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Am J Physiol Renal Physiol 289: F305-F313, 2005. First published April 12, 2005; doi:10.1152/ajprenal.00349.2004
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Differential effects of salt on renal hemodynamics and potential pressure transmission in stroke-prone and stroke-resistant spontaneously hypertensive rats

Isam Abu-Amarah,1 Anil K. Bidani,1 Rifat Hacioglu,2 Geoffrey A. Williamson,2 and Karen A. Griffin1

1Department of Internal Medicine, Loyola University Medical Center and Edward Hines Jr. Veterans Affairs Hospital, Maywood; and 2Department of Electrical and Computer Engineering, Illinois Institute of Technology, Chicago, Illinois

Submitted 16 September 2004 ; accepted in final form 9 March 2005

Salt-supplemented stroke-prone spontaneously hypertensive rats (SHRsp) develop more severe hypertension-induced renal damage (HIRD) compared with their progenitor SHR. The present studies were performed to examine whether in addition to increasing the severity of hypertension salt also enhanced the transmission of such hypertension to the renal vascular bed in the SHRsp. "Step" and "dynamic" renal blood flow (RBF) autoregulation (AR) were examined in ~12-wk-old SHR and SHRsp after 3–5 days of an 8% NaCl diet. During step AR under anesthesia (n = 8–11), RBF was significantly higher in the SHRsp at all perfusion pressures (P < 0.01), but AR capacity was not different. Similarly, in separate conscious chronically instrumented rats (n = 8 each), both blood pressure (BP) and RBF were modestly but significantly higher at baseline before salt in the SHRsp (P < 0.05). However, transfer function analysis did not show significant differences in the admittance gain parameters. However, after 3–5 days of salt, although average BP was not significantly altered in either strain, RBF increased further in the SHRsp and there was a significantly greater transfer of BP into RBF power in the SHRsp. This was reflected in the significantly higher admittance gain parameters at most frequencies including the heartbeat frequency (P < 0.05 maximum). These differential hemodynamic effects of salt have the potential to enhance BP transmission to the renal vascular bed and also contribute to the more severe HIRD observed in the salt-supplemented SHRsp.

autoregulation; myogenic response; genetics; nephrosclerosis



Address for reprint requests and other correspondence: K. A. Griffin, Loyola Univ. Medical Center, 2160 South First Ave., Maywood, IL 60153 (e-mail: kgriffi{at}lumc.edu)




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