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Cardiovascular Research 2001 51(2):217-229; doi:10.1016/S0008-6363(01)00324-8
© 2001 by European Society of Cardiology
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Copyright © 2000, European Society of Cardiology

Cardiac gap junction channels: modulation of expression and channel properties

Toon A.B. van Veen*, Harold V.M. van Rijen and Tobias Opthof

Department of Medical Physiology, University Medical Center Utrecht, Utrecht, The Netherlands

* Corresponding author. Tel.: +31-30-253-8908; fax: +31-30-253-9036

In the heart, intercellular gap junction channels constructed from connexin molecules are crucial for conduction of the electric impulse. Cardiomyocytes can be interconnected by channels composed of three types of connexin proteins: Cx40, Cx43 or Cx45. In mammalian hearts, these three isoforms are regionally differently expressed and even between the species differences exist. Each of these channel-types possesses specific properties and are susceptible to modulation by various mechanisms. In this paper we compare the differences in properties of these channels as deduced from studies on transfected cells and isolated cardiomyocytes and discuss the factors involved in modulation of channel properties. Next, we evaluate the consequences of alterations in expression and modulation of channel properties for cardiac function. Therefore, we have compared reports on genetically engineered animals and discuss this information in relation to various pathophysiological disorders.

KEYWORDS {gamma}j, single channel conductance; gj, gap junctional (macroscopic) conductance; Po, open probability; Vj, transjuctional voltage gradient; Vo, Voltage difference at half-maximal (in)activation); PKC, protein kinase C; PKA, protein kinase A; PKG, protein kinase G; MAP kinase, mitogen activated protein kinase; LY, lucifer yellow (MW 443 dalton; 6CF, 6-carboxyfluorescein; DCF, 2'7'-dichlorofluorescein; mCx40, mCx43, mCx45, mouse connexin 40, –43, –45; rCx40, rCx43, rCx45, rat connexin 40, –43, –45; hCx40, hCx43, hCx45, human connexin 40, –43, –45


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