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HIPK family kinases bind and regulate the function of the CCR4-NOT complex.


ABSTRACT: The serine/threonine kinase HIPK2 functions as a regulator of developmental processes and as a signal integrator of a wide variety of stress signals, such as DNA damage, hypoxia, and reactive oxygen intermediates. Because the kinase is generated in a constitutively active form, its expression levels are restricted by a variety of different mechanisms. Here we identify the CCR4-NOT complex as a new regulator of HIPK2 abundance. Down-regulation or knockout of the CCR4-NOT complex member CNOT2 leads to reduced HIPK2 protein levels without affecting the expression level of HIPK1 or HIPK3. A fraction of all HIPK family members associates with the CCR4-NOT components CNOT2 and CNOT3. HIPKs also phosphorylate the CCR4-NOT complex, a feature that is shared with their yeast progenitor kinase, YAK1. Functional assays reveal that HIPK2 and HIPK1 restrict CNOT2-dependent mRNA decay. HIPKs are well known regulators of transcription, but the mutual regulation between CCR4-NOT and HIPKs extends the regulatory potential of these kinases by enabling posttranscriptional gene regulation.

SUBMITTER: Rodriguez-Gil A 

PROVIDER: S-EPMC4907730 | biostudies-literature | 2016 Jun

REPOSITORIES: biostudies-literature

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HIPK family kinases bind and regulate the function of the CCR4-NOT complex.

Rodriguez-Gil Alfonso A   Ritter Olesja O   Hornung Juliane J   Stekman Hilda H   Krüger Marcus M   Braun Thomas T   Kremmer Elisabeth E   Kracht Michael M   Schmitz M Lienhard ML  

Molecular biology of the cell 20160427 12


The serine/threonine kinase HIPK2 functions as a regulator of developmental processes and as a signal integrator of a wide variety of stress signals, such as DNA damage, hypoxia, and reactive oxygen intermediates. Because the kinase is generated in a constitutively active form, its expression levels are restricted by a variety of different mechanisms. Here we identify the CCR4-NOT complex as a new regulator of HIPK2 abundance. Down-regulation or knockout of the CCR4-NOT complex member CNOT2 lead  ...[more]

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