The present study was attempted to investigate the effects of total ginseng saponin (G75), panaxadiol-type (PDS) and panaxatriol-type saponin (PTS) on contractile responses of vasoconstrictors in aortic smooth muscle stripes of normotensive (NR) and spontaneous hypertensive rats (SHR). Phenylephrine (an adrenergic $alpha$$\_$1/-receptor agonist) and high potassium (a membrane depolarizing agent) caused greatly contractile responses in both NR and AHR aorta, respectively. Phenylephrine- and high potassium-induced contractile responses were greater in NA than those in SHR aortic smooth muscle stripes. In NR, the contractile responses of high potassium (5.6$ imes$10$^$-2/ M) were not affected in the presence of GTS (300 $mu$g/ml), PDS (300 $mu$g/ml), and PTS (300 $mu$g/ml), respectively whereas phenylephrine (10$^$-6/ M)-induced contractile responses were markedly inhibited. In SHR, the contractile responses of high potassium (5.6$ imes$10$^$-2/ M) were not affected in the presence of GTS (300 $mu$g/ml), PDS (300 $mu$g/ml), and moderate doses of PTS (150-300 $mu$g/ml), respectively but greatly blocked by high concentration of PTS (600 $mu$g/ml). Phenylephrine (10$^$-6/ M)-induced contractile responses were inhibited in a dose dependent fashion (150-600 $mu$g/ml) by the pretreatment with PTS while not altered in the presence of GTS (300 $mu$g/ml) and PDS (300 $mu$g/ml), respectively. Taken together, these experimental results suggest that ginseng saponins cause vascular relaxation through blockade of adrenergic $alpha$$\_$1/-receptors and some unknown mechanisms, and that there is some difference in sensitivity of vascular smooth muscle between NR and SHR in responses to ginseng saponins. It seems that panaxatriol type of some ginseng saponins has the greatest potency in vascular relaxation.