Functional and Structural Assessment of Intercellular Communication
- 1 August 1996
- journal article
- research article
- Published by Wolters Kluwer Health in Circulation Research
- Vol. 79 (2) , 174-183
- https://doi.org/10.1161/01.res.79.2.174
Abstract
Remodeling of conduction pathways in the hypertrophic response to myocardial injury is a potential mechanism leading to the development of anatomic substrates of lethal arrhythmias. To delineate the responsible mechanisms and to directly relate changes in intercellular coupling at gap junctions with electrophysiological alterations, we studied the effects of cAMP, a mediator of cardiac hypertrophy, on action potential conduction velocity and connexin expression in neonatal rat ventricular myocyte cultures. Conduction velocity was measured with an optical activation mapping technique in cells loaded with the voltage-sensitive dye RH-237. Action potentials were conducted 24% to 29% more rapidly (P<.005) after incubating cultures for 24 hours with the cAMP analogue dibutyryl cAMP (db-cAMP, 1 mmol/L). However, db-cAMP caused no change in the maximum rate of rise of the action potential upstroke, V̇max. Electron and immunofluorescence microscopy revealed a significant increase in the number and size of gap junctions in db-cAMP–treated cells. Immunoblotting showed that the total amounts of the ventricular gap junction proteins connexin43 and connexin45 (Cx43 and Cx45, respectively) increased 2- to 4-fold. Immunoprecipitation of metabolically labeled connexin proteins revealed a dose-dependent increase in the rate of Cx45 protein synthesis in myocytes exposed to db-cAMP (>2-fold after a 4-hour exposure) but no change in the Cx43 synthesis rate. Northern blot analysis demonstrated a time-dependent increase in the amount of Cx43 mRNA, with a maximum 3.3-fold increase after 4 hours of exposure to 1 mmol/L db-cAMP; cycloheximide did not block this effect. In contrast, Cx45 mRNA levels were not altered significantly after db-cAMP treatment. Thus, cAMP causes a significant increase in conduction velocity that appears to be attributable largely to enhanced expression of proteins responsible for intercellular communication. Cx43 and Cx45 levels appear to be upregulated by cAMP by disparate molecular mechanisms.Keywords
This publication has 30 references indexed in Scilit:
- Retinoic acid enhances connexin43 expression at the post‐transcriptional level in rat liver epithelial cellsCell Biochemistry and Function, 1995
- Conduction Defects and Arrhythmias in Chagas' Disease:Journal of Cardiovascular Electrophysiology, 1994
- Pathophysiology of Gap Junctions in Heart DiseaseJournal of Cardiovascular Electrophysiology, 1994
- Hypertrophy causes delayed conduction in human and guinea pig myocardium: accentuation during ischaemic perfusionCardiovascular Research, 1994
- Differential regulation of multiple gap junction transcripts and proteins during rat liver regeneration.The Journal of cell biology, 1993
- Further studies on the influence of cAMP-dependent protein kinase on junctional conductance in isolated heart cell pairsJournal of Molecular and Cellular Cardiology, 1991
- Na+ channel blockade by cyclic AMP and other 6-aminopurines in neonatal rat heartThe Journal of Membrane Biology, 1991
- Alpha 1-adrenergic receptor stimulation of sarcomeric actin isogene transcription in hypertrophy of cultured rat heart muscle cells.Journal of Clinical Investigation, 1989
- The potassium channel opener cromakalim (BRL 34915) activates ATP-dependent K+ channels in isolated cardiac myocytesBiochemical and Biophysical Research Communications, 1988
- Connexin43: a protein from rat heart homologous to a gap junction protein from liver.The Journal of cell biology, 1987