Ionic currents and endothelin signaling in smooth muscle cells from rat renal resistance arteries

Gordienko, Dmitri; Clausen, Chris; Goligorsky, Michael S.

doi:10.1152/ajprenal.1994.266.2.f325

Cited by 76 publications

(106 citation statements)

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“…Collectively, our findings suggest that in afferent arterioles, phospholipase C-dependent calcium release from endoplasmic reticulum (35) triggers subsequent cellular responses that activate voltage-dependent calcium channels. Electrophysiological studies indicate the presence of calcium-activated chloride channels on preglomerular vessels, including afferent arterioles (10,36). Furthermore, previous data demonstrated that chloride channel blockade inhibited AngII-induced afferent arteriolar constriction (11,37).…”

Section: Discussionmentioning

confidence: 99%

Cellular mechanisms mediating rat renal microvascular constriction by angiotensin II.

Takenaka¹,

Suzuki²,

Fujiwara³

et al. 1997

J. Clin. Invest.

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To assess cellular mechanisms mediating afferent (AA) and efferent arteriolar (EA) constriction by angiotensin II (AngII), experiments were performed using isolated perfused hydronephrotic kidneys. In the first series of studies, AngII (0.3 nM) constricted AAs and EAs by 29 Ϯ 3 ( n ϭ 8, P Ͻ 0.01) and 27 Ϯ 3% ( n ϭ 8, P Ͻ 0.01), respectively. Subsequent addition of nifedipine restored AA but not EA diameter. Manganese (8 mM) reversed EA constriction by 65 Ϯ 9% ( P Ͻ 0.01). In the second group, the addition of N -ethylmaleimide (10 M), a Gi/Go protein antagonist, abolished AngIIinduced EA ( n ϭ 6) but not AA constriction ( n ϭ 6). In the third series of experiments, treatment with 2-nitro-4-carboxyphenyl-N , N -diphenyl-carbamate (200 M), a phospholipase C inhibitor, blocked both AA and EA constriction by AngII ( n ϭ 6 for each). In the fourth group, thapsigargin (1 M) prevented AngII-induced AA constriction ( n ϭ 8) and attenuated EA constriction (8 Ϯ 2% decrease in EA diameter at 0.3 nM AngII, n ϭ 8, P Ͻ 0.05). Subsequent addition of manganese (8 mM) reversed EA constriction. Our data provide evidence that in AAs, AngII stimulates phospholipase C with subsequent calcium mobilization that is required to activate voltage-dependent calcium channels. Our results suggest that AngII constricts EAs by activating phospholipase C via the Gi protein family, thereby eliciting both calcium mobilization and calcium entry. ( J.

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Section: Discussionmentioning

confidence: 99%

Cellular mechanisms mediating rat renal microvascular constriction by angiotensin II.

Takenaka¹,

Suzuki²,

Fujiwara³

et al. 1997

J. Clin. Invest.

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“…Second messengers responsible for the ET-1-mediated vascular response include phospholipase C activation and subsequent calcium mobilization from intracellular stores, as well as phospholipase A 2 stimulation, resulting in production of arachidonic acid metabolites. 1,14,21,25 In freshly isolated smooth muscle cells from large-caliber renal vessels, Gordienko et al 25 demonstrated that ET-1-induced mobilization of intracellular calcium was accompanied by membrane depolarization. ET-1 also stimulated Ca 2ϩ -activated K ϩ channels in renal vascular smooth muscle cells.…”

Section: Discussionmentioning

confidence: 99%

Cytochrome P450 and Cyclooxygenase Metabolites Contribute to the Endothelin-1 Afferent Arteriolar Vasoconstrictor and Calcium Responses

et al. 2000

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Abstract-Arachidonic acid metabolites contribute to the endothelin-1 (ET-1)-induced decrease in renal blood flow, but the vascular sites of action are unknown. Experiments performed in vitro used the rat juxtamedullary nephron preparation combined with videomicroscopy. The response of afferent arterioles to ET-1 was determined before and after cytochrome P450 (CYP450) or cyclooxygenase (COX) inhibition. Afferent arteriolar diameter averaged 20Ϯ1 m (nϭ17) at a renal perfusion pressure of 100 mm Hg. Superfusion with 0.001 to 10 nmol/L ET-1 caused a graded decrease in diameter of the afferent arteriole. Vessel diameter decreased by 30Ϯ2% and 41Ϯ2% in response to 1 and 10 nmol/L ET-1, respectively. The afferent arteriolar response to ET-1 was significantly attenuated during administration of the CYP450 hydroxylase inhibitor , such that afferent arteriolar diameter decreased by 19Ϯ3% and 22Ϯ3% in response to 1 and 10 nmol/L ET-1, respectively. COX inhibition also greatly attenuated the vasoconstriction elicited by ET-1, whereas the CYP450 epoxygenase inhibitor N-methylsulfonyl-6-(2-proparglyoxyphenyl) hexanamide enhanced the ET-1-mediated vascular response. Additional studies were performed using freshly isolated smooth muscle cells prepared from preglomerular microvessels. Renal microvascular smooth muscle cells were loaded with the calcium-sensitive dye fura 2 and studied by use of single-cell fluorescence microscopy. Basal renal microvascular smooth muscle cell [Ca 2ϩ ] i averaged 95Ϯ3 nmol/L (nϭ42). ET-1 (10 nmol/L) increased microvascular smooth muscle cell [Ca 2ϩ ] i to a peak value of 731Ϯ75 nmol/L before stabilizing at 136Ϯ8 nmol/L. Administration of DDMS or the COX inhibitor indomethacin significantly attenuated the renal microvascular smooth muscle cell calcium response to ET-1. These data demonstrate that CYP450 hydroxylase and COX arachidonic acid metabolites contribute importantly to the afferent arteriolar diameter and renal microvascular smooth muscle cell calcium responses elicited by ET-1. Key Words: endothelin-1 Ⅲ renal hemodynamics Ⅲ cytochrome P450 Ⅲ cyclooxygenase Ⅲ cytosolic calcium Ⅲ microcirculation E ndothelin-1 (ET-1) is a 21-amino-acid peptide synthesized by endothelial cells that acts as a potent vasoconstrictor on vascular smooth muscle cells. [1][2][3] Elevations in circulating and tissue ET-1 levels have been implicated in a number of pathological states, including acute renal failure, cyclosporine nephrotoxicity, and hypertension. 4 -6 The ET-1 effects on the renal circulation are consistent with the view that the peptide plays a crucial role in maintaining fluid and electrolyte homeostasis. Intrarenal infusion of ET-1 decreases renal blood flow and glomerular filtration rate while increasing sodium excretion. 3,7,8 Previous studies have demonstrated that ET-1 constricts the afferent arteriole 9 -13 ; however, the preglomerular vascular smooth muscle cellular signaling mechanisms responsible are not well understood. ET-1 activates G proteins that in turn stimulate phospholipase C...

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“…In guinea pig smooth muscle myocytes, endothelin stimulated the activity of a 12-pS channel, that may or may not be carried through T-type channels (181). Endothelin has been reported to have no effect on T-type currents recorded from smooth muscle cells from rat renal resistance arteries (143).…”

Section: B Hormonal Stimulationmentioning

confidence: 97%

“…T-type currents have only been recorded from smooth muscle cells (SMC) isolated from rat interlobular and arcuate arteries (143). Heterogeneity in Ca 2ϩ currents was observed, with approximately one-third of the freshly isolated myocytes displaying only T-type currents ("T-rich"), one-third only L type, and the rest a mixture.…”

Section: Kidneymentioning

confidence: 99%

Molecular Physiology of Low-Voltage-Activated T-type Calcium Channels

Perez‐Reyes

2003

Physiological Reviews

1,501

1,446

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T-type Ca2+ channels were originally called low-voltage-activated (LVA) channels because they can be activated by small depolarizations of the plasma membrane. In many neurons Ca2+ influx through LVA channels triggers low-threshold spikes, which in turn triggers a burst of action potentials mediated by Na+ channels. Burst firing is thought to play an important role in the synchronized activity of the thalamus observed in absence epilepsy, but may also underlie a wider range of thalamocortical dysrhythmias. In addition to a pacemaker role, Ca2+ entry via T-type channels can directly regulate intracellular Ca2+ concentrations, which is an important second messenger for a variety of cellular processes. Molecular cloning revealed the existence of three T-type channel genes. The deduced amino acid sequence shows a similar four-repeat structure to that found in high-voltage-activated (HVA) Ca2+ channels, and Na+ channels, indicating that they are evolutionarily related. Hence, the α1-subunits of T-type channels are now designated Cav3. Although mRNAs for all three Cav3 subtypes are expressed in brain, they vary in terms of their peripheral expression, with Cav3.2 showing the widest expression. The electrophysiological activities of recombinant Cav3 channels are very similar to native T-type currents and can be differentiated from HVA channels by their activation at lower voltages, faster inactivation, slower deactivation, and smaller conductance of Ba2+. The Cav3 subtypes can be differentiated by their kinetics and sensitivity to block by Ni2+. The goal of this review is to provide a comprehensive description of T-type currents, their distribution, regulation, pharmacology, and cloning.

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Ionic currents and endothelin signaling in smooth muscle cells from rat renal resistance arteries

Cited by 76 publications

References 0 publications

Cellular mechanisms mediating rat renal microvascular constriction by angiotensin II.

Cellular mechanisms mediating rat renal microvascular constriction by angiotensin II.

Cytochrome P450 and Cyclooxygenase Metabolites Contribute to the Endothelin-1 Afferent Arteriolar Vasoconstrictor and Calcium Responses

Molecular Physiology of Low-Voltage-Activated T-type Calcium Channels

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