Abstract
Peptide growth factors contribute to the pathogenesis of cardiovascular diseases by inducing a variety of cellular responses including anti-apoptotic effects. Several of the signaling molecules that are activated by growth factor receptors such as Src family kinases (Src), phosphatidylinositol 3'-kinase (PI3K), phospholipase Cgamma (PLCgamma), Ras, and SHP-2 were shown to mediate survival signals. We systematically investigated the relative contribution of each signaling molecule for growth factor-dependent cell survival in vascular smooth muscle cells (VSMC). Our approach was the use of mutated plateletderived growth factor (PDGF) beta-receptors (betaPDGFR) in which the tyrosine residues required for binding of each signaling molecule were individually mutated to phenylalanine. To bypass endogenous PDGFR in VSMC we used chimeric receptors (ChiRs), containing the extracellular domain of the macrophage colony-stimulating factor (M-CSF) receptor and the cytoplasmic domain of the wild type (WT) or mutated betaPDGFR. Selective activation of the ChiR-WT with M-CSF significantly reduced apoptosis to the same extent as PDGF-BB in non-transfected cells. Deletion of the binding site for PI3K, but not for Src, RasGAP, SHP-2, or PLCgamma, completely abolished the anti-apoptotic effect. Consistently, a ChiR mutant that only binds PI3K was fully able to mediate cell survival as efficiently as the ChiR-WT. Furthermore, the PDGF-dependent anti-apoptotic effect in non-transfected cells was completely abolished by the PI3K inhibitor wortmannin, whereas inhibitors of Src, PLCgamma, ERK, or p38 MAP kinase had no effect. The exploration of downstream signaling events revealed that PDGF-BB activates the anti-apoptotic Akt signaling pathway in a PI3K-dependent manner. Moreover, Akt phosphorylates and thus inactivates the pro-apoptotic proteins BAD and Forkhead transcription factors (FKHR, FKHRL1). We conclude that growth factor-dependent cell survival in VSMC is mediated only by activation of the PI3K/Akt pathway, whereas all other receptor-associated signaling molecules do not play a significant role.
Highlights
Peptide growth factors contribute to the pathogenesis of cardiovascular diseases by inducing a variety of cellular responses including anti-apoptotic effects
Characterization of Chimeric CSF1R/PDGFR Mutants—To systematically evaluate the role of each of the PDGFR signaling molecules (Src, phosphatidylinositol 3-kinase (PI3K), RasGAP, SHP-2, and PLC␥) for growth factor-mediated cell survival in a single cell type, we created a series of chimeric receptors (ChiRs) in which the tyrosine residues required for the association of each of the above signaling enzymes were individually mutated to phenylalanine (Fig. 1A)
In the present study we have systematically investigated the relative importance of the signaling enzymes that are recruited to the activated PDGFR for protection against apoptosis in vascular smooth muscle cells (VSMC)
Summary
Peptide growth factors contribute to the pathogenesis of cardiovascular diseases by inducing a variety of cellular responses including anti-apoptotic effects. We conclude that growth factor-dependent cell survival in VSMC is mediated only by activation of the PI3K/Akt pathway, whereas all other receptor-associated signaling molecules do not play a significant role. SHP-2 was shown to be essential for insulin-like growth factor-I- or PDGF-mediated cell survival, as it suppresses caspase 3-dependent apoptosis in fibroblasts [14]. Another well characterized survival pathway is the Ras/Raf/extracellular-regulated kinase (ERK) cascade, which leads to the phosphorylation of BAD [15, 16]. This paper is available on line at http://www.jbc.org ates cell survival via protein kinase C-dependent phosphorylation of Bcl-2 proteins such as Bcl-2 and BAD (18 –20)
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