Distinct properties of atrial natriuretic factor receptor subpopulations in epithelial and fibroblast cell lines
We have characterized two atrial natriuretic factor (ANF) receptor subtypes, designated ANF-R1 and ANF-R2, in two established cell lines that express exclusively one receptor subtype. The ANF-R1 receptor is selectively expressed by the kidney epithelial cell line LLC-PK1. It is a 130-kDa protein tha...
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Veröffentlicht in: | Molecular pharmacology 1989-05, Vol.35 (5), p.584-592 |
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Zusammenfassung: | We have characterized two atrial natriuretic factor (ANF) receptor subtypes, designated ANF-R1 and ANF-R2, in two established
cell lines that express exclusively one receptor subtype. The ANF-R1 receptor is selectively expressed by the kidney epithelial
cell line LLC-PK1. It is a 130-kDa protein that has a much higher affinity for the biologically active forms of ANF than for
its metabolites. The binding of ANF to this subtype is potentiated by amiloride and by divalent cations. The activation of
the ANF-R1 receptor leads to an accumulation of cyclic GMP that is only partially inhibited by methylene blue. The ANF-R2
receptor, which is expressed selectively by the fibroblast cell line NIH-3T3, is a 130-kDa protein composed of two disulfide-linked
subunits of 64-kDa. Activation of this subtype by saturating concentrations of ANF does not appear to elicit cyclic GMP production.
However, supraphysiological concentrations of ANF induce a nonsaturable accumulation of cyclic GMP with an apparent ED50 in
the high micromolar range. In contrast to the ANF-R1 subtype, the stimulation of cyclic GMP production is completely abolished
by methylene blue. This subtype recognizes the active forms of ANF as well as its metabolites, and the binding is insensitive
to amiloride and is decreased by divalent cations. These two cell lines can serve as models for studying the differential
regulatory properties of ANF-R1 and ANF-R2 subtypes. In addition, we have also characterized the two ANF receptor subtypes
in rat kidney glomeruli, where they show the same structure and pharmacological characteristics as in the two model cell lines. |
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ISSN: | 0026-895X 1521-0111 |