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Comparative Study
. 1991 Nov 27;181(1):396-401.
doi: 10.1016/s0006-291x(05)81432-9.

RO 31-8220 and RO 31-7549 show improved selectivity for protein kinase C over staurosporine in macrophages

Affiliations
Comparative Study

RO 31-8220 and RO 31-7549 show improved selectivity for protein kinase C over staurosporine in macrophages

P Dieter et al. Biochem Biophys Res Commun. .

Abstract

Two new potent protein kinase C inhibitors, RO 31-8220 and RO 31-7549, and staurosporine were found to inhibit dose-dependently the phorbol ester-induced formation of prostaglandin E2 and superoxide in cultured liver macrophages. Prostaglandin E2 formation from exogenously added arachidonate was not affected by these compounds. The zymosan-induced formation of inositol phosphates was decreased by simultaneous addition of phorbol ester and was enhanced by prior desensitization of protein kinase C indicating that protein kinase C negatively modulates phospholipase C activation in these cells. While staurosporine suppressed almost totally the zymosan-induced formation of inositol RO 31-8220 and RO 31-7549 inhibited the protein kinase C-mediated effect on inositol phosphate formation, only. Phagocytosis of zymosan was not affected by RO 31-8220 and RO 31-7549 but was decreased by staurosporine. These results demonstrate that two new potent protein kinase C inhibitors, RO 31-8220 and RO 31-7549, are more selective in their actions as staurosporine and are useful tools to determine an involvement of protein kinase C in cellular systems.

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