F. Lebrin et al., CK2 alpha - protein phosphatase 2A molecular complex: Possible interactionwith the MAP kinase pathway, MOL C BIOCH, 191(1-2), 1999, pp. 207-212
Despite its wide range of known substrates, the signaling function of prote
in kinase CK2 is still enigmatic. Mounting evidence suggests that CK2 alpha
, the catalytic subunit of holoenzymic CK2, may exist free of its usual reg
ulatory partner CK2 beta, raising the possibility that 'free' CK2 alpha has
regulation and function distinct from those of the holoenzyme. We previous
ly reported that CK2 alpha could bind to the core dimer of protein phosphat
ase 2A, and indirectly cause down-regulation of the PP2A substrate MEK1, po
ssibly via activation of PP2A and/or targeting of PP2A to some element of t
he Ras/Raf/MEK pathway. Here, these results are confirmed and extended. By
using transfection experiments and immune kinase assays, we show that endog
enous PP2Ac and CK2 beta are the only major substrates associating with epi
tope-tagged CK2 alpha, and that expression of activated Raf results in disr
uption of the CK2 alpha-PP2A association. Such disruption might be a necess
ary step for maximal activation of the MAP kinase pathway by Raf In keeping
with this idea, overexpression of CK2 alpha dose-dependently inhibits the
mitogen-induced activation of cotransfected, epitope-tagged MAP kinase. We
suggest that the CK2 beta free form of CK2 alpha is both a target and a reg
ulator of Raf/MAPK signaling.