Literature DB >> 20647690

Evidence of direct smooth muscle relaxant effects of the fibrate gemfibrozil.

Laura E Phelps1, Jacob D Peuler.   

Abstract

Fibrates are commonly employed to treat abnormal lipid metabolism via their unique ability to stimulate peroxisome proliferator-activated receptor alpha (PPARalpha). Interestingly, they also decrease systemic arterial pressure, despite recent evidence that PPAR alpha may contribute to expression of renin and related hypertension. Yet, mechanisms responsible for their potential antihypertensive activity remain unresolved. Rapid decreases in arterial pressure following bolus intravenous injections of bezafibrate strongly suggest they may relax arterial smooth muscle directly. But since bezafibrate is highly susceptible to photodegradation in aqueous media, it has never been critically tested for this possibility in vitro with isolated arterial smooth muscle preparations. Accordingly, we tested gemfibrozil which is resistant to photodegradation. We examined it over a therapeutically-relevant range (50-400 microM) for both acute and delayed relaxant effects on contractions of the isolated rat tail artery; contractions induced by either depolarizing its smooth muscle cell membranes with high potassium or stimulating its membrane-bound receptors with norepinephrine and arginine-vasopressin. We also examined these same gemfibrozil levels for effects on spontaneously-occurring phasic rhythmic contractile activity, typically not seen in arteries under in vitro conditions but commonly exhibited by smooth muscle of uterus, duodenum and bladder. We found that gemfibrozil significantly relaxed all induced forms of contraction in the rat tail artery, acutely at the higher test levels and after a delay of a few hours at the lower test levels. The highest test level of gemfibrozil (400 microM) also completely abolished spontaneously-occurring contractile activity of the isolated uterus and duodenum and markedly suppressed it in the bladder. This is the first evidence that a fibrate drug can directly relax smooth muscle contractions, either induced by various contractile agents or spontaneously-occurring. These findings are particularly relevant to both the recently renewed concern over the impact of fibrates on hypertension and a new understanding of their gastrointestinal side effects.

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Year:  2010        PMID: 20647690     DOI: 10.1540/jsmr.46.125

Source DB:  PubMed          Journal:  J Smooth Muscle Res        ISSN: 0916-8737


  7 in total

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Journal:  Circ Genom Precis Med       Date:  2018-04

2.  Chronic social isolation in the prairie vole induces endothelial dysfunction: implications for depression and cardiovascular disease.

Authors:  Jacob D Peuler; Melissa-Ann L Scotti; Laura E Phelps; Neal McNeal; Angela J Grippo
Journal:  Physiol Behav       Date:  2012-03-26

3.  PPARα-independent action against metabolic syndrome development by fibrates is mediated by inhibition of STAT3 signalling.

Authors:  Huiying Hua; Julin Yang; Hante Lin; Yang Xi; Manyun Dai; Gangming Xu; Fuyan Wang; Lihong Liu; Tingqi Zhao; Jing Huang; Frank J Gonzalez; Aiming Liu
Journal:  J Pharm Pharmacol       Date:  2018-09-25       Impact factor: 3.765

4.  Effects of trans- versus cis-resveratrol on adrenergic contractions of the rat tail artery and role of endothelium.

Authors:  Ian R VanAntwerp; Laura E Phelps; Jacob D Peuler; Phillip G Kopf
Journal:  Physiol Rep       Date:  2021-01

5.  PPARα-Independent Arterial Smooth Muscle Relaxant Effects of PPARα Agonists.

Authors:  Neerupma Silswal; Nikhil K Parelkar; Michael J Wacker; Mostafa Badr; Jon Andresen
Journal:  PPAR Res       Date:  2012-09-11       Impact factor: 4.964

6.  Resveratrol can both enhance and relax adrenergic contractions of the rat tail artery.

Authors:  Sayra M Stom; Laura E Phelps; Jacob D Peuler
Journal:  J Smooth Muscle Res       Date:  2016

7.  Pharmacological preconditioning with gemfibrozil preserves cardiac function after heart transplantation.

Authors:  Kálmán Benke; Csaba Mátyás; Alex Ali Sayour; Attila Oláh; Balázs Tamás Németh; Mihály Ruppert; Gábor Szabó; Gábor Kökény; Eszter Mária Horváth; István Hartyánszky; Zoltán Szabolcs; Béla Merkely; Tamás Radovits
Journal:  Sci Rep       Date:  2017-10-27       Impact factor: 4.379

  7 in total

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