Leptin promotes K
            <sub>ATP</sub>
            channel trafficking by AMPK signaling in pancreatic β-cells

Park, Sun Hyun; Ryu, Shin Young; Yu, Weon Jin; Han, Young Eun; Ji, Young Sun; Oh, Keunhee; Sohn, Jong Woo; Lim, Ajin; Jeon, Jae Pyo; Lee, Hyunsu; Lee, Kyu-Hee; Lee, Suk Ho; Berggren, Per Olof; Jeon, Ju Hong; Ho, Won Kyung

doi:10.1073/pnas.1216351110

Cited by 70 publications

(110 citation statements)

References 39 publications

(49 reference statements)

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“…Leptin inhibits insulin secretion by increasing the cell-surface expression and the open probability of K ATP channels, resulting in a more hyperpolarized membrane potential (Holz et al, 2013). Leptin also induces an increased surface expression of Kv2.1 channels, leading to a rapid repolarization of membrane potential (Park et al, 2013b). These studies suggest that leptin exerts a coordinated trafficking regulation of K ATP and Kv2.1 channels to inhibit insulin secretion (Wu et al, 2015).…”

Section: Pharmacology Of K Atp Channels In Pancreatic Beta Cellsmentioning

confidence: 87%

“…The mechanism by which leptin activates K ATP channels involves phosphatase and tensin homologe inhibition mediated by phosphoinositide 3 kinase. phosphatase and tensin homologe inhibition induces F-actin depolymerization and, consequently, K ATP channel opening (Park et al, 2013b;Wu et al, 2015).…”

Section: Endogenous Regulation Of K Atp Channels In the Beta Cellmentioning

confidence: 99%

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Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

et al. 2016

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Pancreatic beta cells, unique cells that secrete insulin in response to an increase in glucose levels, play a significant role in glucose homeostasis. Glucose-stimulated insulin secretion (GSIS) in pancreatic beta cells has been extensively explored. In this mechanism, glucose enters the cells and subsequently the metabolic cycle. During this process, the ATP/ADP ratio increases, leading to ATP-sensitive potassium (K ATP ) channel closure, which initiates depolarization that is also dependent on the activity of TRP nonselective ion channels. Depolarization leads to the opening of voltage-gated Na 1 channels (Nav) and subsequently voltage-dependent Ca 21 channels (Cav).The increase in intracellular Ca 21 triggers the exocytosis of insulin-containing vesicles. Thus, electrical activity of pancreatic beta cells plays a central role in GSIS. Moreover, many growth factors, incretins, neurotransmitters, and hormones can modulate GSIS, and the channels that participate in GSIS are highly regulated. In this review, we focus on the principal ionic channels (K ATP , Nav, and Cav channels) involved in GSIS and how classic and new proteins, hormones, and drugs regulate it. Moreover, we also discuss advances on how metabolic disorders such as metabolic syndrome and diabetes mellitus change channel activity leading to changes in insulin secretion.

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Section: Pharmacology Of K Atp Channels In Pancreatic Beta Cellsmentioning

confidence: 87%

Section: Endogenous Regulation Of K Atp Channels In the Beta Cellmentioning

confidence: 99%

Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

et al. 2016

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“…Many proteins pass through early endosomes in the recycling process. K ATP channels likely follow this route, as evidenced by the partial colocalization of internalized Kir6.2 in pancreatic ␤-cells with the early endosome antigen 1 (EEA1) protein, which serves as a marker for this cellular compartment (632). The term early endosome actually refers to two types of endosomes, namely, the sorting endosome and the endocytic recycling compartment (ERC) (549).…”

Section: F Endocytic Recyclingmentioning

confidence: 99%

K_ATPChannels in the Cardiovascular System

Foster

Coetzee

2016

Physiological Reviews

187

222

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KATP channels are integral to the functions of many cells and tissues. The use of electrophysiological methods has allowed for a detailed characterization of KATP channels in terms of their biophysical properties, nucleotide sensitivities, and modification by pharmacological compounds. However, even though they were first described almost 25 years ago (Noma 1983, Trube and Hescheler 1984), the physiological and pathophysiological roles of these channels, and their regulation by complex biological systems, are only now emerging for many tissues. Even in tissues where their roles have been best defined, there are still many unanswered questions. This review aims to summarize the properties, molecular composition, and pharmacology of KATP channels in various cardiovascular components (atria, specialized conduction system, ventricles, smooth muscle, endothelium, and mitochondria). We will summarize the lessons learned from available genetic mouse models and address the known roles of KATP channels in cardiovascular pathologies and how genetic variation in KATP channel genes contribute to human disease.

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“…18 Similar study regarding leptin and glucose regulation of TRPC4 was recently published. 19 In this study, leptin is shown to activate TRPC4 channel and Ca 2C influx through TRPC4 activates AMPK that triggers translocation of ATPdependent K C channel (KATP) to the plasma membrane to hyperpolarize the resting membrane potential in pancreatic b-cell. Leptin activates TRPC4 in POMC, 20,21,22 and kisseptinsecreting hypothalamic neuron.…”

Section: Trpc4 Channelsmentioning

confidence: 99%

“…The finding of TRPC4 current in pancreatic b-cell in response to dexamethasone was interesting since similar study regarding leptin and glucose regulation of TRPC4 was recently published. 19 Leptin was first discovered in 1994 by Zang et al 59 and it is the most important and widely studied hormones in the control of energy balance. 60 Leptin is a 16 kDa protein mostly secreted from adipose tissue which has a critical role regulating body weight and energy homeostasis.…”

Section: The Roles Of Glucocorticoids and Leptin Via Trpc4 In Insulinmentioning

confidence: 99%

The Roles of Rasd1 small G proteins and leptin in the activation of TRPC4 transient receptor potential channels

et al. 2015

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#These authors contributed equally to this work TRPC4 is important regulators of electrical excitability in gastrointestinal myocytes, pancreatic b-cells and neurons. Much is known regarding the assembly and function of these channels including TRPC1 as a homotetramer or a heteromultimer and the roles that their interacting proteins play in controlling these events. Further, they are one of the best-studied targets of G protein-coupled receptors and growth factors in general and Ga i/o and Ga q protein coupled receptor or epidermal growth factor and leptin in particular. However, our understanding of the roles of small G proteins and leptin on TRPC4 channels is still rudimentary. We discuss potential roles for Rasd1 small G protein and leptin in channel activation in addition to their known role in cellular signaling.

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Leptin promotes K _ATP channel trafficking by AMPK signaling in pancreatic β-cells

Cited by 70 publications

References 39 publications

Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

K_ATPChannels in the Cardiovascular System

The Roles of Rasd1 small G proteins and leptin in the activation of TRPC4 transient receptor potential channels

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Leptin promotes K ATP channel trafficking by AMPK signaling in pancreatic β-cells

Cited by 70 publications

References 39 publications

Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

Modulation of Ionic Channels and Insulin Secretion by Drugs and Hormones in Pancreatic Beta Cells

KATPChannels in the Cardiovascular System

The Roles of Rasd1 small G proteins and leptin in the activation of TRPC4 transient receptor potential channels

Contact Info

Product

Resources

About

Leptin promotes K _ATP channel trafficking by AMPK signaling in pancreatic β-cells

K_ATPChannels in the Cardiovascular System