HIGHLIGHTED TOPIC Pulmonary Circulation and Hypoxia Pressure-induced smooth muscle cell depolarization in pulmonary arteries from control and chronically hypoxic rats does not cause myogenic vasoconstriction

Naik, Jay S., Scott Earley, Thomas C. Resta, and Benjimen R. Walker. Pressure-induced smooth muscle cell depolarization in pulmonary arteries from control and chronically hypoxic rats does not cause myogenic vasoconstriction. J Appl Physiol 98: 1119–1124, 2005. First published October 22, 2004; doi:10.1152/japplphysiol.00819. 2004.—Chronic obstructive pulmonary diseases, as well as prolonged residence at high altitude, can result in generalized airway hypoxia, eliciting an increase in pulmonary vascular resistance. We hypothesized that a portion of the elevated pulmonary vascular resistance following chronic hypoxia (CH) is due to the development of myogenic tone. Isolated, pressurized small pulmonary arteries from control (barometric pressure 630 Torr) and CH (4 wk, barometric pressure 380 Torr) rats were loaded with fura 2-AM and perfused with warm (37°C), aerated (21% O2-6% CO2-balance N2) physiological saline solution. Vascular smooth muscle (VSM) intracellular Ca concentration ([Ca ]i) and diameter responses to increasing intraluminal pressure were determined. Diameter and VSM cell [Ca ]i responses to KCl were also determined. In a separate set of experiments, VSM cell membrane potential responses to increasing luminal pressure were determined in arteries from control and CH rats. VSM cell membrane potential in arteries from CH animals was depolarized relative to control at each pressure step. VSM cells from both groups exhibited a further depolarization in response to step increases in intraluminal pressure. However, arteries from both control and CH rats distended passively to increasing intraluminal pressure, and VSM cell [Ca ]i was not affected. KCl elicited a dosedependent vasoconstriction that was nearly identical between control and CH groups. Whereas KCl administration resulted in a dosedependent increase in VSM cell [Ca ]i in arteries taken from control animals, this stimulus elicited only a slight increase in VSM cell [Ca ]i in arteries from CH animals. We conclude that the pulmonary circulation of the rat does not demonstrate pressure-induced vasoconstriction.