Regulation of phospholipase D (PLD) in growth plate chondrocytes by 24R,25-(OH)₂D₃ is dependent on cell maturation state (resting zone cells) and is specific to the PLD2 isoform

Many of the effects of 1α,25-(OH)₂D₃ and 24R,25-(OH)₂D₃ on costochondral chondrocytes are mediated by the protein kinase C (PKC) signal transduction pathway. 1α,25-(OH)₂D₃ activates PKC in costochondral growth zone chondrocytes through a specific membrane receptor (1α,25-mVDR), involving rapid increases in diacylglycerol via a phospholipase C (PLC)-dependent mechanism. 24R,25-(OH)₂D₃ activates PKC in resting zone chondrocytes. Although diacylglycerol is increased by 24R,25-(OH)₂D₃, PLC is not involved, suggesting a phospholipase D (PLD)-dependent mechanism. Here, we show that resting zone and growth zone cells express mRNAs for PLD1a, PLD1b, and PLD2. Both cell types have PLD activity, but levels are higher in resting zone cells. 24R,25-(OH)₂D₃, but not 24S,25-(OH)₂D₃ or 1α,25-(OH)₂D₃, stimulates PLD activity in resting zone cells within 3 min via nongenomic mechanisms. Neither 1α,25-(OH)₂D₃ nor 24R,25-(OH)₂D₃ affected PLD in growth zone cells. Basal and 24R,25-(OH)₂D₃-stimulated PLD were inhibited by the PLD inhibitors wortmannin and EDS. Inhibition of phosphatidylinositol 3-kinase (PI 3-kinase), PKC, phosphatidylinositol-specific PLC (PI-PLC), and phosphatidylcholine-specific PLC (PC-PLC) had no effect on PLD activity. Thus, 24R,25-(OH)₂D₃ stimulates PLD, and PI 3-kinase, PI-PLC and PKC are not involved, whereas PLD is required for stimulation of PKC by 24R,25-(OH)₂D₃. Pertussis toxin, GDPβS, and GTPγS had no effect on 24R,25-(OH)₂D₃-dependent PLD when added to cell cultures, indicating that G-proteins are not involved. These data show that PKC activation in resting zone cells is mediated by PLD and suggest that a functional 24R,25-(OH)₂D₃-mVDR is required. The results also support the conclusion that the 24R,25-(OH)₂D₃-responsive PLD is PLD2, since this PLD isoform is G-protein-independent.