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RXP-E: a connexin43-binding peptide that prevents action potential propagation block
- Source :
- Lewandowski , R , Procida , K , Vaidyanathan , R , Coombs , W , Jalife , J , Nielsen , M S , Taffet , S M & Delmar , M 2008 , ' RXP-E: a connexin43-binding peptide that prevents action potential propagation block ' , Circulation Research , vol. 103 , no. 5 , pp. 519-26 .
- Publication Year :
- 2008
-
Abstract
- Udgivelsesdato: 2008-Aug-29<br />Gap junctions provide a low-resistance pathway for cardiac electric propagation. The role of GJ regulation in arrhythmia is unclear, partly because of limited availability of pharmacological tools. Recently, we showed that a peptide called "RXP-E" binds to the carboxyl terminal of connexin43 and prevents chemically induced uncoupling in connexin43-expressing N2a cells. Here, pull-down experiments show RXP-E binding to adult cardiac connexin43. Patch-clamp studies revealed that RXP-E prevented heptanol-induced and acidification-induced uncoupling in pairs of neonatal rat ventricular myocytes. Separately, RXP-E was concatenated to a cytoplasmic transduction peptide (CTP) for cytoplasmic translocation (CTP-RXP-E). The effect of RXP-E on action potential propagation was assessed by high-resolution optical mapping in monolayers of neonatal rat ventricular myocytes, containing approximately 20% of randomly distributed myofibroblasts. In contrast to control experiments, when heptanol (2 mmol/L) was added to the superfusate of monolayers loaded with CTP-RXP-E, action potential propagation was maintained, albeit at a slower velocity. Similarly, intracellular acidification (pH(i) 6.2) caused a loss of action potential propagation in control monolayers; however, propagation was maintained in CTP-RXP-E-treated cells, although at a slower rate. Patch-clamp experiments revealed that RXP-E did not prevent heptanol-induced block of sodium currents, nor did it alter voltage dependence or amplitude of Kir2.1/Kir2.3 currents. RXP-E is the first synthetic molecule known to: (1) bind cardiac connexin43; (2) prevent heptanol and acidification-induced uncoupling of cardiac gap junctions; and (3) preserve action potential propagation among cardiac myocytes. RXP-E can be used to characterize the role of gap junctions in the function of multicellular systems, including the heart.
Details
- Database :
- OAIster
- Journal :
- Lewandowski , R , Procida , K , Vaidyanathan , R , Coombs , W , Jalife , J , Nielsen , M S , Taffet , S M & Delmar , M 2008 , ' RXP-E: a connexin43-binding peptide that prevents action potential propagation block ' , Circulation Research , vol. 103 , no. 5 , pp. 519-26 .
- Notes :
- English
- Publication Type :
- Electronic Resource
- Accession number :
- edsoai.on1322570327
- Document Type :
- Electronic Resource