Cannabinoid-Induced Hypotension and Bradycardia in Rats Is Mediated by CB1-Like Cannabinoid Receptors

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Vol. 281, Issue 3, 1030-1037, 1997

Cannabinoid-Induced Hypotension and Bradycardia in Rats Is Mediated by CB₁-Like Cannabinoid Receptors¹

Kristy D. Lake, David R. Compton, Karoly Varga, Billy R. Martin and George Kunos

Department of Pharmacology and Toxicology, Medical College of Virginia, Virginia Commonwealth University, Richmond, Virginia

	Abstract

Top Abstract Introduction Methods Results Discussion References

Previous studies indicate that the CB₁ cannabinoid receptor antagonist, N-(piperidin-1-yl)-5-(4-chlorophenyl)-1-(2,4-dichlorophenyl)-4-methyl-1H-pyrazole-3-carboxamideHCl (SR141716A), inhibits the anandamide- and $Delta$ ⁹-tetrahydrocannabinol- (THC) induced hypotension and bradycardiain anesthetized rats with a potency similar to that observed forSR141716A antagonism of THC-induced neurobehavioral effects. Tofurther test the role of CB₁ receptors in the cardiovascular effectsof cannabinoids, we examined two additional criteria for receptor-specificinteractions: the rank order of potency of agonists and stereoselectivity.A series of cannabinoid analogs including the enantiomeric pair(-)-11-OH- $Delta$ ⁹-THC dimethylheptyl (+)-11-OH- $Delta$ ⁹-THC dimethylheptyl were evaluated for their effects on arterialblood pressure and heart rate in urethane anesthetized rats. Sixanalogs elicited pronounced and long lasting hypotension and bradycardiathat were blocked by 3 mg/kg of SR141716A. The rank order of potencywas (-)-11-OH- $Delta$ ⁹-THC dimethylheptyl $>=$ (-)-3-[2-hydroxy-4-(1,1-dimethyl-heptyl)phenyl]-4-[3-hydroxy-propyl]cyclohexan-1-ol> (-)-3-[2-hydroxy-4-(1,1-dimethyl-heptyl)phenyl]-4-[3-hydroxy-propyl]cyclohexan-1-ol> THC > anandamide $>=$ (-)-3-[2-hydroxy-4-(1,1-dimethyl-heptyl)phenyl]-4-[3-hydroxy-propyl]cyclohexan-1-ol,which correlated well with CB₁ receptor affinity or analgesicpotency (r = 0.96-0.99). There was no hypotension or bradycardiaafter palmitoylethanolamine or (+)-11-OH- $Delta$ ⁹-THC dimethylheptyl. An initial pressor response was also observedwith THC and anandamide, which was not antagonized by SR141716A.We conclude that the similar rank orders of potency, stereoselectivityand sensitivity to blockade by SR141716A indicate the involvementof CB₁-like receptors in the hypotensive and bradycardic actionsof cannabinoids, whereas the mechanism of the pressor effect ofTHC and anandamide remains unclear.

	Introduction

Top Abstract Introduction Methods Results Discussion References

In anesthetized animals, the major psychoactive constituent of Cannabis sativa, THC, elicits a transient pressor responsefollowed by hypotension and bradycardia (Dewey et al., 1970; Grahamand Li, 1973; Estrada et al., 1987). In rats with genetic or surgicallyinduced hypertension, THC significantly lowers mean arterial bloodpressure to normotensive levels (Stark and Dews, 1980; Birmingham,1973; Nahas et al., 1973), and it has also been shown to preventimmobilization stress-induced hypertension (Williams and Ng, 1973).

Cannabinoid receptors have been identified in the rat by radioligand binding and autoradiography (Devane et al., 1988; Herkenhamet al., 1990). Subsequently, two cannabinoid receptors have beencloned: the CB₁ receptor located in the brain (Matsuda et al.,1990; Gerard et al., 1991), and in some peripheral organs (Shireet al., 1995; Ishac et al., 1996), and the CB₂ receptor identifiedin macrophages (Munro et al., 1993; Galiegue et al., 1995). Additionally,a splice variant of the CB₁ receptor, the CB_1A receptor has alsobeen described (Shire et al., 1995).

In 1992, an endogenous cannabinoid receptor ligand, anandamide (arachidonyl-2-ethanolamide), was extracted and purified fromporcine brain (Devane et al., 1992). As with THC, anandamide bindsto cannabinoid receptors (Vogel et al., 1993; Felder et al., 1993),inhibits adenylate cyclase via an inhibitory G-protein (Vogelet al., 1993), and inhibits voltage-gated N-type calcium channels(Felder et al., 1993). In neurobehavioral assays, anandamide hasbeen shown to mimic THC in terms of inducing catalepsy, hypomotility,hypothermia and analgesia (Fride et al., 1993; Smith, et al.,1994). We previously demonstrated that in anesthetized rats, anandamidecauses a pressor response followed by hypotension and mild bradycardia(Varga et al., 1995), and similar effects have been observed inboth conscious and anesthetized, spontaneously hypertensive rats(Lake et al., 1997). The hypotensive and bradycardic responsesto anandamide and THC are inhibited by the selective CB₁ receptorantagonist, SR141716A (Rinaldi-Carmona et al., 1994), which suggeststhe involvement of CB₁ receptors (Varga et al., 1995). Activationof these receptors was found to inhibit sympathetic tone via apresynaptic mechanism at peripheral sympathetic nerve terminals(Varga et al., 1996; Ishac et al., 1996). CB₁ receptors in thebrain that mediate the neurobehavioral effects of cannabinoidshave been characterized not only by their susceptibility to inhibitionby SR141716A (Rinaldi Carmona et al., 1994; Compton et al., 1996),but also by their selective interaction with cannabinoid enantiomers(Little et al., 1989). Furthermore, the rank order of potencyof various cannabinoid analogs for eliciting neurobehavioral effectscorrelates well with their binding affinities for the brain cannabinoidreceptor (Compton et al., 1992a, 1993). To further test whetherthe CB₁ receptors mediating neurobehavioral and cardiovasculareffects are pharmacologically similar, we analyzed the cardiovasculareffects of a series of cannabinoid analogs, including enantiomericpairs, in urethane-anesthetized rats. The results indicate thatthe pronounced hypotension and bradycardia induced by structurallydifferent cannabinoids are mediated by receptors that are pharmacologicallysimilar to brain CB₁ receptors mediating neurobehavioral effects.In contrast, the mechanism of the brief pressor response elicitedby some cannabinoids remains unclear.

	Methods

Top Abstract Introduction Methods Results Discussion References

Animals. Adult male Sprague-Dawley rats weighing 280 to 400 g were obtained from Harlan (Indianapolis, IN) and were housed in suspensioncages with food and water ad libitum. The animals were maintainedat 24 to 26°C under a 14:10 hr light/dark cycle and were allowedto acclimate for at least 1 wk before surgery.

Surgical preparation. Anesthesia was induced with diethyl ether and a femoral vein was cannulated for i.v. drug administration. Ether anesthesiawas then discontinued and urethane was administered (0.7 g/kg,i.v. + 0.3 g/kg, s.c.). Urethane administered according to thisprotocol does not depress basal blood pressure and does not interferewith cardiovascular regulatory mechanisms (Maggi and Meli, 1986).The femoral artery was cannulated and the catheter connected toa pressure transducer (Abbott, North Chicago, IL) for continuousmonitoring of BP with a physiograph (Astromed, Cortland, NY).HR was monitored via a tachograph preamplifier driven by the pressurewave. The trachea was cannulated with PE-160 tubing to maintainan open airway. Body temperature was maintained at 37 to 38°Cthroughout the experiments by using a water circulating heatingpad (Gaymar Industries, Orchard Park, NY) and rectal thermometer.

Experimental protocols. After a 30-min stabilization period, the animals received either vehicle or SR14716A (3 mg/kg, i.v.). Twenty min later, asingle dose of an agonist was administered, and the changes inBP and HR were monitored for 60 min. As agonist effects on BPand HR were long lasting for most of the drugs and doses tested,each animal was tested with a single dose of an agonist, aftereither vehicle or SR141716A.

Drugs. The chemical structure of the cannabinoid agonists used is illustrated in Figure 1. Anandamide (arachidonyl-2-ethanolamide)and 4 $'$ -(R)- and 4 $'$ -(S)-OH-diadduct- $Delta$ ⁹-THC (O-502 and O-522, respectively) were synthesized by Dr. RajRazdan (Organix Inc., Woburn, MA). HU-210 and HU-211 were synthesizedby Dr. Raphael Mechoulam (Hebrew University, Jerusalem, Israel).CP-55940 and SR141716A were provided by Dr. John Lowe at PfizerCentral Research. JWH-015 was synthesized by Dr. John Huffman(Clemson University). $Delta$ ⁹-THC was obtained from the National Institute on Drug Abuse. WIN-55212-2was purchased from Research Biochemicals International (Natick,MA). Palmitoylethanolamine was purchased from BIOMOL ResearchLaboratories, Inc. (Plymouth Meeting, PA). All drugs were dissolvedin 1:1:18 or 1:1:8 (emulphor-ethanol-saline). Emulphor (EL-620,a polyoxyethylated vegetable oil, GAF Corporation, Linden, NJ)is currently available as Alkmulphor. The dosing volume was 0.5to 1 ml/kg i.v., followed by a catheter line flush of 0.2 ml saline.Injection of the same volume of vehicle had no effect on bloodpressure or heart rate. All drugs were injected i.v. as bolusdoses over a 10- to 15-sec period.

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Fig. 1. Structure of cannabinoid agonists tested. Classical cannabinoids ( $Delta$ ⁹-THC, HU-210 and enantiomer HU-211), nonclassical compounds (CP-55940,WIN-55212-2, JWH-015, O-502 and stereoisomer O-522) and endogenousethanolamide conjugated fatty acids (anandamide and palmitoylethanolamide).

Data analysis. MAP was calculated as 1/3(systolic-diastolic BP) + diastolic BP. Basal MAP and HR for all groups was 102 ± 4.8 mmHg and 325± 5.4 bpm, respectively (n = 96). Time-dependent, agonist-inducedchanges in MAP and HR in the absence or presence of SR141716Awere compared using analysis of variance followed by Tukey's posthoc test. The ED₅₀ for each agonist was calculated using ALLFIT,a nonlinear sigmoidal curve-fitting program (DeLean et al., 1977).For anandamide and THC, which produce both a pressor and a subsequentdepressor response, ED₅₀s for both components were calculated,using the peak response minus predrug baseline value in both cases.The ED₅₀ for the depressor response to THC was calculated basedon the descending portion of the biphasic curve. Correlation analysisand generation of the Pearson product-moment coefficient was performedusing the StatView statistical package (Brainpower, Inc., AgouraHills, CA). Data are presented as mean ± S.E. of the mean.

	Results

Top Abstract Introduction Methods Results Discussion References

THC (0.02-10 mg/kg, fig. 2A) elicited an initial brief pressor response followed by prolonged and marked hypotension and bradycardia.Dose-response relationships for these latter effects were biphasicwith maximal hypotension (-62 ± 9 mmHg) observed at 2 mg/kg andmaximal bradycardia (-140 ± 24 bpm) observed at 8 mg/kg of THC,beyond which doses the hypotensive and bradycardic effects wereless pronounced (fig. 3). ED₅₀ values were 0.27 ± 0.09 mg/kg forthe hypotension and 0.62 ± 0.10 mg/kg for the bradycardic effect.Maximal decreases in BP and HR took 15 to 25 min to develop afterthe lower doses and 4 min after the 2 mg/kg dose, and each lastedmore than 60 min. Pretreatment with SR141716A (3 mg/kg) blockedthe hypotension and bradycardia elicited by the 4.0 mg/kg dose(fig. 2A). The initial pressor response (ED₅₀ = 2.47 ± 0.85 mg/kg,data not shown) was observed at doses of THC $>=$ 1 mg/kg, and wasnot antagonized by SR141716A (fig. 2A). No animal died followingany dose of THC.

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Fig. 2. Effects of classical cannabinoids on MAP and HR in anesthetized rats. A, Effects of THC (4 mg/kg, i.v.) after pretreatmentwith vehicle ( $black-square$ ) or SR141716A (3 mg/kg, i.v., $square$ ). B, Effects ofHU-210 (0.01 mg/kg i.v.) after vehicle ( $black-square$ ) or SR141716A (3 mg/kg,i.v., $square$ ) or HU-211 (1 mg/kg i.v.) after vehicle ( $black-triangle$ ). Data arepresented as mean ± S.E. (n = 5-9; *P < .05 from baseline, #P< .05 between groups).

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Fig. 3. Dose-dependent hypotension (A) and bradycardia (B) elicited by HU-210 ( $square$ ), CP-55940 ( $black-square$ ), WIN-55212-2 ( $triangle$ ), $Delta$ ⁹-THC ( $black-triangle$ ), anandamide ( $open circle$ ) and JWH-015 ( $bullet$ ). Each dose representsthe mean of three to six experiments. The average S.E. was lessthan 10% of the mean.

The stereoselectivity of cannabinoid-induced hypotension and bradycardia was evaluated using the enantiomers HU-210 and HU-211.At a dose of 0.01 mg/kg, HU-210 caused pronounced and long lastinghypotension and bradycardia without an initial pressor response(fig. 2B). In dose-response studies, HU-210 appeared to be morepotent in causing hypotension than in eliciting bradycardia, theED₅₀s for these being 0.0020 ± 0.0004 and 0.09 ± 0.01 mg/kg, respectively(fig. 3). Like THC, the effects of HU-210 were long lasting (fig.2B), and the maximal decrease in MAP and HR exceeded those ofTHC (fig. 3). Pretreatment with SR141716A (3 mg/kg) blocked thehypotension and bradycardia elicited by the 0.01 mg/kg dose ofHU-210 (fig. 2B). One in four animals died following the 0.3 mg/kgdose of HU-210, but none after lower doses. In contrast, the behaviorallyinactive isomer HU-211 caused no changes in BP at doses of 0.1and 1 mg/kg but, consistent with published observations (Mechoulamet al., 1992), caused a slowly developing increase in HR (fig.2B).

At a dose of 0.3 mg/kg, CP-55940 elicited pronounced hypotension and bradycardia without an initial pressor effect (fig. 4A),which was similar to the effects of HU-210. The ED₅₀ was 0.011± 0.002 mg/kg for the hypotension and 0.11 ± 0.05 mg/kg for thebradycardia. Maximal hypotension (-83 ± 3 mmHg) and bradycardia(-218 ± 10 bpm) developed within 4 to 10 min. Pretreatment withSR141716A (3 mg/kg) blocked both the hypotension and the bradycardiaelicited by 0.3 mg/kg CP-55,940 (fig. 4A). At a dose of 1 mg/kg,WIN-55212-2 also elicited long lasting hypotension and bradycardia,which developed within 1 to 5 min (fig. 4B). Similarly, WIN-55212-2caused no initial pressor effect at any of the doses tested andhad an ED₅₀ of 0.10 ± 0.02 mg/kg for hypotension and 0.29 ± 0.13mg/kg for bradycardia (fig. 3). Pretreatment with SR141716A (3mg/kg) blocked the hypotension, but only partially antagonizedthe bradycardia elicited by the 0.3 mg/kg dose of WIN-55212-2(fig. 4B). One in three animals died after the highest dose tested(10 mg/kg), but none after lower doses. The time-response curvefor both CP-55,940 and WIN-55212-2 was clearly biphasic, the reasonsfor which are not clear. The third compound in this class, JWH-015,was less potent than the first two, having an ED₅₀ of 10.1 ± 1.6mg/kg for hypotension and 16.4 ± 2.2 mg/kg for bradycardia (fig.3). Pretreatment with SR141716A (3 mg/kg) blocked the long lastinghypotension and bradycardia elicited by 10 mg/kg of JWH-015 (fig.4C). One in four animals died after the 20- and 30-mg/kg doses.As with CP-55,940 and WIN-55212-2, no initial pressor responsewas observed at any dose.

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Fig. 4. Effects of nonclassical cannabinoids on MAP and HR in anesthetized rats. A, Effects of CP-55940 (0.3 mg/kg, i.v.) after pretreatmentwith vehicle ( $black-square$ ) or SR141716A (3 mg/kg, i.v., $square$ ). B, Effects ofWIN-55212-2 (1 mg/kg, i.v.) after vehicle ( $black-square$ ) or SR141716A (3mg/kg, i.v., $square$ ). C, Effects of JWH-015 (10 mg/kg, i.v.) aftervehicle ( $black-square$ ) or SR141716A (3 mg/kg, i.v., $square$ ). Points representmeans ± S.E. from four experiments for each treatment group; *P< .05 from baseline and #P < .05 between groups.

The stereoisomers O-502 and O-522 did not elicit any change in BP or HR at doses of 0.5 or 5 mg/kg. At a dose of 30 mg/kg,a brief (<4 min) pressor response was observed after either O-502(+30 ± 6 mmHg) or O-522 (+41 ± 4 mm Hg). Both agents also causedmoderate, but long lasting tachycardia (O-502: +50 ± 4 bpm; O-522:+45 ± 8 bpm) at the 30-mg/kg dose. Neither of these two cannabinoidisomers binds to the CB₁ receptor or elicits neurobehavioral effectsin mice (table 1).

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TABLE 1
Summary of cardiovascular effects, receptor binding affinity in rat brain preparations and neurobehavioral effects in micefor selected cannabinoid compounds; compounds listed in descendingrank order of potency (top to bottom)

As described earlier (Varga et al., 1995), anandamide elicited an initial transient bradycardia followed by a brief pressorand a more prolonged depressor response that lasted less than15 min. During this latter hypotensive phase there was also moderatebradycardia (fig. 5). Dose-response studies yielded an ED₅₀ of2.5 ± 0.3 mg/kg for the hypotension with a peak change of -46± 3 mmHg, and an ED₅₀ of 2.5 ± 0.2 mg/kg for the bradycardia witha peak of -43 ± 15 bpm (fig. 3). Pretreatment with SR141716A (3mg/kg) inhibited the hypotension and parallel bradycardia elicitedby the 4.0-mg/kg dose (fig. 5). The initial transient vagal bradycardia/hypotensionand the subsequent brief pressor response that preceded the hypotensionwere not blocked by SR141716A (fig. 5). No animals died followingup to 30 mg/kg of anandamide. In contrast, palmitoylethanolaminedid not influence BP at doses of 1 to 20 mg/kg and caused a moderatedelayed tachycardia at the 4 and 20 mg/kg doses.

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Fig. 5. Effects of anandamide (4 mg/kg i.v.) on MAP and HR in anesthetized rats pretreated with vehicle ( $black-square$ ) or SR141716A (3 mg/kg,i.v., $square$ ). Points represent mean ± SE (n = 5-9); *P < .05 frombaseline and #P < .05 between groups.

As illustrated in figure 3, the rank order of potency of the six analogs that elicited hypotension and bradycardia was thesame for these two effects: HU-210 $>=$ CP-55940 > WIN-55212-2 >THC > anandamide > JWH-015. In earlier studies, similar rank ordersof potency have been determined for CB₁ receptor binding in ratbrain membranes and for various behavioral effects in mice (table1). Therefore, we determined the correlation between rat brainCB₁ receptor binding affinity (K_i) and the hypotensive and bradycardicED₅₀ values of the above six analogs. A significant positive correlationwas observed between hypotension (r = 0.97) and bradycardia (r= 0.96) to the binding affinity (fig. 6A). A similar, significantpositive correlation could be established between antinociceptivepotency in mice and either the hypotensive (r = 0.99) or the bradycardiceffects (r = 0.96) in rats (fig. 6B). Table 1 includes the absolutepotencies of the various analogs tested for eliciting hypotensionand bradycardia as determined in our study, and their potenciesin eliciting hypothermia, antinociception, ring-immobility andhypoactivity, as well as their receptor binding affinities.

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Fig. 6. A, Linear correlation between log K_i values for displacement of binding of ³H-CP-55,940 to rat brain membranes and log ED₅₀ values for maximalhypotension ( $black-square$ ) or bradycardia ( $bullet$ ), as shown on the abscissa.The correlation coefficient for hypotension was 0.97 (P < .05)and for bradycardia was 0.96 (P < .05). B, Linear correlationbetween log ED₅₀ values for antinociception and log ED₅₀s foreach compound for hypotension ( $black-square$ ) or bradycardia ( $bullet$ ). The correlationcoefficient for hypotension was 0.99 (P < .05) and for bradycardiawas 0.95 (P < .05).

	Discussion

Top Abstract Introduction Methods Results Discussion References

It has long been recognized that the major psychoactive constituent of marijuana, THC, can cause pronounced and long lastinghypotension and bradycardia (Vollmer et al., 1974; Siqueira etal., 1979). More recently, analogous effects have been describedfor the endogenous cannabinoid ligand, anandamide (Varga et al.,1995; 1996). We have reported that these effects are inhibitedby the CB₁ receptor antagonist SR141716A (Varga et al., 1995)and that the inhibitory potency of SR141716A against the hypotensiveresponse to THC or anandamide (Lake et al., 1997) was similarto its inhibitory potency against the neurobehavioral effectsof THC (Rinaldi-Carmona et al., 1994). This has suggested thatthe cannabinoid-induced hypotension and bradycardia are mediatedby CB₁-like receptors. In our study, we sought to further testthis hypothesis by analyzing the cardiovascular effects of a seriesof cannabinoid analogs including two pairs of enantiomers in urethane-anesthetizedrats. The analogs selected for testing belong to three classes:classical cannabinoids (THC, HU-210 and HU-211), nonclassicalcannabinoids (CP-55940, WIN-55212-2, JWH-015, O-502 and O-522),and endogenous ethanolamine-conjugated fatty acids (anandamideand palmitoylethanolamine). This should minimize the possibilitythat their effects may be related to a common structural featureunrelated to their interaction with cannabinoid receptors. Sixof the 10 analogs tested elicited hypotension and bradycardia,and they include compounds from all three classes. With the possibleexception of anandamide, the hypotension and bradycardia werevery pronounced and of long duration, with a clearly establishedrank order of potency. The involvement of specific receptors inthese effects is indicated by their marked stereoselectivity.The behaviorally active analog HU-210 (Little et al., 1989) displayedthe same high potency for hypotension (ED₅₀: 2 µg/kg) as for elicitingneurobehavioral effects (ED₅₀s of 2-4 µg/kg, see table 1), althoughit was somewhat less potent in eliciting bradycardia. A significantlylower potency of HU-210 to elicit hypotension (ED₅₀ $approx$ 50 µg/kg)was noted in Wistar rats, which may be related to the use of pentobarbitalas anesthetic (Vidrio et al., 1996). In contrast, the behaviorallyinactive enantiomer, HU-211, did not elicit hypotension at dosesup to 1 mg/kg, indicating a minimum of 500-fold stereoselectivity.At the 1-mg/kg dose, HU-211 elicited a moderate tachycardic effect,which is similar to earlier findings (Mechoulam et al., 1992),and thus is probably not mediated by cannabinoid receptors.

The ability of SR141716A to inhibit the hypotensive and bradycardic effects of all six analogs is in agreement with earlierobservations with THC and anandamide (Varga et al., 1995; Lakeet al., 1997). In a previous study, the AD₅₀ of SR141716A forinhibiting THC- or anandamide-induced hypotension and bradycardiain anesthetized rats was found to be in the range of 0.1 to 0.3mg/kg iv. (Lake et al., 1997). Our finding that a dose of 3 mg/kgSR141716A completely blocked the effects of most analogs is compatiblewith the involvement of CB₁ receptors in these effects. This possibilityis further supported by the significant positive correlation betweenthe potencies of the six analogs in eliciting hypotension andbradycardia and the binding affinity of these compounds or theiranalgesic potency in mice (fig. 6, table 1). However, despitethis strong correlation there are also some subtle differences.First, it is evident that the absolute potencies of the six analogstested for causing hypotension are slightly but consistently higherthan their potencies for eliciting neurobehavioral effects (table1). Second, the four most potent hypotensive analogs were appreciablyless potent in eliciting bradycardia than hypotension (table 1).Third, the hypotensive ED₅₀s of the three most potent analogs(HU-210 > CP-55940 > WIN-55212-2) vary over two orders of magnitude,whereas their binding K_is for CB₁ receptors are roughly equal(table 1). Finally, a dose of SR141716A that completely blockedthe hypotensive response to 1 mg/kg WIN-55212-2, only partiallyinhibited its bradycardic effect (fig. 4B). Although the existenceof a significant receptor reserve for the hypotensive action ordifferences in receptor coupling mechanisms may explain some ofthese discrepancies, we cannot exclude the possibility that theymay reflect the existence of different isoforms of CB₁ receptors.Such a possibility is also suggested by reports that certain cannabinoidanalogs devoid of neurobehavioral effects can elicit hypotensionin experimental animals (Adams et al., 1976; Zaugg and Kyncl,1983), which we were able to confirm and extend in the case ofabnormal cannabidiol (J. L. Wiley, E. J. N. Ishac, R. K. Razdan,B. R. Martin, K. Varga and G. Kunos, unpublished results).

Apart from the possibility of CB₁ receptor heterogeneity, it is also likely that the effects of some of the analogs are complexand involve more than one mechanism via CB₁ receptors locatedin different tissues. The results of our previous studies suggestthat the hypotensive action of anandamide is due to inhibitionof sympathetic tone (Varga et al., 1995), and a similar mechanismhas been proposed earlier for THC (Vollmer et al., 1974; Siqueiraet al., 1979). Additional evidence has eliminated the centralnervous system, sympathetic ganglia or postsynaptic sites in thevasculature or heart as possible sites of the sympathoinhibitoryaction of anandamide, and has suggested a presynaptic mechanismat sympathetic nerve terminals (Varga et al., 1996). Indeed, thispossibility is strongly supported by the demonstration of a CB₁receptor-mediated inhibition of exocytotic norepinephrine releaseinduced by anandamide or THC in isolated cardiac tissue or vasdeferens, and by the presence of CB₁ receptor mRNA in a sympatheticganglion (Ishac et al., 1996). However, in our experiments thethree most potent hypotensive analogs, CP-55,940, HU-210 and WIN-55212-2lowered MAP by more than 80 mmHg (see table 1), which far exceedsthe decrease in MAP caused by removing sympathetic tone. In aprevious study done in the same strain of rats under identicalconditions, the hypotensive response to anandamide was no longerpresent after alpha-adrenergic blockade with 2 mg/kg phentolamine,which lowered MAP from the same resting level by 51 ± 3 mmHg (Vargaet al., 1995). Therefore, CB₁ receptors other than those locatedpresynaptically on sympathetic nerve terminals must contributeto the hypotensive effect of the more potent and efficacious cannabinoids.

Anandamide has been shown to bind to CB₁ as well as CB₂ receptors in transfected cell lines (Showalter et al., 1996), whereasa saturated analog, palmitoylethanolamine, has been found to bindto the rat CB₂ receptor (Facci et al., 1995) but not to the CB₁receptor (Devane et al., 1992; Felder et al., 1993) or to thehuman CB₂ receptor (Showalter et al., 1996). Our finding thatpalmitoylethanolamine did not elicit any change in blood pressureand caused moderate tachycardia argues against the possible roleof CB₂ receptors in the hypotensive and bradycardic effects. Thelack of CB₂ receptor involvement in these cannabinoid-inducedeffects is also suggested by their potent inhibition by SR141716A,an antagonist with 60-fold lower affinity for CB₂ (K_i: 702 nM)than for CB₁ receptors (K_i: 12.3 nM, Showalter et al., 1996).Conclusive evidence against CB₂ receptor involvement awaits thedevelopment of a selective and potent CB₂ receptor antagonist.

Of the 10 compounds evaluated, only four elicited a transient pressor response: anandamide, THC, O-502 and O-522. The anandamide-and THC-induced pressor response was not CB₁ receptor-mediatedas it was not attenuated by SR141716A. The involvement of CB₂receptors is also unlikely, because JWH and WIN-55212-2 are evenmore potent at CB₂ than at CB₁ receptors (Showalter et al., 1996),yet they produced no pressor effect. O-502 and its stereoisomerO-522, which are both devoid of cannabinoid-like neurobehavioraleffects and do not bind to cannabinoid receptors (table 1), didnot alter MAP or HR at the lower doses tested and caused a moderatepressor response and tachycardia only at a dose of 30 mg/kg. Thissuggests that the pressor and tachycardic effects are not mediatedby cannabinoid receptors and may result from a nonreceptor- mediateddirect effect on vascular smooth muscle, or an indirect effectvia release of a vasoconstrictor agent. Sympathetic activationcan be excluded as the underlying mechanism, in view of the earlierfinding that spinal cord transection or alpha-adrenergic receptorblockade does not attenuate the pressor response to THC (Siqueiraet al., 1979) or anandamide (Varga et al., 1995).

In summary, we have found that several cannabinoids, including anandamide, elicit hypotension and bradycardia. These effectsare dose-dependent, antagonized by SR141716A, enantioselectiveand display a similar same rank order of potency as observed forbinding to CB₁ receptors in rat brain preparations and for elicitingantinociception in mice. All this indicates that the hypotensionand bradycardia elicited by cannabinoids is mediated by a CB₁-likecannabinoid receptor. However, due to subtle differences in agonistpotencies for the different effects of cannabinoids and in theinhibitory effects of SR141617A, the possible existence of CB₁receptor isoforms cannot be excluded. Further studies are aimedat identifying cannabinoid analogs that cause hypotension butare devoid of neurobehavioral effects, and thus may prove of interestin the management of hypertension.

	Acknowledgments

The authors thank Dr. Raj Razdan for the synthesis of anandamide, O-502 and O-522, Dr. John Lowe for providing SR141716A,Dr. John Huffman for synthesis of JWH-015 and Dr. Raphael Mechoulamfor the synthesis of HU-210 and HU-211.

	Footnotes

Accepted for publication February 19, 1997.

Received for publication October 3, 1996.

¹ This work was supported by NIH Grants HL-49938 to G.K., DA-09789 to B.R.M. and AHA Virginia Affiliate Grant VA-96-GS7 to K.V.Support for K.D.L. was by NIH training Grant DA07027.

Send reprint requests to: Dr. G. Kunos, Department of Pharmacology & Toxicology, Medical College of Virginia, Virginia Commonwealth University, P.O. Box 980613, Richmond, VA 23298-0613.

	Abbreviations

THC, $Delta$ ⁹-tetrahydrocannabinol; CP-55, 940, (-)-3-[2-hydroxy-4-(1,1-dimethyl-heptyl)phenyl]-4-[3-hydroxy-propyl]cyclohexan-1-ol; HU-210, (-)-11-OH- $Delta$ ⁹-THC dimethylheptyl; HU-211, (+)-11-OH- $Delta$ ⁹-THC dimethylheptyl; WIN-55212-2, O-502, {(R)-(+)-[2,3-dihydro-5-methyl-3-[(4-morpholinyl)methyl]pyrrolo[1,2,3-de]-1,4-benzoxazin-6-yl]-(1-naphthalenyl) methanone}JWH-015, (-)-3-[2-hydroxy-4-(1,1-dimethyl-heptyl)phenyl]-4-[3-hydroxy-propyl]cyclohexan-1-ol; O-502, 4 $'$ -(R)-OH-diadduct- $Delta$ ⁹-THC; O-522, 4 $'$ -(S)-OH-diadduct- $Delta$ ⁹-THC; SR141716A, N-(piperidin-1-yl)-5-(4-chlorophenyl)-1-(2,4-dichlorophenyl)-4-methyl-1H-pyrazole-3-carboxamide HCl; ABN-CBD, abnormal-cannabidiol; MAP, mean arterial blood pressure; HR, heart rate; bpm, beats per minute; ED₅₀, agonist dose producing half-maximal effect, AD₅₀, antagonist dose causing 50% inhibition of agonist response.

	References

Top Abstract Introduction Methods Results Discussion References

Adams, M. D., Earnhardt, J. T., Dewey, W. L. and Harris, L. S.: Vasoconstrictor actions of $Delta$ ⁸- and $Delta$ ⁹-tetrahydrocannabinol in the rat. J. Pharmacol. Exp. Ther. 196: 649-656, 1976[Abstract/Free Full Text].
Adams, M. D., Earnhardt, J. T., Martin, B. R., Harris, L. S., Dewey, W. L. and Razdan, R. K.: A cannabinoid with cardiovascular activity but no overt behavioral effects. Experientia 33: 1204-1205, 1977[Medline].
Birmingham, M. K.: Reduction by $Delta$ ⁹-tetrahydrocannabinol of the blood pressure of hypertensive rats bearing regenerated adrenal glands. Br. J. Pharmacol. 48: 169-171, 1973[Medline].
Compton, D. R., Gold, L. H., Ward, S. J., Balster, R. L. and Martin, B. R.: Aminoalkylindole analogs: Cannabimimetic activity of a class of compounds structurally distinct from $Delta$ ⁹-tetrahydrocannabinol. J. Pharmacol. Exp. Ther. 263: 1118-1126, 1992a[Abstract/Free Full Text].
Compton, D. R., Johnson, M. R., Melvin, L. S. and Martin, B. R.: Pharmacological profile of a series of bicyclic cannabinoid analogs: Classification as cannabimimetic agents. J. Pharmacol. Exp. Ther. 260: 201-209, 1992b[Abstract/Free Full Text].
Compton, D. R., Rice, K. C., De Costa, B. R., Razdan, R. K., Melvin, L. S., Johnson, M. R. and Martin, B. R.: Cannabinoid structure-activity relationships: Correlation of receptor binding and in vivo activities. J. Pharmacol. Exp. Ther. 265: 218-226, 1993[Abstract/Free Full Text].
Compton, D. R., Aceto, M. D., Lowe, J. and Martin, B. R.: In vivo characterization of a specific cannabinoid receptor antagonist (SR141716A): Inhibition of $Delta$ ⁹-tetrahydrocannabinol-induced responses and apparent agonist activity. J. Pharmacol. Exp. Ther. 277: 586-594, 1996[Abstract/Free Full Text].
DeLean, A., Munson, P. and Rodbard, D.: Simultaneous analysis of families of sigmoidal curves: Application to bioassay, radioligand assay, and physiological dose-response curves. Am. J. Physiol. 235: E97-E102, 1977.
Devane, W. A., Dysarz, F. A., Johnson, M. R., Melvin, L. S. and Howlett, A. C.: Determination and characterization of a cannabinoid receptor in rat brain. Mol. Pharmacol. 34: 605-613, 1988[Abstract].
Devane, W. A., Hanus, L., Breuer, A., Pertwee, R. G., Stevenson, L. A., Griffin, G., Gibson, D., Mandelbaum, A., Etinger, A. and Mechoulam, R.: Isolation and structure of a brain constituent that binds to the cannabinoid receptor. Science 258: 1946-1949, 1992[Abstract/Free Full Text].
Dewey, W. L., Harris, L. S., Howes, J. F., Kennedy, J. S., Granchelli, F. E., Pars, H. G. and Razdan, R. K.: Pharmacology of some marijuana constituents and two heterocyclic analogues. Nature 226: 1265-1276, 1970[Medline].
Estrada, U., Brase, D. A., Martin, B. R. and Dewey, W. L.: Cardiovascular effects of $Delta$ ⁹- and $Delta$ ⁹⁽¹¹⁾-tetrahydrocannabinol and their interaction with epinephrine. Life Sci. 41: 79-87, 1987[Medline].
Facci, L., Toso, D., Romanello, S., Buriani, A., Skaper, S. D. and Leon, A.: Mast cells express a peripheral cannabinoid receptor with differential sensitivity to anandamide and palmitoylethanolamide. Proc. Natl. Acad. Sci. U.S.A. 92: 3376-3380, 1995[Abstract/Free Full Text].
Felder, C. C., Briley, E. M., Axelrod, J., Simpson, J. T., Mackie, K. and Devane, W. A.: Anandamide, an endogenous cannabimimetic eicosanoid, binds to the cloned human receptor and stimulates receptor-mediated signal transduction. Proc. Natl. Acad. Sci. U.S.A. 90: 7656-7660, 1993[Abstract/Free Full Text].
Fride, E. and Mechoulam, R.: Pharmacological activity of the cannabinoid receptor agonist, anandamide, a brain constituent. Eur. J. Pharmacol. 231: 313-314, 1993[Medline].
Galiegue, S., Mary, S., Marchand, J., Dussossoy, D., Carriere, D., Carayon, P., Bouboula, M., Shire, D., Le Fur, G. and Casellas, P.: Expression of central and peripheral cannabinoid receptors in human immune tissues and leukocyte subpopulations. Eur. J. Biochem. 232: 54-61, 1995[Medline].
Gerard, C. M., Mollereau, C., Vassart, G. and Parmentier, M.: Molecular cloning of a human brain cannabinoid receptor which is also expressed in testis. Biochem. J. 279: 129-134, 1991.
Graham, J. D. P. and Li, D. M. F.: Cardiovascular and respiratory effects of cannabis in cat and rat. Br. J. Pharmacol. 49: 1-10, 1973[Medline].
Herkenham, M., Lynn, A. B., Little, M. D., Johnson, M. R., Melvin, L. S., De Costa, B. R. and Rice, K. C.: Cannabinoid receptor localization in brain. Proc. Natl. Acad. Sci. U.S.A. 87: 1932-1936, 1990[Abstract/Free Full Text].
Ishac, E. J. N., Jiang, L., Lake, K. D., Varga, K., Abood, M. A. and Kunos, G.: Inhibition of exocytotic noradrenaline release by presynaptic cannabinoid CB1 receptors on peripheral sympathetic nerves. Br. J. Pharmacol. 118: 2023-2028, 1996[Medline].
Kuster, J. E., Stevenson, J. I., Ward, S. J., D'Ambra, T. E. and Haycock, D. A.: Aminoalkylindole binding in rat cerebellum: Selective displacement by natural and synthetic cannabinoids. J. Pharmacol. Exp. Ther. 264: 1352-1363, 1993[Abstract/Free Full Text].
Lake K. D., Martin, B. R., Kunos, G. and Varga, K.: Cardiovascular effects of anandamide in anesthetized and conscious normotensive and spontaneously hypertensive rats. Hypertension. In press, 1997.
Little, P. J., Compton, D. R., Mechoulam, R. and Martin, B. R.: Stereochemical effects of 11-OH- $Delta$ ⁸-THC-dimethylheptyl in mice and dogs. Pharmacol. Biochem. Behav. 32: 661-666, 1989[Medline].
Little, P. J., Compton, D. R., Johnson, M. R., Melvin, L. S. and Martin, B. R.: Pharmacology and stereoselectivity of structurally novel cannabinoids in mice. J. Pharmacol. Exp. Ther. 247: 1046-11051, 1988[Abstract/Free Full Text].
Maggi, C. A. and Meli, A.: Suitability of urethane for physio-pharmacological investigations in various systems. Experientia 42: 109-115, 1986[Medline].
Matsuda, L. A., Lolait, S. J., Brownstein, M. J., Young, A. C. and Bonner, T. I.: Structure of a cannabinoid receptor and functional expression of the cloned cDNA. Nature 346: 561-564, 1990[Medline].
Mechoulam, R., Devane, W. A. and Glaser, R.: Cannabinoid geometry and biological activity. In: Marijuana/cannabinoids: neurobiology and neurophysiology, ed. by L. Murphy and A. Bartke, pp. 1-33, CRC Press, Boca Raton, FL, 1992.
Munro, S., Thomas, K. L. and Abu-Shaar, M.: Molecular characterization of a peripheral receptor for cannabinoids. Nature 365: 61-65, 1993[Medline].
Nahas, G. G., Schwartz, I. W., Adamec, J. and Manger, W. M.: Tolerance to delta-9-tetrahydrocannabinol in the spontaneously hypertensive rat. Proc. Soc. Exp. Biol. Med. 142: 58-60, 1973[Medline].
Rinaldi-Carmona, M., Barth, F., Heaulme, M., Shire, D., Calandra, B., Congy, C., Martinez, S., Maruani, J., Neliat, G., Caput, D., Ferrara, P., Soubrie, P., Breliere, J. C. and Le Fur, G.: SR141716A, a potent and selective antagonist of the brain cannabinoid receptor. FEBS Lett. 350: 240-244, 1994[Medline].
Shire, D., Carillon, C., Kaghad, M., Calandra, B., Rinaldi-Carmona, M., LeFur, G. and Ferrara, P.: An amino-terminal variant of the central cannabinoid receptor resulting from alternative splicing. J. Biol. Chem. 270: 3726-3731, 1995[Abstract/Free Full Text].
Showalter, V. M., Compton, D. R., Martin, B. R. and Abood, M. A.: Evaluation of binding in a transfected cell line expressing a peripheral cannabinoid receptor (CB₂): Identification of cannabinoid receptor subtype selective ligands. J. Pharmacol. Exp. Ther. 278: 989-999, 1996[Abstract/Free Full Text].
Siqueira, S. W., Lapa, A. J. and Do Valle, J. R.: The triple effect induced by $Delta$ ⁹-tetrahydrocannabinol on the rat blood pressure. Eur. J. Pharmacol. 58: 351-357.
Smith, P. B., Compton, D. R., Welch, S. P., Razdan, R. K., Mechoulam, R. and Martin, B. R.: The pharmacological activity of anandamide, a putative endogenous cannabinoid, in mice. J. Pharmacol. Exp. Ther. 270: 219-227, 1994[Abstract/Free Full Text].
Stark, P. and Dews, P. B.: Cannabinoids II. Cardiovascular effects. J. Pharmacol. Exp. Ther. 214: 131-138, 1980[Free Full Text].
Varga, K., Lake, K., Martin, B. R. and Kunos, G.: Novel antagonist implicates the CB₁ cannabinoid receptor in the hypotensive action of anandamide. Eur. J. Pharmacol. 278: 279-283, 1995[Medline].
Varga, K., Lake, K. D., Huangfu, D., Guyenet, P. G. and Kunos, G.: Mechanism of the hypotensive action of anandamide in anesthetized rats. Hypertension 28: 682-686, 1996[Abstract/Free Full Text].
Vogel, Z., Barg, J., Levy, R., Saya, D., Heldman, E. and Mechoulam, R.: Anandamide, a brain endogenous compound, interacts specifically with cannabinoid receptors and inhibits adenylate cyclase. J. Neurochem. 61: 352-35, 1993[Medline].
Vollmer, R. R., Cavero, I., Ertel, R. J., Solomon, T. A. and Buckley, J. P.: Role of the central autonomic nervous system in the hypotension and bradycardia induced by (-)- $Delta$ ⁹-trans-tetrahydrocannabinol. J. Pharm. Pharmacol. 26: 186-198, 1974[Medline].
Williams, R. B., Ng, J. K. Y., Lamprecht, F., Roth, K. and Kopin, I. J.: $Delta$ ⁹-trans-tetrahydrocannabinol: A hypotensive effect in rats. Psychopharmacology 28: 269-274, 1973.
Vidrio, H., Sanchez-Salvatori, M. A. and Medina, M.: Cardiovascular effects of (-)-11-OH- $Delta$ ⁸-tetrahydrocannabinol-dimethylheptyl in rats. J. Cardiovasc. Pharmacol. 28: 332-336, 1996[Medline].
Zaugg, H. E. and Kyncl, J.: New antihypertensive cannabinoids. J. Med. Chem. 26: 214-217, 1983[Medline].

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Cannabinoid-Induced Hypotension and Bradycardia in Rats Is Mediated by CB1-Like Cannabinoid Receptors1

Cannabinoid-Induced Hypotension and Bradycardia in Rats Is Mediated by CB₁-Like Cannabinoid Receptors¹