What question did this study set out to answer?

The research aims to explore the role of TRPV4 channels in the regulation of nitric oxide release and relaxation in pulmonary arteries.

February 9, 2026Open Access

Involvement of Nitric Oxide in TRPV4-Induced Relaxations of Mouse and Human Pulmonary Arteries

Key Points

The research aims to explore the role of TRPV4 channels in the regulation of nitric oxide release and relaxation in pulmonary arteries.
Isolated pulmonary arteries from wild-type and KCa3.1-deficient mice.
Conducted simultaneous measurements of nitric oxide concentration and relaxation.
Performed isometric tension recordings on isolated human pulmonary arteries.
Utilized TRPV4 activator GSK1016790A and blocker HC06704 to assess their effects on relaxation and nitric oxide levels.
Acetylcholine slightly decreased NO and relaxation in KCa3.1-deficient mouse arteries.
TRPV4 activation equally heightened NO and relaxation in both mouse types.
TRPV4 blockade inhibited NO release and relaxation in KCa3.1-deficient arteries.
Human pulmonary arteries showed endothelium-dependent relaxation in response to NO activators.

Abstract

The transient receptor potential vanilloid 4 channel (TRPV4) is thought to play a pivotal role in pulmonary arterial circulation. The present study hypothesizes that TRPV4 activation increases nitric oxide (NO) release and activates calcium-activated potassium of intermediate conductance (KCa3.1) in pulmonary arteries. Pulmonary arteries were isolated from wild-type mice (wt) and mice deficient in KCa3.1 channels (Kcnn4⁻/⁻) and mounted for simultaneous NO concentration and relaxation measurements. Human small pulmonary arteries were isolated and mounted in microvascular myographs for isometric tension recordings. Acetylcholine-induced increases in NO and relaxation of pulmonary arteries were slightly decreased in pulmonary arteries from Kcnn4⁻/⁻ versus wt mice. An activator of TRPV4 channels, GSK1016790A, increased NO and relaxation to the same degree in pulmonary arteries from wt and Kcnn4⁻/⁻ mice. A blocker of TRPV4 channels, HC06704, inhibited increases in NO concentration with no effect on acetylcholine (ACh) relaxation in pulmonary arteries from wt mice, but blocked increases in NO concentration and relaxation in pulmonary arteries from Kcnn4⁻/⁻ mice and responses to GSK1016790A in pulmonary arteries from wt and Kcnn4⁻/⁻ mice. Concentration-dependent relaxations induced by an inhibitor of sarcoplasmic Ca-ATPase, cyclopiazonic acid, were blocked in the presence of an inhibitor of NO synthase and a blocker of KCa3.1 channels, TRAM-34, in pulmonary arteries from wt mice, but were unaltered in the presence of TRAM-34 in arteries from Kcnn4⁻/⁻ mice, or the presence of a blocker of TRPV4 channels. In small human pulmonary arteries, ACh and sodium nitroprusside (SNP) induced concentration-dependent relaxations, blocked by endothelial cell removal, in the presence of an inhibitor of NO synthase and the KCa3.1 channel blocker TRAM-34. GSK1016790A induced relaxation of human pulmonary arteries with endothelium, but failed to relax arteries without endothelium. The findings suggest that TRPV4 channels are involved in endothelium-dependent relaxation and likely regulate pulmonary vascular tone by modulating NO release.

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