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Literature DB >> 12743165

Potentiated L-type Ca2+ channels rectify.

Valérie Leuranguer¹, Robert T Dirksen, Kurt G Beam.

Abstract

Strong depolarization and dihydropyridine agonists potentiate inward currents through native L-type Ca2+ channels, but the effect on outward currents is less clear due to the small size of these currents. Here, we examined potentiation of wild-type alpha1C and two constructs bearing mutations in conserved glutamates in the pore regions of repeats II and IV (E2A/E4A-alpha1C) or repeat III (E3K-alpha1C). With 10 mM Ca2+ in the bath and 110 mM Cs+ in the pipette, these mutated channels, expressed in dysgenic myotubes, produced both inward and outward currents of substantial amplitude. For both the wild-type and mutated channels, we observed strong inward rectification of potentiation: strong depolarization had little effect on outward tail currents but caused the inward tail currents to be larger and to decay more slowly. Similarly, exposure to DHP agonist increased the amplitude of inward currents and decreased the amplitude of outward currents through both E2A/E4A-alpha1C and E3K-alpha1C. As in the absence of drug, strong depolarization in the presence of dihydropyridine agonist had little effect on outward tail currents but increased the amplitude and slowed the decay of inward tail currents. We tested whether cytoplasmic Mg2+ functions as the blocking particle responsible for the rectification of potentiated L-type Ca2+ channels. However, even after complete removal of cytoplasmic Mg2+, (-)BayK 8644 still potentiated inward current and partially blocked outward current via E2A/E4A-alpha1C. Although zero Mg2+ did not reveal potentiation of outward current by DHP agonist, it did have two striking effects, (a) a strong suppression of decay of both inward and outward currents via E2A/E4A-alpha1C and (b) a nearly complete elimination of depolarization-induced potentiation of inward tail currents. These results can be explained by postulating that potentiation exposes a binding site in the pore to which an intracellular blocking particle can bind and produce inward rectification of the potentiated channels.

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Year: 2003 PMID： 12743165 PMCID： PMC2217356 DOI： 10.1085/jgp.200308833

Source DB: PubMed Journal: J Gen Physiol ISSN： 0022-1295 Impact factor: 4.086

27 in total

1. Temperature-sensitive intracellular Mg2+ block of L-type Ca2+ channels in cardiac myocytes.

Authors: Kaoru Yamaoka; Tsunetsugu Yuki; Kayoko Kawase; Makoto Munemori; Issei Seyama
Journal: Am J Physiol Heart Circ Physiol Date: 2002-03 Impact factor: 4.733

2. Multiple structural elements contribute to voltage-dependent facilitation of neuronal alpha 1C (CaV1.2) L-type calcium channels.

Authors: C Altier; R L Spaetgens; J Nargeot; E Bourinet; G W Zamponi
Journal: Neuropharmacology Date: 2001-06 Impact factor: 5.250

Review 3. Permeation and selectivity in calcium channels.

Authors: William A Sather; Edwin W McCleskey
Journal: Annu Rev Physiol Date: 2002-11-21 Impact factor: 19.318

4. Modulation of the conductance of unitary cardiac L-type Ca(2+) channels by conditioning voltage and divalent ions.

Authors: Ira R Josephson; Antonio Guia; Edward G Lakatta; Michael D Stern
Journal: Biophys J Date: 2002-11 Impact factor: 4.033

5. Modulation of the gating of unitary cardiac L-type Ca(2+) channels by conditioning voltage and divalent ions.

Authors: Ira R Josephson; Antonio Guia; Edward G Lakatta; Michael D Stern
Journal: Biophys J Date: 2002-11 Impact factor: 4.033

6. Different modes of Ca channel gating behaviour favoured by dihydropyridine Ca agonists and antagonists.

Authors: P Hess; J B Lansman; R W Tsien
Journal: Nature Date: 1984 Oct 11-17 Impact factor: 49.962

7. Improved patch-clamp techniques for high-resolution current recording from cells and cell-free membrane patches.

Authors: O P Hamill; A Marty; E Neher; B Sakmann; F J Sigworth
Journal: Pflugers Arch Date: 1981-08 Impact factor: 3.657

8. Potentiation of the cardiac L-type Ca(2+) channel (alpha(1C)) by dihydropyridine agonist and strong depolarization occur via distinct mechanisms.

Authors: C M Wilkens; M Grabner; K G Beam
Journal: J Gen Physiol Date: 2001-11 Impact factor: 4.086

9. Role of calcium permeation in dihydropyridine receptor function. Insights into channel gating and excitation-contraction coupling.

Authors: R T Dirksen; K G Beam
Journal: J Gen Physiol Date: 1999-09 Impact factor: 4.086

10. Mechanism of calcium channel blockade by verapamil, D600, diltiazem and nitrendipine in single dialysed heart cells.

Authors: K S Lee; R W Tsien
Journal: Nature Date: 1983-04-28 Impact factor: 49.962

8 in total

1. FPL 64176 modification of Ca(V)1.2 L-type calcium channels: dissociation of effects on ionic current and gating current.

Authors: Stefan I McDonough; Yasuo Mori; Bruce P Bean
Journal: Biophys J Date: 2004-10-22 Impact factor: 4.033

Potentiated L-type Ca2+ channels rectify.

1. Temperature-sensitive intracellular Mg2+ block of L-type Ca2+ channels in cardiac myocytes.

2. Multiple structural elements contribute to voltage-dependent facilitation of neuronal alpha 1C (CaV1.2) L-type calcium channels.

Review 3. Permeation and selectivity in calcium channels.

4. Modulation of the conductance of unitary cardiac L-type Ca(2+) channels by conditioning voltage and divalent ions.

5. Modulation of the gating of unitary cardiac L-type Ca(2+) channels by conditioning voltage and divalent ions.

6. Different modes of Ca channel gating behaviour favoured by dihydropyridine Ca agonists and antagonists.

7. Improved patch-clamp techniques for high-resolution current recording from cells and cell-free membrane patches.

8. Potentiation of the cardiac L-type Ca(2+) channel (alpha(1C)) by dihydropyridine agonist and strong depolarization occur via distinct mechanisms.

9. Role of calcium permeation in dihydropyridine receptor function. Insights into channel gating and excitation-contraction coupling.

10. Mechanism of calcium channel blockade by verapamil, D600, diltiazem and nitrendipine in single dialysed heart cells.

1. FPL 64176 modification of Ca(V)1.2 L-type calcium channels: dissociation of effects on ionic current and gating current.

2. Properties of Na+ currents conducted by a skeletal muscle L-type Ca2+ channel pore mutant (SkEIIIK).

3. A skeletal muscle L-type Ca²⁺ channel with a mutation in the selectivity filter (Ca_V1.1 E1014K) conducts K<sup/>.

4. Role of extracellular Ca2+ in gating of CaV1.2 channels.

5. The cardiac alpha(1C) subunit can support excitation-triggered Ca2+ entry in dysgenic and dyspedic myotubes.

Review 6. Ca(V)1.1: The atypical prototypical voltage-gated Ca²⁺ channel.

7. The skeletal L-type Ca(2+) current is a major contributor to excitation-coupled Ca(2+) entry.

8. Nitric oxide mediates activity-dependent plasticity of retinal bipolar cell output via S-nitrosylation.