Lovastatin Prevents Development of Hypertension in Spontaneously Hypertensive Rats

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Hypertension. 1997;30:968-974

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(Hypertension. 1997;30:968-974.)
© 1997 American Heart Association, Inc.

Articles

Lovastatin Prevents Development of Hypertension in Spontaneously Hypertensive Rats

Jian Jiang; ; Richard J. Roman

From the Department of Physiology, Medical College of Wisconsin, Milwaukee.

Correspondence to Richard J. Roman, PhD, Department of Physiology, Medical College of Wisconsin, 8701 Watertown Plank Rd, Milwaukee, WI 53226.

Abstract The present study evaluated the effects of lovastatinon renal function and the development of hypertension in spontaneouslyhypertensive rats (SHR). Four-week-old SHR were given lovastatin(10 mg/kg) or vehicle twice daily by gavage. After 4 weeks oftreatment, mean arterial pressure was significantly lower inlovastatin-treated SHR (131±4 mm Hg, n=5) than in controlanimals (160±4 mm Hg, n=12) (P<.05). The fall in arterialpressure in lovastatin-treated rats was accompanied by changesin renal function. The slope of the relationship between arterial pressureand sodium excretion was threefold greater in lovastatin-treatedSHR (n=6) than in control rats (n=6), and this was associatedwith significant elevations in renal medullary blood flow andrenal interstitial hydrostatic pressure. Glomerular filtrationrate was 17% higher in lovastatin-treated SHR (n=6) than incontrol rats (n=6) (0.94±0.05 versus 0.81±0.07mL/min per g of kidney weight, P<.05). The wall-to-lumenarea ratio of renal arterioles was significantly reduced inlovastatin-treated SHR compared with vehicle-treated rats (0.86±0.05versus 1.08±0.04 for vessels with inner diameters <50µm and 0.62±0.02 versus 0.75±0.04 for vesselswith inner diameters of 50 to 100 µm, P<.05). Theseresults indicate that chronic treatment with lovastatin shiftsthe relations between renal medullary blood flow, renal interstitialpressure, sodium excretion, and renal perfusion pressure tolower levels of arterial pressure and attenuates the developmentof hypertension and renal vascular hypertrophy in SHR.

Key Words: lovastatin • hypertension • rats, inbred SHR • natriuresis • hypertrophy

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