Affiliation:
1. From the Division of Nephrology and Hypertension and Hypertension, Kidney, and Vascular Health Center, Georgetown University, Washington, DC.
Abstract
Because defects in renal autoregulation may contribute to renal barotrauma in chronic kidney disease, we tested the hypothesis that the myogenic response is diminished by reduced renal mass. Kidneys from 5/6 nephrectomized mice had only a minor increase in the glomerular sclerosis index. The telemetric mean arterial pressure (108±10 mm Hg) was unaffected after 3 months of high-salt intake (6% salt in chow) or reduced renal mass. Afferent arterioles from 5/6 nephrectomized mice and sham-operated controls were perfused ex vivo during step changes in pressure from 40 to 134 mm Hg. Afferent arterioles developed a constriction and a linear increase in active wall tension above a perfusion pressure of 36±6 mm Hg, without a plateau. The slope of active wall tension versus perfusion pressure defined the myogenic response, which was similar in sham mice fed normal or high-salt diets for 3 months (2.90±0.22 versus 3.22±0.40 dynes · cm
−1
/mm Hg;
P
value not significant). The myogenic response was unaffected after 3 days of reduced renal mass on either salt diet (3.39±0.61 versus 4.04±0.47 dynes · cm
−1
/mm Hg) but was reduced (
P
<0.05) in afferent arterioles from reduced renal mass groups fed normal and high salt at 3 months (2.10±0.28 and 1.35±0.21 dynes · cm
−1
/mm Hg). In conclusion, mouse renal afferent arterioles develop a linear increase in myogenic tone around the range of ambient perfusion pressures. This myogenic response is impaired substantially in the mouse model of prolonged reduced renal mass, especially during high salt intake.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Cited by
30 articles.
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