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-adrenoceptors able to desensitize? Acute
and chronic effects of
-agonists in neonatal heart and liver
Department of Pharmacology and Cancer Biology, Duke University Medical Center, Durham, North Carolina 27710
During fetal and
neonatal development,
-adrenergic receptors (
-ARs) appear to be
resistant to desensitization by
-agonist drugs. To determine the
mechanisms underlying the regulatory differences between adults and
neonates, we administered isoproterenol, a mixed
1/
2-AR agonist, and terbutaline, a
2-selective agonist. Effects were examined in the
ensuing 4 h after a single injection, or after the last of four
daily injections. We prepared cell membranes from heart (predominantly
1-ARs) and liver (predominantly
2-ARs) and assessed signal transduction in the adenylyl cyclase (AC) pathway.
In the first few hours after a single administration of isoproterenol
to adult rats, cardiac
-ARs showed activation of G proteins
(elevated AC response to forskolin) and desensitization of
-AR-mediated responses; after the fourth injection, heterologous desensitization emerged, characterized by a loss of signaling mediated
either through
-ARs or glucagon receptors. Terbutaline evoked an
increase in the forskolin response but no desensitization of
receptor-mediated responses. When we gave the same treatments to
neonatal rats, we observed cardiac G protein activation, but there was
neither homologous nor heterologous desensitization of
-ARs or
glucagon receptors. In the adult liver, isoproterenol and terbutaline
both failed to evoke desensitization, regardless of whether the drugs
were given once or for 4 days. In neonates, however, acute or chronic
treatment elicited homologous desensitization of
-AR-mediated AC
signaling, while sensitizing the response to glucagon. These results
show that neonatal
-ARs are inherently capable of
desensitization in some, but not all, cell types; cellular responses
can be maintained through heterologous sensitization of signaling
proteins downstream from the receptor. Differences from adult patterns
of response are highly tissue selective and are likely to depend on
ontogenetic differences in subtypes of
-ARs and AC.
adenylyl cyclase; adenosine 3',5'-cyclic monophosphate; development; isoproterenol; terbutaline
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