Analgesic, Respiratory and Heart Rate Effects of Cannabinoid and Opioid Agonists in Rhesus Monkeys: Antagonist Effects of SR 141716A

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HEROIN
TETRAHYDROCANNABINOL

Vol. 286, Issue 2, 697-703, August 1998

Analgesic, Respiratory and Heart Rate Effects of Cannabinoid and Opioid Agonists in Rhesus Monkeys: Antagonist Effects of SR 141716A¹^,²

Jeffrey A. Vivian, Shiroh Kishioka³, Eduardo R. Butelman⁴, Jillian Broadbear, Katherine O. Lee and James H. Woods

Departments of Psychology and Pharmacology, University of Michigan Medical School, Ann Arbor, Michigan

	Abstract

Top Abstract Introduction Methods Results Discussion References

This study characterized the antinociceptive, respiratory and heart rate effects of the cannabinoid receptor agonists $Delta$ -9-tetrahydrocannabinol( $Delta$ -9-THC) and WIN 55212 {(R)-(+)-2,3-dihydro-5-methyl-3-[(4-morpholinyl)methyl]pyrol-[1,2,3-de]-1,4-benzoxazin-6-yl)(1-naphtalenyl)methanonemonomethanesulfonate}, N-arachidonyl ethanolamide (anandamide)and the mu and kappa opioid receptor agonists heroin and U69593,alone and in conjunction with a cannabinoid receptor antagonist,SR 141716A [N-(piperidin-1-1-yl)-5-(4-chlorophenyl)-1(2,4-dichlorophenyl)-4-methyl-1H-pyrazole-3-carboxamidehydrochloride] and an opioid receptor antagonist, quadazocine,in rhesus monkeys (Macaca mulatta). Using 12 adult rhesus monkeys,latencies to remove the tail from a 50°C water bath, respirationin 5% CO₂ and heart rate were measured. When administered alone,SR 141716A (1.8, 5.6 mg/kg i.m.) did not alter nociception, respirationor heart rate. $Delta$ -9-THC (0.1-10 mg/kg i.m.) and WIN 55212 (0.1-10mg/kg i.m.) dose-dependently increased antinociception and dose-dependentlydecreased respiratory minute and tidal volumes and heart rate.These antinociceptive, respiratory and heart rate effects werereversed by SR 141716A but not by the opioid antagonist quadazocine(1 mg/kg i.m.). Anandamide (10 mg/kg i.m.) also produced antinociception.Heroin (0.01-10 mg/kg i.m.) and U69593 (0.01-3.2 mg/kg i.m.) alsodose-dependently increased antinociception and decreased respiratoryand heart rate measures; these effects were antagonized by quadazocinebut not by SR 141716A. These results demonstrate selective andreversible antagonism of cannabinoid behavioral effects by SR141716A in rhesus monkeys.

	Introduction

Top Abstract Introduction Methods Results Discussion References

Acute administration of cannabinoid receptor agonists such as $Delta$ -9-THC, WIN 55212 {(R)-(+)-2,3-dihydro-5-methyl-3-[(4-morpholinyl)methyl]pyrol-[1,2,3-de]-1,4-benzoxazin-6-yl)(1-naphtalenyl)methanonemonomethanesulfonate} and CP 55940 [( $-$ )-cis-3-[2-hydroxy-4(1,1-dimethyl-heptyl)phenyl]-trans-4-(3-hydroxypropyl)cyclohexanol]reliably produces antinociception (Herzberg et al., 1997; Pughet al., 1997) and discriminative effects (Wiley et al., 1995a,1995b), impairs tasks involving memory (Terranova et al., 1996;Lichtman and Martin, 1996) and reduces locomotor activity (Comptonet al., 1996; Stark and Dews, 1980) and body temperature (Fanet al., 1994) in rodents. Chronic administration of $Delta$ -9-THC revealsthe development of tolerance to the acute effects, and a withdrawalsyndrome has been demonstrated (Aceto et al., 1996; Tsou et al.,1995).

Recently, a cannabinoid receptor antagonist has been synthesized and proved to be effective in reversing the effects of $Delta$ -9-THC.In vivo, pretreatment with SR 141716A blocks the antinociceptive(Compton et al., 1996), discriminative stimulus (Wiley et al.,1995c, 1995d), memory impairing (Lichtman and Martin, 1996) andhypolocomotor effects produced by $Delta$ -9-THC (Compton et al., 1996).SR 141716A also precipitates a withdrawal syndrome in rats treatedchronically with $Delta$ -9-THC (Aceto et al., 1996). In vitro, SR 141716Abinds selectively to central cannabinoid receptors (CB1) withhigh affinity (K_i = 2 nM), and blocks the inhibitory effects ofcannabinoid receptor agonists in the mouse vas deferens, dopamine-stimulatedadenylyl cyclase (Rinaldi-Carmona et al., 1994) and WIN 55212-stimulatedGTP $gamma$ S binding (Selley et al., 1996).

Many of the previous in vivo investigations involving compounds targeting cannabinoid receptors have been performed in nonprimatespecies. The objectives of the current experiments were (1) tomore fully characterize the antinociceptive, respiratory and heartrate effects of the cannabinoid receptor agonists $Delta$ -9-THC andWIN 55212 and (2) to evaluate the ability and selectivity of SR141716A to block the antinociceptive, respiratory and heart rateeffects of the cannabinoid agonists $Delta$ -9-THC and WIN 55212 andthe opioid receptor agonists heroin and U69593 in rhesus monkeys.

	Methods

Top Abstract Introduction Methods Results Discussion References

Subjects

Twelve adult rhesus monkeys (Macaca mulatta) with complex experimental and drug histories were individually housed with freeaccess to water in a vivarium maintained at 21 ± 1°C, 30% to 50%humidity and a 12:12-hr light/dark cycle. Monkeys were fed ~30biscuits (Purina Monkey Chow) daily and fresh fruit twice weekly.

Apparatus and Procedure

Warm water tail withdrawal assay. Monkeys (n = 6) were seated in primate chairs, and the lower 10 cm of the shaved tail was immersed in a flask containing watermaintained at either 40°, 50° or 55°C (Dykstra and Woods, 1986).Tail withdrawal latencies were timed manually, and a maximum latencyof 20 sec was allowed to prevent tissue damage. Noninjection base-linewithdrawal latencies were determined at each water temperaturein a random order among the monkeys. Subsequent to base-line determinations,drugs were administered using a cumulative dosing procedure, withascending doses of a test compound being administered at 30- (opioids)or 60- (cannabinoids) min intervals. Tail withdrawal latencieswere determined at each of the three water temperatures in a randomfashion ~25 (opioids) or ~55 (cannabinoids) min after drug administration.In antagonist studies, quadazocine or SR 141716A were administered30 or 60 min before agonist administration, respectively.

Respiration and heart rate. Monkeys (n = 6) were seated in primate chairs and placed in ventilated, sound-attenuating primate chambers with custom-madepolycarbonate respiratory helmets placed over their head (Howellet al., 1988). The helmet was sealed around the neck of the monkeyswith two polycarbonate shields. Gas (air or a mixture of 5% CO₂in air) was pumped through the helmet and removed at a rate of10 liters/min. Pressure changes and displacement within the helmetwere detected with a pressure transducer and integrator connectedto a polygraph (Grass models 7E and 7P122E), respectively, andthe data were recorded on a polygraph trace and a PC-compatiblecomputer. Respiratory data included f, V_e and V_t (V_e/f) and wereobtained for consecutive 3-min periods.

Sessions consisted of several consecutive cycles, with each cycle composed of a 23-min air exposure followed by a 7-min 5%CO₂ exposure (opioids) or a 53-min air exposure followed by a7-min 5% CO₂ exposure (cannabinoids). Noninjection base-line respirationmeasures were determined; subsequently, vehicle and drugs wereadministered at the beginning of each cycle using a cumulativedosing procedure. In antagonist experiments, quadazocine or SR141716A were administered 30 and 60 min before agonist administration,respectively.

Heart rate data were collected concurrently with respiration data. Monkeys were connected to electrocardiogram electrodesconnected to a polygraph trace, from which the heart rate wascalculated graphically.

Drugs

$Delta$ -9-THC (National Institute for Drug Abuse, Rockville, MD), WIN 55212 (Sterling Winthrop, Rensselaer, NY), N-arachidonyl-ethanolamine(anandamide; Organix, Woburn, MA) and SR 141716A (Sanofi Recherche,Montpellier, France) were dissolved in a vehicle containing emulphor,ethanol and distilled water (1:1:9). Heroin (National Institutefor Drug Abuse), U69593 (Upjohn, Kalamazoo, MI), and quadazocinemethanesulfate (Sterling Winthrop) were dissolved in distilledwater. Pilot work revealed that tolerance developed to the antinociceptiveeffects of the cannabinoids rapidly; for this reason, cannabinoidtest compounds were not administered more than once every 3 weeks.All drugs were administered intramuscularly at a volume of 0.1ml/kg b.wt.

Data Analysis

Tail-withdrawal data were converted to percent maximum possible effect (% MPE) with the calculation: % MPE = 100 × [(testlatency $-$ control latency)/(cutoff latency $-$ control latency)].Respiratory data were from the last 3-min exposure to air and5% CO₂ and heart rate data were from the last 3-min exposure toair, during each cycle was converted to percent of vehicle control,and all data were analyzed with a one-factor (dose) repeated-measuresANOVA. When significant effects were demonstrated, post-hoc Dunnett'st tests were performed. The $alpha$ value was .05 (two-tailed).

	Results

Top Abstract Introduction Methods Results Discussion References

Antinociception. The cannabinoid receptor agonists $Delta$ -9-THC and WIN 55212 and the mu and kappa opioid receptor agonists heroin and U69593 dose-dependentlyincreased the latency to remove the tail from a 50° and 55°C waterbath (figs. 1 and 2). In 50°C water, $Delta$ -9-THC and WIN 55212 produceda 71% and 79% MPE [ $Delta$ -9-THC: F(4,8) = 5.49, P < .05; WIN 55212:F(3,6) = 11.2, P < .05], whereas both heroin and U69593 produceda 100% MPE [heroin: F(5,10) = 11.4, P < .05; U69593: F(6,12) =11449.0, P < .05], respectively. Base-line tail-withdrawal latenciesare presented in table 1.

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Fig. 1. Antinociceptive effects of the cannabinoid receptor agonists $Delta$ -9-THC (A) and WIN 55212 (B) in 50° and 55°C. Each value represents the mean (n = 3), and error bars represent 1 S.E.M. *, Significant differences (P < .05) from control.

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Fig. 2. Antinociceptive effects of the opioid receptor agonists heroin (A) and U69593 (B) in 50° and 55°C. Each value represents the mean (n = 3), and error bars represent 1 S.E.M. *, Significant differences (P < .05) from control. Note: In 55°C, the antinociceptive effects of heroin alone were similar to those in the presence of SR 141716A (top right).

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TABLE 1
Control values for tail-withdrawal latencies, respiratory frequency, tidal, minute volumes and heart rate before drug administration
Each value represents the mean (n = 3) and S.E.M.

In 55°C water, the cannabinoids were less effective in producing antinociception than they were at 50°C and compared withthe effects of the opioids at 55°C. At the highest doses tested, $Delta$ -9-THC (3.2 mg/kg) and WIN 55212 (1 mg/kg) produced a 15% and9% MPE [ $Delta$ -9-THC: F(4,8) = 6.02, P < .05; WIN 55212: F(3,6) = 7.65,P < .05], respectively. In contrast, the opioids were effectivein abolishing the tail-withdrawal reflex [heroin: F(5,10) = 600.0,P < .05; U69593: F(6,12) = 26.9, P < .05].

In the presence of their respective antagonists (cannabinoids: SR 141716A, opioids: quadazocine), the antinociceptive potenciesof $Delta$ -9-THC, WIN 55212, heroin and U69593 were reduced. After SR141716A (1.8 mg/kg) pretreatment, $Delta$ -9-THC did not reliably produceantinociception, and the antinociceptive effects of WIN 55212were shifted approximately one-half log unit to the right at 50°C[F(4,8) = 10.1, P < .05] and 55°C [F(4,8) = 7.83, P < .05]. Inthe presence of SR 141716A (5.6 mg/kg), WIN 55212 did not produceantinociception. In contrast, SR 141716A (1.8 mg/kg) did not alterthe antinociceptive effects of heroin or U69593; heroin and U69593dose-dependently increased tail-withdrawal latencies at 50°C [F(5,10)= 12.5, P < .05; F(4,8) = 30.0, P < .05, respectively] and 55°C[F(5,10) = 1340.0, P < .05; F(4,8) = 259.5, P < .05, respectively].

The opioid antagonist quadazocine (1 mg/kg) did not alter the antinociceptive effects of $Delta$ -9-THC. In the presence of the quadazocine(0.1 mg/kg), heroin dose-dependently increased tail-withdrawallatencies [50°C: F(5,10) = 10.7, P < .05; 55°C: F(5,10) = 4.7,P < .05], albeit at a reduced potency. In the presence of quadazocine(1 mg/kg), U69593 dose-dependently increased tail-withdrawal latencies(50°C: F(6,12) = 55.7, P < .05; 55°C: F(6,12) = 786.4, P < .05],also at a reduced potency. Neither SR 141716A nor quadazocinealtered base-line tail-withdrawal latencies when administeredalone at these doses (data not shown).

In a separate time course study, the initial exposure to the putative endogenous cannabinoid agonist anandamide (10 mg/kgi.m.) produced a 100% MPE 30 to 60 min after administration in50°C [F(12,24) = 7.44, P < .05]. In subsequent weekly anandamidechallenges (1, 3.2 and 5.6 mg/kg), modest but not dose-relatedantinociceptive effects (<35% MPE) were observed. Anandamide (10mg/kg) administered 4 weeks after the initial 10 mg/kg administrationfailed to produce an antinociceptive effect. Anandamide did notalter tail-withdrawal latencies in 55°C at any time point tested.

Respiration. Increased respiratory f, V_t and V_e during 5% CO₂ breathing were observed and are depicted in table 1. Drug effects on respiratorymeasures during air/5% CO₂ breathing were similar; only the respiratorydata during 5% CO₂ challenges are presented. $Delta$ -9-THC, WIN 55212,heroin and U69593 dose-dependently decreased V_t and V_e and didnot produce reliable decreases in f (figs. 3 and 4). At the highestdoses tested, $Delta$ -9-THC produced a 64% suppression of V_t [1 mg/kg;F(4,8) = 6.16, P < .05], WIN 55212 produced a 40% [1 mg/kg; F(3,6)= 25.8, P < .05], heroin produced a 40% suppression of V_t [0.32mg/kg; F(4,8) = 19.0, P < .05] and U69593 produced a 42% suppressionof V_t [0.32 mg/kg; F(5,10) = 18.4, P < .05]. Similarly, $Delta$ -9-THCproduced a 60% suppression of V_e [F(4,8) = 9.47, P < .05], WIN55212 produced a 40% suppression of V_e [F(3,6) = 16.0, P < .05],heroin produced a 40% suppression of V_e [F(4,8) = 40.2, P < .05]and U69593 produced a 43% suppression of V_e [F(5,10) = 10.6, P< .05]. Respiratory (and heart rate) effects of anandamide werenot evaluated.

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Fig. 3. Respiratory suppressant effects of $Delta$ -9-THC (A) and WIN 55212 (B). Each value represents the mean (n = 3), and error bars represent 1 S.E.M. *, Significant differences (P < .05) from control.

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Fig. 4. Respiratory suppressant effects of heroin (A) and U69593 (B). Each value represents the mean (n = 3), and error bars represent 1 S.E.M. *, Significant differences (P < .05) from control.

In the presence of their respective antagonists, the respiratory suppressant effects of $Delta$ -9-THC, WIN 55212, heroin and U69593were reduced. After SR 141716A (1.8 mg/kg) pretreatment, $Delta$ -9-THCdose-dependently decreased V_t and V_e, now requiring a dose of10 mg/kg to produce a 27% and 39% suppression of these measures,respectively [V_t: F(4,8) = 6.16, P < .05; V_e: F(4,8) = 9.47, P> .05]. Two doses of SR 141716A were evaluated in conjunctionwith WIN 55212. SR 141716A (0.56 and 1.8 mg/kg) produced a dose-relatedinhibition of WIN 55212 respiratory depressant effects. Afterpretreatment with the lower dose of SR 141716A, WIN 55212 (1 mg/kg)produced a 20% suppression of V_t [F(3,6) = 5.94, P < .05] anda 29% suppression of V_e [F(3,6) = 15.9, P < .05], and pretreatmentwith the higher dose of SR 141716A abolished the ability of WIN55212 to suppress these respiratory measures. In contrast, SR141716A (1.8 mg/kg) did not alter the respiratory suppressanteffects of heroin or U69593; heroin and U69593 dose-dependentlydecreased V_t [F(4,8) = 6.08, P < .05; F(5,10) = 5.17, P < .05,respectively] and V_e [F(4,8) = 9.98, P < .05; F(5,10) = 4.48,P < .05, respectively].

Quadazocine (1 mg/kg) did not alter the respiratory suppressant effects of $Delta$ -9-THC or WIN 55212. In the presence of quadazocine, $Delta$ -9-THC and WIN 55212 dose-dependently decreased V_t [F(4,8) =8.92, P < .05; F(3,6) = 9.34, P < .05, respectively] and V_e [F(4,8)= 34.3, P < .05; F(3,6) = 21.1, P < .05, respectively]. Afterpretreatment with quadazocine (0.1 mg/kg), the potency of herointo reduce V_t and V_e was decreased [F(4,8) = 4.95, P < .05; F(4,8)= 7.33, P < .05, respectively]. Similarly, pretreatment with quadazocine(1 mg/kg) reduced the potency of U69593 to decrease V_t [F(5,10)= 9.12, P < .05] and V_e (P = N.S.). Neither SR 141716A nor quadazocinealtered base-line respiratory measures (data not shown).

Heart rate. $Delta$ -9-THC dose-dependently decreased heart rate (fig. 5). At the highest doses tested, $Delta$ -9-THC and WIN 55212 reduced heart rateto 70% of control [ $Delta$ -9-THC: F(4,8) = 11.6, P < .05; WIN 55212:P = N.S.], and heroin and U69593 reduced heart rate to 80% ofcontrol [heroin: F(4,8) = 4.03, P < .05; U69593: P = N.S.].

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Fig. 5. Cardiovascular effects of $Delta$ -9-THC (A), WIN 55212 (B), heroin (C) and U69593 (D). Each value represents the mean (n = 3), and error bars represent 1 S.E.M. *, Significant differences (P < .05) from control.

SR 141716A (1.8 mg/kg), but not quadazocine (1 mg/kg), reduced the potency of $Delta$ -9-THC to reduce heart rate [F(5,10) = 3.52,P < .05; F(4,8) = 30.3, P < .05, respectively]. In contrast, quadazocine(0.1 mg/kg), but not SR 141716A (1.8 mg/kg), reversed the suppressiveeffects of heroin on heart rate [F(5,10) = n.s.; F(4,8) = 3.61,P < .05, respectively]. Neither SR 141716A nor quadazocine alteredthe base-line heart rate (data not shown).

	Discussion

Top Abstract Introduction Methods Results Discussion References

The current experiments reveal that cannabinoid receptor agonists such as $Delta$ -9-THC, WIN 55212 and anandamide produce antinociceptionand suppress respiratory function and heart rate. These effectswere reversed with the cannabinoid receptor antagonist SR 141716Abut not the opioid receptor antagonist quadazocine, thus revealinga cannabinoid receptor mechanism of action. Despite data thatsupport the proposal that cannabinoid and opioid systems may modulatecommon behavioral events (e.g., antinociception; Reche et al.,1996a; Welch, 1994), the current data were ineffective in revealingsuch an interaction.

The antinociceptive effects of acutely administered cannabinoid receptor agonists are quite reliable. Previously, $Delta$ -9-THC,WIN 55212, CP 55940 and anandamide were effective in increasingtail-flick latencies and reducing stretch reflexes induced byp-phenylquinone in rats and mice (Herzberg et al., 1997; Pughet al., 1997; Compton et al., 1996; Smith et al., 1994). Similarly,these agonists produced antinociception in rhesus monkeys, yettheir efficacy as antinociceptive agents was limited. As observedin the current experiment, all three of the tested cannabinoidsfailed to produce an antinociceptive effect against more intensethermal stimuli, specifically 55°C water. This is in contrastto heroin and U69593, which produced 100% MPE values at the highestdoses tested. Pretreatment with SR 141716A reduced the antinociceptivepotency of $Delta$ -9-THC and WIN 55212, but not heroin and U69593, providingfurther in vivo evidence that SR 141716A is an effective and selectivecannabinoid receptor antagonist.

The interaction of antinociceptive effects produced by cannabinoids and opioids in mice is well documented. The mu opioidreceptor agonists morphine and DAMGO produced parallel and leftwardshifts in the antinociceptive effects produced by $Delta$ -9-THC (Recheet al., 1996a), and the administration of $Delta$ -9-THC decreased theantinociceptive ED₅₀ values produced by morphine (Pugh et al.,1997; Welch and Stevens, 1992). Furthermore, dynorphin antisera,a kappa opioid antisense oligonucleotide, and the kappa opioidreceptor antagonist norbinaltorphamine blocked $Delta$ -9-THC antinociceptionin rodents (Pugh et al., 1995, 1997; Reche et al., 1996b). SR141716A has been found to inhibit morphine antinociception (Comptonet al., 1996). In the current experiments, there was no evidencefor a cannabinoid/opioid interaction because SR 141716A failedto alter the antinociception produced by heroin or U69593 andquadazocine, at a dose that targeted both mu and kappa receptortypes, failed to alter the antinociceptive effects of $Delta$ -9-THC.Previously, failure of nonselective opioid antagonists to altercannabinoid-induced antinociception has been demonstrated, andinteractions between opioids and cannabinoids have been most evidentthrough the use of selective kappa antagonists and intrathecaladministration of cannabinoid agonists (Welch et al., 1995; Welch,1994).

In humans, $Delta$ -9-THC produced inconsistent effects on respiratory measures: decreased tidal volume (Johnstone et al., 1975),no change in tidal volume (Malit et al., 1975) and increased respirationrate (Mathew et al., 1992) have been observed. In rats, $Delta$ -9-THCand $Delta$ -8-THC dose-dependently decreased respiration rate (Estradaet al., 1987), yet cannabinoid receptor agonist effects on respirationin rhesus monkeys are undocumented. In the current experiments,both $Delta$ -9-THC and WIN 55212 produced dose-related decreases inminute and tidal volume, while not affecting respiratory frequency.These respiratory suppressant effects were prevented by SR 141716A,but not quadazocine, revealing a cannabinoid mechanism of action.Similar to the results from the antinociceptive experiments (describedabove), there were no indications of an interaction between thecannabinoid and opioid systems influencing respiratory functionin that quadazocine did not alter cannabinoid respiratory effectsand SR 141716A failed to change the respiratory effects of bothheroin and U69593.

Heart rate effects of $Delta$ -9-THC are robust in rats and humans, although the direction of the effect diverges. In humans, smokedmarijuana produced tachycardia, and this increased heart ratewas further demonstrated after oral administration of $Delta$ -9-THC(e.g., Chait and Burke, 1994; Zacny and Chait, 1992). In rats,bradycardia was observed after cannabinoid administration: $Delta$ -9-THC, $Delta$ -8-THC and HU-210 [( $-$ )-11-OH- $Delta$ -8-tetrahydrocannabinol-dimethylheptyl]decreased the heart rate in rats (Vidrio et al., 1996; Estradaet al., 1987; Hine et al., 1977). In monkeys, increased and decreasedheart rates have been observed after the administration of $Delta$ -9-THC.When administered intraperitoneally, $Delta$ -9-THC (0.75-4 mg/kg) dose-dependentlydecreased heart rate, producing a maximal (40%) suppression atthe highest dose tested (Matsuzaki et al., 1987). Conversely,when administered intravenously, $Delta$ -9-THC (0.5 mg/kg) producedan increase in heart rate (Fredericks et al., 1981). In the currentexperiment, intramuscular $Delta$ -9-THC and WIN 55212 dose-dependentlydecreased heart rate, an effect that was antagonized in the presenceof SR 141716A, suggesting cannabinoid receptor mediation. Whetherthe route of administration is an important factor for the heartrate effects of $Delta$ -9-THC remains unknown. Although quadazocinefailed to alter the heart rate effect of $Delta$ -9-THC, there is evidencethat cross-tolerance develops to the THC- and morphine-induceddecrease in heart rate after a regimen of morphine (50 mg/kg/day× 23 days) or $Delta$ -9-THC (10 mg/kg/day × 7 days; Hine, 1985). Theuse of selective opioid antagonists in conjunction with acutelyor chronically administered cannabinoids might help to furtherilluminate cannabinoid-opioid interactions on heart rate.

The current experiments demonstrated the ability of SR 141716A to selectively block cannabinoid antinociceptive, respiratoryand heart rate effects in rhesus monkeys. In general, each ofthe tested agonists (cannabinoids and opioids) produced dose-relatedeffects that were reversed through the use of the appropriateantagonist. SR 141716A is an important tool in the understandingof cannabinoid pharmacology and neurobiology, and its apparentaffinity for the central cannabinoid receptor (CB1; Rinaldi-Carmonaet al., 1996, 1995) will help to elucidate central and peripheralactions of cannabinoid receptor systems. Although the neurobiologyof cannabinoids is becoming better understood, it must be notedthat the effectiveness of $Delta$ -9-THC as an analgesic agent is limited.Most important, $Delta$ -9-THC is not particularly effective as an analgesicagainst more intense pain, and untoward side effects, includingrespiratory suppression and the rapid development of tolerance,are manifest at doses that produce analgesic effects.

	Footnotes

Accepted for publication April 9, 1998.

Received for publication November 4, 1997.

¹ This work was supported by United States Public Health Service Grants DA00254, DA07268, DA05773 and GM07767.

² Animals used in these studies were maintained in accordance with the University of Michigan Committee on Animal Care and Guidelinesof the Committee on the Care and Use of Laboratory Animal Resources,National Health Council (Department of Health, Education and Welfare,ISBN 0-309-05377-3, revised 1996).

³ Present address: Department of Pharmacology, Wakayama Medical College, 9-Banch 27, Wakayama-city, Wakayama 640, Japan.

⁴ Present address: Box 171, Rockefeller University, 1230 York Avenure, New York, NY 10021.

Send reprint requests to: Dr. J. A. Vivian, Department of Pharmacology, University of Michigan Medical School, 1301 MSRB III, Ann Arbor, MI 48109-0632. E-mail: jvivian{at}umich.edu

	Abbreviations

$Delta$ -9-THC, $Delta$ -9-tetrahydrocannabinol; $Delta$ -8-THC, $Delta$ -8-tetrahydrocannabinol; f, frequency; V_e, minute volume; V_t, tidal volume.

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Analgesic, Respiratory and Heart Rate Effects of Cannabinoid and Opioid Agonists in Rhesus Monkeys: Antagonist Effects of SR 141716A¹^,²