Wang D, Huang H J, Kazlauskas A, Cavenee W K
Ludwig Institute for Cancer Research, University of California-San Diego, 92093-0660, USA.
Cancer Res. 1999 Apr 1;59(7):1464-72.
Increased numbers of platelet-derived growth factor beta receptors betaPPDGFRs) on neovascular endothelial cells is a common occurrence in several pathological conditions including wound healing, inflammation, and glioma tumorigenesis. Here we sought to test the biological significance of this by determining whether expression of wild-type betaPDGFR by normal aortic endothelial cells affected the expression of the vascular endothelial growth factor (VEGF), a critical angiogenesis regulator and mitogen for such cells. The results showed that PDGF could increase transcription and secretion of VEGF by betaPDGFR-expressing endothelial cells. Moreover, we further demonstrated a requirement for the activation of phosphatidylinositol 3-kinase (PI3K) in this response by using chemical inhibitors of PI3K, mutant PDGFR, and dominant-negative PI3K. These studies suggest a novel mechanism by which PDGF induces VEGF expression in endothelial cells, define VEGF as a downstream target for PI3K, and invoke a role for PI3K in angiogenesis.
新生血管内皮细胞上血小板衍生生长因子β受体(βPPDGFRs)数量增加在包括伤口愈合、炎症和胶质瘤肿瘤发生在内的多种病理状况中很常见。在此,我们试图通过确定正常主动脉内皮细胞中野生型βPDGFR的表达是否影响血管内皮生长因子(VEGF)的表达来测试其生物学意义,VEGF是此类细胞的关键血管生成调节因子和有丝分裂原。结果表明,血小板衍生生长因子(PDGF)可增加表达βPDGFR的内皮细胞中VEGF的转录和分泌。此外,我们通过使用磷脂酰肌醇3激酶(PI3K)的化学抑制剂、突变型PDGFR和显性负性PI3K进一步证明了PI3K激活在此反应中的必要性。这些研究提示了一种新机制,即PDGF在内皮细胞中诱导VEGF表达,将VEGF定义为PI3K的下游靶点,并揭示了PI3K在血管生成中的作用。
