Chronic red laser treatment induces hypotensive effect in two-kidney one-clip model of renovascular hypertension in rat.

Abstract

To evaluate whether the chronic effect of photobiomodulation therapy (PBM) onsystolic arterial pressure (SAP)from two kidneys one clip (2K-1C) hypertension animal models can cause a hypotensive effect. Serum levels of nitric oxide were also analyzed and the assessment of lipid peroxidation of the thoracic aorta artery. Male Wistar rats were used. Hypertensive animals (2K-1C) with Systolic arterial pressure (SAP) greater than or equal to 160mmHg were used. Systolic arterial pressure (SAP) was determined by the tail plethysmography technique. Normotensive (2K) and hypertensive (2K-1C) rats were treated to PBM for 4weeks using a laser whose irradiation parameters were: red wavelength (λ) = 660nm: operating continuously; 56s per point (3 points) spot size = 0.0295 cm2; average optical power of 100 mW; energy of 5.6J per point; irradiance of 3.40 W/cm2; fluency of 190J/cm2 per point. The application was on the animals tails, at 3 different points simultaneously, in contact with the skin. To assess serum nitrite and nitrate (NOx) levels, blood collection was performed after chronic PBM treatment, 24h after the last laser application. The evaluation of the lipid peroxidation of the thoracic aorta artery was performed by measuring the concentration of hydroperoxide by the FOX method. Chronic photobiomodulation therapy (PBM) by red laser (660nm) can induce a hypotensive effect in 64% of 2K-1C hypertensive animals, which we say responsive animals. There was no difference in serum NO levels 24h after the last red laser application, between treated and non-treated groups. Aortic rings from 2K-1C hypertensive animals present a higher lipid peroxidation. The chronic PBM treatment by red laser decreased aortic rings lipid peroxidation in hypertensive responsive groups, compared to control. our results indicate that chronic PBM made by red laser has an important hypotensive effect in renovascular hypertensivemodels, by a mechanism that involves decrease in oxidative stress from vascular beds.