9430
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KK1273 |
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CGC/Ken Kemphues |
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NWG0316 |
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This paper |
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NWG0124 |
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This paper |
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Oligos for
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AATGTTCTGATTGACGCTGA
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CACATAAAACTGACAGATTA
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(AluI restriction site introduced) |
TCATTCTCGCGGAATCATTTATCGTGATCTCAAATTGGAC
AACGTCTTAATCGATGCAGAAGGACATATCA
GACTACGGAATGTGTAAAGAGAATATTAAGGATGGAGA TTTAACTTCA |
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Oligos for
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GCTTCCGTTGCTGTTGCATG
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CGAATTCGATGACAAAGAAC
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(MspI restriction site introduced) |
AAAATTTTAAACCAAAATTTTGATAATTTCAGACCGAATC
CTGATGTTTCACATGCAACAGCAACGGAAGCTTCCAGAA GAGCACGCTCGA |
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Primers for genotyping (covers both I331A and T394A sites) | |
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Forward primer (screening) |
CCACAATTCCCTTCCTCGCT |
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Reverse primer (screening) |
TCGAATGGAGATCGACCAGC |
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* underlined base pairs in the crRNA denotes the PAM sequence, which needs to be removed before purchasing crRNA from IDT
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