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      Ras GTPase is EssentiaI for Fas-Mediated Activation of Phospholipase D in A20 Cells

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      https://www.riss.kr/link?id=E1064409

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      We have previously reported that Fas cross-linking resulted in an increase in phospholipase D activity in A20 murine cells(Han, J.-S. et al(1999) Arch Biochem. Biophys. 367, 233-239). In an attempt to explore the Fas downstream factor contributing to the activation of phospholipase D, we have investigated the possible involvement of a small GTP biding protein Ras in signaling events that were triggered by Fas cross-linking. Upon adenoviral expression of dominant negative mutant of Ras(N17Ras), an increase in phospholipase D activity by anti-Fas monoclonal antibody was diminished. Also, the Fas-downstream signaling events triggered by Fas cross-linking such as the activation of phosphatidylcholine-specific phospholipase C, the increase in diacylglycerol level and the translocation of protein kinase C to membrane fraction, were all reduced by N17Ras expression. When parellel experiments were performed with manumycin-A, a Ras farnensyltransferase inhibitor, almost identical inhibitory effects on Fas downstream signaling were exhibited. These data suggest that Ras GTPase is essential in transmitting phospholipase D activation signal induced by Fas cross-linking and is located at phosphatidylcholine-specific phospholipase C upstream in Fas signaling cascades.
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      We have previously reported that Fas cross-linking resulted in an increase in phospholipase D activity in A20 murine cells(Han, J.-S. et al(1999) Arch Biochem. Biophys. 367, 233-239). In an attempt to explore the Fas downstream factor contributing to ...

      We have previously reported that Fas cross-linking resulted in an increase in phospholipase D activity in A20 murine cells(Han, J.-S. et al(1999) Arch Biochem. Biophys. 367, 233-239). In an attempt to explore the Fas downstream factor contributing to the activation of phospholipase D, we have investigated the possible involvement of a small GTP biding protein Ras in signaling events that were triggered by Fas cross-linking. Upon adenoviral expression of dominant negative mutant of Ras(N17Ras), an increase in phospholipase D activity by anti-Fas monoclonal antibody was diminished. Also, the Fas-downstream signaling events triggered by Fas cross-linking such as the activation of phosphatidylcholine-specific phospholipase C, the increase in diacylglycerol level and the translocation of protein kinase C to membrane fraction, were all reduced by N17Ras expression. When parellel experiments were performed with manumycin-A, a Ras farnensyltransferase inhibitor, almost identical inhibitory effects on Fas downstream signaling were exhibited. These data suggest that Ras GTPase is essential in transmitting phospholipase D activation signal induced by Fas cross-linking and is located at phosphatidylcholine-specific phospholipase C upstream in Fas signaling cascades.

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