Modulation of Kv1.5 Currents by Protein Kinase A, Tyrosine Kinase, and Protein Tyrosine Phosphatase Requires an Intact Cytoskeleton

Mason, Helen S.; Latten, Mark J.; Godoy, L. D.; Horowitz, Burton; Kenyon, James L.

doi:10.1124/mol.61.2.285

Cited by 52 publications

(42 citation statements)

References 39 publications

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“…It has been established that this type of regulation involves the production of cAMP and subsequent phosphorylation by protein kinase A (PKA). Tyrosine kinases have also been reported to modulate the activity of cardiac ion channels (Shuba & McDonald, 1997;Zhou et al, 1997;Wang & Lipsius, 1998;Hool et al, 1998;Maier et al, 1999;Mason et al, 2002;Tiran et al, 2003). We previously demonstrated that genistein, a tyrosine kinase inhibitor, can increase the sensitivity of cardiac ion channels to b 1 -AR stimulation, suggesting that basal tyrosine kinase activity inhibits badrenergic responsiveness in cardiac myocytes (Hool et al, 1998).…”

Section: Introductionmentioning

confidence: 98%

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide

Sims

Harvey

2004

British J Pharmacology

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1 Phenylarsine oxide (PAO) is commonly used to inhibit tyrosine phosphatase activity. However, PAO can affect a variety of different processes because of its ability to promote sulfhydryl oxidation. In the present study, we investigated the effects that PAO has on basal and b-adrenergically stimulated L-type Ca 2 þ channel activity in isolated cardiac myocytes. 2 Extracellular application of PAO transiently stimulated the basal L-type Ca 2 þ channel activity, whereas it irreversibly inhibited protein kinase A (PKA)-dependent regulation of channel activity by isoproterenol, forskolin and 8-CPT-cAMP (8-p-chlorophenylthioadenosine 3 0 ,5 0 -cyclic monophosphate). PAO also inhibited channel activity irreversibly stimulated in the presence of adenosine 5 0 -(3-thiotriphosphate) tetralithium salt. 3 Neither the stimulatory nor the inhibitory effects of PAO were affected by the tyrosine kinase inhibitor lavendustin A, suggesting that tyrosine phosphorylation is not involved. 4 Extracellular application of the sulfhydryl-reducing agent dithiothreitol (DTT) antagonized both the stimulatory and inhibitory effects of PAO. Yet, following intracellular dialysis with DTT, only the inhibitory effect of PAO was antagonized. 5 The inhibitory effect of PAO was mimicked by intracellular, but not extracellular application of the membrane impermeant thiol oxidant 5,5 0 -dithio-bis(2-nitrobenzoic acid).6 These results suggest that the stimulatory effect of PAO results from oxidation of sulfhydryl residues at an extracelluar site and the inhibitory effect is due to redox regulation of an intracellular site that affects the response of the channel to PKA-dependent phosphorylation. It is concluded that the redox state of the cell may play a critical role in modulating b-adrenergic responsiveness of the Ltype Ca 2 þ channel in cardiac myocytes.

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Section: Introductionmentioning

confidence: 98%

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide

Sims

Harvey

2004

British J Pharmacology

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“…A myriad of studies over the past 40 years have identified hundreds (if not thousands) of PKA substrates, both in the nucleus and in the cytoplasm (Budovskaya et al 2005, Huang et al 2007, Neuberger et al 2007, Gao et al 2008. Like other post-translational protein modifications, PKAmediated phosphorylation can affect any aspect of target protein function, including activity, localization, and stability (Huang et al 2000, Mason et al 2002, Higuchi et al 2003, Qiao et al 2003, Hoang et al 2004, Hino et al 2005, Rolli-Derkinderen et al 2005, such that PKA exerts complex effects on most biologic systems. For this reason, pharmacologic or genetic manipulation in tissue culture cells may produce only a limited understanding of the pleomorphic role of PKA signaling.…”

Section: Introductionmentioning

confidence: 99%

Mouse models of altered protein kinase A signaling

Kirschner¹,

Yin²,

Jones³

et al. 2009

Endocrine-Related Cancer

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Protein kinase A (PKA) is an evolutionarily conserved protein which has been studied in model organisms from yeast to man. Although the cAMP-PKA signaling system was the first mammalian second messenger system to be characterized, many aspects of this pathway are still not well understood. Owing to findings over the past decade implicating PKA signaling in endocrine (and other) tumorigenesis, there has been renewed interest in understanding the role of this pathway in physiology, particularly as it pertains to the endocrine system. Because of the availability of genetic tools, mouse modeling has become the pre-eminent system for studying the physiological role of specific genes and gene families as a means to understanding their relationship to human diseases. In this review, we will summarize the current data regarding mouse models that have targeted the PKA signaling system. These data have led to a better understanding of both the complexity and the subtlety of PKA signaling, and point the way for future studies, which may help to modulate this pathway for therapeutic effect.

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“…Cardiac Kv1.5 channels also couple to the actin cytoskeleton, which regulates current density and channel localization (20). Recently, it has been shown that modulation of Kv1.5 currents by protein kinase A requires an intact cytoskeleton (21). Specific disruptors for cytoskeletons have been used in analyzing the functional roles of the cytoskeleton, including modulation of ion channel activities.…”

Section: Discussionmentioning

confidence: 99%

“…There are several previous reports (20,21,33,37) showing the regulation of ion channels by cytoskeleton. Maruoka et al (20) have reported that disruption of the actin cytoskeleton with cytochalasin B or cytochalasin D significantly increases Kv1.5-dependent K ϩ currents in Kv1.5-expressing human embryonic kidney cells.…”

Section: Discussionmentioning

confidence: 99%

Direct block of cloned hKv1.5 channel by cytochalasins, actin-disrupting agents

Choi¹,

Park²,

Lee³

et al. 2005

American Journal of Physiology-Cell Physiology

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The action of cytochalasins, actin-disrupting agents on human Kv1.5 channel (hKv1.5) stably expressed in Ltk Ϫ cells was investigated using the whole cell patchclamp technique. Cytochalasin B inhibited hKv1.5 currents rapidly and reversibly at ϩ60 mV in a concentration-dependent manner with an IC 50 of 4.2 M. Cytochalasin A, which has a structure very similar to cytochalasin B, inhibited hKv1.5 (IC 50 of 1.4 M at ϩ60 mV). Pretreatment with other actin filament disruptors cytochalasin D and cytochalasin J, and an actin filament stabilizing agent phalloidin had no effect on the cytochalasin B-induced inhibition of hKv1.5 currents. Cytochalasin B accelerated the decay rate of inactivation for the hKv1.5 currents. Cytochalasin B-induced inhibition of the hKv1.5 channels was voltage dependent with a steep increase over the voltage range of the channel's opening. However, the inhibition exhibited voltage independence over the voltage range in which channels are fully activated. Cytochalasin B produced no significant effect on the steady-state activation or inactivation curves. The rate constants for association and dissociation of cytochalasin B were 3.7 M/s and 7.5 s Ϫ1 , respectively. Cytochalasin B produced a use-dependent inhibition of hKv1.5 current that was consistent with the slow recovery from inactivation in the presence of the drug. Cytochalasin B (10 M) also inhibited an ultrarapid delayed rectifier K ϩ current (IK,ur) in human atrial myocytes. These results indicate that cytochalasin B primarily blocks activated hKv1.5 channels and endogenous IK,ur in a cytoskeleton-independent manner as an open-channel blocker.

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Modulation of Kv1.5 Currents by Protein Kinase A, Tyrosine Kinase, and Protein Tyrosine Phosphatase Requires an Intact Cytoskeleton

Cited by 52 publications

References 39 publications

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide

Mouse models of altered protein kinase A signaling

Direct block of cloned hKv1.5 channel by cytochalasins, actin-disrupting agents

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Modulation of Kv1.5 Currents by Protein Kinase A, Tyrosine Kinase, and Protein Tyrosine Phosphatase Requires an Intact Cytoskeleton

Cited by 52 publications

References 39 publications

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca2+ channel activity by phenylarsine oxide

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca2+ channel activity by phenylarsine oxide

Mouse models of altered protein kinase A signaling

Direct block of cloned hKv1.5 channel by cytochalasins, actin-disrupting agents

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Product

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Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide

Redox modulation of basal and β‐adrenergically stimulated cardiac L‐type Ca²⁺ channel activity by phenylarsine oxide