Role of spinal {alpha}1-adrenoceptor subtypes in the bladder reflex in anesthetized rats

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Role of spinal $alpha$ ₁-adrenoceptor subtypes in the bladder reflex in anesthetized rats

Mitsuharu Yoshiyama¹^,²^,³ and William C. De Groat¹

¹ Department of Pharmacology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, 15261; ² Department of Neurology, Chiba University Graduate School of Medicine, Chiba, 260 - 8670; and ³ Department of Neurology, Chiba-Higashi National Hospital, Chiba, 260 - 8712, Japan

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The contribution of different subtypes of $alpha$ ₁-adrenoceptors in the lumbosacral spinal cord to the control of the urinary bladderwas examined in urethane-anesthetized rats. Bladder pressure wasrecorded via a transurethral catheter under isovolumetric conditions.Drugs were administered intrathecally at the L₆-S₁ segmental levelof spinal cord. RS-100329 (an $alpha$ _1A-antagonist) in doses of 25,50, and 100 nmol significantly decreased bladder-contraction amplitudeby 38%, 52%, and 95%, respectively, whereas (+)-cyclazosin (an $alpha$ _1B-antagonist) significantly decreased bladder-contraction amplitude(48% reduction) only in a 50-nmol but not a 100-nmol dose. Fiftynanomoles of RS-100329 and (+)-cyclazosin increased bladder-contractionfrequency by 54% and 44%, respectively. BMY7378 (an $alpha$ _1D-antagonist),in doses of 25, 50, and 100 nmol, did not change bladder activity.These studies suggest that reflex-bladder activity is modulatedby two types of spinal $alpha$ ₁-adrenergic mechanisms: 1) $alpha$ _1A- or $alpha$ _1B-inhibitorycontrol of the frequency of voiding reflexes presumably mediatedby an alteration in the processing of bladder afferent input and2) $alpha$ _1A-facilitatory modulation of the descending efferent limbof the micturition-reflex pathway. Spinal $alpha$ _1D-adrenoceptors donot appear to have a significant role at eithersite.

afferents; descending efferents; locus ceruleus

	INTRODUCTION

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

MODULATION OF MICTURITION by central noradrenergic pathways has been a topic of interest because it was reported that sympatheticand parasympathetic nuclei in the lumbosacral cord receive inputsfrom noradrenergic neurons in the brain stem (2). A large partof this input arises from neurons in the locus ceruleus (LC) (2,16, 18, 19, 25), which has been implicated in the supraspinalcontrol of micturition (3, 29, 30). In anesthetized cats,electrical stimulation of the LC induced bladder contractionsthat were blocked by the intrathecal injection of prazosin, an $alpha$ ₁-adrenoceptor antagonist (29, 30). In addition, destructionof noradrenergic cells in the LC by microinjection of 6-hydroxydopamine,a toxin for catecholaminergic neurons, produced a hypoactive bladder,and this effect was partially reversed by the intrathecal injectionof phenylephrine, an $alpha$ ₁-adrenoceptor agonist (30). On the basisof these studies, it was proposed that bulbospinal noradrenergicinputs to the sacral parasympathetic nucleus played an essentialrole in voiding function. Although these findings were not confirmedin conscious cats (5, 6), they indicated that under certainconditions, $alpha$ ₁-adrenergic mechanisms in the spinal cord couldmodulate voiding function. Studies in anesthetized (4, 35)and conscious (11) rats also support thisconclusion.

Our previous studies in anesthetized rats revealed that reflex-bladder activity is modulated by two types of spinal $alpha$ ₁-adrenergicmechanisms: 1) inhibitory control of the frequency of reflex-bladdercontractions presumably due to modulation of afferent processingin the spinal cord and 2) excitatory modulation of the amplitudeof bladder contractions due to regulation of the descending glutamatergiclimb of the spinobulbospinal bladder-reflex pathway (4, 35).These mechanisms could involve activation of three subtypes of $alpha$ ₁-adrenoceptors: $alpha$ _1A, $alpha$ _1B, and $alpha$ _1D (10). This was examinedin the present experiments by studying the effects on reflex-bladderactivity of intrathecal administration of drugs that selectivelyblock different subtypes of $alpha$ ₁-adrenoceptors.

A preliminary account of this work has been presented in an abstract (34).

	MATERIALS AND METHODS

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

Animal preparation. Experiments were performed on urethane-anesthetized (1.2 g/kg sc) female Sprague-Dawley rats weighing 250-300 g. The tracheawas cannulated with a polyethylene tube (PE-240) to facilitaterespiration, and an intrathecal catheter was inserted accordingto the technique of Yaksh and Rudy (28). The occipital crestof the skull was exposed and the atlanto-occipital membrane wasincised at the midline using the tip of a 16-gauge needle as acutting edge. A catheter (PE-10) filled with artificial cerebrospinalfluid (CSF) (7, 17) was inserted through the slit and passedcaudally to the L₆ level of the spinal cord. At the end of theexperiment, a laminectomy was performed to verify the locationof the cathetertip.

A transurethral bladder catheter (PE-90) connected to a pressure transducer was used to record the bladder pressure isovolumetricallywith the urethral outlet ligated. The bladder was filled via thebladder catheter by incremental volumes of physiological salineuntil spontaneous bladder contractions occurred (total volume:0.8-1.5 ml). For isovolumetric recording, the ureters were tieddistally, cut, and the proximal ends cannulated (PE-10) and drainedexternally. This procedure prevented the bladder from fillingwith urine during theexperiment.

The protocols in these studies were approved by the Animal Care and Use Committee of the University ofPittsburgh.

Drugs. Drugs used in these studies included urethane (ethyl carbamate, Sigma, St. Louis, MO), N-[(2-trifluoroethoxy)phenyl],N'-(3-thyminylpropyl)piperazinehydrochloride (RS-100329, Roche Bioscience, Palo Alto, CA) (12,26), [4-(4-amino-6,7-dimethoxyquinazolin-2-yl)-cis-octahydroquinoxalin-1-yl]furan-2-ylmethanone[(+)-cyclazosin, Roche Bioscience] (8, 12, 21), and 8-[2-[4-(2-methoxyphenyl)-1-piperazinyl]ethyl]-8-azaspiro[4.5]decane-7,9-dionedihydrochloride (BMY 7378 Research Biochemicals International,Natick, MA) (9). Urethane was dissolved in distilled water(0.5 g/ml solution). RS-100329 and (+)-cyclazosin were dissolvedin 100% DMSO (20 mM solutions), and BMY 7378-HCl was dissolvedin artificial CSF (10 and 100 mM solutions). Drug doses were calculatedfor the base of each compound. Drugs were administered in smallvolumes (<5 µl), and then the intrathecal catheter was flushedby artificial CSF (7.5 µl).

Multiple doses of drugs or vehicles starting with the smallest amounts were injected in each animal. Increasing amounts wereadministered after bladder contractions recovered to control.Injections were spaced at intervals of at least 30 min even whenbladder activity was notaltered.

Evaluation and statistical analysis. The effects of RS-100329, (+)-cyclazosin, and BMY 7378 were evaluated on the amplitude and frequency of reflex-bladder contractionsrecorded under isovolumetric conditions. The effects of vehiclesolutions [100% DMSO for RS-100329 and (+)-cyclazosin and artificialCSF with pH adjusted to 1.6 or 4.0 for BMY 7378] were also examined.All values are expressed as means ± SE. For statistical data analysis,ANOVA and paired t-test were used to compare the values beforeand after drug administration. Two-way ANOVA and unpaired t-testwere applied to compare the differences between the effects ofdrug and vehicle solution. For all statistical tests, P < 0.05was consideredsignificant.

	RESULTS

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Animals with implanted intrathecal catheters (n = 30) exhibited rhythmic bladder contractions (mean amplitude: 33 ± 2 cmH₂O;range: 17-51 cmH₂O) at a mean frequency of 0.84 ± 0.04 contractions/min(range: 0.43-1.34 contractions/min) under isovolumetric conditionswhen the bladder was filled with 0.8-1.5 ml ofsaline.

Effects of vehicles (100% DMSO or acidic CSF) on bladder activity. The vehicle for RS-100329 and (+)-cyclazosin (up to 5 µl of 100% DMSO followed by 7.5 µl artificial CSF injection) did notalter the frequency of bladder contractions, but a large volumeof vehicle decreased the amplitude of bladder contractions (seeFig. 2). The volume of vehicle for 50- and 100-nmol doses reducedbladder-contraction amplitude by 4.1 ± 1.2% (n = 10) and by 30.1± 11.0% (n = 11), respectively. Therefore, two-way ANOVA (followedby unpaired t-test) was used to compare the dose-response curvesfor vehicle (100% DMSO) with the dose-response curves for RS-100329or (+)-cyclazosin. The dose-response curves for BMY 7378 and itsvehicle (artificial CSF adjusted to pH 1.6 or 4) were comparedin the same manner, although the vehicle for BMY 7378 did notchange bladder activity at any volume (n = 3-6).

Effects of RS-100329, (+)-cyclazosin, or BMY 7378 on bladder activity. RS-100329 in 25-, 50-, and 100-nmol doses decreased the amplitude of bladder contractions by 16-85% (average: 38 ± 9%), 18-100%(average: 52 ± 10%), and 84-100% (average: 95 ± 2%), respectively,whereas smaller doses of the drug (6.25 and 12.5 nmol) had noeffect (Figs. 1 and 2A). The depressant effect occurred within1 min after the administration of the drug and persisted for 7-53min depending on the dose (25 nmol, average: 15 ± 2 min; 50 nmol,average: 18 ± 3 min; 100 nmol, average: 34 ± 4 min). RS-100329in the 50-nmol dose significantly increased (average: 51 ± 14%,range: 4-131%) the frequency of bladder contractions; however,smaller doses (6.25, 12.5, and 25 nmol) and a larger dose (100nmol) had no significant effect (Figs. 1 and 2B).

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Fig. 1. The effects of RS-100329 (6.25, 25, and 50 nmol intrathecal) on bladder activity under isovolumetric conditions in a urethane-anesthetized rat. Note that the 25 and 50 nmol of the drug decreased the bladder-contraction amplitude and 50 nmol increased the bladder-contraction frequency, whereas the small dose (6.25 nmol) had no effect on bladder activity.

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Fig. 2. Graphs showing the effects of intrathecal (it) administration of RS-100329 (n = 7-10), (+)-cyclazosin (n = 3-9), and vehicles (100% DMSO, n = 8-11) for these drugs on amplitude and frequency of bladder contractions under isovolumetric conditions in urethane-anesthetized rats. *P < 0.05, **P < 0.01 (comparison between vehicle and each drug by unpaired t-test following 2-way ANOVA). *Significant differences between measurements taken before and after each drug injection (by paired t-test).

The effects of (+)-cyclazosin were variable between animals and not dose dependent (Fig. 3). The 50-nmol dose significantlydecreased the amplitude of bladder contractions (average: 45 ±11%, range: 6-79%) and increased the bladder-contraction frequency(average: 57 ± 20%, range: 19-145%) for periods ranging from 5to 14 min (average: 9 ± 1 min); whereas smaller and larger doses(25 and 100 nmol) had no significant effect (Fig. 2, A and B)compared with vehicle. However, it should be noted that therewas considerable variation in the effect of the 100-nmol dosethat in three experiments completely blocked bladder contractionsand in three other experiments had minimal effects on bladder-contractionamplitude. Thus the effects of the 100-nmol dose of (+)-cyclazosinon bladder-contraction frequency could be evaluated in only threerats (Fig. 2B). In these animals, the drug produced 35% increasein frequency, which was not statistically significant (P = 0.1361).

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Fig. 3. The effects of (+)-cyclazosin (25 and 50 nmol it) on bladder activity under isovolumetric conditions in an urethane-anesthetized rat. Note that 50 nmol of the drug increased the bladder-contraction frequency. The bladder-contraction amplitude was slightly reduced in this rat; however, the effect of the drug on amplitude varied in different animals. The 25 nmol did not change either the bladder-contraction amplitude or frequency.

BMY 7378 (25, 50, and 100 nmol) did not significantly alter the amplitude or the frequency of bladder contractions (Fig. 4).

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Fig. 4. Graphs showing the effects of it administration of BMY 7378 (n = 6) and drug vehicle (acidic cerebrospinal fluid, n = 3-6) on amplitude and frequency of bladder contractions under isovolumetric conditions in urethane-anesthetized rats. BMY 7378 produced no significant effect on either parameter (comparison between vehicle and drug by unpaired t-test following 2-way ANOVA).

	DISCUSSION

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

In our previous studies in anesthetized rats (4, 35), phenylephrine (an $alpha$ ₁-adrenoceptor agonist) increased the intercontractioninterval (i.e., the time between bladder contractions) and pressurethreshold for inducing micturition during continuous infusioncystometrograms. Under isovolumetric conditions, the drug abolishedbladder activity. On the other hand, doxazosin (a nonselective $alpha$ ₁-adrenoceptor antagonist) decreased intercontraction intervalsduring cystometrograms and increased the bladder-contraction frequencyand decreased bladder-contraction amplitude under isovolumetricconditions. These results indicated that two types of spinal $alpha$ ₁-adrenergicmechanisms are involved in reflex-bladder activity: 1) inhibitorycontrol of the bladder-contraction frequency presumably due tomodulation of afferent processing in the spinal cord and 2) excitatorymodulation of bladder-contraction amplitude due to regulationof the descending limb of the spinobulbospinal bladder-reflexpathway. The present experiments have provided insights into the $alpha$ ₁-adrenoceptor subtypes involved in these modulatorymechanisms.

Intrathecal administration of RS-100329, an $alpha$ _1A-adrenoceptor antagonist, suppressed bladder-contraction amplitude in a dose-dependentmanner, indicating that the descending limb of the micturition-reflexpathway is facilitated by bulbospinal noradrenergic inputs actingon $alpha$ _1A-adrenoceptors. Certain doses of RS-100329 or (+)-cyclazosin,an $alpha$ _1B-adrenoceptor antagonist, significantly increased the bladder-contractionfrequency, indicating that $alpha$ _1A- or $alpha$ _1B-adrenoceptors modulatethe spinal processing of afferent input from bladder mechanoreceptors.It is likely that these adrenergic modulatory mechanisms regulateN-methyl-D-aspartate (NMDA) and non-NMDA glutamatergic synapsesthat play an essential role in the micturition-reflex pathway(31-33).

Although RS-100329, which has a high affinity and selectivity for the $alpha$ _1A-adrenoceptor versus the $alpha$ _1B- and $alpha$ _1D-adrenoceptorsubtypes (26), suppressed bladder-contraction amplitude in adose-dependent manner, only the 50-nmol dose significantly increasedthe frequency of bladder contractions. Smaller and larger doses(25 and 100 nmol) were ineffective. The lack of effect on thisparameter by the largest dose (100 nmol) raises the possibilitythat $alpha$ _1A-adrenoceptors are not involved or that the high dosenonselectively affected other transmitter mechanisms to negatethe effects of the lowerdose.

In contrast to the prominent effect of RS-100329 on bladder activity, the $alpha$ _1D-antagonist BMY 7378 had no significant effect.This indicates that $alpha$ _1D-adrenoceptors do not play an importantrole in controlling reflex-bladder activity under the conditionsof our experiments. On the other hand, the role of $alpha$ _1B-adrenoceptorsis less clear. The effects of (+)-cyclazosin were complicated.The 50-nmol dose had significant effects on bladder-contractionamplitude and frequency, whereas lower and higher doses did notproduce significant changes. There may be several reasons forthis unusual dose-response relationship. First, the vehicle (100%DMSO) may have interfered with the effect of the drug. Second,(+)-cyclazosin may not be sufficiently selective at $alpha$ _1B-adrenoceptors.Radioligand binding studies indicated that (+)-cyclazosin wasa potent and selective ligand for the $alpha$ _1B-adrenoceptor subtype(8), whereas functional studies indicated that (+)-cyclazosindisplayed low potency and did not act as a competitive antagonist(21). The lack of any effect on either parameter by 100 nmolmay be due to the interaction with other receptor(s). Furthermore,in the present studies, the largest volume of the vehicle (100%DMSO) for RS-100329 and (+)-cyclazosin significantly decreasedthe amplitude of bladder contractions. Therefore, the vehiclecould have interacted synergistically with the drugs to enhancethe depression of bladder-contraction amplitude and converselyto antagonize the facilitatory drug effects on the frequency ofbladdercontractions.

The present results suggesting that $alpha$ _1A-adrenoceptors are the most important and that $alpha$ _1B-adrenoceptors are of lesser importancein the regulation of reflex-bladder activity are consistent withthe previous studies using a radioligand binding assay (24),which revealed that in the rat lumbar spinal cord, the $alpha$ _1A- and $alpha$ _1B-adrenoceptor populations comprised 70% and 30%, respectively,of the total population of $alpha$ ₁-adrenoceptors in the spinal ventraland dorsal horns and that $alpha$ _1D-adrenoceptors were expressed atvery lowlevels.

In other spinal systems, $alpha$ _1A-adrenoceptors also seem to play a major role. For example, in vivo experiments in rats indicatedthat spinal $alpha$ _1A-adrenoceptors mediated the spontaneous tail flicksinduced by 8-hydroxy-2-(di-n-propylamino)tetralin (1), andexperiments on the rat lumbar spinal cord slice preparation revealedthat $alpha$ _1A-adrenoceptors were essential for adrenergic facilitationof spinal motoneuron activity (23). On the contrary, Wilsonand Minneman (27) reported that in the in vitro cervical spinalcord preparation, 42% of $alpha$ ₁-adrenoceptors were inactivated bychloroethylclonidine, an $alpha$ _1B/1D-adrenoceptor antagonist, suggestinga somewhat lower proportion of $alpha$ _1A-adrenoceptors at this levelof thecord.

Because bladder activity in the present studies was evaluated under isovolumetric conditions in which reflex-bladder contractionsoccurred against a closed outlet, it might be questioned whetherthis bladder activity is elicited via different mechanisms than"normal" voiding reflexes. For example, isovolumetric contractionsmight activate high-threshold bladder afferents that, in turn,stimulate nociceptive pathways in the spinal cord. Thus the effectsof adrenergic drugs on this type of bladder activity might reflectadrenergic modulation of visceral nociceptive mechanisms ratherthan the control of normal micturition. However, we believe thatthis is unlikely because isovolumetric bladder contractions, likevoiding reflexes, are dependent on similar central mechanismsincluding glutamatergic transmission and a spinobulbospinal-reflexpathway (31-33). In addition, doxazosin, a nonselective $alpha$ ₁-adrenoceptorantagonist, decreased micturition pressure in conscious rats duringcontinuous-infusion cystometrograms (CMGs) with an open urethraloutlet (11), and phenylephrine, $alpha$ ₁-adrenoceptor agonist, alteredthe profile of bladder contractions in anesthetized rats duringcontinuous CMGs with the bladder catheter inserted through a ureter(14). Thus $alpha$ ₁-adrenergic drugs are still effective in modulatingthe activity of rat bladder even under conditions in which voidingis unobstructed and bladder afferent activity is entirelynonnoxious.

In summary, the present results taken together with previous studies (4, 35) indicate that two types of spinal $alpha$ ₁-adrenergicmechanisms are involved in the control of reflex activity in anesthetizedrats: 1) $alpha$ _1A- or $alpha$ _1B-adrenergic inhibitory control of afferentprocessing in the spinal cord and 2) $alpha$ _1A-adrenergic excitatorymodulation of the descending limb of bladder-reflex pathway (Fig.5). These two mechanisms possibly involving $alpha$ _1A- and $alpha$ _1B-adrenoceptorsacting in concert would facilitate urine storage by increasingbladder capacity and also enhance voiding efficiency by increasingparasympathetic nerve activity and the amplitude of bladder contractions.

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Fig. 5. Scheme showing putative mechanisms using $alpha$ ₁-adrenoceptor subtypes in the L₆-S₁ spinal cord that contribute to the control of reflex activity of the urinary bladder in the rat. PGN, preganglionic neurons; PMC, pontine micturition center. Descending noradrenergic pathways from the brain stem may excite inhibitory interneurons to regulate the sensory pathways from the bladder and excitatory interneurons to regulate the efferent pathway to the bladder.

Perspectives

In clinical urology, nonselective $alpha$ ₁-adrenergic antagonists have been used in the treatment of benign prostatic hypertrophy(15). This therapy was initially designed to block adrenergicreceptors in the proximal urethra and prostate gland and therebyreduce urethral resistance and increase urine flow. It was discoveredthat the drugs not only improved urine flow but also reduced irritativebladder symptoms. However, the changes in urinary flow rates werenot correlated with the improvement in symptoms (15). This raisesthe possibility that the two effects might occur by differentmechanisms. The reduction in abnormal bladder sensations couldbe mediated by a suppression of unstable bladder contractionsdue to an effect on efferent pathways to the bladder. This couldoccur as a result of actions at various sites including 1) thespinal cord, as suggested by the present experiments, 2) at presynaptic $alpha$ ₁-adrenergic facilitatory receptors on efferent parasympatheticnerve terminals in the bladder wall (20, 22), or 3) at $alpha$ ₁-adrenergicfacilitatory receptors in bladder parasympathetic ganglia (13).Thus $alpha$ ₁-adrenergic receptors at various sites in the peripheraland central nervous system, as well as in smooth muscle, may playa role in voidingfunction.

	ACKNOWLEDGEMENTS

We acknowledge Drs. A. P. D. W. Ford and T. J. Williams (Center for Biological Research, Roche Bioscience, Palo Alto, CA)for the gift of the drugs used in the present studies and helpfuldiscussions during thisproject.

	FOOTNOTES

This work was supported by National Institute of Diabetes and Digestive and Kidney Diseases Grants DK-49430 and DK- 51402(W. de Groat) and a research grant from Roche Bioscience (W. deGroat).

Address for reprint requests and other correspondence: M. Yoshiyama, Dept. of Neurology, Chiba Univ. Graduate School of Medicine,1-8-1 Inohana, Chuo-ku, Chiba, 260-8670, Japan (E-mail: PXN15164{at}nifty.ne.jp).

The costs of publication of this article were defrayed in part by the payment of page charges. The article must thereforebe hereby marked "advertisement" in accordance with 18 U.S.C.Section 1734 solely to indicate thisfact.

Received 3 August 2000; accepted in final form 13 December 2000.

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