Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation

Yau Chi Chan; Fung Ping Leung; Wing Tak Wong; Xiao Yu Tian; Lai Ming Yung; Chi Wai Lau; Suk Ying Tsang; Xiaoqiang Yao; Zhen Yu Chen; Yu Huang

doi:10.1161/ATVBAHA.110.203935

Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation

Yau Chi Chan, Fung Ping Leung, Wing Tak Wong, Xiao Yu Tian, Lai Ming Yung, Chi Wai Lau, Suk Ying Tsang, Xiaoqiang Yao, Zhen Yu Chen, Yu Huang

Research output: Journal Publications and Reviews › RGC 21 - Publication in refereed journal › peer-review

26 Citations (Scopus)

Abstract

Objective-: Selective estrogen receptor modulators (SERMs) inhibit constriction of mammalian conduit arteries. However, it is unknown whether SERMs at therapeutically achievable concentrations could reduce vascular tone in resistance arteries. The present study aimed to examine roles of Ca influx in endothelium and endothelial nitric oxide synthase (eNOS) activation in dilatations induced by raloxifene, a second-generation SERM in myogenically active arteries.Methods and results-: Small mesenteric arteries from Sprague-Dawley rats were isolated and mounted in a pressure myograph for measurement of changes in vessel diameter. [Ca]i images on native endothelial cells of intact arteries were determined by the fluorescence imaging technique, and phosphorylation of eNOS was assayed by Western blotting. Raloxifene (0.3 to 10 nmol/L) produced dilatations on established steady myogenic constriction. Female rat arteries dilated significantly more in response to raloxifene than male arteries. Raloxifene-induced dilatations of female arteries were blunted by N-nitro-l-arginine methyl ester but unaffected by 1400W, charybdotoxin plus apamin, wortmannin, or LY294002. Raloxifene (3 nmol/L) triggered rises in endothelial cell [Ca]i and increased eNOS phosphorylation at Ser1177. Both effects were greater in arteries from female rats than in arteries from male rats. Increases in endothelial cell [Ca]i and in eNOS phosphorylation were prevented by removal of extracellular Ca ions. Finally, ICI 182,780 did not affect the raloxifene-stimulated rise in endothelial cell [Ca]i, eNOS phosphorylation, and vasodilatations. Chronic raloxifene treatment reduced myogenic constriction in arteries from female but not male rats. Conclusion-: Raloxifene at therapeutically relevant concentrations inhibits myogenic constriction by an NO-dependent mechanism that causally involves the elevated [Ca]i in endothelial cells and subsequent eNOS activation. Raloxifene dilates resistance arteries more effectively in female rats, indicating its significant gender-related action on endothelial cells in microcirculation. © 2010 American Heart Association, Inc.

Original language	English
Pages (from-to)	992-999
Journal	Arteriosclerosis, Thrombosis, and Vascular Biology
Volume	30
Issue number	5
DOIs	https://doi.org/10.1161/ATVBAHA.110.203935
Publication status	Published - May 2010
Externally published	Yes

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Research Keywords

Endothelial nitric oxide synthase
Mesenteric artery
Myogenic tone
Raloxifene
Selective estrogen receptor modulator

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Chan, Y. C., Leung, F. P., Wong, W. T., Tian, X. Y., Yung, L. M., Lau, C. W., Tsang, S. Y., Yao, X., Chen, Z. Y., & Huang, Y. (2010). Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation. Arteriosclerosis, Thrombosis, and Vascular Biology, 30(5), 992-999. https://doi.org/10.1161/ATVBAHA.110.203935

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title = "Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation",

abstract = "Objective-: Selective estrogen receptor modulators (SERMs) inhibit constriction of mammalian conduit arteries. However, it is unknown whether SERMs at therapeutically achievable concentrations could reduce vascular tone in resistance arteries. The present study aimed to examine roles of Ca influx in endothelium and endothelial nitric oxide synthase (eNOS) activation in dilatations induced by raloxifene, a second-generation SERM in myogenically active arteries.Methods and results-: Small mesenteric arteries from Sprague-Dawley rats were isolated and mounted in a pressure myograph for measurement of changes in vessel diameter. [Ca]i images on native endothelial cells of intact arteries were determined by the fluorescence imaging technique, and phosphorylation of eNOS was assayed by Western blotting. Raloxifene (0.3 to 10 nmol/L) produced dilatations on established steady myogenic constriction. Female rat arteries dilated significantly more in response to raloxifene than male arteries. Raloxifene-induced dilatations of female arteries were blunted by N-nitro-l-arginine methyl ester but unaffected by 1400W, charybdotoxin plus apamin, wortmannin, or LY294002. Raloxifene (3 nmol/L) triggered rises in endothelial cell [Ca]i and increased eNOS phosphorylation at Ser1177. Both effects were greater in arteries from female rats than in arteries from male rats. Increases in endothelial cell [Ca]i and in eNOS phosphorylation were prevented by removal of extracellular Ca ions. Finally, ICI 182,780 did not affect the raloxifene-stimulated rise in endothelial cell [Ca]i, eNOS phosphorylation, and vasodilatations. Chronic raloxifene treatment reduced myogenic constriction in arteries from female but not male rats. Conclusion-: Raloxifene at therapeutically relevant concentrations inhibits myogenic constriction by an NO-dependent mechanism that causally involves the elevated [Ca]i in endothelial cells and subsequent eNOS activation. Raloxifene dilates resistance arteries more effectively in female rats, indicating its significant gender-related action on endothelial cells in microcirculation. {\textcopyright} 2010 American Heart Association, Inc.",

keywords = "Endothelial nitric oxide synthase, Mesenteric artery, Myogenic tone, Raloxifene, Selective estrogen receptor modulator",

author = "Chan, {Yau Chi} and Leung, {Fung Ping} and Wong, {Wing Tak} and Tian, {Xiao Yu} and Yung, {Lai Ming} and Lau, {Chi Wai} and Tsang, {Suk Ying} and Xiaoqiang Yao and Chen, {Zhen Yu} and Yu Huang",

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year = "2010",

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doi = "10.1161/ATVBAHA.110.203935",

language = "English",

volume = "30",

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Chan, YC, Leung, FP, Wong, WT, Tian, XY, Yung, LM, Lau, CW, Tsang, SY, Yao, X, Chen, ZY & Huang, Y 2010, 'Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation', Arteriosclerosis, Thrombosis, and Vascular Biology, vol. 30, no. 5, pp. 992-999. https://doi.org/10.1161/ATVBAHA.110.203935

Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation. / Chan, Yau Chi; Leung, Fung Ping; Wong, Wing Tak et al.
In: Arteriosclerosis, Thrombosis, and Vascular Biology, Vol. 30, No. 5, 05.2010, p. 992-999.

Research output: Journal Publications and Reviews › RGC 21 - Publication in refereed journal › peer-review

TY - JOUR

T1 - Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation

AU - Chan, Yau Chi

AU - Leung, Fung Ping

AU - Wong, Wing Tak

AU - Tian, Xiao Yu

AU - Yung, Lai Ming

AU - Lau, Chi Wai

AU - Tsang, Suk Ying

AU - Yao, Xiaoqiang

AU - Chen, Zhen Yu

AU - Huang, Yu

N1 - Publication details (e.g. title, author(s), publication statuses and dates) are captured on an “AS IS” and “AS AVAILABLE” basis at the time of record harvesting from the data source. Suggestions for further amendments or supplementary information can be sent to [email protected].

PY - 2010/5

Y1 - 2010/5

N2 - Objective-: Selective estrogen receptor modulators (SERMs) inhibit constriction of mammalian conduit arteries. However, it is unknown whether SERMs at therapeutically achievable concentrations could reduce vascular tone in resistance arteries. The present study aimed to examine roles of Ca influx in endothelium and endothelial nitric oxide synthase (eNOS) activation in dilatations induced by raloxifene, a second-generation SERM in myogenically active arteries.Methods and results-: Small mesenteric arteries from Sprague-Dawley rats were isolated and mounted in a pressure myograph for measurement of changes in vessel diameter. [Ca]i images on native endothelial cells of intact arteries were determined by the fluorescence imaging technique, and phosphorylation of eNOS was assayed by Western blotting. Raloxifene (0.3 to 10 nmol/L) produced dilatations on established steady myogenic constriction. Female rat arteries dilated significantly more in response to raloxifene than male arteries. Raloxifene-induced dilatations of female arteries were blunted by N-nitro-l-arginine methyl ester but unaffected by 1400W, charybdotoxin plus apamin, wortmannin, or LY294002. Raloxifene (3 nmol/L) triggered rises in endothelial cell [Ca]i and increased eNOS phosphorylation at Ser1177. Both effects were greater in arteries from female rats than in arteries from male rats. Increases in endothelial cell [Ca]i and in eNOS phosphorylation were prevented by removal of extracellular Ca ions. Finally, ICI 182,780 did not affect the raloxifene-stimulated rise in endothelial cell [Ca]i, eNOS phosphorylation, and vasodilatations. Chronic raloxifene treatment reduced myogenic constriction in arteries from female but not male rats. Conclusion-: Raloxifene at therapeutically relevant concentrations inhibits myogenic constriction by an NO-dependent mechanism that causally involves the elevated [Ca]i in endothelial cells and subsequent eNOS activation. Raloxifene dilates resistance arteries more effectively in female rats, indicating its significant gender-related action on endothelial cells in microcirculation. © 2010 American Heart Association, Inc.

AB - Objective-: Selective estrogen receptor modulators (SERMs) inhibit constriction of mammalian conduit arteries. However, it is unknown whether SERMs at therapeutically achievable concentrations could reduce vascular tone in resistance arteries. The present study aimed to examine roles of Ca influx in endothelium and endothelial nitric oxide synthase (eNOS) activation in dilatations induced by raloxifene, a second-generation SERM in myogenically active arteries.Methods and results-: Small mesenteric arteries from Sprague-Dawley rats were isolated and mounted in a pressure myograph for measurement of changes in vessel diameter. [Ca]i images on native endothelial cells of intact arteries were determined by the fluorescence imaging technique, and phosphorylation of eNOS was assayed by Western blotting. Raloxifene (0.3 to 10 nmol/L) produced dilatations on established steady myogenic constriction. Female rat arteries dilated significantly more in response to raloxifene than male arteries. Raloxifene-induced dilatations of female arteries were blunted by N-nitro-l-arginine methyl ester but unaffected by 1400W, charybdotoxin plus apamin, wortmannin, or LY294002. Raloxifene (3 nmol/L) triggered rises in endothelial cell [Ca]i and increased eNOS phosphorylation at Ser1177. Both effects were greater in arteries from female rats than in arteries from male rats. Increases in endothelial cell [Ca]i and in eNOS phosphorylation were prevented by removal of extracellular Ca ions. Finally, ICI 182,780 did not affect the raloxifene-stimulated rise in endothelial cell [Ca]i, eNOS phosphorylation, and vasodilatations. Chronic raloxifene treatment reduced myogenic constriction in arteries from female but not male rats. Conclusion-: Raloxifene at therapeutically relevant concentrations inhibits myogenic constriction by an NO-dependent mechanism that causally involves the elevated [Ca]i in endothelial cells and subsequent eNOS activation. Raloxifene dilates resistance arteries more effectively in female rats, indicating its significant gender-related action on endothelial cells in microcirculation. © 2010 American Heart Association, Inc.

KW - Endothelial nitric oxide synthase

KW - Mesenteric artery

KW - Myogenic tone

KW - Raloxifene

KW - Selective estrogen receptor modulator

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M3 - RGC 21 - Publication in refereed journal

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SN - 1079-5642

VL - 30

SP - 992

EP - 999

JO - Arteriosclerosis, Thrombosis, and Vascular Biology

JF - Arteriosclerosis, Thrombosis, and Vascular Biology

IS - 5

ER -

Therapeutically relevant concentrations of raloxifene dilate pressurized rat resistance arteries via calcium-dependent endothelial nitric oxide synthase activation

Abstract

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