AI Article Synopsis
- Calcium influx through CaV1.2 channels is essential for controlling vascular smooth muscle contraction, which helps maintain blood pressure and myogenic tone.
- Alternative splicing of the CaV1.2 channel can be influenced by the RNA-binding protein Rbfox1, whose role in vascular smooth muscle cells (VSMCs) had not been clearly defined before.
- Rbfox1 is shown to reduce splicing changes in CaV1.2, and its knockdown leads to increased vascular constriction in hypertensive conditions, suggesting it could be a potential target for hypertension therapy.
Article Abstract
Calcium influx from depolarized CaV1.2 calcium channels triggers the contraction of vascular smooth muscle cells (VSMCs), which is important for maintaining vascular myogenic tone and blood pressure. The function of CaV1.2 channel can be subtly modulated by alternative splicing (AS), and its aberrant splicing involves in the pathogenesis of multiple cardiovascular diseases. The RNA-binding protein Rbfox1 is reported to regulate the AS events of CaV1.2 channel in the neuronal development, but its potential roles in vascular CaV1.2 channels and vasoconstriction remain undefined. Here, we detect Rbfox1 is expressed in rat vascular smooth muscles. Moreover, the protein level of Rbfox1 is dramatically decreased in the hypertensive small arteries from spontaneously hypertensive rats in comparison with normotensive ones from Wistar-Kyoto rats. In VSMCs, Rbfox1 could dynamically regulate the AS of CaV1.2 exons 9* and 33. By whole-cell patch clamp, we identify knockdown of Rbfox1 induces the hyperpolarization of CaV1.2 current-voltage relationship curve in VSMCs. Furthermore, siRNA-mediated knockdown of Rbfox1 increases the K+-induced constriction of rat mesenteric arteries. In summary, our results indicate Rbfox1 modulates vascular constriction by dynamically regulating CaV1.2 alternative exons 9* and 33. Therefore, our work elucidates the underlying mechanisms for CaV1.2 channels regulation and provides a potential therapeutic target for hypertension.
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| http://dx.doi.org/10.1042/CS20220226 | DOI Listing |
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