1. ¹Research Laboratories, Kyoto Pharmaceutical Industries, Ltd., Kyoto, Japan,
2. ²The Second Department of Medicine, University of Tokyo, Tokyo, Japan,
3. ³Fuji Biomedix Incorporated, Yamanashi, Japan.

Correspondence: Hiroaki Shirahase, PhD, Research Laboratories, Kyoto Pharmaceutical Industries, Ltd, 38, Nishinokyo Tsukinowa-cho, Nakakyo-ku, Kyoto 604, Japan.

Received 26 June 1996; Revised  0000; Accepted 14 January 1997.

Abstract

Iganidipine, a new water-soluble calcium antagonist, was administered at a nonhypotensive dose (NHD) of 0.3 mg/kg/day, a moderate-hypotensive dose (MHD) of 1.0 mg/kg/day, and a sustained-hypotensive dose (SHD) of 3.0 mg/kg/day to Dahl salt-sensitive (Dahl-S) rats fed a high-salt diet for 8 weeks. The effects on survival, and on renal and cerebral injuries, were then examined. Iganidipine completely prevented hypertensive death at the SHD and tended to increase the survival at the NHD and MHD. Iganidipine reduced glomerulosclerosis and renal arterial and tubular injuries in a dose-dependent manner. Iganidipine at the SHD, but not NHD or MHD, improved plasma creatinine, serum urea nitrogen, and glomerular filtration rate. Iganidipine at all doses examined increased the urinary prostaglandin (PG) I₂ and PGE₂, but not PGF₂ or thromboxane B₂, and decreased plasma angiotensin II (AII) level and renin activity. The renal glomerular, tubular, and arterial injuries were significantly correlated with blood pressure (r = 0.56 to 0.80) and plasma AII level (r = 0.50 to 0.71) but not with urinary prostanoids. Iganidipine also reduced the incidence of cerebral infarction. The infarction area was slightly and significantly correlated with urinary PGI₂ (r = 0.42) and PGE₂ (r = 0.41) but not with blood pressure or plasma AII. In conclusion, iganidipine prevented renal and cerebral injuries in Dahl-S rats. In addition to the reduced blood pressure, the reduction of plasma AII and the increase of vasodilatory prostanoids may also partially contribute to the renal and cerebral protective effects of iganidipine.