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Journal of Lipid Research, Vol 26, 127-134, Copyright © 1985 by Lipid Research, Inc.
B Richelsen and H Beck-Nielsen
The effect of treatment of isolated rat adipocytes with prostaglandin E2
(PGE2) on subsequent [3H]PGE2 binding was studied. In addition, the
antilipolytic effects of was studied. In addition, the antilipolytic
effects of PGE2, adenosine, and insulin were studied in control and
PGE2-treated adipocytes. Treatment of adipocytes with PGE2 (1 microM)
decreased the binding of [3H]PGE2 by 61% (from 11.0 to 4.6 fmol/10(6)
cells, P less than 0.005). Scatchard analysis of the binding data
demonstrated that the decrease of PGE2 receptor binding was due to a
decrease in the apparent number of PGE2 receptors while the apparent
receptor affinity was unaltered. Reduction of the PGE2 receptor binding was
specifically regulated inasmuch as structurally related compounds such as
PGF2 alpha and arachidonic acid had only minor effects on subsequent
[3H]PGE2 receptor binding. Reduction of the available receptor number was
associated with a significant decrease in the antilipolytic effect of PGE2
on the isoproterenol-stimulated lipolysis (P less than 0.05). The maximal
antilipolytic effect of PGE2 was decreased by 45%. Desensitization of the
biological effect of PGE2 (antilipolysis) was only partially specifically
regulated inasmuch as the antilipolytic compound phenylisopropyladenosine
also had reduced antilipolytic effect in PGE2-treated cells. However, the
antilipolytic effect of insulin was similar in control and PGE2-treated
cells. It was found that the PGE2-induced decrease of [3H]PGE2 receptor
binding may be due to a very tight coupling between the PGE2 molecule and
its specific receptor. This tight coupling may then represent an occupancy
of the receptor rather than a true loss of receptors.(ABSTRACT TRUNCATED AT
250 WORDS)
ARTICLES
Decrease of prostaglandin E2 receptor binding is accompanied by reduced antilipolytic effects of prostaglandin E2 in isolated rat adipocytes
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