SPAK, a STE20/SPS1-related kinase that activates the p38 pathway
Details
Publication Year 2000-08-31,Volume 19,Issue #37,Page 4290-4297
Journal Title
ONCOGENE
Publication Type
Journal Article
Abstract
We have cloned a member of the STE20/SPS1 protein kinase family from a transformed rat pancreatic beta cell line. SPAK (STE20/SPS1-related, proline alanine-rich kinase) belongs to the SPS1 subfamily of STE20 kinases and is highly conserved between species. SPAK is expressed ubiquitously, although preferentially in brain and pancreas. Biochemical characterization of SPAK catalytic activity demonstrates that is a serine/threonine kinase that can phosphorylate itself and an exogenous substrate in vitro. SPAK is immunoprecipitated from transfected mammalian cells as a complex with another, as yet uncharacterized, serine/threonine kinase which is capable of phosphorylating catalytically-inactive SPAK and myelin basic protein in an in vitro kinase assay. SPAK specifically activates the p38 pathway in cotransfection assays. Like MST1 and MST2, SPAK contains a putative caspase cleavage site at the junction of the catalytic domain and the C-terminal region. Full-length SPAK is expressed in the cytoplasm in transfected cells, while a mutant corresponding to caspase-cleaved SPAK is expressed predominantly in the nucleus. The similarity of SPAK to other SPS1 family members, its ability to activate the p38 pathway, in addition to its putative caspase cleavage site, provide evidence that SPAK may act as a novel mediator of stress-activated signals.
Publisher
NATURE PUBLISHING GROUP
Keywords
STE20-LIKE PROTEIN-KINASE; GERMINAL CENTER KINASE; N-TERMINAL KINASE; SACCHAROMYCES-CEREVISIAE; APOPTOSIS; CLONING; LYMPHOCYTES; DOWNSTREAM; COMPONENTS; PROTEASES
Terms of Use/Rights Notice
Refer to copyright notice on published article.


Creation Date: 2000-08-31 12:00:00
An error has occurred. This application may no longer respond until reloaded. Reload 🗙