Treatment of essential hypertension and hypertension associated with renal impairment with pinacidil: A new vasodilator

Breen, E. G.; Mulhall, D.; Keogh, J. A. B.

doi:10.1007/bf00544354

Cited by 5 publications

(2 citation statements)

References 18 publications

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“…is a nitric oxide (NO•) donor. Initially, these drugs were developed as hypotensive compounds that relax smooth muscle by stimulating the K+ influx to smooth muscle [53][54][55]. Therefore, pinacidil, diazoxide, minoxidil, and nicorandil are used in clinical praxis for treatment of hypertension [18,53,55].…”

Section: Katp Channel Blockersmentioning

confidence: 99%

“…Initially, these drugs were developed as hypotensive compounds that relax smooth muscle by stimulating the K+ influx to smooth muscle [53][54][55]. Therefore, pinacidil, diazoxide, minoxidil, and nicorandil are used in clinical praxis for treatment of hypertension [18,53,55]. KCOs are categorized as follows for their ability to induce relaxation of the aorta: rilmakalim > P1075 > bimakalim > levcromakalim > nicorandil, (À)-pinacidil > aprikalim > minoxidil > (+)-pinacidil > diazoxidel [18].…”

Section: Katp Channel Blockersmentioning

confidence: 99%

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K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

Maslov

Popov

Naryzhnaya

et al. 2023

Fundamemntal Clinical Pharma

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BackgroundThe use of percutaneous coronary intervention (PCI) in patients with ST‐segment elevation myocardial infarction (STEMI) is associated with a mortality rate of 5%–7%. It is clear that there is an urgent need to develop new drugs that can effectively prevent cardiac reperfusion injury. ATP‐sensitive K+ (KATP) channel openers (KCOs) can be classified as such drugs.ResultsKCOs prevent irreversible ischemia and reperfusion injury of the heart. KATP channel opening promotes inhibition of apoptosis, necroptosis, pyroptosis, and stimulation of autophagy. KCOs prevent the development of cardiac adverse remodeling and improve cardiac contractility in reperfusion. KCOs exhibit antiarrhythmic properties and prevent the appearance of the no‐reflow phenomenon in animals with coronary artery occlusion and reperfusion. Diabetes mellitus and a cholesterol‐enriched diet abolish the cardioprotective effect of KCOs. Nicorandil, a KCO, attenuates major adverse cardiovascular event and the no‐reflow phenomenon, reduces infarct size, and decreases the incidence of ventricular arrhythmias in patients with acute myocardial infarction.ConclusionThe cardioprotective effect of KCOs is mediated by the opening of mitochondrial KATP (mitoKATP) and sarcolemmal KATP (sarcKATP) channels, triggered free radicals' production, and kinase activation.

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Section: Katp Channel Blockersmentioning

confidence: 99%

Section: Katp Channel Blockersmentioning

confidence: 99%

K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

Maslov

Popov

Naryzhnaya

et al. 2023

Fundamemntal Clinical Pharma

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ATP‐Sensitive Potassium Channels and Their Physiological and Pathophysiological Roles

Tinker

Aziz

et al. 2018

Comprehensive Physiology

111

112

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ATP sensitive potassium channels (K ) are so named because they open as cellular ATP levels fall. This leads to membrane hyperpolarization and thus links cellular metabolism to membrane excitability. They also respond to MgADP and are regulated by a number of cell signaling pathways. They have a rich and diverse pharmacology with a number of agents acting as specific inhibitors and activators. K channels are formed of pore-forming subunits, Kir6.1 and Kir6.2, and a large auxiliary subunit, the sulfonylurea receptor (SUR1, SUR2A, and SUR2B). The Kir6.0 subunits are a member of the inwardly rectifying family of potassium channels and the sulfonylurea receptor is part of the ATP-binding cassette family of proteins. Four SURs and four Kir6.x form an octameric channel complex and the association of a particular SUR with a specific Kir6.x subunit constitutes the K current in a particular tissue. A combination of mutagenesis work combined with structural studies has identified how these channels work as molecular machines. They have a variety of physiological roles including controlling the release of insulin from pancreatic β cells and regulating blood vessel tone and blood pressure. Furthermore, mutations in the genes underlie human diseases such as congenital diabetes and hyperinsulinism. Additionally, opening of these channels is protective in a number of pathological conditions such as myocardial ischemia and stroke. © 2018 American Physiological Society. Compr Physiol 8:1463-1511, 2018.

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Pinacidil

Simmons

2009

xPharm: The Comprehensive Pharmacology Reference

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Treatment of essential hypertension and hypertension associated with renal impairment with pinacidil: A new vasodilator

Cited by 5 publications

References 18 publications

K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

ATP‐Sensitive Potassium Channels and Their Physiological and Pathophysiological Roles

Pinacidil

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Treatment of essential hypertension and hypertension associated with renal impairment with pinacidil: A new vasodilator

Cited by 5 publications

References 18 publications

KATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

KATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

ATP‐Sensitive Potassium Channels and Their Physiological and Pathophysiological Roles

Pinacidil

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Product

Resources

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K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury

K_ATP channels are regulators of programmed cell death and targets for the creation of novel drugs against ischemia/reperfusion cardiac injury