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            Current and Spontaneous Activity in Mouse Embryonic Ventricular Myocytes

Yasui, Kohichiroh; Liu, Weiran; Opthof, Tobias; Kada, Kenji; Lee, Jong-Kook; Kamiya, Kaichiro; Kodama, Itsuo

doi:10.1161/01.res.88.5.536

Cited by 143 publications

(127 citation statements)

References 27 publications

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“…A minority of myocytes isolated from the hearts of adult rats express I f , which, when present, was of small amplitude. In accordance with data reported in the fetal mouse (Yasui et al, 2001;Mommersteeg et al, 2007;Schweizer et al, 2009), expression analysis in the rat documented that both HCN4 and HCN2 isoforms account for the majority of total HCN transcript in the neonatal ventricle, while HCN1 and HCN3 isoforms are not expressed at detectable levels . Interestingly, HCN4 is down-regulated during rat heart maturation, but in association with HCN2 it undergoes a clear-cut up-regulation after cardiac infarction (Suffredini et al, 2009).…”

Section: Funny Channel Over-expression In Cardiomyocytes Is a Marker supporting

confidence: 89%

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

Sartiani¹,

Cerbai²,

Mugelli³

2011

Modern Pacemakers - Present and Future

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Section: Funny Channel Over-expression In Cardiomyocytes Is a Marker supporting

confidence: 89%

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

Sartiani¹,

Cerbai²,

Mugelli³

2011

Modern Pacemakers - Present and Future

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“…7,14,15 A higher expression of HCN4 was detected in CO-exposed rat hearts at 4 days after birth (2.73±0.54 vs 1.04±0.11) (Figure 5a); this was accompanied by a relative upregulation of the mRNA coding for MinK-related peptide 1 (MiRP-1) (2.06 ± 0.02 vs 1.03 ± 0.2 at 4 days) (Figure 5c). MiRP-1 is a b-subunit that enhances the expression and speeds up the kinetics of activation of the HCN-derived proteins; in the adult heart, MiRP-1 is expressed in the sinus node region but hardly detectable in the ventricle.…”

Section: Molecular Properties Of F-channels In Co-exposed Neonatal Ratsmentioning

confidence: 98%

“…To get a functional correlate, we evaluated the temporal pattern of expression of f-current. In fact, I f is overexpressed in rodent ventricular myocytes during the fetal life but is downregulated after birth 13,14 ; eventually, I f expression is reinduced when adult cardiomyocytes undergo 'pathological' hypertrophic growth such as in cardiac diseases. 8 Figure 3 shows typical action potentials (upper panels) and currents (lower panels) recorded in myocytes isolated from control and CO-exposed rat hearts at 2 (panels a and b) and 40 (panels c and d) days after birth.…”

Section: Sustained Functional Expression Of F-channels In Co-exposed mentioning

confidence: 99%

Prenatal exposure to carbon monoxide delays postnatal cardiac maturation

Sartiani

Stillitano

Luceri

et al. 2010

Laboratory Investigation

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Prenatal exposure to toxicants, such as maternal smoking, may impair cardiovascular autonomic maturation in infants. We recently showed that exposure of pregnant rats to a mild concentration of carbon monoxide (CO), a component of cigarette smoke, delays postnatal electrophysiological maturation of ventricular myocytes from newborns rats, likely predisposing to life-threatening arrhythmias. To get a comprehensive view of developmental molecular abnormalities induced, at cardiac level, by prenatal CO exposure, we used microarray analysis approach on the rat heart at 4, 7 and 20 days postnatal life. The relationship between molecular and functional alterations was investigated by assessing the ventricular expression of f-current, an electrophysiological marker of immature cardiac phenotype. Rats were prenatally exposed to 0 (CTR) or 150 p.p.m. CO and mRNA obtained from ventricular samples. Differential analysis and biological pathway analysis of microarray data were performed by using Newton's approach and the GENMAPP/MAPPFinder, respectively. The real-time RT-PCR reactions were performed by TaqMan probe-based chemistry. Freshly isolated patch-clamped ventricular cardiomyocytes were used to measure I f . Genes and pathways controlling cell cycle and excitation-contraction coupling were significantly modified in CO-exposed rats. The higher effect was observed in cardiomyocytes harvested from 7-day-old rats, in which mRNA expression for crucial sarcomeric proteins (myosin and actin subunits, troponin I), transporters (Ca 2 þ transporting ATPase) and enzymes (aldolase) were significantly downregulated. Accordingly, the molecular and functional expression of f-channels, which represents a marker of fetal ventricular phenotype, was transiently greater in CO-exposed rats ( þ 200%) than in control ones. In conclusion, our study provides new insights into the molecular and functional mechanisms underlying cardiac maturation and its impairment by prenatal exposure to toxic components of smoking, such as CO.

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“…Molecularly, the extinction of Tbx3 leads to the appearance of "high conductance" proteins [11][12][13] , such as the connexins Cx40 and Cx43 [14] , and the replacement of the Land T-type Ca 2+ channels by the fast voltage-activated sodium channel Scn5a (Nav1.5) [15] . HCN4 expression is also strongly decreased in the working myocardium, as this tissue loses its intrinsic pacemaker activity [16][17][18] . The ventricular conduction is provided by the trabecular myocardium from the dorsal part of atrioventricular canal, which expresses the fast-conducting connexins [19,20] .…”

Section: Development Of the Human Cardiac Conduction Systemmentioning

confidence: 99%

Mechanisms underlying the cardiac pacemaker: the role of SK4 calcium-activated potassium channels

et al. 2016

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The proper expression and function of the cardiac pacemaker is a critical feature of heart physiology. The sinoatrial node (SAN) in human right atrium generates an electrical stimulation approximately 70 times per minute, which propagates from a conductive network to the myocardium leading to chamber contractions during the systoles. Although the SAN and other nodal conductive structures were identified more than a century ago, the mechanisms involved in the generation of cardiac automaticity remain highly debated. In this short review, we survey the current data related to the development of the human cardiac conduction system and the various mechanisms that have been proposed to underlie the pacemaker activity. We also present the human embryonic stem cellderived cardiomyocyte system, which is used as a model for studying the pacemaker. Finally, we describe our latest characterization of the previously unrecognized role of the SK4 Ca 2+ -activated K + channel conductance in pacemaker cells. By exquisitely balancing the inward currents during the diastolic depolarization, the SK4 channels appear to play a crucial role in human cardiac automaticity.

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I _f Current and Spontaneous Activity in Mouse Embryonic Ventricular Myocytes

Cited by 143 publications

References 27 publications

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

Prenatal exposure to carbon monoxide delays postnatal cardiac maturation

Mechanisms underlying the cardiac pacemaker: the role of SK4 calcium-activated potassium channels

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I f Current and Spontaneous Activity in Mouse Embryonic Ventricular Myocytes

Cited by 143 publications

References 27 publications

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

The Funny Current in Cardiac Non-Pacemaker Cells: Functional Role and Pharmacological Modulation

Prenatal exposure to carbon monoxide delays postnatal cardiac maturation

Mechanisms underlying the cardiac pacemaker: the role of SK4 calcium-activated potassium channels

Contact Info

Product

Resources

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I _f Current and Spontaneous Activity in Mouse Embryonic Ventricular Myocytes