Antiarrhythmic effect and its underlying ionic mechanism of 17β‐estradiol in cardiac myocytes

Nakajima, Toshiaki; Iwasawa, Kuniaki; Oonuma, Hitoshi; Morita, Toshihiro; Goto, Akitoshi; Wang, Yuepeng; Hazama, Hisanori

doi:10.1038/sj.bjp.0702576

Cited by 77 publications

(53 citation statements)

References 56 publications

(73 reference statements)

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“…The profound inhibition of I Ca,L by raloxifene over the range of potentials tested is similar to previously documented direct actions of 17b-oestradiol on cardiac myocytes (Jiang et al, 1992;Grohe et al, 1996;Nakajima et al, 1999a). However, raloxifene did not significantly shift the steady-state activation or inactivation curves.…”

Section: Discussionsupporting

confidence: 87%

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Liew

Stagg

MacLeod

et al. 2004

British J Pharmacology

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1 The selective oestrogen (ER) receptor modulator, raloxifene, is widely used in the treatment of postmenopausal osteoporosis, but may also possess cardioprotective properties. We investigated whether it directly suppresses myocyte contractility through Ca 2 þ channel antagonism in a similar way to 17b-oestradiol. 2 Cell shortening and Ca 2 þ transients were measured in single guinea-pig ventricular myocytes fieldstimulated (1 Hz, 371C) in a superfusion chamber. Electrophysiological recordings were performed using single electrode voltage-clamp. 3 Raloxifene decreased cell shortening (EC 50 2.4 mM) and the Ca 2 þ transient amplitude (EC 50 6.4 mM) in a concentration-dependent manner. At a concentration of 1 mM, raloxifene produced a 3372% (mean7s.e.m) and 2472% reduction, respectively (Po0.001, n ¼ 14 for both parameters). 4 These inhibitory actions were not observed in myocytes that had been incubated with the specific antagonist, ICI 182,780 (10 mM) (n ¼ 11). 5 Raloxifene (1 mM) shortened action potential durations at 50 and 90% repolarisation (Po0.05 and o0.001, respectively; n ¼ 27) and decreased peak L-type Ca 2 þ current by 45%, from À5.170.5 pA/pF to À2.870.3 pA/pF (Po0.001, n ¼ 18). 6 Raloxifene did not significantly alter sarcoplasmic reticulum Ca 2 þ content, as assessed by integrating the Na þ /Ca 2 þ exchanger currents following rapid caffeine application. 7 The present study provides evidence for direct inhibitory actions of raloxifene on ventricular myocyte contractility, mediated through Ca 2 þ channel antagonism.

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Section: Discussionsupporting

confidence: 87%

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Liew

Stagg

MacLeod

et al. 2004

British J Pharmacology

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“…However, a Kir blocker terikalant has no effect on the current of ATP-sensitive K ϩ channel (Escande, 1989). Thus, it is not surprising that although 17␤-estradiol did not exert any effect on Kir channels (Nakajima et al, 1999;Tanabe et al, 1999), it can activate ATP-sensitive K ϩ channels. Many agonists have been shown to trigger the opening of ATP-sensitive K ϩ channels, including adenosine, bradykinin, opioids, and free radicals (Downey and Cohen, 1997).…”

Section: Discussionmentioning

confidence: 99%

“…17␤-Estradiol has been shown to activate K ϩ channels in some (Sudhir et al, 1995;Hugel et al, 1999) but not all studies (Nakajima et al, 1999;Tanabe et al, 1999). The ATP-sensitive K ϩ channel, a member of the superfamily of Kir channels, is a heteromultimer composed of a pore-forming K ϩ channel core and a regulating ATP-binding cassette protein (Jovanovic et al, 1999).…”

Section: Discussionmentioning

confidence: 99%

Differential Effects of Sarcolemmal and Mitochondrial K_ATP Channels Activated by 17β-Estradiol on Reperfusion Arrhythmias and Infarct Sizes in Canine Hearts

Tsai

Su²,

Chou³

et al. 2002

J Pharmacol Exp Ther

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We have demonstrated the effects of estrogen on modulation of ATP-sensitive K ϩ channels; however, the subcellular location of these channels is unknown. The purpose of the present study was to investigate the role of the sarcolemmal and mitochondrial ATP-sensitive K ϩ channels in a canine model of myocardial infarction after stimulation with 17␤-estradiol. Anesthetized dogs were subjected to 60 min of the left anterior descending coronary artery occlusion followed by 3 h of reperfusion. Infarct size was markedly reduced in estradiol-treated dogs compared with controls (14 Ϯ 6 versus 42 Ϯ 6%, P Ͻ 0.0001), indicating the effective dose of estradiol administrated. Pretreatment with the mitochondrial ATP-sensitive K ϩ channel antagonist 5-hydroxydecanoate completely abolished estradiol-induced cardioprotection. The sarcolemmal ATP-sensitive K ϩ channel antagonist 1-15-12-(5-chloro-o-anisamido)ethylmethoxyphenyl)sulfonyl-3-methylthiourea (HMR 1098) did not significantly attenuate estradiol-induced infarct size limitation.In addition, estradiol administration significantly reduced the incidence and duration of reperfusion-induced ventricular tachycardia and ventricular fibrillation. Although 5-hydroxydecanoate alone caused no significant effect on the incidence of reperfusion arrhythmias in the presence or absence of estradiol, the administration of HMR 1098 abolished estrogen-induced improvement of reperfusion arrhythmias. Pretreatment with the estrogen-receptor antagonist faslodex (ICI 182,780) did not alter estrogen-induced infarct-limiting and antiarrhythmic effects. These results demonstrate that estrogen is cardioprotective against infarct sizes and fatal reperfusion arrhythmias by different ATP-sensitive K ϩ channels for an estrogen receptor-independent mechanism. The infarct size-limiting and antiarrhythmic effects of estrogen were abolished by 5-hydroxydecanoate and HMR 1098, suggesting that the effects may result from activation of the mitochondrial and sarcolemmal ATP-sensitive K ϩ channels, respectively.

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“…The female hormone progesterone (P4) activates the principal calcium channel of sperm (CatSper) (2)(3)(4)(5) and blocks the potassium channel KSper (6) via these nongenomic pathways (7). The modulation of ion channel functions by steroid hormones has been reported in the heart (8,9), neurons (10)(11)(12), smooth muscle (13), and pancreatic beta cells (14). In marine invertebrates, the sulfated steroid cholestane acts as a chemoattractant for sea squirt sperm, which also happens via the nongenomic pathway (15).…”

mentioning

confidence: 99%

Regulation of the sperm calcium channel CatSper by endogenous steroids and plant triterpenoids

Mannowetz

Miller

Lishko

2017

Proc. Natl. Acad. Sci. U.S.A.

102

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The calcium channel of sperm (CatSper) is essential for sperm hyperactivated motility and fertility. The steroid hormone progesterone activates CatSper of human sperm via binding to the serine hydrolase ABHD2. However, steroid specificity of ABHD2 has not been evaluated. Here, we explored whether steroid hormones to which human spermatozoa are exposed in the male and female genital tract influence CatSper activation via modulation of ABHD2. The results show that testosterone, estrogen, and hydrocortisone did not alter basal CatSper currents, whereas the neurosteroid pregnenolone sulfate exerted similar effects as progesterone, likely binding to the same site. However, physiological concentrations of testosterone and hydrocortisone inhibited CatSper activation by progesterone. Additionally, testosterone antagonized the effect of pregnenolone sulfate. We have also explored whether steroid-like molecules, such as the plant triterpenoids pristimerin and lupeol, affect sperm fertility. Interestingly, both compounds competed with progesterone and pregnenolone sulfate and significantly reduced CatSper activation by either steroid. Furthermore, pristimerin and lupeol considerably diminished hyperactivation of capacitated spermatozoa. These results indicate that (i) pregnenolone sulfate together with progesterone are the main steroids that activate CatSper and (ii) pristimerin and lupeol can act as contraceptive compounds by averting sperm hyperactivation, thus preventing fertilization.CatSper | steroids | lupeol | triterpenoids | pristimerin S teroid hormones control fundamental organism functions such as development, metabolism, inflammation, ion homeostasis, and reproduction. According to the conventional model, steroid hormones signal through a corresponding genomic receptor, which upon binding to a steroid hormone initiates the translocation of the hormone-receptor complex to the nucleus. There it acts as a transcription factor by altering gene expression, and such a process can take hours (1). However, there is another, much faster pathway that is initiated by steroid hormone binding to its membrane receptor on the extracellular side of the cell. The latter signaling involves second messengers and signal-transduction cascades, which often result in the activation of ion channels (1). The female hormone progesterone (P4) activates the principal calcium channel of sperm (CatSper) (2-5) and blocks the potassium channel KSper (6) via these nongenomic pathways (7). The modulation of ion channel functions by steroid hormones has been reported in the heart (8, 9), neurons (10-12), smooth muscle (13), and pancreatic beta cells (14). In marine invertebrates, the sulfated steroid cholestane acts as a chemoattractant for sea squirt sperm, which also happens via the nongenomic pathway (15). The latter represents an unconventional chemoattractant for ascidian sperm, as such factors are usually proteins or peptides and not steroids. In humans, pregnenolone sulfate (PregS), a sulfated steroid hormone similar in structure to P4, i...

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Antiarrhythmic effect and its underlying ionic mechanism of 17β‐estradiol in cardiac myocytes

Cited by 77 publications

References 56 publications

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Differential Effects of Sarcolemmal and Mitochondrial K_ATP Channels Activated by 17β-Estradiol on Reperfusion Arrhythmias and Infarct Sizes in Canine Hearts

Regulation of the sperm calcium channel CatSper by endogenous steroids and plant triterpenoids

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Antiarrhythmic effect and its underlying ionic mechanism of 17β‐estradiol in cardiac myocytes

Cited by 77 publications

References 56 publications

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Raloxifene acutely suppresses ventricular myocyte contractility through inhibition of the L‐type calcium current

Differential Effects of Sarcolemmal and Mitochondrial KATP Channels Activated by 17β-Estradiol on Reperfusion Arrhythmias and Infarct Sizes in Canine Hearts

Regulation of the sperm calcium channel CatSper by endogenous steroids and plant triterpenoids

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Product

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Differential Effects of Sarcolemmal and Mitochondrial K_ATP Channels Activated by 17β-Estradiol on Reperfusion Arrhythmias and Infarct Sizes in Canine Hearts