AI Article Synopsis
- There are significant daily variations in heart rhythm, but few studies link cardiac genes to biological clocks.
- Researchers studied mice with brain lesions and autonomic nervous system blockages to explore this connection.
- Control mice showed regular 24-hour patterns in specific clock and ion channel genes; however, those patterns disappeared in SCNX mice, while ANSB mice showed dampened rhythms but retained some circadian patterns.
Article Abstract
Significant circadian variations exist in the frequency of cardiac arrhythmia, but few studies have examined the relation between cardiac ion channels genes and biological clocks. We investigated this relation using suprachiasmatic nuclei lesion (SCNX) and pharmacological autonomic nervous system block (ANSB) mice. Significant 24-h variations were observed in the expression of clock genes Per2, Bmal1, and Dbp and ion channel genes KCNA5, KCND2, KCHIP2, and KCNK3 in the control mice hearts. In the SCNX mice, all genes examined lost circadian rhythm. In the ANSB mice, the expressions of the three clock genes were dampened significantly but still had circadian rhythm, whereas the four ion channel gene expressions lost rhythm. Heart rate also lost circadian rhythm in both the SCNX and ANSB mice. These results suggest that some ion channel gene expressions might be regulated by the central clock in the SCN through the ANS but not the peripheral clock in the heart.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3570950 | PMC |
| http://dx.doi.org/10.1080/09291016.2012.704801 | DOI Listing |
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