Effects of Ethanol on Recombinant Human Neuronal Nicotinic Acetylcholine Receptors Expressed in Xenopus Oocytes

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Vol. 289, Issue 2, 774-780, May 1999

**Effects of Ethanol on Recombinant Human Neuronal Nicotinic Acetylcholine Receptors Expressed in Xenopus Oocytes¹**

Rita A. Cardoso, Susan J. Brozowski, Laura E. Chavez-Noriega, Michael Harpold, C. Fernando Valenzuela and R. Adron Harris

Department of Neurosciences, University of New Mexico Health Sciences Center, Albuquerque, New Mexico (R.A.C., C.F.V.); Department of Pharmacology, University of Colorado Health Sciences Center, Denver, Colorado (S.J.B.); SIBIA Neurosciences, Inc., La Jolla, California (L.E.C.-N.); National Center for Genome Resources, Santa Fe, New Mexico (M.H.); and Institute for Cellular and Molecular Biology, University of Texas, Austin, Texas (R.A.H.)

	Abstract

Top Abstract Introduction Materials and Methods Results Discussion References

Alcohol and tobacco use is highly correlated in humans, and studies with animal models suggest an interaction of alcohol withneuronal nicotinic acetylcholine receptors (nAChRs). The aim ofthe present study was to characterize the effect of acute ethanoltreatment on different combinations of human nAChR (hnAChR) subunitsexpressed in Xenopus oocytes. Ethanol (75 mM) potentiated ACh-inducedcurrents in $alpha$ ₂ $beta$ ₄, $alpha$ ₄ $beta$ ₄, $alpha$ ₂ $beta$ ₂, and $alpha$ ₄ $beta$ ₂ receptors. This effectwas due to an increase in E_max, without a change in the EC₅₀ orHill coefficient. hnAChR $alpha$ ₂ $beta$ ₄ did not develop tolerance to repeatedapplications of ethanol or continuous exposure (10 min). The $alpha$ ₃ $beta$ ₂and $alpha$ ₃ $beta$ ₄ combinations were insensitive to ethanol. Low concentrationsof ethanol (25 and 50 mM) significantly inhibited homomeric $alpha$ ₇receptor function, but these receptors showed highly variableresponses to ethanol. These results indicate that ethanol effectson hnAChRs depend on the receptor subunit composition. In lightof recent evidence indicating that nAChRs mediate and modulatesynaptic transmission in the central nervous system, we postulatethat acute intoxication might involve ethanol-induced alterationsin the function of thesereceptors.

	Introduction

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There is a high correlation between alcohol and tobacco use in humans (reviewed in Istvan and Matarazzo, 1984). Alcoholicsare more likely to use tobacco than nonalcoholics, and alcoholicsmokers consume more cigarettes per day than nonalcoholic smokers(reviewed in Istvan and Matarazzo, 1984; DiFranza and Guerrera,1990). In laboratory animals, nicotine treatment increases ethanolconsumption (Blomqvist et al., 1996). Mouse and rat lines wereselectively bred for differences in ethanol sensitivity, and itwas found that animals that have high sensitivity to ethanol alsohave high sensitivity to nicotine (De Fiebre et al., 1987, 1990,1991). Recently, Collins et al. (1996) suggested that cross-tolerancebetween nicotine and ethanol in laboratory animals might involvea change in neuronal nicotinic acetylcholine receptor (nAChR)function. The studies mentioned above suggest that common geneproducts are involved in the interaction between ethanol and nicotine,and there is considerable interest in determining whether thisinteraction is mediated, at least in part, bynAChRs.

nAChRs are members of a superfamily of ligand-gated ion channels. A gene family of 11 nAChR subunits ( $alpha$ _2-9, $beta$ _2-4)has been identified (McGehee and Role, 1995). Receptors containing $alpha$ _2-6 subunits are usually expressed as heteromers in combinationwith $beta$ _2-4 subunits (reviewed in Role and Berg, 1996). Themajority of heteromeric neuronal nicotinic binding sites expressedin the central nervous system possess the $alpha$ ₄ $beta$ ₂ or $alpha$ ₄ $alpha$ ₅ $beta$ ₂ subunitcombinations (Flores et al., 1992; Zoli et al., 1998). Recentexperiments with $beta$ ₂ mutant mice suggest that $alpha$ ₂ $beta$ ₂ and $alpha$ ₃ $beta$ ₂ receptorsare expressed in the interpeduncular nucleus and the hippocampus(Zoli et al., 1998). The $alpha$ ₃ $beta$ ₄ or $alpha$ ₃ $alpha$ ₅ $beta$ ₄ subunit combinations arepredominantly expressed in the medial habenula, interpeduncularnucleus, and dorsal medula (Zoli et al., 1998). The $alpha$ ₄ $beta$ ₄ or $alpha$ ₂ $beta$ ₄subunit combinations are predominantly expressed in the lateralmedial habenula and dorsal interpeduncular nucleus, respectively(Zoli et al., 1998). The $alpha$ ₇, $alpha$ ₈, and $alpha$ ₉ subunits can form homomericreceptors (reviewed in Role and Berg, 1996). nAChRs receptorscontaining $alpha$ ₇ subunits are the major binding sites for $alpha$ -bungarotoxin( $alpha$ -BGT) in the mammalian central nervous system and are predominantlyexpressed in the cortex and limbic areas (Orr-Urtreger et al.,1997; Zoli et al., 1998).

The acute effects of ethanol on nAChRs have been studied previously with conflicting results. It was recently reported thatethanol (5-100 mM) inhibits the function of $alpha$ ₇ nAChRs expressedin Xenopus oocytes by a mechanism that involves the amino-terminaldomain of the receptor (Yu et al., 1996). In rat pheochromocytoma(PC12) cells, continuous bath application of low concentrationsof ethanol (0.1-10 mM) produced an increase in desensitizationof nAChR responses, with variable changes in the current peakamplitude (Nagata et al., 1996). Recently, Covernton and Connolly(1997) showed that different combinations of rat nAChRs subunitsexpressed in Xenopus oocytes are sensitive to acute exposure toethanol under some experimental conditions. The aim of the presentstudy was to characterize the effect of acute ethanol treatmenton the recently characterized human nAChRs (hnAChR; Chavez-Noriegaet al., 1997) and to assess the effects of ethanol on receptorswith different subunitcompositions.

	Materials and Methods

Top Abstract Introduction Materials and Methods Results Discussion References

Materials. Xenopus laevis female frogs were purchased from Xenopus I (Ann Arbor, MI) or Nasco (Fort Atkinson, WI). Acetylcholine chloride,atropine sulfate, collagenase type 1A, streptomycin/penicillin,gentamicin, and other reagents were purchased from Sigma ChemicalCo. (St. Louis, MO). Ethanol was from Aaper Alcohol and Chemical(Shelbyville, KY). XL-1 Blue cells were from Stratagene (La Jolla,CA). The QIAFilter Maxi kit was from Qiagen (Chatworth, CA), andthe mCAP mRNA capping kit was from Stratagene (La Jolla,CA).

cDNA and cRNA Preparation. The hnAChR subunits $alpha$ ₂, $alpha$ ₃, $alpha$ _4, $alpha$ ₇, $beta$ ₂, and $beta$ ₄ were cloned from cDNA libraries prepared from human brain and the human IMR32neuroblastoma cell line and subcloned into different expressionvectors, $alpha$ ₂ and $alpha$ ₃ in pCMV-T7 to 3; $alpha$ ₄, $alpha$ ₇, and $beta$ ₄ in pcDNA3;and $beta$ ₂ in pSP64T (Elliott et al., 1996). XL-1 Blue cells weretransformed with the cDNAs, and amplified plasmid was purifiedwith the QIAFilter Maxi kit. In vitro transcripts were preparedusing the mRNA cappingkit.

Eletrophysiological Recording of Xenopus Oocytes. Isolation and injection of Xenopus laevis oocytes were performed as described previously by Mascia et al. (1996). Oocyteswere injected with 40 nl of diethyl pyrocarbonate-treated watercontaining 20 to 100 ng of $alpha$ _x $beta$ _y subunit combinations of cRNA ina 1:1 ratio or 50 ng of $alpha$ ₇cRNA.

For electrophysiological recording, oocytes were placed in a rectangular chamber (~100 µl) and perfused (2 ml/min) with bufferND96 (96 mM NaCl, 2 mM KCl, 1 mM MgCl₂, 1.8 mM CaCl₂, and 10 mMHEPES, pH 7.4) containing 1 µM atropine sulfate. Oocytes wereimpaled with two glass electrodes (0.5-10 M $Omega$ ) filled with 3 MKCl and clamped at $-$ 70 mV using a Warner Instruments (Hamden,CT) oocyte clamp (model OC-725C).

Agonist (acetylcholine or nicotine) was applied for 20 s at 5-min intervals. Unless indicated otherwise, ethanol was preappliedfor 2 min to allow complete equilibration in the bath and thenimmediately coapplied with agonist for 20 s. All solutions wereprepared on the day of theexperiment.

Statistical Analysis. Results are expressed as percentages of change from control responses, which were measured before and after each ethanol applicationto take into account possible shifts in the control current throughoutthe experiment. The "n" values refer to number of oocytes studied.Each experiment was carried out with oocytes from at least twodifferent frogs. Effects of ethanol were analyzed by either one-sampleStudent's t test (against a theoretical mean of zero) or one-wayANOVA. Statistical analysis and curve fitting were performed usingGraphPad Prism software (San Diego, CA). To analyze dose/responsecurves, a four-parameter logistic equation (sigmoid) with variableslope was used (Y = Bottom + (Top $-$ Bottom)/(1+ 10^{((Log EC50-X) · (Hill
Slope))}), where X is the logarithm of concentration, and Y is the response).The best fit for the data was obtained without fixing any of theparameters in this equation. Data are presented as mean ± S.E.M.

	Results

Top Abstract Introduction Materials and Methods Results Discussion References

Effects of Ethanol on hnAChRs Are Reproducible and Reversible. Our first goal was to evaluate whether the effects of ethanol were reproducible and reversible. Concentration-response curvesfor acetylcholine were obtained for the different hnAChR subunitcombinations. Currents induced by an EC₃₀ dose of ACh in $alpha$ ₂ $beta$ ₄were equally potentiated after 2, 5, and 10 min of preincubationwith 75 mM ethanol, and essentially the same level of potentiationwas obtained after washout and re-exposure to ethanol (Fig. 1;ANOVA, p > .05).

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Fig. 1. Currents induced by an EC₃₀ ACh in $alpha$ ₂ $beta$ ₄ are equally potentiated after 2, 5, and 10 min of preincubation with 75 mM ethanol, and the same level of potentiation is obtained after washout and re-exposure to ethanol. Top panel, representative current tracing obtained from a single Xenopus oocyte. The bars represent the period of application of drugs. In the bottom panel, ethanol was preapplied for 2, 5, and 10 min before coapplication for 20 s with ACh (23 µM). Control responses to ACh were measured 5 min before and after ethanol. After that, oocytes were subjected to 5 min of washout and 2 min of preincubation with ethanol, and they were re-exposed to ACh+EtOH. After 5 min, a new ACh control response was determined. Values are mean ± S.E.M. from four to six oocytes.

Effects of Ethanol Depend on the hnAChR Subunit Composition. The effects of 75 mM ethanol on ACh concentration curves in oocytes expressing six different combinations of hnAChR subunitsare shown in Figs. 2-4 and Table 1. Ethanol potentiated ACh-gatedcurrents in $alpha$ ₂ $beta$ ₂ and $alpha$ ₄ $beta$ ₂, and this was independent of the concentrationof ACh (ANOVA, p > .05), and characterized by an increase in theE_max without change in the EC₅₀ or Hill coefficient. Ethanol alsoinduced a significant increase in the E_max of $alpha$ ₂ $beta$ ₄ and $alpha$ ₄ $beta$ _4, anddid not change the EC₅₀ or Hill coefficient for ACh. The potentiationof agonist responses produced by ethanol in both of these receptorconfigurations was inversely proportional to ACh concentration(ANOVA, p $<=$ .001 and p $<=$ .05, respectively).

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Fig. 2. Ethanol selectively potentiates some hnAChR subunit combinations. Representative tracings of ACh-induced currents before and after preincubation with 75 mM ethanol. Oocytes were stimulated with ACh for 20 s, followed by 5 min of wash, then 2 min of preincubation with EtOH, which was immediately coapplied with ACh and once more washed for 5 min and re-exposed to ACh. Note that the effect of ethanol in all receptors was reversible. Bars represent period of treatment with drugs.

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Fig. 3. Effect of 75 mM ethanol in the ACh concentration-response curve in Xenopus oocytes expressing $alpha$ ₂ $beta$ ₂ (top), $alpha$ ₃ $beta$ ₂ (middle), and $alpha$ ₄ $beta$ ₂ (bottom). Drug application protocols are the same as in Fig. 2. ACh concentration-response curves were fitted using GraphPad Prism software, as described in Materials and Methods. Values are mean ± S.E.M. from five to seven oocytes. Shown in the inset is the percentage of potentiation (mean ± S.E.M.) produced by ethanol as a function of ACh concentration. Error bars not visible are smaller than symbols.

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Fig. 4. Effect of 75 mM ethanol on the ACh concentration-response curve in Xenopus oocytes expressing $alpha$ ₂ $beta$ ₄ (top), $alpha$ ₃ $beta$ ₄ (middle), and $alpha$ ₄ $beta$ ₄ (bottom). Drug application protocols are the same as in Fig. 2. ACh concentration-response curves were fitted using GraphPad Prism software, as described in Materials and Methods. Values are mean ± S.E.M. from 6 to 12 oocytes. Shown in the inset is the percentage of potentiation (mean ± S.E.M.) produced by ethanol as a function of ACh concentration. Error bars not visible are smaller than symbols.

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TABLE 1
Effect of EtOH on different parameters of ACh response in hnAchRs

Receptors formed by the $alpha$ ₃ $beta$ ₂ combination of hnAChR subunits were insensitive to ethanol, as well as $alpha$ ₃ $beta$ ₄ receptors at submaximalagonist concentrations. A small but statistically significantdecrease in E_max induced by 75 mM ethanol ( $-$ 13.8 ± 3.9%) was observedwith $alpha$ ₃ $beta$ ₄.

Potentiation by Ethanol of $alpha$ ₂ $beta$ ₄ and $alpha$ ₄ $beta$ ₂ hnAChRs Is Concentration Dependent. To study the ethanol concentration-response relationship, we chose $alpha$ ₄ $beta$ ₂ and $alpha$ ₃ $beta$ ₄ as nAChR subtype combinations that are thoughtto be abundantly expressed in the central nervous system and peripheralnervous system (McGehee and Role, 1995), and differ in ethanolsensitivity (present results). We also included the $alpha$ ₂ $beta$ ₄ combination,because it allowed us to determine whether the $alpha$ or $beta$ subunitwas critical for the alcohol resistance of the $alpha$ ₃ $beta$ ₄ receptor.To evaluate the concentration-response effect of ethanol on hnAChRs,we used an ACh concentration corresponding to the EC₃₀ for eachreceptor, which was 23 µM for $alpha$ ₂ $beta$ ₄, 0.5 µM for $alpha$ ₄ $beta$ ₂, and 127 µMfor $alpha$ ₃ $beta$ ₄. ACh-induced currents in $alpha$ ₂ $beta$ ₄ and $alpha$ ₄ $beta$ ₂ were potentiatedin a concentration-dependent manner by ethanol. The lowest ethanolconcentration that produced a statistically significant potentiationwas 50 mM for both subunit combinations. In contrast, $alpha$ ₃ $beta$ ₄ receptorswere insensitive to all concentrations of ethanol tested underthese recording conditions (Fig. 5)

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Fig. 5. Effect of different concentrations of ethanol on ACh-induced currents in oocytes expressing $alpha$ ₂ $beta$ ₄, $alpha$ ₃ $beta$ ₄, and $alpha$ ₄ $beta$ ₂. Ethanol was applied for 2 min before coapplication with ACh for 20 s. An EC₃₀ dose of ACh was used for each receptor: 23 µM for $alpha$ ₂ $beta$ ₄, 127 µM for $alpha$ ₃ $beta$ ₄, and 0.5 µM for $alpha$ ₄ $beta$ ₂. Values are mean ± S.E.M. from 7 to 11 oocytes. Error bars not visible are smaller than symbols. *, lowest concentration of ethanol with a significant (p $<=$ .05) effect on $alpha$ ₂ $beta$ ₄ and $alpha$ ₄ $beta$ ₂.

Low Concentrations of Ethanol Inhibit Homomeric $alpha$ ₇ hnAChRs. We also tested different concentrations of ethanol (25-200 mM) on the nicotine-gated currents mediated by homomeric hnAChR $alpha$ ₇. These receptors presented a highly variable response to ethanol,with changes ranging from 43% inhibition to 17% potentiation at25 mM ethanol and from 75% inhibition to 40% potentiation at 200mM ethanol. Despite the large variability in the responses, statisticalanalysis of average effects showed that low concentrations ofethanol significantly inhibited these receptors (25 mM: $-$ 17 ±6% and 50 mM: $-$ 29 ± 6%; Student's t test, p $<=$ .05), but higherconcentrations did not alter its function (Fig. 6).

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Fig. 6. Effect of different concentrations of ethanol on nicotine-induced currents in oocytes expressing hnAChR $alpha$ ₇. Nicotine (Nic) was applied for 20 s, and after 5 min of washout, oocytes were pre-exposed to 75 mM EtOH for 2 min before coapplication of Nic+EtOH. The nicotine concentration used was the EC₃₀ (32 µM) for $alpha$ ₇. Top, each point represents data from a single oocyte. Bottom, values are mean ± S.E.M. from 8 to 14 oocytes. *p $<=$ .05, Student's t test.

	Discussion

Top Abstract Introduction Materials and Methods Results Discussion References

Our results demonstrate that recombinant hnAChRs with distinct subunit configurations are differentially affected by pharmacologicallyrelevant doses of ethanol (concentrations $<=$ 100 mM; Deitrich andHarris, 1996). The $alpha$ ₂ $beta$ ₄ and $alpha$ ₄ $beta$ ₂ combinations were the most sensitivereceptors to potentiation by ethanol, and the $alpha$ ₄ $beta$ ₄ and $alpha$ ₂ $beta$ ₂ combinationswere slightly less sensitive. Interestingly, receptors containingthe $alpha$ ₃ subunit plus either the $beta$ ₂ or $beta$ ₄ subunits were insensitiveto ethanol. Homomeric $alpha$ ₇ receptors displayed highly variable responsesto ethanol, and the average effect of ethanol was inhibitory atlow ethanol concentrations. From these results, we conclude thatthe sensitivity to ethanol of hnAChRs depends on the subunit compositionof the receptorsexpressed.

The effects of ethanol on rat nAChR were previously suggested to be dependent on the subunit composition of the receptor (Coverntonand Connolly, 1997). It was found that the $alpha$ ₃ $beta$ ₄ combination ofrat nAChR had highly variable responses (ranging from potentiationto inhibition) to low concentrations of ethanol. The authors alsoreported that the $alpha$ ₇, $alpha$ ₃ $beta$ ₂, $alpha$ ₄ $beta$ ₂, and $alpha$ ₄ $beta$ ₄ receptors were lesssensitive to low concentrations of ethanol than $alpha$ ₃ $beta$ ₄ receptors.We obtained similar results in our initial studies (data not shown).However, variability was minimized, and results were different(see above) than those of Covernton and Connolly (1997) when ethanolwas preapplied. We decided to preapply ethanol because, in vivo,the receptors are not only exposed to ethanol at the time theyare activated by acetylcholine, but they would be expected tobe in contact with ethanol before activation. Covernton and Connolly(1997) found that $alpha$ ₃ $beta$ ₄ receptors developed tolerance to repeatedexposure to ethanol, which was not seen in our experiments. Thesedifferences might be due to either experimental protocol or speciesdifferences. Indeed, Chavez-Noriega et al. (1997) showed thathuman clones of nAChR have distinct pharmacological profiles comparedwith clones from other species. It should be noted that we obtainedsimilar results as Covernton and Connolly (1997) with rat $alpha$ ₇ receptors,which were modulated in a variable manner by ethanol. Interestingly,we found that the average effect of low concentrations of ethanolwas inhibitory, which is in agreement with the findings of anotherstudy (Yu et al., 1996).

The differential sensitivity of hnAChRs with different subunit compositions to ethanol may be the basis for the observationsthat ethanol potentiates the excitatory responses to nicotinein the substantia nigra reticulata and ventral pallidum (Criswellet al., 1993) but inhibits them in the locus ceruleus (Fröhlichet al., 1994). The differential sensitivity of distinct nAChRconfigurations to ethanol might also explain why ethanol inhibitsnAChR-dependent firing of Purkinje neurons (Freund and Palmer,1997). Unfortunately, the precise subunit composition of functionalnAChRs present in those regions has not yet been elucidated. Also,it is not clear whether alcohol acts on pre- or postsynaptic receptors,orboth.

It is interesting to compare the magnitude of the acute effects of ethanol on nAChRs versus its effects on other members ofthis superfamily of ligand-gated ion channels studied previouslyin Xenopus oocytes. Homomeric glycine $alpha$ ₁ receptors were potentiatedby 25 to 200 mM ethanol by 20 to 110% at glycine EC₂ concentrations(Mascia et al., 1996), whereas GABA_A receptors with differentsubunit compositions were potentiated by 0 to 60% at submaximalagonist concentrations (Mihic et al., 1994, 1997; Harris et al.,1997). 5-HT₃ receptors were potentiated by 25 to 200 mM ethanolby 25 to 40% at submaximal agonist concentrations (Machu and Harris,1994). A striking difference is that ethanol alters the functionof glycine, GABA_A, and 5-HT₃ receptors by changing the neurotransmitterEC₅₀ with no change in the E_max (Machu and Harris,1994; Mihicet al., 1994; Mascia et al., 1996). Thus, ethanol appears to havea rather unique action on hnAChRs dose/response curves when comparedwith other members of this family of ligand-gated ionchannels.

Significance. A number of recent studies found that $alpha$ -BGT-sensitive as well as $alpha$ -BGT-insensitive nAChRs modulate neurotransmitter releasefrom presynaptic terminals (reviewed in Role and Berg, 1996).Therefore, it is possible that the effects of ethanol on presynapticnAChRs result in alterations in the function of pathways involvinga number of different neurotransmitters. For instance, nicotineenhances glutamatergic, cholinergic, and monoaminergic synaptictransmission by activation of presynaptic nAChRs that contain,at least in part, the $alpha$ ₇ subunit (McGehee et al., 1995; Gray etal., 1996; Guo et al., 1998; Li et al., 1998). Experiments with $alpha$ -conotoxin MII, which is a selective inhibitor of $alpha$ ₃ $beta$ ₂ nAChRs,suggest that these receptors mediate nicotine-stimulated dopaminerelease in rat striatal synaptosomes (Kulak et al., 1997). Experimentswith $alpha$ -conotoxin AuIB, which is a selective blocker of $alpha$ ₃ $beta$ ₄ nAChRs,suggest that these receptors mediate nicotine-induced releaseof norepinephrine in rat hippocampal synaptosomes (Luo et al.,1998). In our studies, the $alpha$ ₃ $beta$ ₂ and $alpha$ ₃ $beta$ ₄ receptor configurationswere insensitive to ethanol, which suggests that ethanol doesnot act by modulating neurotransmitter release mediated by thesereceptors. However, ethanol could affect neurotransmitter releasemediated by $alpha$ ₇ receptors, which were inhibited by it at low concentrations.Ethanol could also enhance neurotransmitter release controlledby $alpha$ ₄ $beta$ ₂ nAChRs; Alkondon et al. (1997) recently postulated thatactivation of $alpha$ ₄ $beta$ ₂ receptors might induce GABA release from hippocampalinterneurons. A similar finding was reported by Yang et al. (1996)in the rat medialseptum.

Finally, it is interesting that most, if not all, drugs of abuse stimulate dopamine neurotransmission in the mesolimbic system,including nicotine and alcohol (Pontieri et al., 1996

; Blomqvistet al., 1997

). It has been suggested that the stimulation of dopaminergictransmission in the mesolimbic system by ethanol involves theactivation of nAChRs in the ventral tegmental area; unfortunately,the subunit composition of mesolimbic nAChRs has not yet beenaddressed (Blomqvist et al., 1996

, 1997

). A better understandingof the regional distribution of different subunit combinationsof nAChRs as well as of molecular interactions between ethanoland nAChRs might provide targets for the development of pharmacologicaltools to control alcohol and tobaccoaddictions.

	Footnotes

Accepted for publication December 30, 1998.

Received for publication October 1, 1998.

¹ Supported by NIH Grants K01-AA00227 (C.F.V.), AA06399 (R.A.H.), AA03527 (R.A.H.).

Send reprint requests to: R. Adron Harris, PhD, Institute for Cellular and Molecular Biology, University of Texas at Austin, 2500 Speedway, Austin, TX 78712-1095.

	Abbreviations

nAChR, neuronal nicotinic acetylcholine receptor; BGT, bungarotoxin; GABA, $gamma$ -aminobutyric acid; 5-HT, 5-hydroxytryptamine; ACh, acetylcholine; Nic, nicotine; HEPES, 4-(2-hydroxyethyl)-1-piperazine-ethanesulfonic acid; EtOH, ethanol.

	References

Top Abstract Introduction Materials and Methods Results Discussion References

Alkondon M, Pereira EFR, Barbosa CTF and Albuquerque EX (1997) Neuronal nicotinic acetylcholine receptor activation modulates $gamma$ -aminobutyric acid release from CA1 neurons of rat hippocampal slices. J Pharmacol Exp Ther 283: 1396-1411[Abstract/Free Full Text].
Blomqvist O, Ericson M, Johnson DH, Engel JA and Söderpalm B (1996) Voluntary ethanol intake in the rat: Effects of nicotinic acetylcholine receptor blockade or subchronic nicotine treatment. Eur J Pharmacol 314: 257-267[Medline].
Blomqvist O, Ericson M, Engel JA and Söderpalm B (1997) Accumbal dopamine overflow after ethanol: Localization of the antagonizing effect of mecamylamine. Eur J Pharmacol 334: 149-156[Medline].
Chavez-Noriega LE, Crona JH, Washburn MS, Urrutia A, Elliott KJ and Johnson EC (1997) Pharmacological characterization of recombinant human neuronal nicotinic acetylcholine receptors h $alpha$ 2 $beta$ 2, h $alpha$ 2 $beta$ 4, h $alpha$ 3 $beta$ 2, h $alpha$ 3 $beta$ 4, h $alpha$ 4 $beta$ 2, h $alpha$ 4 $beta$ 4 and h $alpha$ 7 expressed in Xenopus oocytes. J Pharmacol Exp Ther 280: 346-356[Abstract/Free Full Text].
Collins AC, Wilkins LH, Slobe BS, Cao J-Z and Bullock AE (1996) Long-term ethanol and nicotine treatment elicit tolerance to ethanol. Alcohol Clin Exp Res 20: 990-999[Medline].
Covernton PJO and Connolly JG (1997) Differential modulation of rat neuronal nicotinic receptor subtypes by acute application of ethanol. Br J Pharmacol 122: 1661-1668[Medline].
Criswell HE, Simson PE, Duncan GE, McCown TJ, Herbert JS, Morrow AL and Breese GR (1993) Molecular basis for regionally specific action of ethanol on $gamma$ -aminobutyric acid_A receptors: Generalization to other ligand-gated ion channels. J Pharmacol Exp Ther 267: 522-537[Abstract/Free Full Text].
De Fiebre CM, Medhurst LJ and Collins AC (1987) Nicotine response and nicotinic receptors in long-sleep and short-sleep mice. Alcohol 4: 493-501[Medline].
De Fiebre CM, Marks MJ and Collins AC (1990) Ethanol-nicotine interactions in long-sleep and short-sleep mice. Alcohol 7: 249-257[Medline].
De Fiebre CM, Romm E, Collins JT, Draski LJ, Deitrich RA and Collins AC (1991) Response to cholinergic agonists of rats selectively bred for differential sensitivity to ethanol. Alcohol Clin Exp Res 15: 270-276[Medline].
Deitrich RA and Harris RA (1996) How much alcohol should I use in my experiments? Alcohol Clin Exp Res 20: 1-2[Medline].
DiFranza JR and Guerrera MP (1990) Alcoholism and smoking. J Stud Alcohol 51: 130-135[Medline].
Elliott KJ, Ellis SB, Berckhan KJ, Urrutia A, Chavez-Noriega LE, Johson EC, Velicelebi G and Harpold M (1996) Comparative structure of human neuronal $alpha$ 2- $alpha$ 7 and $beta$ 2- $beta$ 4 nicotinic acetylcholine receptor subunits and functional expression of the $alpha$ 2, $alpha$ 3, $alpha$ 4, $alpha$ 7, $beta$ 2 and $beta$ 4 subunits. J Mol Neurosci 7: 217-228[Medline].
Flores CM, Rogers SW, Pabreza LA, Wolfe BB and Kellar KJ (1992) A subtype of nicotinic cholinergic receptor in rat brain is composed of alpha 4 and beta 2 subunits and is up-regulated by chronic nicotine treatment. Mol Pharmacol 41: 31-37[Abstract].
Freund RK and Palmer MR (1997) Ethanol depression of cerebellar Purkinje neuron firing involves nicotinic acetylcholine receptors. Exp Neurol 143: 319-322[Medline].
Fröhlich R, Patzelt C and Illes P (1994) Inhibition by ethanol of excitatory amino acid receptors and nicotinic acetylcholine receptors at rat locus coeruleus neurons. Naunyn-Schmiedeberg's Arch Pharmakol 350: 626-631[Medline].
Gray R, Rajan AS, Radcliffe KA, Yakehiro M and Dani JA (1996) Hippocampal synaptic transmission enhanced by low concentrations of nicotine. Nature (London) 383: 713-716[Medline].
Guo J-Z, Tredway TL and Chiappinelli VA (1998) Glutamate and GABA release are enhanced by different subtypes of presynaptic nicotinic receptors in the lateral geniculate nucleus. J Neurosci 18: 1963-1969[Abstract/Free Full Text].
Harris RA, Mihic SJ, Brozowski SJ, Hadingham K and Whiting PJ (1997) Ethanol, flunitrazepam, and pentobarbital modulation of GABA_A receptors expressed in mammalian cells and Xenopus oocytes. Alcohol Clin Exp Res 21: 444-451[Medline].
Istvan J and Matarazzo JD (1984) Tobacco, alcohol, and caffeine use: a review of their interrelationships. Psychol Bull 95: 301-326[Medline].
Kulak JM, Nguyen TA, Olivera BM and McIntosh JM (1997) $alpha$ -Conotoxin MII blocks nicotine-stimulated dopamine release in rat striatal synaptosomes. J Neurosci 17: 5263-5270[Abstract/Free Full Text].
Li X, Rainnie DG, McCarley RW and Greene RW (1998) Presynaptic nicotinic receptors facilitate monoaminergic transmission. J Neurosci 18: 1904-1912[Abstract/Free Full Text].
Luo S, Kulak JM, Cartier GE, Jacobsen RB, Yoshikami D, Olivera BM and McIntosh JM (1998) $alpha$ -Conotoxin AuIB selectively blocks $alpha$ 3 $beta$ 4 nicotinic acetylcholine receptors and nicotine-evoked norepinephrine release. J Neurosci 18: 8571-8579[Abstract/Free Full Text].
Machu TK and Harris RA (1994) Alcohols and anesthetics enhance the function of 5-hydroxytryptamine₃ receptors expressed in Xenopus laevis oocytes. J Pharmacol Exp Ther 271: 898-905[Abstract/Free Full Text].
Mascia MP, Mihic SJ, Valenzuela CF, Schofield PR and Harris RA (1996) A single amino acid determines differences in ethanol actions on strychnine-sensitive glycine receptors. Mol Pharmacol 50: 402-406[Abstract].
McGehee DS and Role LW (1995) Physiological diversity of nicotinic acetylcholine receptors expressed by vertebrate neurons. Annu Rev Physiol 57: 521-546[Medline].
McGehee DS, Heath MJS, Gelber S, Devay P and Role LW (1995) Nicotine enhancement of fast excitatory synaptic transmission in CNS by presynaptic receptors. Science (Wash DC) 269: 1692-1696[Abstract/Free Full Text].
Mihic SJ, Whiting PJ and Harris RA (1994) Anaesthetic concentrations of alcohols potentiate GABA_A receptor-mediated currents: lack of subunit specificity. Eur J Pharmacol 268: 209-214[Medline].
Mihic SJ, Ye Q, Wick MJ, Koltchine VV, Finn SE, Hanson K, Mascia MP, Valenzuela CF, Harris RA and Harrison NL (1997) Sites of alcohol and volatile anesthetic action on GABA_A and glycine receptors. Nature (London) 389: 385-389[Medline].
Nagata K, Aistrup GL, Huang C-S, Marszalec W, Song J-H, Yeh JZ and Narahashi T (1996) Potent modulation of neuronal nicotinic acetylcholine receptor-channel by ethanol. Neurosci Lett 217: 189-193[Medline].
Orr-Urtreger A, Göldner FM, Saeki M, Lorenzo I, Goldberg L, De Biasi M, Dani JA, Patrick JW and Beaudet AL (1997) Mice deficient in the $alpha$ 7 neuronal nicotinic acetylcholine receptor lack $alpha$ -bungarotoxin binding sites and hippocampal fast nicotinic currents. J Neurosci 17: 9165-9171[Abstract/Free Full Text].
Pontieri FE, Tanda G, Orzi F and Di Chiara G (1996) Effects of nicotine on the nucleus accumbens and similarity to those of addictive drugs. Nature (London) 382: 255-257[Medline].
Role LW and Berg DK (1996) Nicotinic receptors in the development and modulation of CNS synapses. Neuron 16: 1077-1085[Medline].
Yang X, Criswell HE and Breese GR (1996) Nicotinic-induced inhibition in medial septum involves activation of presynaptic nicotinic cholinergic receptors on $gamma$ -aminobutyric acid-containing neurons. J Pharmacol Exp Ther 276: 482-489[Abstract/Free Full Text].
Yu D, Zhang L, Eiselé J-L, Bertrand D, Changeux J-P and Weight FF (1996) Ethanol inhibition of nicotinic acetylcholine type $alpha$ ₇ receptors involves the amino-terminal domain of the receptor. Mol Pharmacol 50: 1010-1016[Abstract].
Zoli M, Léna C, Picciotto MR and Changeux J-P (1998) Identification of four classes of brain nicotinic receptors using $beta$ 2 mutant mice. J Neurosci 18: 4461-4472[Abstract/Free Full Text].

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				T. Flatscher-Bader, N. Zuvela, N. Landis, and P.A. Wilce Smoking and alcoholism target genes associated with plasticity and glutamate transmission in the human ventral tegmental area Hum. Mol. Genet., January 1, 2008; 17(1): 38 - 51. [Abstract] [Full Text] [PDF]

				P. Steensland, J. A. Simms, J. Holgate, J. K. Richards, and S. E. Bartlett Varenicline, an {alpha}4beta2 nicotinic acetylcholine receptor partial agonist, selectively decreases ethanol consumption and seeking PNAS, July 24, 2007; 104(30): 12518 - 12523. [Abstract] [Full Text] [PDF]

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				M. Oz, S. N. Jackson, A. S. Woods, M. Morales, and L. Zhang Additive Effects of Endogenous Cannabinoid Anandamide and Ethanol on {alpha}7-Nicotinic Acetylcholine Receptor-Mediated Responses in Xenopus Oocytes J. Pharmacol. Exp. Ther., June 1, 2005; 313(3): 1272 - 1280. [Abstract] [Full Text] [PDF]

				C. M. Butt, N. M. King, J. A. Stitzel, and A. C. Collins Interaction of the Nicotinic Cholinergic System with Ethanol Withdrawal J. Pharmacol. Exp. Ther., February 1, 2004; 308(2): 591 - 599. [Abstract] [Full Text] [PDF]

				C. M. Borghese, L. A. Henderson, V. Bleck, J. R. Trudell, and R. A. Harris Sites of Excitatory and Inhibitory Actions of Alcohols on Neuronal {alpha}2{beta}4 Nicotinic Acetylcholine Receptors J. Pharmacol. Exp. Ther., October 1, 2003; 307(1): 42 - 52. [Abstract] [Full Text] [PDF]

				T. Suzuki, K. Ueta, M. Sugimoto, I. Uchida, and T. Mashimo Nitrous Oxide and Xenon Inhibit the Human ({alpha}7)5 Nicotinic Acetylcholine Receptor Expressed in Xenopus Oocyte Anesth. Analg., February 1, 2003; 96(2): 443 - 448. [Abstract] [Full Text] [PDF]

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				B. Buisson and D. Bertrand Chronic Exposure to Nicotine Upregulates the Human {alpha}4{beta}2 Nicotinic Acetylcholine Receptor Function J. Neurosci., March 15, 2001; 21(6): 1819 - 1829. [Abstract] [Full Text] [PDF]

				E. L. Godden, R. A. Harris, and T. V. Dunwiddie Correlation between Molecular Volume and Effects of n-Alcohols on Human Neuronal Nicotinic Acetylcholine Receptors Expressed in Xenopus Oocytes J. Pharmacol. Exp. Ther., March 1, 2001; 296(3): 716 - 722. [Abstract] [Full Text]

				J. A. Stitzel, M. Jimenez, M. J. Marks, T. Tritto, and A. C. Collins Potential Role of the alpha 4 and alpha 6 Nicotinic Receptor Subunits in Regulating Nicotine-Induced Seizures J. Pharmacol. Exp. Ther., April 1, 2000; 293(1): 67 - 74. [Abstract] [Full Text]

Effects of Ethanol on Recombinant Human Neuronal Nicotinic Acetylcholine Receptors Expressed in Xenopus Oocytes1

**Effects of Ethanol on Recombinant Human Neuronal Nicotinic Acetylcholine Receptors Expressed in Xenopus Oocytes¹**