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Complementation of byrl in fission yeast by mammalian MAP kinase
kinase requires coexpression of Raf kinase David A. Hughes, Alan Ashworth & Christopher J. Marshall
Section of Cell and Molecular
Biology, Chester Beatty Laboratories, Institute of Cancer Research, London SW3
6JB, UK
INTRACELLULAR signalling from receptor tyrosine kinases in
mammalian cells involves the activation of a signal cascade which includes
p21ras and the protein kinases
p74raf-1, MAP kinase kinase and MAP
kinases1–8. In the yeasts Schizosaccharomyces pombe
and Saccharomyces cerevisiae the response to mating pheromones requires
the Spkl and KSS1/FUS3 kinases, which have sequence homology to vertebrate MAP
kinases9–12. The recent cloning of complementary DNAs for
mammalian13–15 and frog16 MAP kinase
kinases has shown that they are homologous to the S. pombe Byr1 (ref.
17) and S. cerevisiae STE7 (ref. 18) kinases, which have been proposed
to function upstream of Spk1 and KSS1/FUS3,
respectively19–22. We have investigated whether these
apparently similar kinase pathways are functionally conserved between
vertebrates and S. pombe. We report here that expression of mammalian
MAP kinase kinase alone fails to complement a byr1 mutant of S.
pombe. When coexpressed with Raf kinase, however, MAP kinase kinase is
activated by phosphorylation and the mating defect of the byr1 mutant is
rescued. This suggests that the pathways are functionally homologous and that
Raf kinase may directly phosphorylate and activate MAP kinase kinase.
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