Literature DB >> 1359124

Dopamine D2 receptor stimulation differentially affects voltage-activated calcium channels in rat pituitary melanotropic cells.

J A Keja1, J C Stoof, K S Kits.   

Abstract

1. Whole-cell voltage clamp recordings were made from 141 rat pituitary melanotropic cells in short-term, serum-free, primary culture. The effects of the dopamine D2 receptor agonist, LY 171555, on sodium, potassium and barium currents were investigated. 2. Application of 1 microM-LY 171555 did not affect the inward sodium and outward potassium currents. 3. Application of LY 171555 reversibly inhibited barium currents, with the strongest inhibition on the early inward current. The effect was dose dependent (IC50 = 4 x 10(-8) M), maximal inhibition of the total current was 30% and the LY 171555-induced block (1 microM) was reversibly antagonized by (+/-)sulpiride (4 microM). 4. Using barium-selective saline solutions, different types of barium current (T, N, and two L components) were identified on the basis of their voltage-dependent kinetics. Their relative amplitudes differed between cells. 5. The T-type current activated at potentials positive to -60 mV, reaching peak amplitude between -20 and -10 mV. At -30 mV, this current was inhibited up to 30% by 1 microM-LY 171555. The time constants of activation (10-3 ms) and inactivation (50-20 ms) as well as the voltage dependence of inactivation (potential of half-maximal inactivation (H), -61 mV; slope factor (S), 4.9 mV) were not affected by LY 171555 application. 6. A rapidly inactivating (time constants 100-50 ms), high threshold current component was identified as an N-type current. This current activated at command potentials positive to -30 mV and reached a maximal amplitude at +10 mV. The steady-state inactivation was described by a single Boltzmann equation with H = -65 mV and S = 11.7 mV. Application of 1 microM-LY 171555 completely suppressed this current. 7. The slowly inactivating (time constants > 1500 ms), high-threshold, L-type current displayed the same voltage dependence of activation as the N current. The voltage dependence of inactivation was modelled by the sum of two Boltzmann equations (L1: H1 = -45 mV, S1 = 13.0 mV; L2:H2 = -11 mV, S2 = 6.0 mV), indicating the existence of two L channel populations. Neither time course, nor voltage dependence of inactivation were influenced by LY 171555. However, LY 171555 induced a slow-down in the time course of activation, which necessitated the use of two time constants to model the activation kinetics. One of these (approximately 2 ms) was also observed under control conditions.(ABSTRACT TRUNCATED AT 400 WORDS)

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Year:  1992        PMID: 1359124      PMCID: PMC1176129          DOI: 10.1113/jphysiol.1992.sp019134

Source DB:  PubMed          Journal:  J Physiol        ISSN: 0022-3751            Impact factor:   5.182


  40 in total

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5.  Dihydropyridine inhibition of neuronal calcium current and substance P release.

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6.  Kinetics and selectivity of a low-voltage-activated calcium current in chick and rat sensory neurones.

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7.  Dopamine inhibits two characterized voltage-dependent calcium currents in identified rat lactotroph cells.

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Journal:  Endocrinology       Date:  1990-09       Impact factor: 4.736

8.  Effects of dopamine on voltage-dependent potassium currents in identified rat lactotroph cells.

Authors:  P M Lledo; P Legendre; J Zhang; J M Israel; J D Vincent
Journal:  Neuroendocrinology       Date:  1990-12       Impact factor: 4.914

9.  Action potentials in gland cells of rat pituitary pars intermedia: inhibition by dopamine, an inhibitor of MSH secretion.

Authors:  W W Douglas; P S Taraskevich
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10.  Voltage-activated calcium channels that must be phosphorylated to respond to membrane depolarization.

Authors:  D Armstrong; R Eckert
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  18 in total

1.  All classes of calcium channel couple with equal efficiency to exocytosis in rat melanotropes, inducing linear stimulus-secretion coupling.

Authors:  H D Mansvelder; K S Kits
Journal:  J Physiol       Date:  2000-07-15       Impact factor: 5.182

2.  Pattern changes of pituitary peptides in rat after salt-loading as detected by means of direct, semiquantitative mass spectrometric profiling.

Authors:  C R Jiménez; K W Li; K Dreisewerd; H D Mansvelder; A B Brussaard; B B Reinhold; R C Van der Schors; M Karas; F Hillenkamp; J P Burbach; C E Costello; W P Geraerts
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4.  Multiple modulatory effects of dopamine on calcium channel kinetics in adult rat sensory neurons.

Authors:  A Formenti; M Martina; A Plebani; M Mancia
Journal:  J Physiol       Date:  1998-06-01       Impact factor: 5.182

5.  Ionic currents influencing spontaneous firing and pacemaker frequency in dopamine neurons of the ventrolateral periaqueductal gray and dorsal raphe nucleus (vlPAG/DRN): A voltage-clamp and computational modelling study.

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6.  Dopamine (D2) receptor regulation of intracellular calcium and membrane capacitance changes in rat melanotrophs.

Authors:  A K Lee
Journal:  J Physiol       Date:  1996-09-15       Impact factor: 5.182

7.  Depression of high-threshold calcium currents by activation of human D2 (short) dopamine receptors expressed in differentiated NG108-15 cells.

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8.  Ca2+ channel Ca(2+)-dependent inactivation in a mammalian central neuron involves the cytoskeleton.

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9.  Mechanism of dopamine mediated inhibition of neuropeptide Y release from pheochromocytoma cells (PC12 cells).

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10.  Dopamine D2 receptor stimulation alters G-protein expression in rat pituitary intermediate lobe melanotropes.

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