GABA A and GABA B sites in bovine adrenal medulla membranes

1 The function of y-aminobutyric acidB (GABAB) receptors in modulation of catecholamine secretion by chromaffin cells and the possible mechanism involved in this action have been examined. 2 The GABAB agonists (-)-baclofen and 3-aminopropylphosphinic acid (3-APPA) were found to induce a dose-dependent increase of basal catecholamine secretion. The ECms were 151 ± 35 1LM and 225 ± 58 tIM for baclofen and 3-APPA, respectively. This stimulatory effect was specific since it could be blocked by 0.5 mM of the specific GABAB antagonist CGP-35348. 3 In contrast, preincubation of chromaffin cells with the GABAB agonists was found to inhibit, in a dose-dependent manner, the catecholamine secretion evoked by 10 jaM nicotine and 200 JiM muscimol.4 The effects of GABAB agonists on both basal and evoked catecholamine secretion were found to be accompanied by parallel changes in intracellular calcium concentration ([Ca2+]J). GABAB agonists produced a dose-dependent increase in [Ca2+]i which was partially blocked by CGP 35348, but they produced a strong inhibition of the [Ca2+]i increase induced by nicotine and muscimol.5 The GABAB agonists also produced a dose-dependent increase in intracellular cyclic AMP levels, there being a direct correlation between both increase in catecholamine secretion and in intracellular cyclic AMP levels. 6 The pretreatment of chromaffin cells with pertussis toxin doubled the catecholamine secretion and increased by four times the intracellular cyclic AMP levels evoked by GABAB agonists. 7 The possible involvement of adenylate cyclase in the mechanism of GABAB receptor modulation of catecholamine secretion is discussed.

Section: Resultsmentioning

confidence: 74%

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

GABA_B receptors modulate catecholamine secretion in chromaffin cells by a mechanism involving cyclic AMP formation

Oset-Gasque

Parramón

González

1993

“…Many substances, including opioid peptides, substance P. y-aminobutyric acid and peptides derived from cromogranin A, appear to modulate acetylcholine-mediated catecholamine (CA) release from these cells (Mizobe et al, 1979;Kumakura et al, 1980;Castro et al, 1988;Simon et al, 1988).…”

Section: Introductionmentioning

confidence: 99%

Effect of diadenosine polyphosphates on catecholamine secretion from isolated chromaffin cells

Castro

Torres

Miras‐Portugal

et al. 1990

Self Cite

1 The action of several diadenosine polyphosphates (AP3A, AP4A and AP5A) on basal, and on nicotineand high K+-evoked, catecholamine (CA) release has been investigated. Each of the three diadenosine polyphosphates weakly but significantly increased basal CA secretion. This enhancement represented about 10% of the response evoked by 2 J1M nicotine. 2 The evoked secretory response to diadenosine polyphosphates had an absolute requirement for extracellular Ca2".3 In contrast, these compounds had an inhibitory action on nicotine-evoked release. This response was concentration-dependent, EC50 values being 3.2 + 0.4OAM, 4.0 + 1.6./M and 19.3 + 4.0/AM for AP A AP4A, and AP5A, respectively. The lower the concentration of nicotine used to evoke secretion, the higher the inhibitory power of these compounds.4 The CA secretion evoked by K+-rich solutions was further enhanced by AP3A and APA, whereas AP4A inhibited it. The possible physiological role of these dual actions is discussed.

“…This is the case with the adrenal medulla, where GABA regulates catecholamine (CA) secretion (Castro et al, 1989). This function is mainly mediated by binding to GABAA receptors (Kataoka et al, 1984;Castro et al, 1988), through a mechanism dependent on the membrane potential (Gonzalez et al, 1992).…”

mentioning

confidence: 99%

Pharmacological modulation of adrenal medullary GABA_A receptor: consistent with its subunit composition

Parramón¹,

González²

1995

5 Pregnanolone and related neuroactive steroids enhanced muscimol-evoked catecholamine secretion by up to 87%, in a dose-dependent fashion. In contrast pregnenolone weakly inhibited muscimol-evoked catecholamine secretion. 6 Zn2+ did not affect GABAA receptor-induced catecholamine secretion. 7 These pharmacological results are absolutely concordant with the theoretical properties given by the GABAA receptor subunit composition of bovine adrenal medulla -al, a4, f1-3, Y2-previously characterized by Western blot analysis.