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Publication : Reciprocal regulation of protein kinase C isoforms results in differential cellular responsiveness.

First Author  Sudan R Year  2012
Journal  J Immunol Volume  188
Issue  5 Pages  2328-37
PubMed ID  22271653 Mgi Jnum  J:181276
Mgi Id  MGI:5310686 Doi  10.4049/jimmunol.1101678
Citation  Sudan R, et al. (2012) Reciprocal regulation of protein kinase C isoforms results in differential cellular responsiveness. J Immunol 188(5):2328-37
abstractText  Immunological homeostasis is often maintained by counteractive functions of two different cell types or two different receptors signaling through different intermediates in the same cell. One of these signaling intermediates is protein kinase C (PKC). Ten differentially regulated PKC isoforms are integral to receptor-triggered responses in different cells. So far, eight PKC isoforms are reported to be expressed in macrophages. Whether a single receptor differentially uses PKC isoforms to regulate counteractive effector functions has never been addressed. As CD40 is the only receptor characterized to trigger counteractive functions, we examined the relative role of PKC isoforms in the CD40-induced macrophage functions. We report that in BALB/c mouse macrophages, higher doses of CD40 stimulation induce optimum phosphorylation and translocation of PKCalpha, betaI, betaII, and epsilon whereas lower doses of CD40 stimulation activates PKCdelta, zeta, and lambda. Infection of macrophages with the protozoan parasite Leishmania major impairs PKCalpha, betaI, betaII, and epsilon isoforms but enhances PKCdelta, zeta, and lambda isoforms, suggesting a reciprocity among these PKC isoforms. Indeed, PKCalpha, betaI, betaII, and epsilon isoforms mediate CD40-induced p38MAPK phosphorylation, IL-12 expression, and Leishmania killing; PKCdelta and zeta/lambda mediate ERK1/2 phosphorylation, IL-10 production, and parasite growth. Treatment of the susceptible BALB/c mice with the lentivirally expressed PKCdelta- or zeta-specific short hairpin RNA significantly reduces the infection and reinstates host-protective IFN-gamma-dominated T cell response, defining the differential roles for PKC isoforms in immune homeostasis and novel PKC-targeted immunotherapeutic and parasite-derived immune evasion strategies.
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