1981
DOI: 10.1073/pnas.78.6.3664
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Specific receptors for platelet-derived growth factor on cells derived from connective tissue and glia.

Abstract: A cellular receptor for platelet-derived growth factor (PDGF) was demonstrated by incubation of "MI-labeled PDGF with human foreskin fibroblast cultures followed by liberation of cell-bound radioactivity with Triton X-100. The cellular binding of labeled PDGF in the presence of increasing amounts ofunlabeled PDGF showed saturation; Scatchard analysis ofbinding data indicated a single class of receptors having kd = 1 x 10-9 M. The number of PDGF binding sites was -3 X 105/cell. Labeled PDGF binding reached an a… Show more

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Cited by 352 publications
(169 citation statements)
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“…PDGF was labeled with 125 I (Heldin et al, 1981) and PDGF receptor competing activity in fractionated W9 CM was measured as inhibition of binding of [ 125 I]PDGF to con¯uent cultures of CRL 1477 ®broblasts as described previously (Peres et al, 1987;Bronzert et al, 1987). Puri®ed PDGF and EGF served as competition controls.…”
Section: Pdgf Receptor Binding Assaymentioning
confidence: 99%
“…PDGF was labeled with 125 I (Heldin et al, 1981) and PDGF receptor competing activity in fractionated W9 CM was measured as inhibition of binding of [ 125 I]PDGF to con¯uent cultures of CRL 1477 ®broblasts as described previously (Peres et al, 1987;Bronzert et al, 1987). Puri®ed PDGF and EGF served as competition controls.…”
Section: Pdgf Receptor Binding Assaymentioning
confidence: 99%
“…Platelet-derived growth factor (PDGF) is a potent mitogen for cells of mesenchymal origin, and has recently been shown to act also on other types of cells (Beits et al, 1991;Do et al, 1992;Heldin et al, 1981;Henriksen et al, 1993;Ra et al, 1988;Smits et al, 1991). It is implicated in normal embryonic development and wound healing, as well as in development of pathological conditions such as tumors, in¯ammatory diseases and atherosclerosis (Heldin and Westermark, 1994;Ross, 1993).…”
Section: Introductionmentioning
confidence: 99%
“…However, to our knowledge, this has not been observed for PDGF or other ligands that engage receptor tyrosine kinases. PDGF-BB binds to cell membranes or immobilized PDGF receptor extracellular domains with an observed K D ϳ 0.1-1 nM (11,39,(42)(43)(44), yet inhibition of cell responses at much higher concentrations has not been observed. NIH 3T3 cells were stimulated with 3 nM PDGF-BB for the times indicated.…”
Section: Figmentioning
confidence: 99%