The Selective Dopamine D1 Receptor Agonist A-86929 Maintains Efficacy with Repeated Treatment in Rodent and Primate Models of Parkinson's Disease

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Vol. 281, Issue 1, 454-459, 1997

The Selective Dopamine D1 Receptor Agonist A-86929 Maintains Efficacy with Repeated Treatment in Rodent and Primate Models of Parkinson's Disease

K. E. Asin, E. F. Domino, A. Nikkel and K. Shiosaki

Abbott Laboratories, Neuroscience Research Division (K.E.A., A.N., K.S.), Dept. 47U, Bldg. AP-9A, Abbott Park, Illinois and Department of Pharmacology (E.F.D.), University of Michigan, Ann Arbor, Michigan

	Abstract

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The ability of the selective dopamine D1 receptor agonist (5aR,11bS)-4,5,5a,6,7,11b-hexahydro-2-propyl-3-thia-5-azacyclopent-1-ena[c]-phenanthrene-9,10-diol(A-86929) to induce contralateral rotation after repeated administrationwas determined in rodent and primate models of Parkinson's disease.Testing was conducted in rats previously given unilateral 6-hydroxydopamineinjections and in macaques previously given unilateral, intracarotidinfusions of the neurotoxin 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine.Both treatments have been shown to reduce forebrain dopamine levelson the side of the infusion. Such animals rotate contralaterallyafter injections of direct-acting dopamine receptor agonists.Rats were administered A-86929 (0.11 or 0.22 µmol/kg s.c.) threetimes daily for 10 days, with injections spaced 3 h apart, androtation was measured across a 9-h period on various treatmentdays. Initially, monkeys were given various doses of A-86929 (0.03,0.10 or 0.30 µmol/kg i.m.), and rotation was monitored for 3 hafter each dose. Significant, dose-dependent levels of contralateralrotation were achieved. Monkeys were next treated three timesdaily at 3-h intervals with A-86929 (0.3 µmol/kg). Analysis oftotal, daily rotation scores indicated that the magnitude of thebehavioral response did not change significantly across the 10-daytreatment period in monkeys, although it increased in rats (0.22µmol/kg). The first daily injection tended to elicit greater andlonger-lived responses than the subsequent daily injections inboth species. In monkeys, this was particularly true on the firsttest day and was not seen by the last test. This study suggeststhat a selective D1 receptor agonist, such as A-86929, with fullintrinsic activity relative to dopamine, may be useful for thetreatment of Parkinson's disease.

	Introduction

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A-86929 is a selective ligand for the DA D1 receptor with full agonist activity relative to DA (Shiosaki et al., 1996); thediacetyl derivative, ABT-431, is currently under development forthe treatment of PD. One useful model for testing compounds forpotential antiparkinsonian properties involves the use of ratsor nonhuman primates with unilateral DA depletions. In such animals,direct-acting DA receptor agonists induce rotation away from thelesioned side, presumably because of the increased sensitivityof postsynaptic DA receptors on the denervated side. In rats,unilateral injections of the neurotoxin 6-OHDA reduce forebrainDA levels, whereas in primates, unilateral brain depletions ofDA can be achieved through the intracarotid infusion of the neurotoxinMPTP. Results generated in the MPTP primate model have, in particular,proved useful for extrapolation to humans. Although the partialagonist SKF 38393 proved efficacious in rat models of PD, it wasunable to ameliorate parkinsonian signs in MPTP-treated primates,perhaps because of its partial agonist activity (Bédard and Boucher,1989; Braun et al., 1986; Falardeau et al., 1988). Subsequently,D1 receptor agonists with greater intrinsic activity have beendemonstrated to relieve parkinsonian signs and symptoms in MPTP-treatedprimates and in PD patients (Blanchet et al., 1993; Emre et al.,1992; Gnanalingham et al., 1995; Luquin et al., 1994; Taylor etal., 1991; Temlett et al., 1989) and to induce dose-dependentcontralateral rotation in monkeys rendered hemiparkinsonian viaunilateral, intracarotid infusions of MPTP (Domino and Sheng,1993a,b; Johnson et al., 1995; Vermeulen et al., 1993; 1995).The behavioral effects of these compounds after repeated dailytreatment have not been reported.

The ability of A-86929 to produce rotation in rats bearing unilateral 6-OHDA lesions and in nonhuman primates rendered hemiparkinsonianthrough intracarotid infusions of MPTP was investigated in thepresent study. Rotation was examined across a thrice-daily, repeated-treatmentregimen across a 10-day period. The results indicate that a D1receptor agonist with full intrinsic activity may be useful asa chronic treatment for PD.

	Materials and Methods

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Subjects

Twelve adult male Sprague-Dawley rats (Charles River, Portage, MI), weighing approximately 300 g, were used as subjects. Animalswere single-housed in hanging wire-mesh cages, with food and wateravailable ad libitum. The light:dark schedule was 12:12 h.

Five adult female Macaca nemstrina (pig-tailed macaque) monkeys weighing 5.4 to 6.9 kg at the time of study were originallyobtained from Charles River Co., Port Washington, NY. The animalcare and use program conforms to the standards in the Guide forthe Care and Use of Laboratory Animals (1985), and we followedthe B Virus Working Group Guidelines for Prevention of HerpesVirus Simian Infection in Monkey Handlers (1988). Animals weresingle housed and maintained on a 12:12 light:dark schedule, withwater and monkey chow available ad libitum each morning, and fruitsupplements, as warranted.

Surgery

Rats. Twenty minutes after an injection of desmethylimipramine HCl (25 mg/kg ip), rats were anesthetized with sodium pentobarbital(50 mg/kg) and given unilateral injections of 6-OHDA into themedial forebrain bundle, as described previously (Asin et al.,1995). Rats were prescreened for rotation in response to apomorphineabout 2 to 3 weeks after lesioning, as also described elsewhere(Asin et al., 1995). Animals were used in the present studiesapproximately 2 months after surgery. There were six animals ineach of the two treatment groups.

Monkeys. The method of Bankiewicz et al. (1986) was used to infuse MPTP unilaterally into one common carotid artery (also see Dominoand Sheng, 1993a,b). Animals were anesthetized with ketamine hydrochloride(5-10 mg/kg, base dose) followed by 30 mg/kg i.v. sodium pentobarbitalto maintain deep anesthesia. Animals were secured on the operatingtable, and one common carotid artery was exposed at its bifurcation.MPTP HCl (approximately 3 mg in 60 ml) was infused slowly overa 20-min period, and the wound was then closed. Each animal wasgiven 300,000 U sterile penicillin G benzathine and penicillinG procaine in an aqueous suspension. At the time of the currentstudies, animals had been displaying hemiparkinsonian symptomsfor 3 to 5 years and had been given various selective D1 and D2DA receptor agonists and other compounds (e.g., amphetamine, cocaine,ketamine, phencyclidine and MK-801) during this time. However,animals had been free of medication for approximately 1 monthbefore the present study.

Apparatus and Procedure

Rats. Animals were tested for rotation in automated rotometers (San Diego Instruments, San Diego, CA), as described previously (Asinet al., 1995). Animals were allowed to habituate to the rotometerbowls for approximately 20 min before the first daily injectionof A-86929 (0.11 or 0.22 µmol/kg s.c.); the second and third injectionswere administered at 3-h intervals. These doses are approximately50% and 100%, respectively, of the ED₅₀ value for this compoundto induce rotation (Shiosaki et al., 1996). During the 10 daysof treatment, rotation was measured on days 1, 3, 5, 8 and 10for 3 h after each injection (total test time of 9 h); on theremaining days, rats were given the three daily injections intheir home cages.

Monkeys. Methods were similar to those described elsewhere (see Domino and Sheng, 1993a,b). Briefly, monkeys were placed individuallyinto a standard primate cage modified with a clear plexiglas front.Gross animal behaviors were observed and recorded via three colorvideo cameras (Panasonic VHS model PV-420; Magnavox VR 9344-AV01and Sears LX-1 model 1934) connected individually to videocassetterecorders (Mitsubishi model U-32 VCR). The behavior of the animalswas recorded for 30 min after vehicle injection and for 3 h aftereach drug injection without humans present. Videotapes were scoredfor the number and direction of complete, 360° turns demonstratedby each animal during each consecutive 5-min period.

Initially, we administered A-86929 in doses of 0.03, 0.10 and 0.30 µmol/kg i.m. and gave it in increasing doses in order todetermine the effect and the duration of action of each dose.A 2- to 3-day washout period intervened between tests. On thebasis of the results of the dose-response determination, the 0.30-µmol/kgdose was chosen for use in the repeated-treatment study. Thisdose was administered thrice daily for 10 days at approximately9:00 A.M., noon and 3:00 P.M. At approximately 8:30 A.M. eachday, animals were given a control injection of 5% dextrose inwater (i.m.) followed 30 min later by the active drug.

Compounds

A-86929 was synthesized at Abbott Laboratories (Michaelides et al., 1995). It was administered to rats in sterile water andto monkeys in sterile 5% glucose in water, purchased from AbbottLaboratories (Abbott Park, IL). 6-OHDA and desmethyl-imipramineHCl were purchased from Sigma Chemical (St. Louis, MO), and MPTPHCl was purchased from Aldrich Chemical Co (Milwaukee, WI).

	Results

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Rats

Separate one-way ANOVAs with repeated measures for each of the two doses of A-86929 were conducted on the total net numberof contralateral rotations (contralateral minus ipsilateral) shownby 6-OHDA-lesioned rats. There was a significant effect of Daysfor both the low [F(4,20) = 4.16; P < .02] and the high [F(4,20)= 5.73; P < .003] doses. Post hoc analysis (Tukey HSD) indicatedthat for the lower dose, the mean total number of responses ondays 3 and 8 differed from each other, whereas for the higherdose, responses on days 8 and 10 both differed significantly fromthe response on day 1 (P < .05) (see fig. 1).

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Fig. 1. Mean (± S.E.) daily (9 h) total net numbers of contralateral rotations (contralateral minus ipsilateral) demonstrated by 6-OHDA-lesionedrats after three daily injections of A-86929. *From Michaelideset al., 1995

Separate two-way ANOVAs (Injection number × Days) on rotation scores after the three daily injections across the five testingdays were also conducted for each dose. For the low dose, therewere significant effects of Days [F(4,20) = 4.16; P < .02] andInjection number [F(2,10) = 23.12; P < .001] and a significantDays × Injection number interaction [F(8,40) = 4.75; P < .001].For the high dose, there were also significant effects of Days[F(4,20) = 5.73; P < .003] and Injection number [F(2,10) = 13.62;P < .001] and a significant Days × Injection number interaction[F(8,40) = 3.72; P < .002]. As can be seen in figure 2, and asborne out in post-hoc analysis (one-way ANOVAs with repeated measuresconducted across days for each dose and each injection number),the behavioral response to the first daily injection increasedsignificantly across days for both the low [F(4,20) = 4.28; P< .02] and the high [F(4,20) = 3.85; P < .02] doses. The levelsof rotation seen over days in response to the second daily injectionremained unchanged at the low dose [F(4,20) < 1.0] but increasedsignificantly at the high dose [F(4,20) = 5.82; P < .004]. Theresponse to the third daily injection tended to decline in ratsadministered the low dose [F(4,20) = 2.60; p < .07] and remainedunchanged at the high dose [F(4,20) < 1.0].

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Fig. 2. Mean (± S.E.) net numbers of contralateral rotations across days in rats after each of the three daily injections of A-86929A) 0.11 µmol/kg. B) 0.22 µmol/kg.

In order to compare the initial and final rotation responses over time after the three daily injections, three-way ANOVAs(Injection number × Time × Days) were also conducted for eachdose on rotation scores after each injection on treatment days1 and 10 (fig. 3). For the low dose, there were significant effectsof Injection number [F(2,10) = 10.89; P < .004] and Time [F(5,25)= 12.37; P < .001] but not Days [F(1,5) < 1.0]. Significant interactionswere obtained for Days × Injection number [F(2,10) = 5.35; p <.03], Injection number × Time [F(10,50) = 9.03; P < .001] butnot Days × Time [F(5,25) < 1.0]. The Days × Injection number ×Time interaction was also significant [F(10,50) = 3.13; P < .005].The results of the ANOVA conducted on the lower dose can be summarizedas follows: On the first day of treatment, the response over timeto the three injections was similar. By Day 10, post-hoc analysis(Tukey HSD) indicated that the third injection elicited a smaller,shorter-lived response, both within and between days (P < .01),although the overall total number of rotations did not differsignificantly between the first and last treatment days.

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Fig. 3. Mean (± S.E.) net number of contralateral rotations demonstrated by rats over time after each of the three daily A-86929 injectionson the first and last treatment days. A) 0.11 µmol/kg. B) 0.22µmol/kg.

For the high dose, there were significant effects of Days [F(1,5) = 7.85; P < .04] and Time [F(5,25) = 76.14; P < .001] butnot Injection number [F(2,10) = 2.70; P > .10]. Significant interactionsterms were obtained for Days × Injection number [F(2,10) = 21.60;P < .001] and Days × Time [F(5,25) = 12.43; P < .001] but notInjection number × Time [F(10,50) < 1.0]. The Days × Injectionnumber × Time interaction was not statistically significant [F(10,50)= 1.08; P > .35]. The results of the ANOVA conducted on data fromrats at the higher dose can be summarized as follows: The totalnumber of rotations was greater on day 10 than on day 1, and thiswas true across each of the three injections (although there wasno difference within a day in the behavioral response occurringafter each injection). As may be seen in figure 3, response sensitizationoccurred over the treatment period and was approximately equalin magnitude after each of the three injections.

Monkeys

Dose-response determination. A one-way ANOVA with repeated measures was conducted on the total net number of contralateral rotations (contralateral minusipsilateral) demonstrated by monkeys at each dose. A-86929 producedsignificant, dose-dependent increases in the net number of contralateralrotations demonstrated by each monkey (F(2,8) = 9.71; P < .008)(table 1). The duration of action was also dose-dependent (fig.4). These results indicate that acute administration of A-86929is able to produce robust contralateral rotation in a primatemodel of Parkinson's disease.

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TABLE 1
Mean net number of contralateral rotations shown by hemiparkinsonian monkeys across a 3-h period after A-86929

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Fig. 4. Time course of the behavioral response to various doses of A-86929 in MPTP-lesioned primates. Graphed are the mean (± S.E.)net number of contralateral rotations (contralateral minus ipsilateral).

Repeated treatment. On the basis of the initial dose-response study, a dose of 0.30 µmol/kg was chosen for the repeated-administration study.The data generated in the former study indicated that althoughthe duration of the rotation at this dose was approximately 3h, the duration was reduced to approximately 2 h in the repeated-treatmentstudy after the first day of treatment. Therefore, only data recordedacross the 2-h period after each drug injection were analyzed.Initially, the total, net number of contralateral rotations forthe first, second and third daily injections were summed and analyzedover days. This one-way (Days) ANOVA with repeated measures failedto indicate a significant effect of Days [F(9,36) = 1.60; P >.15], which indicated that there was no significant change inthe effects of A-86929 across the 10-day injection period (fig.5A). A second ANOVA (Injection number × Days, with repeated measureson both factors) was conducted on the net number of contralateralrotations shown by each monkey during the 2-h period after thefirst, second and third daily injection (fig. 5B). There was amarginally significant effect of Injection number [F(2,8) = 4.03;P $<=$ .06]. As expected, there was no significant effect of Days[F(9,36) = 1.60; P > .15] and no Injection number × Days interaction[F(18,72) = 1.40; P > .15]. A graph of the data (fig. 5B) indicatesthat although there was no change in drug efficacy over days,the first daily injection tended to elicit greater contralateralrotation than the second and third daily injections. Because thisdifference in response magnitude appeared to diminish over time,additional data analyses were performed on the data generatedon the first and tenth treatment days. For each day, a two-way(Injection number × Time) ANOVA was conducted on 30-min rotationscores after each injection (fig. 6). On day 1 of treatment, therewas a significant effect of Time (F(3,12) = 14.16; P < .001) anda marginally significant effect of Injection number (F(2,8) =3.96; P < .065). The interaction between Injection number andTime was significant (F(2.52; p < .05). These results indicatea significant difference between the response pattern over timeafter the three injections. In contrast, only a significant effectof Time (F(3,12) = 7.65; P < .005) was obtained from the analysisof data from day 10 [Injection number (F(2,8) = 2.78; P > .10;Injection number × Time (F(6,24) = 1.31; P > .25)]. Thus, by thelast treatment day, the responses to the three daily injectionswere statistically similar. In contrast to the robust contralateralrotation seen after treatment with A-86929, treatment with vehicleelicited ipsilateral rotation during the 30-min period after injection(mean ± S.E.M. = 12.40 ± 5.70).

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Fig. 5. A) Mean (± S.E.) daily total numbers of net contralateral rotations across the 10 days of repeated treatment in primates.Total testing time was 6 h. B) Mean (± S.E.) net numbers of contralateralrotations 2 h after the first, second and third daily injections.

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Fig. 6. Magnitude and duration of the behavioral response in primates to three daily injections of A-86929.1 on the first and lastdays of the repeated-treatment study.

	Discussion

Top Abstract Introduction Materials & Methods Results Discussion References

In the present study, thrice-daily injections of the full DA D1 receptor agonist A-86929 promoted rotation across a 10-daytreatment period in both rats and primates bearing unilateralforebrain DA depletions. The daily total number of rotations didnot decline over the 10-day period, and in rats, evidence forresponse sensitization was obtained with the higher dose (0.22µmol/kg). These observations are unlike those we reported previouslyafter daily treatment of lesioned rats with other DA D1 receptoragonists (A-77636 and A-85653) (Asin and Wirtshafter, 1993; Asinet al., 1995), which produced rapid development of behavioraltolerance. In contrast, daily treatment with either SKF 82958or SKF 38393 may lead to either response sensitization (Silverman,1991, 1992) or, for the case of SKF 38393, tolerance (Engber etal., 1993). Clearly, the behavioral effects of repeated DA agonisttreatment rely on a number of factors, including drug doses andtreatment regimen, as well as pharmacokinetic and pharmacologicproperties of the administered compound (Castro et al., 1985).As we saw in the present study, species differences in the responseto repeated treatment may also exist, perhaps as a consequenceof differences in drug metabolism and/or distribution. It is notablethat both A-77636 and A-85653 have durations of action in 6-OHDA-lesionedrats (measured behaviorally) ranging from 6 to 18 h and that thesecompounds produce behavioral tolerance after repeated treatment(Asin and Wirtshafter, 1993; Asin et al., 1995). This durationof action is considerably longer than that seen with A-86929 inthe present study. Persistent receptor activation contributesto the receptor desensitization produced by A-77636 (Lin et al.,1996).

The hypothesis that a D1 receptor agonist may prove useful for the treatment of Parkinson's disease was tested almost a decadeago using the partial agonist SKF 38393, and, unlike what wasseen in rats, the data collected from primates were not encouraging(Braun et al., 1986). However, subsequent studies have indicatedthat the problem lay not with the hypothesis but with the pharmacologyand pharmacokinetics of the compound tested. Thus, although SKF38393 proved efficacious in rat models of PD, it was unable toameliorate parkinsonian signs in primates (Bédard and Boucher,1989; Braun et al., 1986; Falardeau et al., 1988; Nomoto et al.,1985); this compound's partial agonist activity (Anderson andJansen, 1990; Pifl et al., 1991) and poor blood brain barrierpermeability have been offered as possible explanations for itsinactivity. Since the original studies with SKF 38393, agonistswith greater intrinsic activity (e.g., SKF 82958, CY 208-243 andA-77636) have been demonstrated to relieve parkinsonism in MPTP-treatedprimates or in humans (Akai et al., 1995; Blanchet et al., 1993;Kebabian et al., 1992; Luquin et al., 1994; Temlett et al., 1989).Additionally, the D1 receptor agonists A-77636, dihydrexidineand SKF 81297, but not SKF 38393 (Barone et al., 1987), promotedose-dependent contralateral rotation in monkeys rendered hemiparkinsonianvia unilateral, intracarotid infusions of MPTP (Domino and Sheng,1993a; Johnson et al., 1995; Vermeulen et al., 1993). The resultsof these more recent studies using D1 receptor agonists with fullintrinsic activity certainly suggest that such compounds may beefficacious in treating PD.

In MPTP-lesioned monkeys given repeated L-dopa treatment, D2 receptor agonists, including quinpirole, bromocriptine and (+)-4-propyl-9-hydroxynaphthoxazinewere found to alleviate parkinsonian symptoms but also to inducedyskinesias, as a consequence of L-dopa priming. In contrast,the D1 receptor agonists SKF 82958 and A-77636 also alleviatedparkinsonian symptoms but had less propensity for inducing dyskinesias(Blanchet et al., 1993). Although somewhat controversial (Luquinet al., 1994), selective D1 receptor agonists may therefore producefewer dyskinetic movements than D2 selective agonists in L-dopa-primedanimals, and they appear even to potentiate the antiparkinsonianeffects of selective D2 agonists (Blanchet et al., 1993; Gagnonet al., 1995; Rouillard et al., 1990) in MPTP-treated primates.

Luquin et al. (1996) recently reported that the behavioral response of MPTP-treated monkeys to the partial D1 agonist CY 208-243decayed when animals were given four drug injections spaced 3h apart. The decay was primarily due to a more rapid decline inthe motor response to the drug relative to the first injection.A diminution in behavioral efficacy was not seen after (+)-PHNOadministered under similar conditions, which suggests that thebehavioral tolerance seen in MPTP-treated monkeys after repeatedapomorphine injections may involve D1 receptor mechanisms (Luquinet al., 1993). In the present study, the first daily injectionof A-86929 tended to elicit a greater and longer-lived responsethan either the second or the third injection across the 10-daytreatment period. In monkeys, this difference was particularlyapparent on the first day of treatment, where the magnitude ofthe rotation during the first 30 min after the first injectionwas greater than that after the second and third injections. Bythe tenth treatment day, however, there was no temporal differencein the behavioral response to the first, second or third dailyinjections, although the response did decay more rapidly aftereach injection on the tenth day than on the first day. Thus thereduction in the behavioral response seen after short-term, repeatedD1 agonist treatment in both this study and the study by Luquinet al. (1996) may subsequently plateau during longer-term treatment.If so, it may be possible to overcome this reduction through doseadjustment.

	Acknowledgments

The authors would like to acknowledge the efforts of J. Sheng in the studies involving primates. We also thank Dr. M. Michaelidesand Dr. Y. Hong for preparing A-86929.

	Footnotes

Accepted for publication December 30, 1996.

Received for publication November 1, 1996.

Send reprint requests to: Dr. K. E. Asin, Dept. of Toxicology, Abbott Laboratories, Dept. 468, Bldg. AP13A, 100 Abbott Park Rd., Abbott Park, IL 60064-3500.

	Abbreviations

A86929, (5aR,11bS)-4,5,5a,6,7,11b-hexahydro-2-propyl-3-thia-5-azacyclopent-1-ena[c]-phenanthrene-9,10-diol; DA, dopamine; MPTP, 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine; 6-OHDA, 6-hydroxydopamine; PD, Parkinson's disease; ANOVA, analysis of variance.

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