Gene/Protein Disease Symptom Drug Enzyme Compound
Pivot Concepts:   Target Concepts:
Query: EC:4.6.1.1 (adenylate cyclase)
19,190 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

The indirect immunofluorescence technique was used to study the cellular localization of DARPP-32, a dopamine- and cyclic AMP-regulated phosphoprotein, in brown adipose tissue of newborn piglets. Clusters of strongly DARPP-32-immunoreactive cells were found in brown adipose tissue from the interscapular area and around lymph nodes close to the kidneys, adrenal glands, descending aorta, and great veins in the neck. The DARPP-32-immunoreactive cells contained multilocular lipid droplets, had round, centrally located nuclei, and were polygonal in shape, thus possessing characteristics and location sites typical for brown fat cells. The results indicate that brown adipose tissue from the newborn pig contains DARPP-32, an intracellular third messenger for dopamine. Together with recent functional data, these results strongly suggest that dopaminergic D1 mechanisms--i.e., activation of adenylate cyclase and formation of cyclic AMP--may be involved in cold-induced, nonshivering, and/or diet-induced thermogenesis.
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PMID:Immunohistochemical evidence for the existence of a dopamine- and cyclic AMP-regulated phosphoprotein (DARPP-32) in brown adipose tissue of pigs. 284 73

The inherited disorders of rd mice and affected Irish setter dogs are characterized by the accumulation of cyclic GMP (cGMP). Since the cGMP level in normal retinal rods is regulated by a light-activated enzyme cascade involving rhodopsin, transducin, and phosphodiesterase, an abnormality associated with any of these three proteins would cause cGMP accumulation. In order to determine the relationship between different forms of retinal degeneration and the transducin content in the affected retinas, affinity-purified antibodies directed against the individual subunits of bovine transducin were prepared. These antibodies, which recognized transducin in many vertebrate species, were used to compare the retinal content of this protein at various stages of inherited photoreceptor degeneration. In each of the disorders studied (rd and rds mice, RCS rat, and affected Irish setter dog), retinas at early stages of degeneration displayed two characteristics similar to those of normal control retinas. First, all three subunits of transducin were detected and found to have normal electrophoretic mobility, suggesting that these disorders are unlikely to be due to changes in the composition of transducin subunits. Second, the amount of cross-reactive T beta always exceeded those of T alpha and T gamma. This disproportionately higher amount of T beta-like protein became more pronounced as the visual cells degenerated. In retinas which had undergone complete photoreceptor degeneration, cross-reactive T alpha and T gamma were undetectable. In contrast, anti-T beta gamma antibodies detected an amount of T beta-like polypeptide corresponding to 10-25% of the control. Since our anti-T beta gamma antibodies recognize the beta subunit of the GTP-binding N proteins of the adenylate cyclase system, this finding suggests that this residual T beta-like protein, which is not part of transducin, may be associated with other GTP-binding regulatory proteins.
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PMID:Immunological determination of transducin content in retinas exhibiting inherited degeneration. 347 Jan 93

Recent work has demonstrated that stimulation of cAMP production via A2-adenosine receptors is reduced in cultured retinal pigment epithelial cells from the RCS rat. Cultured rat RPE cells are also shown to possess beta 2-adrenergic receptors positively coupled to cAMP production. Isoproterenol and salbutamol both stimulate cAMP levels with half maximal (EC50) values of 0.5 and 0.2 microM, respectively. Isoproterenol action is attenuated most effectively by the beta 2-antagonist, ICI 118551, while the beta 1-antagonist, CGP 20712A, is only partially effective. Isoproterenol-stimulated cAMP production is markedly reduced in the RCS rat RPE when compared to control cultures. In passaged RCS rat RPE cells cAMP stimulation by 10 microM isoproterenol was 6.4% of that by control cultures and in primary cultures it was around 75% of controls. The observed EC50 values were 0.4 and 1.3 microM for passaged control and RCS rat RPE cells, respectively. Melatonin negatively influences cAMP production in the RPE via Gi-proteins. Melatonin attenuated the action of forskolin by 51.1% in control rat RPE but only by 18.6% in the RCS rat RPE. The dose-response curve for melatonin shows an approximate 1000-fold shift in potency in the RCS rat. bFGF also has an inhibitory effect on rat RPE cells. bFGF (50ng/ml) attenuated forskolin-stimulated cAMP levels by 61.9% in control rat RPE but had not effect on the action of forskolin in RCS rat RPE. Serotonin (100 microM) potentiates the forskolin-induced stimulation of cAMP by 140.1%. However, unlike isoproterenol, melatonin and bFGF, the action of serotonin on adenylate cyclase appears normal in the RCS rat RPE. We conclude that the defect in the RCS rat RPE is likely to be due to impaired coupling of the components of the adenylate cyclase system and that this is most probably an abnormal interaction of adenylate cyclase with G-protein alpha-subunits.
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PMID:Agonist-induced effects on cyclic AMP metabolism are affected in pigment epithelial cells of the Royal College of Surgeons rat. 852 Apr 64

The relationship between tyrosine hydroxylase (TH), dopamine (DA) and cyclic AMP-regulated phosphoprotein-32 (DARPP-32) immunoreactive (IR) neuronal structures and D1 receptor antagonist binding sites has been analysed in various brain regions in the male rat, using immunocytochemistry and receptor autoradiography with the iodinated analogue of SCH 23390 ([(125)I]SCH 23982) as radioligand. Two-colour immunocytochemistry was used to establish in detail the relationship between DARPP-32 and the TH IR neuronal structures in mes-, di- and telencephalon. The analysis reveals complex matches and mismatches between central DARPP-32 immunoreactive neurones, DA neurones and D1 DA receptors. The results inter alia indicate a probable release of DA from the dendritic plexus of the zona reticulata of the substantia nigra to reach D1 DA receptors via extracellular pathways. DA released from the few DA terminals present in the entopeduncular nucleus and from adjacent dopamine axons may also reach D1 DA receptors in this nucleus by extracellular diffusion. A similar situation may also exist in the globus pallidus. Thus, DA may in some regions be released as a paracrine signal to reach distant D1 DA receptors. This type of chemical transmission has been called volume transmission and D1 receptors may thus participate in volume transmission. The mismatch obtained in, for example, the amygdaloid cortex and hypothalamus between D1 receptor antagonist binding sites and DARPP-32 IR nerve cell profiles, is compatible with the possibility that some D1 receptors linked to adenylate cyclase may not involve DARPP-32 as a substrate protein for the cyclic AMP-dependent protein kinase. In addition the possibility should be considered that D1 receptors may not always be linked to adenylate cyclase. Finally, the mismatch in the median eminence between [(125)I]SCH 23982 binding sites and DARPP-32 IR profiles may indicate the existence of D1 receptors which are masked under basal conditions in the male rat.
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PMID:Studies on the relationship of tyrosine hydroxylase, dopamine and cyclic amp-regulated phosphoprotein-32 immunoreactive neuronal structures and d1 receptor antagonist binding sites in various brain regions of the male rat-mismatches indicate a role of d1 receptors in volume transmission. 2050 Dec 87