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Molecular Immunophysiology Unit, URA-1961, National Center for
Scientific Research, Pasteur Institute, Paris, France (T.P., R.G.),
Pharmaceutical Research and Development Group, Kyowa Hakko Kogyo, Ltd.,
Chiyoda-ku, Tokyo, Japan (K.I.), and
Endotoxin Group, URA-1116,
National Center for Scientific Research, University of Paris-Sud,
Centre d'Etudes Pharmaceutiques, 92290 Châtenay-Malabry (D.C.)
and
91405 Orsay (R.C.), France
We established previously that lipopolysaccharide (LPS) can induce the
expression of LPS-binding sites on bone marrow cells (BMC). We now
report that staurosporine (STP), a glycosylated indolocarbazole
alkaloid with potent inhibitory activity for various protein kinases,
can induce the same effect. With both agents, the newly expressed LPS
receptor was found to be CD14. The STP-induced effect was independent
of its protein kinase inhibitory activity because several other protein
kinase inhibitors, such as the indolocarbazole K-252a, the
bisindolylmaleimide RO-31-8220, the perylenequinone calphostin C, and
the isoquinolinesulfonamide H7, did not induce CD14 expression. The
observation that the STP analog K-252a with an identical polyaromatic
aglycon moiety was inactive yet the analog UCN-01 with an identical
glycoside ring was active suggests that the induction of CD14
expression is triggered by the sugar moiety of STP. Three lines of
evidence show that the mechanism of CD14 expression induced by STP
differs from that induced by LPS: (i) unlike LPS, STP can stimulate BMC
from LPS-unresponsive C3H/HeJ mice, (ii) LPS and STP effects are
additive at a saturating dose of LPS, and (iii) the protein kinase
inhibitor K-252a inhibits the LPS-induced but not STP-induced
stimulation. Therefore, our findings show that both a protein
kinase-dependent (LPS-induced) and a protein kinase-independent
(STP-induced) mechanism can lead to the expression of the LPS receptor
CD14 on BMC. We also found that the STP-induced stimulation of BMC is
modulated by cyclosporin A, vinblastine, and verapamil. This
observation may suggest that the inducible effect of STP could be
initiated by its interaction with P-glycoprotein, a membrane pump with
drug efflux function that plays a critical role in the multidrug
resistance of cancer cells.
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T. Pedron, R. Girard, and R. Chaby Down-Modulation of L-Selectin by Lipopolysaccharide Is Not Required for Lipopolysaccharide-Induced Expression of CD14 in Mouse Bone Marrow Granulocytes Infect. Immun., July 1, 2001; 69(7): 4287 - 4294. [Abstract] [Full Text] [PDF]
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