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Reference - PMID:29249658 - Mechanisms Connecting the Conserved Protein Kinases Ssp1, Kin1, and Pom1 in Fission Yeast Cell Polarity and Division.

Reference summary

PubMed ID
PMID:29249658
Title
Mechanisms Connecting the Conserved Protein Kinases Ssp1, Kin1, and Pom1 in Fission Yeast Cell Polarity and Division.
Authors
Lee ME, Rusin SF, Jenkins N, Kettenbach AN, Moseley JB
Citation
Curr Biol 2018 Jan 08;28(1):84-92.e4
Publication year
2018
Abstract
Connections between the protein kinases that function within complex cell polarity networks are poorly understood. Rod-shaped fission yeast cells grow in a highly polarized manner, and genetic screens have identified many protein kinases, including the CaMKK-like Ssp1 and the MARK/PAR-1 family kinase Kin1, that are required for polarized growth and cell shape, but their functional mechanisms and connections have been unknown [1-5]. We found that Ssp1 promotes cell polarity by phosphorylating the activation loop of Kin1. Kin1 regulates cell polarity and cytokinesis through unknown mechanisms [4-7]. We performed a large-scale phosphoproteomic screen and found that Kin1 phosphorylates itself and Pal1 to promote growth at cell tips, and these proteins are interdependent for localization to growing cell tips. Additional Kin1 substrates for cell polarity and cytokinesis (Tea4, Mod5, Cdc15, and Cyk3) were also phosphorylated by a second kinase, the DYRK family member Pom1 [8]. Kin1 and Pom1 were enriched at opposite ends of growing cells, and they phosphorylated largely non-overlapping sites on shared substrates. Combined inhibition of both Kin1and Pom1 led to synthetic defects in their shared substrates Cdc15 and Cyk3, confirming a non-redundant functional connection through shared substrates. These findings uncover a new Ssp1-Kin1 signaling pathway, and define its functional and mechanistic connection with Pom1 signaling for cell polarity and cytokinesis. These kinases are conserved in many eukaryotes including humans, suggesting that similar connections and mechanisms might operate in a broad range of cells.

Annotation

GO molecular function

GO:0005515 - protein binding

Genes:

GO:0004674 - protein serine/threonine kinase activity

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Modification

MOD:00047 - O-phospho-L-threonine

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MOD:00696 - phosphorylated residue

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Multi-locus phenotype

FYPO:0001118 - abnormal vegetative cell morphology

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Genotypes:

FYPO:0005501 - abolished protein localization to cell cortex, with protein mislocalized to cytoplasm, during vegetative growth

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Genotypes:

FYPO:0001880 - abolished protein localization to cell division site

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FYPO:0002699 - decreased protein localization to actomyosin contractile ring

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Genotypes:

FYPO:0000118 - multiseptate vegetative cell

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Genotypes:

FYPO:0000013 - T-shaped vegetative cell with normal cell length

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Single locus phenotype

FYPO:0001384 - abolished protein kinase activity

Genes:

Genotypes:

FYPO:0006502 - abolished protein localization to cell cortex of cell tip during vegetative growth

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Genotypes:

FYPO:0005501 - abolished protein localization to cell cortex, with protein mislocalized to cytoplasm, during vegetative growth

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Genotypes:

FYPO:0001585 - abolished protein localization to cell tip during vegetative growth

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FYPO:0002678 - abolished protein phosphorylation

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FYPO:0000705 - abolished protein-protein interaction

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FYPO:0003150 - decreased NETO

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FYPO:0005798 - decreased protein localization to cell cortex of cell tip during vegetative growth

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FYPO:0003208 - decreased protein localization to cell tip, with protein distributed in plasma membrane or cortex

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FYPO:0002679 - decreased protein phosphorylation

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FYPO:0002021 - dispersed actin cortical patch localization during vegetative growth

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FYPO:0000223 - elongated multiseptate vegetative cell

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FYPO:0003532 - increased monopolar index

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FYPO:0000224 - lemon-shaped cell

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FYPO:0001587 - normal protein localization to cell tip during vegetative growth

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FYPO:0001315 - normal vegetative cell morphology

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FYPO:0003710 - swollen pear-shaped vegetative cell

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