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. 1991 Dec 2;294(1-2):144-8.
doi: 10.1016/0014-5793(91)81362-c.

Catalytic fragment of protein kinase C exhibits altered substrate specificity toward smooth muscle myosin light chain

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Free article

Catalytic fragment of protein kinase C exhibits altered substrate specificity toward smooth muscle myosin light chain

H Nakabayashi et al. FEBS Lett. .
Free article

Abstract

Smooth muscle myosin light chain (LC) can be phosphorylated by myosin light chain kinase (MLCK) at Ser19 and Thr18 and by protein kinase C (PKC) at Thr9 and Ser1 or Ser2 under the in vitro assay conditions. Conversion of PKC to the spontaneously active protein kinase M (PKM) by proteolysis resulted in a change in the substrate specificity of the kinase. PKM phosphorylated both sets of sites in LC recognized by MLCK and PKC as analyzed by peptide mapping analysis. The PKM-catalyzed phosphorylation of these sites was not greatly affected by a MLCK inhibitor, ML-9, nor by the activators of MLCK, Ca2+ and calmodulin.

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