Publication | Open Access
Stimulation of the chemotactic migration of human fibroblasts by transforming growth factor beta.
780
Citations
13
References
1987
Year
Epidermal Growth FactorChemotactic MigrationImmunologyCell ProliferationCell GrowthCellular PhysiologyTumor BiologyGrowth Factor BetaFibroblast Growth FactorMatrix BiologyFibrosisCell BiologyTumor MicroenvironmentDevelopmental BiologyCell MigrationWound HealingPure Tgf-beta BlockHuman FibroblastsMedicineExtracellular Matrix
Transforming growth factor beta (TGF-beta) is a potent chemoattractant in vitro for human dermal fibroblasts. Intact disulfide and perhaps the dimeric structure of TGF-beta is essential for its ability to stimulate chemotactic migration of fibroblasts, since reduction with 2-ME results in a marked loss of its potency as a chemoattractant. Although epidermal growth factor (EGF) appears to be capable of modulating some effects of TGF-beta, it does not alter the chemotactic response of fibroblasts to TGF-beta. Specific polyvalent rabbit antibodies to homogeneously pure TGF-beta block its chemotactic activity but has no effect on the other chemoattractants tested (platelet-derived growth factor, fibronectin, and denatured type I collagen). Since TGF-beta is secreted by a variety of neoplastic and normal cells including platelets, monocytes/macrophages, and lymphocytes, it may play a critical role in vivo in embryogenesis, host response to tumors, and the repair response that follows damage to tissues by immune and nonimmune reactions.
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