Biochemical Characterization of Phospholipids, Sulfatide and Heparin as Potent Stimulators for Autophosphorylation of GSK-3{beta} and the GSK-3{beta}-Mediated Phosphorylation of Myelin Basic Protein In vitro

doi:10.1093/jb/mvm228

Journal of Biochemistry Advance Access originally published online on November 26, 2007
Journal of Biochemistry 2008 143(3):359-367; doi:10.1093/jb/mvm228

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Biochemical Characterization of Phospholipids, Sulfatide and Heparin as Potent Stimulators for Autophosphorylation of GSK-3β and the GSK-3β-Mediated Phosphorylation of Myelin Basic Protein In vitro

Fumitaka Kawakami¹, Akira Yamaguchi¹, Kanzo Suzuki¹, Takayuki Yamamoto² and Kenzo Ohtsuki¹^,*

¹Laboratory of Genetical Biochemistry and Signal Biology, Graduate School of Medical Sciences; and ²Biological Laboratory, Center for Natural Sciences, Kitasato University, Sagamihara 228-8555, Japan

*To whom correspondence should be addressed. Tel/Fax: +81-42-778-8863, E-mail: ken{at}kitasato-u.ac.jp

Received October 21, 2007; Accepted November 13, 2007

Abstract

The stimulatory effects of SH (sulfatide and heparin) and twophospholipids (PI and PS) on autophosphorylation of GSK-3βand the GSK-3β-mediated phosphorylation of myelin basicprotein (MBP) and two synthetic MBP peptides (M86 and M156)were comparatively examined in vitro. It was found that (i)both PI and SH highly stimulated the GSK-3β-mediated phosphorylationof MBP, but not glycogen synthase, and two MBP peptides throughtheir direct binding to these substrates and (ii) both PI andheparin, as compared with sulfatide, highly stimulated autophosphorylationof GSK-3β. The K_m value of MBP for GSK-3β was highlyreduced and the V_max value was significantly increased in thepresence of these acidic modulators, which augmented furtherphosphorylation of MBP by the kinase. Under our experimentalcondition, similar stimulatory effects of PI and heparin wereobserved with the GSK-3β-mediated phosphorylation of tauprotein (TP) in vitro. These results presented here suggestthat these two phospholipids and SH may function as effectivestimulators for autophosphorylation of GSK-3β and for theGSK-3β-mediated high phosphorylation of SH-binding proteins,including MBP and TP, in the highly accumulated levels of theseacidic and sulfated modulators in the brain.

Key Words: glycogen synthase, glycogen synthase kinase 3, heparin, myelin basic protein, phospholipid, sulfatide, tau-kinase, tau protein

Abbreviations: AD, Alzheimer's disease; A-kinase, cAMP-dependent protein kinase; CDK-5, cycline-dependent protein kinase-5; CH-3S, cholesterol-3-sulfate; CK1, casein kinase 1; C-kinase, Ca²⁺/phospholipid-dependent protein kinase; DTT, dithiothreitol; GS, glycogen synthase; GSK-3β, glycogen synthase kinase-3β; MBP, myelin basic protein; PI, phosphatidylinositol; PS, phosphatidylserine; QCM, quarts crystal microbalance; SH, sulfatide and heparin; TP, tau protein

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