쥐의 적출 대동맥에 자외선 조사로 유발된 photorelaxation 기작의 생리학적 특성

Physiological characterization of mechanism on UV light-induced photorelaxation in isolated rat aorta

  • Lee Han-Ki (Department of Physical Therapy, Masan College) ;
  • Hong Yong-geun (Department of Physical Therapy, Masan College) ;
  • Kim Kyung (Department of Physical Therapy, Seoul Health College)
  • 발행 : 2003.06.01

초록

Isolated rat thoracic aorta which is pharmacologically precontracted by phenylephrine induces photorelaxation when exposed to long wave length UV-light. The aim of the present study was to characterize the mechanism of UV-light induced by photorelaxation in the rat aorta. 1. UV light relaxed both endothelium-intact and -denuded rat aortic rings contracted by phenylephrine. The magnitude of relaxation on UV light was dependent on the exposure time and slightly greatly in endothelium-denuded rings than in endothelium-intact preparations. 2. L-NAME (10 nM - 100 $\mu$M) but not D-NAME completely inhibited the photorelaxation in a concentration dependent manner. 3. The UV-induced relaxation was inhibited by methylene blue (1 - 100 uM), and verapamil (100 nM), and removal of extracellular $Ca^{2+}$. In contrast, UV-light induced photorelaxation was potentiated by $N^{w}$-nitro-L-arginine (L-NNA) treatment. These results suggest that UV light-induced photorelaxation may be due to nitric oxide from exogenously administered L-arginine as well as endogenous nitric oxide donors such as amino acid and arginine derivatives

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