Gender Differences in the Effect of Age on Electrical Field Stimulation (EFS)-Induced Adrenergic Vasoconstriction in Rat Mesenteric Resistance Arteries

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Vol. 296, Issue 3, 782-788, March 2001

Gender Differences in the Effect of Age on Electrical Field Stimulation (EFS)-Induced Adrenergic Vasoconstriction in Rat Mesenteric Resistance Arteries

Jennifer C. Sullivan and Cathy A. Davison

Center for Cardiovascular Sciences, Albany Medical College, Albany, New York

	Abstract

Top Abstract Introduction Materials and Methods Results Discussion References

The objective of this study was to examine the effects of gender and age on electrical field stimulation (EFS)-induced vasoconstriction.Fisher 344 rats were studied: young females (YF, n = 38), youngmales (YM, n = 29), old females (OF, n = 33), and old males (OM,n = 30). Isolated mesenteric resistance arteries (endothelium-intactor denuded) were pressurized, and outer diameter was monitored.Dose-response curves were performed to KCl and phenylephrine (PE).EFS (0.1-16 Hz) responses were expressed as percentage of constrictionfrom baseline. Area under the curve (AUC) was calculated and comparisonswere made using analysis of variance and t tests. Females becameless responsive to EFS-induced constriction with age, whereasconstrictor responses among males were unaffected (AUC: YF = 454± 15, OF = 284 ± 22, p < 0.001; YM = 391 ± 35, OM = 357 ± 31,p = 0.22). Endothelial denudation produced a significant increasein EFS-induced constriction in OF and OM. Endothelium removalin OF increased the EFS constrictor response to the level seenin arteries from YF. BQ 123 (ET_A receptor antagonist) significantlydecreased EFS-induced constriction in YM and OM. In YM, SQ 29,548[thromboxane A₂ (TXA₂)/PGH₂ receptor antagonist] and indomethacindepressed constrictor responses. There were no differences amonggroups in the sensitivity to KCl, but YF were the most sensitiveto PE. In conclusion, EFS-induced vasoconstriction declined withage among females but not males. The decrease in EFS constrictorresponses in OF may be due to a selective decrease in vascularsmooth muscle sensitivity to adrenergic agonists and an increasein the production of an endothelium-derived vasodilator. Amongmales there is also an endothelin-1 and TXA₂/PGH₂ component toEFS-induced constriction that is absent amongfemales.

	Introduction

Top Abstract Introduction Materials and Methods Results Discussion References

Cardiovascular function is altered with age in men and women. It is well established that advancing age is a risk factor forthe development of cardiovascular disease. With advancing agethere are a number of structural alterations in the vasculature,which occur in otherwise healthy individuals as part of the normalaging process. With advancing age vascular function and reactivityare impaired, resulting in increased stiffness, decreased distensibilityand compliance, wall thickening (Folkow and Svanborg, 1993; Marin,1995), and impaired endothelial function (Egashira et al., 1993;Taddei et al., 1995; Gerhard et al., 1996).

Epidemiological evidence suggests that aging affects the cardiovascular system of men and women differently. Women have beenreported to lag behind men in coronary heart disease morbidity,as well as mortality rates, by approximately a decade (Castelli,1988; Celermajer et al., 1994). Castelli (1988) reported thatmen and women differ in the development of atherosclerotic lesions,with lesion onset occurring a decade earlier in men. Celermajeret al. (1994) reported that endothelial dysfunction occurs a decadeearlier in men than in women as assessed by flow-mediated dilationin response to reactivehyperemia.

In this study, we examined the effect of age on vascular adrenergic function in male and female rats. Animal studies examiningelectrical field stimulation (EFS) of adrenergic nerves in isolatedtail arteries have reported that arteries from male rats are moreresponsive to EFS-induced vasoconstriction compared with thosefrom females (Li and Duckles, 1994; Garcia-Villalon et al., 1996;Li et al., 1997). Li and Duckles (1994) reported that the observedgender difference in EFS-induced vasoconstriction was abolishedby ovariectomy of females, but unaffected by orchidectomy in males.An effect of gender on vascular smooth muscle sensitivity to adrenergicagonists has also been examined. Sensitivity and maximum responseto the $alpha$ -adrenergic receptor agonist norepinephrine has been reportedto be unaffected by gender in the rat tail artery, although followingorchidectomy in males, maximum response is decreased (Li and Duckles,1994). In the rat aorta sensitivity to norepinephrine is unaffectedby gender, however the maximum response is enhanced in males (Stalloneet al., 1991). These findings suggest that male sex hormones increasevascular smooth muscle sensitivity to adrenergic vasoconstriction.In regard to age, EFS-induced vasoconstriction has been reportedto decrease with age in isolated tail arteries from male Ivanos(Fouda and Atkinson, 1986), Wistar, and Fisher 344 rats (Thorinet al., 1994). In contrast, EFS-induced vasoconstriction has beenreported to be unaffected by advancing age in both femoral andrenal arteries isolated from male rats (Duckles et al., 1985;Duckles, 1987). In experiments examining the effect of age onadrenergic receptor sensitivity, the majority has revealed thatadvancing age does not alter vascular smooth muscle sensitivityto adrenergic agonists (Duckles et al., 1985; Docherty and Hyland,1986; Duckles, 1987; Elliott, 1988; Tsai et al., 1993). However,in the rat tail artery (Fouda and Atkinson, 1986) and aorta (Docherty,1988), advancing age has been reported to decrease vasoconstrictorsensitivity to $alpha$ -adrenergic receptoragonists.

Although studies have been done examining the effects of age or gender on the functional response of arteries to adrenergicnerve-induced vasoconstriction, no studies have examined the interactionof age and gender. A majority of the work that has been done toexamine the effect of gender on EFS-induced vasoconstriction hasfocused on responses in young animals. Studies that have beenperformed to examine the effects of aging on EFS-induced constrictorresponses have exclusively used male animals. Since cardiovascularfunction is known to be altered with advancing age, our studywas designed to examine the effects of age on EFS-induced vasoconstrictionin both male and female animals. We hypothesized that the effectof aging on EFS-induced vasoconstriction would differ in malesandfemales.

	Materials and Methods

Top Abstract Introduction Materials and Methods Results Discussion References

Animals

Male and female Fisher 344 rats of two different ages were used in this study: 3-month-old (young rats) and 26-month-old (senescent)rats. The rats were obtained from the colonies at the NationalInstitute on Aging and were barrier-raised. The rats were housedin individual Thoren cages (laminar airflow, autoclaved food,water, and bedding) in temperature- and humidity-controlled, light-cycled(6:00 AM-6:00 PM) quarters with ad libitum access to standardrat chow and water. Rats were fasted overnight before sacrifice.All procedures involving the use of animals were approved by theInstitutional Animal Care and Use Committee and conform to federal,state, and institutionalguidelines.

Preparation of Vascular Tissue

The rats were weighed and then euthanized using an overdose of sodium pentobarbital (120 mg/kg i.p.) followed by thoracotomy.A portion of the small intestine was removed and placed in coldphysiological salt solution of the following composition: 130mmol/l NaCl, 4.7 mmol/l KCl, 1.17 mmol/l MgSO₄·7H₂O, 1.18 mmol/lKH₂PO₄, 14.9 mmol/l NaHCO₃, 5.5 mmol/l dextrose, 0.03 mmol/l NaCa₂EDTA,and 1.6 mmol/l CaCl₂·2H₂O. Using a dissecting microscope, a mesentericresistance artery was isolated, cleared of fat and connectivetissue, and placed in a chamber of a dual-chambered arteriograph(Living Systems Instrumentation, Burlington, VT). One end of thevessel was cannulated with a glass microcannula and the vessellumen was rinsed with physiological salt solution to remove theblood. The distal end of the artery was then secured to anotherglass microcannula. The artery was secured to the cannulae usingnylon ties. The vessel was pressurized to 60 mm Hg and the pressurewas maintained using an automatic servo device (Living SystemsInstrumentation).

The artery was bathed by warmed (37°C), gassed (95% O₂, 5% CO₂) physiological salt solution, at a flow rate of 20 ml/min.The arteriograph was placed on the stage of an inverted microscopeand the outer diameter of the vessel was monitored using computerizedimage analysis consisting of a Framegrabber card (PCVision Plus)and appropriate software (Microsciences Incorporated, Seattle,WA). The vessel was allowed to equilibrate for 45 min. At thispoint the viability of the vessel was determined by contractingthe vessel with 1 µM phenylephrine (PE) followed by 10 µM acetylcholineto relax thevessel.

Electrical Field Stimulation-Induced Vasoconstriction

Electrical field stimulation was performed by securing two parallel platinum electrodes (Living Systems Instrumentation) oneither side of the isolated artery in the arteriograph. The electricalcurrent was driven by a Grass S48 stimulator set to the followingparameters: 0.3-ms delay, 0.5-ms duration, 10 V, and 60 mA. Betweenthe stimulator and the electrodes was placed a Stimu-SplitterII (Med-Lab Instruments, Loveland, CO), a device that serves tomodulate wave form distortion and allows for measurement of currentat theelectrodes.

The arteries were stimulated at each frequency (0.1, 0.5, 1, 2, 4, 8, and 16 Hz) until a steady-state response was obtainedand allowed to rest between stimulations (approximately 5 min)until the artery returned to the resting diameter. Following afrequency-response curve the artery was allowed to reequilibratefor 30 min and then a second curve was performed in the presenceof a pharmacological inhibitor. Preliminary studies confirmedthat multiple frequency-response curves could be performed reliably.To verify that adrenergic nerves mediated the response, frequency-responsecurves were performed in the absence and presence of the neurotoxintetrodotoxin (300 nM; Kawasaki et al., 1990) and the adrenergicnerve inhibitor guanethidine (5 µM; Li and Duckles, 1992).

Role of the Endothelium

To examine the role of the endothelium, frequency-response curves were performed in endothelium-denuded arteries. Endotheliumdenudation was accomplished by first rubbing the vessel lumenwith a human hair and then passing air bubbles through the lumen(Osol et al., 1989; Case and Davison, 1999). Denudation was verifiedby the absence of a vasodilator response to acetylcholine in avessel preconstricted with PE. The role of endothelium-derivedvasoactive factors was determined by performing frequency-responsecurves in the absence and presence of pharmacological inhibitors.Frequency-response curves were performed following a 10-min incubationwith the inhibitor. Endothelial-derived constricting factors wereexamined using the selective ET_A receptor antagonist BQ 123 (10µM; Awane-Igata et al., 1997) and the TXA₂/PGH₂ receptor antagonistSQ 29,548 (1 µM; Ward et al., 1990). The ET_A receptor has beendemonstrated to mediate ET-1-induced vasoconstriction, whereasthe TXA₂/PGH₂ receptor mediates the contractile responses of endogenouseicosanoids (Ward et al., 1990; Awane-Igata et al., 1997; Ergulet al., 1998). Endothelial-derived nitric oxide was examined usingthe nitric-oxide synthase inhibitor N-nitro-L-arginine (LNA; 100 µM; Case and Davison, 1999). The roleof endothelial-derived cyclooxygenase products was examined usingthe cyclooxygenase inhibitor indomethacin (10 µM; Case and Davison,1999).

Vasoconstrictor Studies

Cumulative concentration-response curves were performed in endothelium-intact arteries to 1) the $alpha$ -adrenergic receptor agonistPE (1 nM-10 µM) and 2) KCl [4.7-100 mM, in the presence of phentolamine(1 µM)]. Each concentration of agonist was added only after thevessel had reached a plateau from the previous dose. The vesselwas then rinsed with fresh physiological salt solution and allowedto reequilibrate for 30min.

Drugs

Acetylcholine, PE, LNA, indomethacin, tetrodotoxin, guanethidine, BQ 123, and phentolamine were all purchased from Sigma ChemicalCo. (St. Louis, MO). Buffer reagents, including KCl, were purchasedfrom Fisher Scientific (Pittsburgh, PA). SQ 29,548 was purchasedfrom Cayman Chemicals (Ann Arbor, MI). Stock solutions of acetylcholine(100 mM), phenylephrine (10 mM), LNA (10 mM), tetrodotoxin (1mM), guanethidine (5 mM), and KCl (3 M) were all made in distilledwater. Stock solutions for indomethacin (10 mM) and SQ 29,548(1 mM) were made in 95% ethanol. All further dilutions were madein water. The maximum ethanol concentration in the bath did notexceed 0.1%.

Statistical Analysis

Electrical Field Stimulation. All data are expressed as mean ± S.E.M. Frequency-response curves are expressed as percentage of constriction from baselinediameter. Curves were analyzed by calculating the area under thecurve (AUC; GraphPad Prism 2.01; GraphPad, San Diego, CA). Allstatistical analyses were performed using STATISTICA for Windows4.0 (StatSoft, Inc., Tulsa, OK). Control responses between thefour rat groups were compared using a two-way ANOVA (factor 1,age; factor 2, gender). Individual comparisons were then performedusing a Student-Newman-Keuls test. To analyze the effects of pharmacologicalinhibitors on the AUC, within-group comparisons were made usinga t test for dependent samples. Between-group comparisons weremade using repeated-measures ANOVA followed by t tests for independentsamples.

Dose-Response Curves. KCl and PE concentration-response curves are expressed as percentage of the maximum response. KCl and PE concentration-responsecurves were analyzed with nonlinear regression of sigmoidal dose-responsecurves (GraphPad Prism), which was used to calculate the EC₅₀(concentration of agonist that elicited 50% of the maximum response),maximum response, and slope. The negative log EC₅₀ values (pD₂)for KCl were compared using a two-way ANOVA. Since there weresignificant differences in the slope of the PE curves betweengroups, PE sensitivity was analyzed by calculating percentageof constriction at a threshold concentration of PE (0.16 µM).The percentage of constrictions was compared using a two-way ANOVA.Individual comparisons for both KCl and PE were then performedusing a Student-Newman-Keuls test. For all comparisons, p < 0.05was consideredsignificant.

	Results

Top Abstract Introduction Materials and Methods Results Discussion References

Effect of Age on EFS-Induced Adrenergic Vasoconstriction in Female and Male Rats. Frequency-response curves for arteries from females and males are shown in Fig. 1, A and B, respectively. Shown in Fig. 2are the integrated AUC values for the four rat groups. Baselinediameters (in µm) of the arteries at the beginning of the experimentwere as follows: young females (YF), 252 ± 5, and old females(OF), 280 ± 6; young males (YM), 261 ± 7, and old males (OM),276 ± 8. Arteries from YF were slightly but significantly smallerthan arteries isolated from OF and OM (YF versus OF, p = 0.0083;YF versus OM, p = 0.023). EFS produced a frequency-dependent vasoconstrictionin all rat groups (Fig. 1). Among the females there was a significantdecrease in EFS-induced adrenergic vasoconstriction with age (Figs.1A and 2). Advancing age had no effect on adrenergic vasoconstrictionamong the males (Figs. 1B and 2). YF were significantly more responsiveto EFS-induced constriction compared with the other rat groups,as indicated by a significantly greater AUC (Fig. 2). OF weresignificantly less responsive, indicated by a significantly lowerAUC compared with the other three rat groups (Fig. 2, AUC values,and Fig. 2, legend for p values). The adrenergic nature of theresponse was verified by complete blockade with either tetrodotoxinor guanethidine in all four rat groups (data not shown).

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Fig. 1. Effect of age on EFS-induced adrenergic vasoconstriction. Females exhibited a significant decline in EFS-induced vasoconstriction with advancing age (A). EFS-induced constriction was unaltered by age in males (B). See Fig. 2 for AUC values. Number in parentheses refers to the number of rats in each group. Values represent means ± S.E.M.

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Fig. 2. Responsiveness to EFS-induced vasoconstriction. YF were significantly more responsive to EFS compared with the other rat groups, as indicated by the asterisk (*) (YF versus OF, p < 0.001; YF versus YM, p = 0.024; YF versus OM, p = 0.0014). Old females were significantly less sensitive to EFS-induced vasoconstriction compared with the other groups, as indicated by the double asterisk (**) (OF versus YM, p = 0.00037; OF versus OM, p = 0.0090). Number in parentheses refers to the number of rats in each group. Values represent means ± S.E.M.

Effect of the Vascular Endothelium on EFS-Induced Adrenergic Vasoconstriction. Endothelial denudation significantly increased EFS-induced vasoconstriction in OF and OM, whereas constrictor responses inYF and YM were unaltered (Fig. 3, AUC values). Removal of theendothelium in OF increased the EFS constrictor responses to thelevel seen in denuded arteries from YF (N.S., p = 0.56).

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Fig. 3. Effect of endothelial denudation on EFS-induced vasoconstriction. Control ( $black-square$ ) and denuded (

). Denudation significantly increased EFS-induced vasoconstriction in OF (p = 0.0051) and OM (p = 0.047). Constrictor responses among YF (N.S., p = 0.47) and YM (N.S., p = 0.33) were not significantly altered. *Indicates significant difference from control. **Indicates significant difference between groups. n = 13 for YF and YM, n = 10 for OF and OM. Values represent means ± S.E.M.

The role of endothelial-derived vasoactive factors in modulating the EFS response was examined by incubating the arterieswith pharmacological inhibitors of endothelial-derived dilatorsand constrictors. The nitric-oxide synthase inhibitor LNA (100µM) did not alter EFS-induced vasoconstriction in any of the ratgroups (data not shown). The ET_A receptor antagonist BQ 123 significantlyreduced EFS-induced vasoconstriction in YM and OM, but did noteffect constrictor responses in YF or OF (Fig. 4A). The TXA₂/PGH₂receptor antagonist SQ 29,548 (Fig. 4B) and the cyclooxygenaseinhibitor indomethacin (Fig. 4C), significantly inhibited EFS-inducedconstriction only in YM. Constrictor responses among the remainingrat groups were not altered by either SQ 29,548 or indomethacin.

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Fig. 4. Effect of pharmacological inhibitors of endothelial-derived vasoconstrictors on EFS-induced vasoconstriction. BQ 123 (10 µM; A) significantly inhibited vasoconstriction in YM (p = 0.040) and OM (p = 0.020). Constrictor responses in YF (N.S., p = 0.60) and OF (N.S., p = 0.77) were unaffected. SQ 29,548 (1 µM, B) and indomethacin (10 µM, C) significantly inhibited EFS-induced constriction only in YM (SQ 29,548, p = 0.020; indomethacin, p = 0.0038). Constrictor responses in YF, OF, and OM were unaffected (YF: SQ 29,548, p = 0.86; indomethacin, p = 0.62; OF: SQ 29,548, p = 0.93; indomethacin, p = 0.07; OM: SQ 29,548, p = 0.17; indomethacin, p = 0.56). *Indicates significant difference from control. **Indicates significant difference between groups. Numbers in parentheses refer to the number of rats in each group. Values represent means ± S.E.M.

Effect of Gender and Age on Agonist-Induced Vasoconstriction. Cumulative concentration-response curves to PE in young and old, male and female rats are shown in Fig. 5. Baseline diameters(in µm) of the arteries at the beginning of the experiment wereas follows: YF, 265 ± 17; OF, 317 ± 16; YM, 259 ± 17; and OM,315 ± 13. Arteries from OM were slightly but significantly largerthan arteries isolated from YF and YM (OM versus YF, p = 0.029;OM versus YM, p = 0.036). Since we found the slope of the PE curveincreased significantly with age (data not shown), data were analyzedby calculating the constrictor response to PE at a threshold concentration(1.6 × 10⁷ M). Arteries isolated from YF were significantly more sensitiveto PE compared with arteries from the other three rat groups (Fig.5, see legend for % constriction values). There were no differencesin absolute maximum responses to PE (% constriction from baseline:YF, 50 ± 2; OF, 53 ± 2; YM, 51 ± 2; and OM, 55 ± 2) (N.S., p =0.62 for the effect of gender and p = 0.084 for the effect ofage).

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Fig. 5. Effect of gender and age on phenylephrine dose-response curves. YF were significantly more sensitive to a threshold concentration of PE than the other three rat groups (% constriction from baseline at 1.6 × 10⁷ M: YF = 39 ± 8, OF = 10 ± 5, YM = 16 ± 5, OM = 0.3 ± 0.2) (YF versus OF, p = 0.0066; YF versus YM, p = 0.013; YF versus OM, p = 0.00078). Numbers in parentheses refer to the number of rats in each group. Values represent means ± S.E.M.

Cumulative concentration-response curves to KCl are shown in Fig. 6. Baseline diameters (in µm) of the arteries at the beginningof the experiment were as follows: YF, 254 ± 11; OF, 306 ± 10;YM, 272 ± 12; and OM, 315 ± 10. Arteries isolated from YF andYM were slightly but significantly smaller than arteries isolatedfrom OF and OM (YF versus OF, p = 0.0076; YF versus OM, p = 0.0033;YM versus OF, p = 0.040; YM versus OM, p = 0.029). In responseto cumulative additions of KCl, there were no significant differencesin the pD₂ values among the rat groups (Fig. 6, see legend forpD₂ values). OF and OM had a significantly greater maximum responseto KCl compared with YF (% constriction from baseline: YF, 53± 2; OF, 58 ± 2; YM, 58 ± 2; and OM, 61 ± 2) (OF versus YF, p= 0.045; OM versus YF, p = 0.010).

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Fig. 6. Effect of gender and age on KCl dose-response curves. There were no significant differences in the pD₂ values for KCl between the rat groups (pD₂ values: YF = $-$ 1.3 ± 0.04, OF = $-$ 1.2 ± 0.04, YM = $-$ 1.2 ± 0.01, OM = $-$ 1.2 ± 0.02) (N.S., p = 0.64 for the effect of gender and p = 0.20 for the effect of age). Numbers in parentheses refer to the number of rats in each group. Values represent means ± S.E.M.

	Discussion

Top Abstract Introduction Materials and Methods Results Discussion References

In this study we found that in isolated mesenteric resistance arteries, there is a gender difference in EFS-induced adrenergicvasoconstriction. Arteries isolated from young females were moreresponsive to constriction relative to arteries isolated fromyoung males. With advancing age, there was a decline in EFS-inducedconstriction among females; however, advancing age has no effecton constrictor responses among males. These data suggest thatadvancing age effects vascular reactivity differently in malesand females. In addition, there were gender- and age-dependentalterations in the role of the vascular endothelium to modulateEFS-inducedvasoconstriction.

A selective enhancement in vascular smooth muscle sensitivity to $alpha$ -adrenergic receptor agonists among YF appears to accountfor the observed gender difference to EFS-induce vasoconstriction,as there were no differences in KCl sensitivity. There are a numberof possible mechanisms that may mediate the enhanced sensitivityamong YF. Adrenergic vasoconstriction is mediated primarily bythe binding of norepinephrine to $alpha$ ₁-adrenergic receptors locatedon vascular smooth muscle cells. Arteries from young females maypossess more $alpha$ ₁-adrenergic receptors than arteries from males,resulting in a greater amplification of the signal and enhancedvasoconstriction. Norepinephrine-mediated vasoconstriction isdependent upon increasing intracellular levels in Ca²⁺. Knot et al. (1999) reported that [Ca²⁺]_i is greater in endothelial cells of coronary arteries isolatedfrom female rats compared with males. Therefore, it is possiblethat vascular smooth muscle cells from females also have higher[Ca²⁺]_i, which would result in enhanced vasoconstriction. In addition,although in this study we only examined the overall constrictorresponse to EFS and postjunctional adrenergic receptor sensitivity,our data do not rule out the possibility of prejunctional neuronalchanges with advancingage.

In contrast to our findings, other investigators have reported a gender difference to EFS-induced vasoconstriction with tailarteries from young females being less responsive relative toarteries from males (Li and Duckles, 1994; Garcia-Villalon etal., 1996; Li et al., 1997). Li et al. (1997) reported that ovariectomy,but not orchidectomy, abolished this gender difference. Garcia-Villalonet al. (1996) reported no effect of gonadectomy on EFS-inducedvasoconstriction, although incubation of arteries with estradiolsignificantly decreased constrictor responses in males and females.These studies suggest that ovarian hormones depress adrenergicvasoconstriction. In reference to adrenergic agonists, in therat tail artery, sensitivity, as well as fractional norepinephrinerelease (Garcia-Villalon et al., 1996; Garcia-Villalon et al.,1997), have been reported to be unaffected by gender (Li and Duckles,1994; Li et al., 1997). In the rat mesentery, PE sensitivity hasbeen reported to decrease following estrogen replacement in ovariectomizedrats (Meyer et al., 1997; Zhang and Davidge, 1999).

Published experiments examining EFS-induced adrenergic vasoconstriction have primarily been performed using isolated rat tailarteries. Tail arteries are typically used in these studies dueto the fact that they are richly innervated by adrenergic nerves.Mesenteric arteries, however, are innervated by both adrenergicnerves as well as sensory nerves. In addition, tail and mesentericarteries serve very different functions in the body. The rat tailis a thermoregulatory organ. The tail artery allows the animalto modulate its body temperature by adjusting the amount of bloodin the tail via arterial constriction/dilation. Mesenteric arterieson the other hand have been demonstrated to be important in thecontrol of blood flow and regulation of systemic vascular resistance.For these reasons, responses found in the tail artery would notnecessarily be expected to be reproduced in resistancearteries.

With advancing age, we found a decrease in EFS-responsiveness and PE sensitivity among females but not males. In contrastto our results, published studies report that in other vascularbeds, EFS-induced vasoconstriction either declines or is unaffectedby advancing age. EFS-induced vasoconstriction in isolated tailarteries has been reported to decrease with age in male Ivanos,Wistar, and Fisher 344 rats (Fouda and Atkinson, 1986; Thorinet al., 1994) as well as subcutaneous resistance arteries fromhumans (Nielsen et al., 1992). In femoral and renal arteries isolatedfrom male Fisher 344 rats, EFS-induced vasoconstriction has beenreported to be independent of age (Duckles et al., 1985; Duckles,1987). In experiments examining vascular smooth muscle sensitivityto adrenergic agonists, investigators have reported either noeffect (Duckles et al., 1985; Docherty and Hyland, 1986; Duckles,1987; Elliott, 1988; Tsai et al., 1993) or a decrease in sensitivitywith age (Fouda and Atkinson, 1986; Docherty, 1988).

Although the basis for these discrepancies between our results and those of others is not obvious, possibilities include differencesin vascular beds and rat strains. Within Fisher 344 rats EFS-inducedvasoconstriction has been reported to decrease with age in tailarteries, whereas constrictor responses in femoral and renal arteriesare maintained. These results support the proposal that the vascularbed influences arterial reactivity. Our results however, do supportthe postulate that advancing age affects the vasculature of malesand females differently. More specifically, age-related alterationsin the vasculature enhance vasoconstriction in males relativeto females. The selective decline in adrenergic vasoconstrictionamong females with advancing age is mediated, at least in part,by a decrease in vascular smooth muscle sensitivity to adrenergicagonists. The mechanism mediating this decline may involve $alpha$ ₁-adrenergicreceptors, the signal transduction pathway or alterations in [Ca²⁺]_i.

We examined the role of the vascular endothelium in adrenergic nerve-induced vasoconstriction. Among YF the endothelium doesnot have a role to modulate constrictor responses. In YM, removalof the endothelium has no net effect on EFS-induced vasoconstriction.Among YM, however, the use of pharmacological inhibitors suggeststhat ET-1, constrictor cyclooxygenase products, and TXA₂ are releasedfrom the endothelium and enhance EFS-induced vasoconstriction.Since the magnitudes of the indomethacin and SQ 29,548 effectsare similar, it is possible that the constrictor cyclooxygenaseproduct is TXA₂. Therefore there is a gender difference in therole of the endothelium to modulate EFS-induced vasoconstriction,among males the endothelium liberates vasoconstrictors that enhanceEFS-inducedconstriction.

This finding suggests that the ET-1 and TXA₂/PGH₂ pathways of vasoconstriction are controlled differently in males and females.Although this study did not assess the functionality of the ET-1and TXA₂/PGH₂ pathways or receptors, the evidence suggests thatperhaps ET_A and TXA₂/PGH₂ receptors in arteries from males aremore sensitive to stimulation in response to EFS than in arteriesfrom females. Ergul et al. (1998) have demonstrated that in humansaphenous veins men have a greater density of ET_A receptors comparedwith women and a 2-fold greater contractile response to exogenousET-1. In addition, testosterone has been reported to increaseTXA₂/PGH₂ receptor density and sensitivity (Halushka et al., 1995).These studies suggest that the male gender has a greater contractileresponse to ET-1 and TXA₂/PGH₂, which may account for the genderdifference observed in our study in the effects of BQ 123 andSQ 29,548 on EFS-inducedvasoconstriction.

The fact that endothelial denudation has no net effect on EFS-induced vasoconstriction among YM, combined with evidence supportinga role for endothelium-derived constrictors, suggests that endothelium-derivedvasodilators are also being released, which counteract the effectof the constrictors. Cyclooxygenase inhibition decreased constriction,and inhibition of nitric-oxide synthase did not significantlyalter constriction, indicating that neither prostaglandin I₂ orNO are modulating constriction. Therefore, it is likely that EDHFis being liberated and is acting to dampen the constrictorresponse.

In contrast to our findings, there is evidence in the literature that the vascular endothelium functions, in part, to suppressadrenergic nerve-induced vasoconstriction. In the rat tail artery(Bucher et al., 1992; Li and Duckles, 1992), rat mesenteric artery(Nase and Boegehold, 1997), mesenteric arteries from monkeys (Tsuchiyaet al., 1994), and cerebral arteries from humans (Aldasoro etal., 1996) it has been reported that removal of the endothelium,or incubation with nitric-oxide synthase inhibitors, enhancesEFS-induced vasoconstriction. The enhanced EFS-induced vasoconstrictionin rat tail arteries (Vo et al., 1991; Li and Duckles, 1992),caudal arteries (Vo et al., 1992), and mesenteric arteries (Naseand Boegehold, 1997) following incubation with nitric-oxide synthaseinhibitors was lost in arteries denuded of their endothelium.Additionally, Boric et al. (1999) have recently demonstrated adirect correlation between EFS-induced norepinephrine releaseand increases in NO release and cGMP levels in the perfused ratmesentery. These studies suggest that endothelial-derived NO depressesconstrictorresponses.

Our study does not support a large role for endothelial modulation of adrenergic responses in young animals. However, a majorityof the studies described above were performed using only malerats. Those studies that did include female rats did not differentiatetheir findings between the genders. In addition, endothelial NOhas primarily been examined. Although our results do not supporta role for NO modulation of EFS-induced vasoconstriction, theendothelium-dependent vasodilator EDHF does appear to modulateconstrictor responses among YM. The ability of endothelium-derivedvasoconstrictors and EDHF to modulate EFS-induced constrictionhas been largely unexplored before this study and is a novel findingof thisstudy.

Endothelial denudation abolished the observed age effect among females and uncovered an age effect among males. The enhancedconstrictor response among old males and females following denudationsuggests that with advanced age there is an increase in the productionof an endothelium-derived vasodilator that normally acts to opposeconstriction. Pharmacological inhibitors of nitric-oxide synthaseand cyclooxygenase failed to enhance EFS-induced adrenergic vasoconstriction,suggesting that with advanced age there is an increase in theproduction of EDHF, which acts to antagonize vasoconstriction.Among old males there also appears to be a loss of endothelium-derivedTXA₂. The mechanism of this effect, either via a direct alterationin the function of the receptor or through a change in the signalingpathway, was not investigated in this study. Although there doesstill appear to be an ET-1 component to EFS-induced constrictionwith age in males, the overall effect of the endothelium is todepress, and not enhance, constriction. Therefore, taken together,the contribution of ET-1 to EFS-induced constriction may be negligible.These results do however support the postulate that endothelialfunction is altered differently in males and females with advancingage.

We conclude that there is a gender difference in EFS-induced adrenergic vasoconstriction, with YF being more sensitive toconstriction relative to YM. Advancing age affects adrenergicvasoconstriction differently in males and females. Among femalesthere is a decline in EFS-induced constriction with age, whereasadvancing age has no effect on constrictor responses among males.The decreased response among females is likely mediated by a decreasein vascular smooth muscle sensitivity to $alpha$ -adrenergic receptoragonists as well as an increase in the production of an EDHF fromthe vascular endothelium. In addition, there is a gender differencein the role of the endothelium to modulate EFS-induced vasoconstriction.Among YM, the endothelium liberates both vasodilators as wellas vasoconstrictors, whereas the endothelium has no role in EFS-mediatedconstrictor responses among YF. Furthermore, in both males andfemales, with advancing age the complement of factors releasedfrom the endothelium isaltered.

	Acknowledgment

We acknowledge the excellent technical assistance of Carlos O.Rivera.

	Footnotes

Accepted for publication November 3, 2000.

Received for publication July 28, 2000.

This work was supported by grants (to C.A.D.) from the National Institutes of Health (AG15658), the American Heart Association(9950341N), and (to J.C.S) Pharmaceutical Research and Manufacturersof AmericaFoundation.

This work is a part of the doctoral thesis of Jennifer C.Sullivan.

A portion of this work was previously presented in abstract form at Experimental Biology 2000 [Sullivan JC and Davison CA(2000) Effect of age and gender on electrical field stimulation(EFS)-induced vasoconstriction. FASEB J 14:A482.12].

Send reprint requests to: Dr. Jennifer C. Sullivan, Center for Cardiovascular Sciences, Albany Medical College, 47 New Scotland Ave., Albany, NY 12208. E-mail: jsullivan{at}mcg.edu

	Abbreviations

EFS, electrical field stimulation; PE, phenylephrine; ET, endothelin; TXA₂, thromboxane A₂; PGH₂, prostaglandin endoperoxide 2; LNA, N-nitro-L-arginine; AUC, area under the curve; ANOVA, analysis of variance; YF, young female; OF, old female; YM, young male; OM, old male; NO, nitric oxide; EDHF, endothelium-derived hyperpolarizing factor.

	References

Top Abstract Introduction Materials and Methods Results Discussion References

Aldasoro M, Martinez C, Vila JM, Medina P and Lluch S (1996) Influence of endothelial nitric oxide on adrenergic contractile responses of human cerebral arteries. J Cereb Blood Flow Metab 16: 623-628[Medline].
Awane-Igata Y, Ikeda S and Watanabe T (1997) Inhibitory effects of TAK-044 on endothelin induced vasoconstriction in various canine arteries and porcine coronary arteries: A comparison with selective ETA and ETB receptor antagonists. Br J Pharmacol 120: 516-522[Medline].
Boric MP, Figueroa XF, Donoso MV, Paredes A, Poblete I and Huidobro-Toro JP (1999) Rise in endothelium-derived NO after stimulation of rat perivascular sympathetic mesenteric nerves. Am J Physiol 277: H1027-H1035[Abstract/Free Full Text].
Bucher B, Ouedraogo S, Tschopl M, Paya D and Stoclet JC (1992) Role of L-arginine-NO pathway and of cyclic GMP in electrical field-induced noradrenaline release and vasoconstriction in the rat tail artery. Br J Pharmacol 107: 976-982[Medline].
Case J and Davison CA (1999) Estrogen alters relative contributions of nitric oxide and cyclooxygenase products to endothelium-dependent vasodilation. J Pharmacol Exp Ther 291: 524-530[Abstract/Free Full Text].
Castelli WP (1988) Cardiovascular disease in women. Am J Obstet Gynecol 158: 1553-1560[Medline], 1566-1567.
Celermajer DS, Sorensen KE, Spiegelhalter DJ, Georgakopoulos D, Robinson J and Deanfield JE (1994) Aging is associated with endothelial dysfunction in healthy men years before the age-related decline in women. J Am Coll Cardiol 24: 471-476[Abstract].
Docherty JR (1988) The effects of ageing on vascular $alpha$ -adrenoceptors in pithed rat and rat aorta. Eur J Pharmacol 146: 1-5[Medline].
Docherty JR and Hyland L (1986) $alpha$ -Adrenoceptor responsiveness in the aged rat. Eur J Pharmacol 126: 75-80[Medline].
Duckles SP (1987) Effects of norepinephrine uptake blockade on contractile responses to adrenergic nerve stimulation of isolated rat blood vessels: Influence of age. J Pharmacol Exp Ther 243: 521-526[Abstract/Free Full Text].
Duckles SP, Carter BJ and Williams CL (1985) Vascular adrenergic neuroeffector function does not decline in aged rats. Circ Res 56: 109-116[Abstract/Free Full Text].
Egashira K, Inou T, Hirooka Y, Kai H, Sugimachi M, Suzuki S, Kuga T, Urabe Y and Takeshita A (1993) Effects of age on endothelium-dependent vasodilation of resistance coronary artery by acetylcholine in humans. Circulation 88: 77-81[Abstract/Free Full Text].
Elliott HL (1988) $alpha$ ₁-Adrenoceptor responsiveness: The influence of age. J Cardiovasc Pharmacol 12 (Suppl 8): S116-S120.
Ergul A, Shoemaker K, Puett D and Tackett RL (1998) Gender differences in the expression of endothelin receptors in human saphenous veins in vitro. J Pharmacol Exp Ther 285: 511-517[Abstract/Free Full Text].
Folkow B and Svanborg A (1993) Physiology of cardiovascular aging. Pharmacol Rev 73: 725-755.
Fouda AK and Atkinson J (1986) Sensitivity to noradrenaline and electrical stimulation decreases with age in the rat tail artery. Naunyn-Schmiedeberg's Arch Pharmacol 334: 37-39[Medline].
Garcia-Villalon AL, Buchholz JN, Duckles SP and Krause DN (1997) Noradrenaline content and release in male and female rat tail arteries. J Cardiovasc Pharmacol 29: 93-96[Medline].
Garcia-Villalon AL, Buchholz JN, Krause DN and Duckles SP (1996) Sex differences in the effects of 17 $beta$ -estradiol on vascular adrenergic responses. Eur J Pharmacol 314: 339-345[Medline].
Gerhard M, Roddy MA, Creager SJ and Creager MA (1996) Aging progressively impairs endothelial-dependent vasodilation in forearm resistance vessels of humans. Hypertension 27: 849-853[Abstract/Free Full Text].
Halushka PV, Matsuda K, Masuda A, Ruff A, Morinelli TA and Mathur RS (1995) Testosterone regulation of platelet and vascular thromboxane A2 receptors. Agents Actions Suppl 45: 19-26[Medline].
Kawasaki H, Nuki C, Saito A and Takasaki K (1990) Role of calcitonin gene-related peptide-containing nerves in the vascular adrenergic neurotransmission. J Pharmacol Exp Ther 252: 403-409[Abstract/Free Full Text].
Knot HJ, Lounsbury KM, Brayden JE and Nelson MT (1999) Gender differences in coronary artery diameter reflect changes in both endothelial Ca²⁺ and ecNOS activity. Am J Physiol 276: H961-H969[Abstract/Free Full Text].
Li Y and Duckles SP (1992) Effect of endothelium on the actions of sympathetic and sensory nerves in the perfused rat mesentery. Eur J Pharmacol 210: 23-30[Medline].
Li Z and Duckles SP (1994) Influence of gender on vascular reactivity in the rat. J Pharmacol Exp Ther 268: 1426-1431[Abstract/Free Full Text].
Li Z, Krause DN, Doolen S and Duckles SP (1997) Ovariectomy eliminates sex differences in rat tail artery response to adrenergic nerve stimulation. Am J Physiol 272: H1819-H1825[Abstract/Free Full Text].
Marin J (1995) Age-related changes in vascular responses: A review. Mech Ageing Dev 79: 71-114[Medline].
Meyer MC, Cummings K and Osol G (1997) Estrogen replacement attenuates resistance artery adrenergic sensitivity via endothelial vasodilators. Am J Physiol 272: H2264-H2270[Abstract/Free Full Text].
Nase GP and Boegehold MA (1997) Endothelium-derived nitric oxide limits sympathetic neurogenic constriction in intestinal microcirculation. Am J Physiol 273: H426-H433[Abstract/Free Full Text].
Nielsen H, Hasenkam JM, Pilegaard HK, Aalkjaer C and Mortensen FV (1992) Age-dependent changes in $alpha$ -adrenoceptor-mediated contractility of isolated human resistance arteries. Am J Physiol 263: H1190-H1196[Abstract/Free Full Text].
Osol G, Cipolla M and Knutson S (1989) A new method for mechanically denuding the endothelium of small (50-150 µm) arteries with a human hair. Blood Vessels 26: 320-324[Medline].
Stallone JN, Crofton JT and Share L (1991) Sexual dimorphism in vasopressin-induced contraction of the rat aorta. Am J Physiol 266: H453-H458.
Taddei S, Virdis A, Mattei P, Ghiadoin L, Gennari A, Fasolo CB, Sudano I and Salvetti A (1995) Aging and endothelial function in normotensive subjects and patients with essential hypertension. Circulation 91: 1981-1987[Abstract/Free Full Text].
Thorin E, Capdeville-Atkinson C, Corman B and Atkinson J (1994) Sympathetic neurotransmission in the tail artery of aging rats. Br J Pharmacol 113: 363-368[Medline].
Tsai H, Buchholz J and Duckles SP (1993) Postjunctional $alpha$ ₂-adrenoceptors in blood vessels: Effect of age. Eur J Pharmacol 237: 311-316[Medline].
Tsuchiya K, Urabe M, Yamamoto R, Asada Y and Lee TJF (1994) Effects of N $omega$ -nitro-L-arginine and capsaicin on neurogenic vasomotor responses in isolated mesenteric arteries of the monkey. J Pharm Pharmacol 46: 155-157[Medline].
Vo PA, Reid JJ and Rand MJ (1991) Endothelial nitric oxide attenuates vasoconstrictor responses to nerve stimulation and noradrenaline in the rat tail artery. Eur J Pharmacol 199: 123-125[Medline].
Vo PA, Reid JJ and Rand MJ (1992) Attenuation of vasoconstriction by endogenous nitric oxide in rat caudal artery. Br J Pharmacol 107: 1121-1128[Medline].
Ward P, Ewan GB, Jordan CC, Ireland SJ, Hagan RM and Brown JR (1990) Potent and highly selective neurokinin antagonists. J Med Chem 33: 1848-1851[Medline].
Zhang Y and Davidge ST (1999) Effect of estrogen replacement on vasoconstrictor responses in rat mesenteric arteries. Hypertension 34: 1117-1122[Abstract/Free Full Text].

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