Intravascular flow stimulates PKD2 (polycystin-2) channels in endothelial cells to reduce blood pressure.
Charles E MacKayM Dennis LeoCarlos Fernandez-PenaRaquibul HasanWen YinAlejandro Mata-DaboinSimon BulleyJesse GammonsSalvatore MancarellaJonathan H JaggarPublished in: eLife (2020)
PKD2 (polycystin-2, TRPP1), a TRP polycystin channel, is expressed in endothelial cells (ECs), but its physiological functions in this cell type are unclear. Here, we generated inducible, EC-specific Pkd2 knockout mice to examine vascular functions of PKD2. Data show that a broad range of intravascular flow rates stimulate EC PKD2 channels, producing vasodilation. Flow-mediated PKD2 channel activation leads to calcium influx that activates SK/IK channels and eNOS serine 1176 phosphorylation in ECs. These signaling mechanisms produce arterial hyperpolarization and vasodilation. In contrast, EC PKD2 channels do not contribute to acetylcholine-induced vasodilation, suggesting stimulus-specific function. EC-specific PKD2 knockout elevated blood pressure in mice without altering cardiac function or kidney anatomy. These data demonstrate that flow stimulates PKD2 channels in ECs, leading to SK/IK channel and eNOS activation, hyperpolarization, vasodilation and a reduction in systemic blood pressure. Thus, PKD2 channels are a major component of functional flow sensing in the vasculature.
Keyphrases
- polycystic kidney disease
- blood pressure
- endothelial cells
- high glucose
- heart rate
- electronic health record
- coronary artery
- magnetic resonance imaging
- magnetic resonance
- hypertensive patients
- big data
- adipose tissue
- nitric oxide
- metabolic syndrome
- drug induced
- nitric oxide synthase
- vascular endothelial growth factor
- computed tomography
- deep learning
- artificial intelligence
- stress induced
- glycemic control