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Superoxide Excess in Hypertension and Aging
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There is evidence in humans that hypertension and aging similarly impair endothelial function, although the mechanism remains unclear. Superoxide anion (O
2
−
) is a major determinant of nitric oxide (NO) bioavailability and thus endothelial function. We sought to determine the relationship between endothelial function, O
2
−
, and age in normotensive Wistar-Kyoto (WKY) and stroke-prone spontaneously hypertensive rats (SHRSP). Aortic rings were removed from female WKY and SHRSP at 3 to 4 months (young) and 9 to 12 months (old). O
2
−
generation by aortic rings was measured before and after removal of the endothelium or incubation with
N
G
nitro-
l
-arginine methyl ester, diphenyleneiodonium, or apocynin. Levels of p22phox were studied with immunohistochemistry and used as a marker of NAD(P)H oxidase expression. NO bioavailability was significantly lower in old WKY compared with young WKY (
P
=0.0009) and in old SHRSP compared with young SHRSP (
P
=0.005). O
2
−
generation was significantly greater in old WKY compared with young WKY (
P
=0.0001). Removal of the endothelium and
N
G
nitro-
l
-arginine methyl ester treatment resulted in a significant reduction in O
2
−
generation in old SHRSP (
P
=0.009 and 0.001, respectively). Diphenyleneiodonium significantly reduced O
2
−
generation in 12-month WKY (
P
=0.008) and 12-month SHRSP (
P
=0.009). Apocynin attenuated O
2
−
generation by older WKY (
P
=0.038) and SHRSP (
P
=0.028). p22phox was increased in older animals compared with young. We conclude that NO bioavailability decreases with age in female WKY and SHRSP. O
2
−
generation increases with age in WKY and is higher in SHRSP and may contribute to the reduced NO by scavenging. NAD(P)H oxidase may contribute to the age-related increase in O
2
−
.
Ovid Technologies (Wolters Kluwer Health)
Title: Superoxide Excess in Hypertension and Aging
Description:
There is evidence in humans that hypertension and aging similarly impair endothelial function, although the mechanism remains unclear.
Superoxide anion (O
2
−
) is a major determinant of nitric oxide (NO) bioavailability and thus endothelial function.
We sought to determine the relationship between endothelial function, O
2
−
, and age in normotensive Wistar-Kyoto (WKY) and stroke-prone spontaneously hypertensive rats (SHRSP).
Aortic rings were removed from female WKY and SHRSP at 3 to 4 months (young) and 9 to 12 months (old).
O
2
−
generation by aortic rings was measured before and after removal of the endothelium or incubation with
N
G
nitro-
l
-arginine methyl ester, diphenyleneiodonium, or apocynin.
Levels of p22phox were studied with immunohistochemistry and used as a marker of NAD(P)H oxidase expression.
NO bioavailability was significantly lower in old WKY compared with young WKY (
P
=0.
0009) and in old SHRSP compared with young SHRSP (
P
=0.
005).
O
2
−
generation was significantly greater in old WKY compared with young WKY (
P
=0.
0001).
Removal of the endothelium and
N
G
nitro-
l
-arginine methyl ester treatment resulted in a significant reduction in O
2
−
generation in old SHRSP (
P
=0.
009 and 0.
001, respectively).
Diphenyleneiodonium significantly reduced O
2
−
generation in 12-month WKY (
P
=0.
008) and 12-month SHRSP (
P
=0.
009).
Apocynin attenuated O
2
−
generation by older WKY (
P
=0.
038) and SHRSP (
P
=0.
028).
p22phox was increased in older animals compared with young.
We conclude that NO bioavailability decreases with age in female WKY and SHRSP.
O
2
−
generation increases with age in WKY and is higher in SHRSP and may contribute to the reduced NO by scavenging.
NAD(P)H oxidase may contribute to the age-related increase in O
2
−
.
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