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KMID : 0617220010120010063
Duksung Bulletin Phamaceutical Sciences
2001 Volume.12 No. 1 p.63 ~ p.66
Both Platelet-Derived Growth Factor Receptor (PDGFR)-¥á and PDGFR-¥â Promote Murine Fibroblast Cell Migration
Yu, Jiuhong
Moon, Aree/Kim Choi, Reh Hyeong
Abstract
Cell motility plays a critical role for many physiological and pathological processes including wound healing, fibrosis, angiogenesis, and tumor metastasis. Platelet-derived growth factor (PDGF) is among the most potent stimuli for mesenchymal cell migration. The PDGF B-chain homodimer PDGF BB activates both ¥á- and ¥â-receptor subunits (¥á-PDGFR and ¥â-PDGFR), and promotes cell migration in many cell types including fibroblasts and smooth muscle cells. PDGF-A chain homodimer PDGF AA activates ¥á-PDGFR only, and its role for cell migration is still debatable. PDGF BB, but not PDGF AA, induces smooth muscle cell migration. Interestingly, ¥á-PDGFR was shown to antagonize ¥â-PDGFR-induced smooth muscle cell migration. In the present study, we investigated the role of ¥á-PDGFR and ¥â-PDGFR in PDGF-mediated cell migration of murine fibroblasts (NIH3T3). Unlike smooth muscle cells, both PDGF AA and PDGF BB promoted NIH 3T3 cell migration. The effect of PDGF BB activation of ¥â-PDGFR alone for cell migration was examined using previously established NIH 3T3 clones in which ¥á-PDGFR signaling is inhibited by a dominant-negative ¥á-PDGFR, or an antisense construct of ¥á-PDGFR. PDGF BB activation of ¥â-PDGFR alone was sufficient to induce cell migration, but the efficiency was significantly lower compared to PDGF actlvation of both receptors. These results showed that both ¥á- and ¥â-PDG
FRs promote fibroblast cell migration and their effects are additive. Taken together, we propose that cell-type specific ¥á-PDGFR signaling is critical for regulation of mesenchymal cell migration in response to PDGF isoform, whereas ¥â-PDGFR mainly promotes cell migration.
¨Ï 2001 Academic Press
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