Abstract:Previous studies have shown that protein kinase C (PKC) alpha, beta II (βII) and zeta inhibition attenuates polymorphonuclear leukocyte (PMN) superoxide (SO) release, whereas PKC delta inhibition augments this response via inhibiting phosphorylation of PMN NADPH oxidase (NOX‐2). However, to date, there is no information regarding the role of PKCβII peptide activator on regulating PMN SO release. PKCβII activator and inhibitor peptides work by augmenting or attenuating PKCβII translocation after stimulation by … Show more
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