par Pochet, Roland 
;Green, D A;Goka, T J;Clark, R B;Barber, R;Dumont, Jacques Emile ;Butcher, R W
Référence Journal of cyclic nucleotide research, 8, 2, page (83-89)
Publication Publié, 1982
;Green, D A;Goka, T J;Clark, R B;Barber, R;Dumont, Jacques Emile ;Butcher, R WRéférence Journal of cyclic nucleotide research, 8, 2, page (83-89)
Publication Publié, 1982
Article révisé par les pairs
| Résumé : | The beta-adrenergic receptors of the intact human lung diploid fibroblast line Wl-38 and an SV-40 transformed clone of Wl-38, Wl-38-VA-13-2RA (VA13), were estimated in experiments utilizing the beta-adrenergic ligand, 125l-hydroxybenzylpindolol (125IHYP). When specific 125IHYP binding was measured in cells grown to relatively low population densities (0.15x10(6)cells/35mm dish), both Wl-38 and VA13 cells had approximately 40,000 beta-adrenergic receptors per cell. Wl-38 cells, when cultured to a high population density (0.5x10(6) cells/35/mm dish) had clearly diminished numbers of beta-adrenergic receptors and greatly decreased cAMP responses to epinephrine stimulation. On the other hand, in VA13 cells, neither the receptor number nor the beta-adrenergic response was affected by cell population density. In Wl-38 cells, the diminished cAMP response to epinephrine paralleled the decrease in number of beta-adrenergic receptors. Prostaglandin E1 (PGE1) stimulation of cAMP levels was unaffected by cell population density in either Wl-38 or VA13 cells. Thus, increased cell population density, perhaps related to density dependent inhibition of growth, caused a specific diminution in 125IHYP binding concomitant with decreased cAMP responses to epinephrine. |
