TY - JOUR
T1 - Oral atorvastatin therapy increases nitric oxide-dependent cutaneous vasodilation in humans by decreasing ascorbate-sensitive oxidants
AU - Holowatz, Lacy A.
AU - Kenney, W. Larry
PY - 2011/9
Y1 - 2011/9
N2 - Elevated low-density lipoproteins (LDL) are associated with cutaneous microvascular dysfunction partially mediated by increased arginase activity, which is decreased following a systemic atorvastatin therapy. We hypothesized that increased ascorbate-sensitive oxidant stress, partially mediated through uncoupled nitric oxide synthase (NOS) induced by upregulated arginase, contributes to cutaneous microvascular dysfunction in hypercholesterolemic (HC) humans. Four microdialysis fibers were placed in the skin of nine HC (LDL = 177 ± 6 mg/dl) men and women before and after 3 mo of a systemic atorvastatin intervention and at baseline in nine normocholesterolemic (NC) (LDL = 95 ± 4 mg/dl) subjects. Sites served as control, NOS inhibited, L-ascorbate, and arginase-inhibited +L-ascorbate. Skin blood flow was measured while local skin heating (42°C) induced NO-dependent vasodilation. After the established plateau in all sites, 20 mM «ngname» was infused to quantify NO-dependent vasodilation. Data were normalized to maximum cutaneous vascular conductance (CVC) (sodium nitroprusside + 43°C). The plateau in vasodilation during local heating (HC: 78 ± 4 vs. NC: 96 ±2% CVCmax,, P < 0.01) and NO-dependent vasodilation (HC: 40 ± 4 vs. NC: 54 ± 4% CVCmax,, P < 0.01) was reduced in the HC group. Acute L-ascorbate alone (91 ± 5% CVCmax,, P < 0.001) or combined with arginase inhibition (96 ±3% CVCmax,, P < 0.001) augmented the plateau in vasodilation in the HC group but not the NC group (ascorbate: 96 ±2; combo: 93 ± 4% CVCmax,, both P > 0.05). After the atorvastatin intervention NO-dependent vasodilation was augmented in the HC group (HC postatorvastatin: 64 ±4% CVCmax,, P < 0.01), and there was no further effect of ascorbate alone (58 4% CVCmax,, P > 0.05) or combined with arginase inhibition (67 ±4% CVCmax,, P > 0.05). Increased ascorbate-sensitive oxidants contribute to hypercholesteromic associated cutaneous microvascular dysfunction which is partially reversed with atorvastatin therapy.
AB - Elevated low-density lipoproteins (LDL) are associated with cutaneous microvascular dysfunction partially mediated by increased arginase activity, which is decreased following a systemic atorvastatin therapy. We hypothesized that increased ascorbate-sensitive oxidant stress, partially mediated through uncoupled nitric oxide synthase (NOS) induced by upregulated arginase, contributes to cutaneous microvascular dysfunction in hypercholesterolemic (HC) humans. Four microdialysis fibers were placed in the skin of nine HC (LDL = 177 ± 6 mg/dl) men and women before and after 3 mo of a systemic atorvastatin intervention and at baseline in nine normocholesterolemic (NC) (LDL = 95 ± 4 mg/dl) subjects. Sites served as control, NOS inhibited, L-ascorbate, and arginase-inhibited +L-ascorbate. Skin blood flow was measured while local skin heating (42°C) induced NO-dependent vasodilation. After the established plateau in all sites, 20 mM «ngname» was infused to quantify NO-dependent vasodilation. Data were normalized to maximum cutaneous vascular conductance (CVC) (sodium nitroprusside + 43°C). The plateau in vasodilation during local heating (HC: 78 ± 4 vs. NC: 96 ±2% CVCmax,, P < 0.01) and NO-dependent vasodilation (HC: 40 ± 4 vs. NC: 54 ± 4% CVCmax,, P < 0.01) was reduced in the HC group. Acute L-ascorbate alone (91 ± 5% CVCmax,, P < 0.001) or combined with arginase inhibition (96 ±3% CVCmax,, P < 0.001) augmented the plateau in vasodilation in the HC group but not the NC group (ascorbate: 96 ±2; combo: 93 ± 4% CVCmax,, both P > 0.05). After the atorvastatin intervention NO-dependent vasodilation was augmented in the HC group (HC postatorvastatin: 64 ±4% CVCmax,, P < 0.01), and there was no further effect of ascorbate alone (58 4% CVCmax,, P > 0.05) or combined with arginase inhibition (67 ±4% CVCmax,, P > 0.05). Increased ascorbate-sensitive oxidants contribute to hypercholesteromic associated cutaneous microvascular dysfunction which is partially reversed with atorvastatin therapy.
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U2 - 10.1152/ajpregu.00220.2011
DO - 10.1152/ajpregu.00220.2011
M3 - Article
C2 - 21715698
AN - SCOPUS:80052416869
SN - 0363-6119
VL - 301
SP - R763-R768
JO - American Journal of Physiology - Regulatory Integrative and Comparative Physiology
JF - American Journal of Physiology - Regulatory Integrative and Comparative Physiology
IS - 3
ER -