International Union of Pharmacology. XXXIII. Mammalian γ-Aminobutyric AcidB Receptors: Structure and Function | Pharmacological Reviews

Advertisement

Abstract

The γ-aminobutyric acid_B(GABA_B) receptor was first demonstrated on presynaptic terminals where it serves as an autoreceptor and also as a heteroreceptor to influence transmitter release by suppressing neuronal Ca²⁺ conductance. Subsequent studies showed the presence of the receptor on postsynaptic neurones where activation produces an increase in membrane K⁺ conductance and associated neuronal hyperpolarization. (−)-Baclofen is a highly selective agonist for GABA_B receptors, whereas the established GABA_Areceptor antagonists, bicuculline and picrotoxin, do not block GABA_B receptors. The receptor is G_i/G_o protein-coupled with mixed effects on adenylate cyclase activity. The receptor comprises a heterodimer with similar subunits currently designated 1 and 2. These subunits are coupled via coiled-coil domains at their C termini. The evidence for splice variants is critically reviewed. Thus far, no unique pharmacological or functional properties have been assigned to either subunit or the variants. The emergence of high-affinity antagonists for GABA_B receptors has enabled a synaptic role to be established. However, the antagonists have generally failed to establish the existence of pharmacologically distinct receptor types within the GABA_B receptor class. The advent of GABA_B1 knockout mice has also failed to provide support for multiple receptor types.

I. Introduction

The GABA_B ¹receptor was originally defined on the basis of pharmacological responses to GABA and related agonists, including baclofen (Bowery et al., 1981). In studies focusing on control of transmitter release, it was noted that a GABA receptor responsible for modulating evoked release in a variety of isolated tissue preparations differed pharmacologically from the receptor responsible for the Cl⁻-dependent actions of GABA. Thus, the ability of GABA to inhibit neurotransmitter release from these preparations was not blocked by bicuculline, was not mimicked by isoguvacine, and was not dependent on Cl⁻, all of which are characteristic of the classical GABA receptor. Most striking was the finding that baclofen (β-parachlorophenyl GABA), a clinically employed spasmolytic (Bein, 1972; Keberle and Faigle, 1972), mimicked, in a stereoselective manner, the effect of GABA in these systems. Furthermore, ligand-binding studies provided direct evidence of distinct attachment sites for baclofen on central neuronal membranes (Hill and Bowery, 1981). The term GABA_B was coined to distinguish this site from the bicuculline-insensitive receptor, which was, in turn, designated GABA_A(Hill and Bowery, 1981).

A major distinction between GABA_A and GABA_B receptors is that the former are ligand-gated ion channels, whereas the latter are coupled to G proteins (Wojcik and Neff, 1984; Hill, 1985; Karbon and Enna, 1985). Hence, GABA_B receptors can be defined as metabotropic, whereas GABA_A receptors form part of the ionotropic receptor superfamily. Characterization of the GABA_B receptor has led to new insights into the structural and functional properties of seven-transmembrane receptors in general. Contained in this report is an overview of selected studies on the properties of GABA_B receptors. Readers desiring additional information on particular aspects of this topic are urged to consult other sources (e.g., Enna, 1997; Enna and Bowery, 1997; Marshall et al., 1999a; Bowery and Enna, 2000; Enna, 2000). Characteristics of the GABA_B receptor, which are described in detail in this review, are summarized in Table1.

View this table:

Table 1

GABA_B receptor characteristics

II. γ-Aminobutyric Acid_B Receptor Structure

Functional G protein-coupled receptors are expressed in cell membranes in different ways. In some cases they may be present as a single protein, whereas in others they may form homodimers (Bouvier, 2001). The structural characterization of the metabotropic GABA_B receptor revealed a third possibility. In this case, the receptor exists as a heterodimer with the subunits designated GABA_B1 and GABA_B2 (Jones et al., 1998; Kaupmann et al., 1998a; White et al., 1998; Kuner et al., 1999; Martin et al., 1999; Ng et al., 1999). The heterodimeric nature of the GABA_B receptor was not initially appreciated when the GABA_B1 subunit was first cloned (Kaupmann et al., 1997). Although shown to be a high molecular weight, seven-transmembrane spanning protein with homology to metabotropic glutamate receptors, the recombinant GABA_B1protein exhibited binding affinities for agonists that were 1000-fold lower than those for wild-type GABA_B receptors. Moreover, the coupling to presumed GABA_B effector systems in heterologous cells was surprisingly inefficient (Kaupmann et al., 1997, 1998b). Subsequent studies revealed that the GABA_B1 protein is not transported to the plasma membrane but remains associated with the endoplasmic reticulum (Couve et al., 1998). This, and the inefficient coupling to effector systems, led to the hypothesis that a trafficking protein, such as a RAMP (receptor activity modifying protein) (McLatchie et al., 1998), might be required for the efficient functional expression of the GABA_B site. Ultimately, the discovery of a second GABA_B receptor subunit, GABA_B2, provided the necessary explanation (seeMarshall et al., 1999a ). The GABA_B2protein has 54% similarity and 35% homology to GABA_B1 and has many of the structural features of the GABA_B1 subunit, including a high molecular weight (110 kDa), seven-transmembrane domains, and a long extracellular chain at the N terminus. The GABA_B2 protein not only serves to escort GABA_B1 to the cell surface, it appears to be the receptor component that links to the G protein, whereas the GABA_B1 subunit is necessary for agonist activation (Margeta-Mitrovic et al., 2000; Calver et al., 2001;Galvez et al., 2001; Pagano et al., 2001). It appears, therefore, that the agonist binds to a component of the GABA_B1subunit, producing a conformational change in the protein complex that allows GABA_B2 to engage and activate the G protein-coupled signaling system. In support of this model, it has been shown that GABA_B2 must remain linked to GABA_B1 after the dimer is inserted into the cell membrane to maintain receptor function ( Margeta-Mitrovic et al., 2000; Calver et al., 2001; Pagano et al., 2001 ). Recombinant GABA_B2 is expressed at the cell surface in the absence of GABA_B1, and early reports suggested that it could display some functionality under this condition (Kaupmann et al., 1998a; Kuner et al., 1999; Martin et al., 1999). Although it now appears unlikely that wild-type GABA_B2 subunits can function alone in this way (Prosser et al., 2001; Schuler et al., 2001), there is no doubt that the coupling of GABA_B2 with GABA_B1 yields a fully functional GABA_B receptor, with the GABA_B1, rather than the GABA_B2 component, displaying a high affinity for radiolabeled ligands (Kaupmann et al., 1998a; White et al., 1998). Indeed, the GABA_B1 isoform, when expressed as part of the heterodimer, has increased agonist affinity similar to that of the wild-type receptor (Kaupmann et al., 1998a; White et al., 1998).

Several proteins other than GABA_B2 have been shown to interact with GABA_B1 (Nehring et al., 2000; White et al., 2000; Couve et al., 2001), but none of these complexes yields a functional receptor. It is possible that the interaction of GABA_B1 or GABA_B2 with transcription factors, such as activating transcription factor-4, may serve to regulate gene expression through a novel signal transduction pathway (Nehring et al., 2000; White et al., 2000).

The interaction of GABA_B1 and GABA_B2 within the cells appears crucial for the correct assembly of the heterodimer on the membrane surface. This has been demonstrated for both recombinant and wild-type GABA_B receptors (Marshall et al., 1999b; Filippov et al., 2000; Chronwall et al., 2001). The interaction of the C-terminal coiled-coil domains, by masking the action of the retention motif RXRR present in the C terminus of GABA_B1, ensures that only correctly assembled receptor complexes traffic to the cell surface (Margeta-Mitrovic et al., 2000; Pagano et al., 2001). Expression of the coupled heterodimer in cell membranes can occur even when the GABA_B1 and/or GABA_B2 C-terminal domains are missing (Calver et al., 2001; Pagano et al., 2001), suggesting that the coiled-coil structures are not essential for heterodimerization per se. Although it has been proposed that mGlu4R can associate with GABA_B1 and traffic it to the cell surface (Sullivan et al., 2000), this finding could not be replicated in a subsequent study using a different experimental approach (Pagano et al., 2001). The critical importance of the GABA_B1subunit is supported by the finding that tissue from mice lacking the gene for this protein fails to respond to GABA_Bagonists and shows a loss of detectable pre- and postsynaptic responses (Prosser et al., 2001; Schuler et al., 2001). Importantly, the GABA_B2 subunit is heavily down-regulated in GABA_B1 null-mutant mice. This requirement of GABA_B1 for stable GABA_B2expression supports the notion that in wild-type mice virtually all GABA_B2 protein is associated with GABA_B1, in agreement with previous biochemical studies (Benke et al., 1999). The null-mutant mice generated on the 129Sv background only survive for 3 to 4 weeks postnatally, apparently due to recurrent seizures (Prosser et al., 2001), whereas those generated on the BALB/c background survive through adulthood even though they exhibit spontaneous seizures, hyperalgesia, hyperlocomotor activity, and memory impairment (Schuler et al., 2001). The viability of BALB/c mice lacking the GABA_B1 subunit has allowed their characterization in GABA_B receptor paradigms. GABA_B agonist administration to BALB/c null-mutant mice failed to produce the typical muscle relaxation, hypothermia, or delta electroencephalogram waves observed in wild-type animals. These behavioral findings were paralleled by a loss of all biochemical and electrophysiological GABA_Bresponses in the null-mutant mice. This demonstrates that GABA_B1 is an essential component of pre- and postsynaptic GABA_B receptors and indicates that most, probably all, brain GABA_B receptors incorporate the GABA_B1 subunit. Moreover, from the analysis of the GABA_B1 null-mutant mice it follows that GABA_B2 is unlikely to function as an autonomous receptor. Although these results are in line with previous work that failed to find any evidence for pharmacologically distinct GABA_B receptor subtypes (Waldmeier et al., 1994), there remains the possibility that unidentified splice variants or GABA_B1-associated proteins generate diversity.

Numerous splice variants of the GABA_B1 subunit have been identified (Kaupmann et al., 1997; Isomoto et al., 1998;Pfaff et al., 1999; Calver et al., 2000; Schwarz et al., 2000; Wei et al., 2001a,b) with sometimes different names in rat and human. A comprehensive description of these variants is made possible by the complete sequence of the human and mouse GABA_B1genes, which are contained within GenBank accession numbers AL031983and AL078630, respectively, and the nearly complete rat gene (Pfaff et al., 1999). The 1a splice variant in all three species contains all 23 conserved exons of the gene, with the first exon being untranslated and the transmembrane domains being encoded by exons 15 to 21. It should be noted that this number of exons differs from much of the literature because Pfaff et al. (1999), apparently through assembly errors in their rat gene sequence (GenBank accession numbers AF110796 andAF110797), failed to recognize introns that split exons 7 and 11 each into two exons. The existence of these exons can be confirmed using sequence from the rat genome sequencing project (http://www.ncbi.nlm.nih.gov/genome/seq/RnBlast.html). In addition,Pfaff et al. (1999) did not use any 5′ untranslated cDNA sequence and, thus, did not identify the first exon. The 1b splice variant initiates 5′ of exon 6, thereby producing an extended exon 6, which contains a new initiation codon, giving rise to an alternative amino-terminal sequence for the 1b protein. The amino-terminal sequence unique to the 1b variant is 47 versus 162 amino acids for the sequence unique to the 1a variant. Isoform-specific antibodies have shown both variants to be expressed in rat brain with 1a predominating before birth and 1b predominating in adults (Fritschy et al., 1999). A third variant, called 1e in both rat and human, skips exon 15, which leads to premature termination prior to the first transmembrane domain. Although this isoform can heterodimerize with GABA_B2subunits, it appears to be unable to activate G protein-coupled, inwardly rectifying potassium channels or to inhibit cAMP production when coexpressed with GABA_B1 subunits (Schwarz et al., 2000). Several variants have been observed in only one species. In humans, a variant called 1c is similar to the 1a variant but skips exon 4, resulting in the deletion of 63 amino acids. It is expressed at much higher levels in fetal brain than in adult brain (Calver et al., 2000;Martin et al., 2001). A rat variant, also called 1c, corresponds to an insertion of a 93-base exon located between exons 19 and 20, which results in the insertion of 31 amino acids into the beginning of transmembrane domain 5. Although the homologous region can be identified in the mouse gene, it is too poorly conserved to be functional due to the insertion of two bases, which disrupts the reading frame. No homologous exon is evident in the human gene. Thus, although the rat variant has been reported to be functional in vitro (Pfaff et al., 1999), it is unclear if it is functional in vivo. Rat variant 1d has a 567-base insertion corresponding to the failure to splice out intron 22. Rat variant 1f skips exon 5, resulting in the deletion of seven amino acids. Rat variant 1g has a 124-base insertion that extends the 5′ end of exon 5 by using an alternative splice acceptor. This insertion shifts the reading frame and results in a severely truncated protein. Aside from variants 1a and 1b, it is presently unknown whether any of these variants act as a subunit of physiological receptors. The 1a and 1b variants are not, strictly speaking, splice variants but instead appear to be transcription start site variants that originate in high guanosine-cytosine content (∼80%) regions of the gene separated by about 5 kilobases. Although such high GC content makes it difficult to make full-length cDNA, to map the transcription start sites, and could easily cause artifacts, variant-specific antibodies have provided critical evidence that both proteins are physiologically expressed at significant levels. Thus, it is appropriate to use the IUPHAR nomenclature reserved for significant splice variants, i.e., GABA_B1(a) and GABA_B1(b), for these two variants.

Partial cDNAs corresponding to two potential splice variants of the human GABA_B2 subunit, called 2b and 2c, which delete 81 and 78 bases of the carboxyl-terminal encoding portion of the cDNA have been reported (Clark et al., 2000). Subsequent analysis of the human GABA_B2 gene (Martin et al., 2001) has demonstrated that neither of the deleted regions correspond to an independent exon but instead reside within the last exon of the gene. There are no appropriate splice donor or acceptor consensus sequences that might act as alternative splice sites. The lack of such sites and the presence of short (4–5 bases) repeated sequences at the ends of the deletion regions suggest that they are polymerase chain reaction artifacts. Thus, there is currently no good evidence for splice variants of the GABA_B2 subunit.

Although there is a 1:1 stoichiometry between GABA_B1 and GABA_B2 subunits in the functional receptor, production of the subunits appears to be regulated, at least in part, independent of one another (McCarson and Enna, 1999). Thus, whereas expression of GABA_B1and GABA_B2 mRNA increases in rat dorsal spinal cord following 24 h of hind paw inflammation, the increase in GABA_B2 mRNA is significantly greater than for GABA_B1. This supports the notion that GABA_B receptor subunits may serve a variety of functions in the cell and could indicate that other, as yet unidentified, proteins may form functional heterodimers with GABA_B1 subunits to form a functional receptor.

III. γ-Aminobutyric Acid_B Receptor Effector Mechanisms

Effector mechanisms associated with neural GABA_B receptors are the adenylate cyclase system and Ca²⁺ and K⁺ ion channels (Hill et al., 1984; Karbon et al., 1984; Hill, 1985; Inoue et al., 1985; Andrade et al., 1986; Xu and Wojcik, 1986; Dolphin et al., 1990; Bindokas and Ishida, 1991; Gage, 1992). GABA_B receptor activation is mediated by G proteins that are members of the pertussis toxin-sensitive family G_iα/G_oα, in particular G_i2α (Odagaki et al., 2000; Odagaki and Koyama, 2001). However, some pertussis toxin-insensitive effects of baclofen have been noted in, for example, the magnocellular neurons of the paraventricular and supraoptic nuclei of the rat (Noguchi and Yamashita, 1999; Cui et al., 2000). In particular, it has been reported that presynaptic, compared with postsynaptic, GABA_B receptor mechanisms are insensitive to pertussis toxin (Harrison et al., 1990). It has also been found that whereas exposure of spinal cord membranes to baclofen results in an increase in guanosine 5′-3-O-(thio)triphosphate binding in young rats, no such response can be obtained in membranes from animals older than 21 days. This would suggest that there may be a developmental change in the coupling of GABA_Breceptors and G proteins in the cord (Moran et al., 2001).

A. Adenylate Cyclase

GABA_B agonists inhibit basal and forskolin-stimulated neuronal adenylate cyclase in brain slices (Xu and Wojcik, 1986; Knight and Bowery, 1996) through a G protein-dependent mechanism that results in a reduced level of intracellular cAMP. Activation of the GABA_B receptor can also enhance cAMP formation in response to G_s-coupled receptor agonists, such as isoprenaline, in brain slices but not in isolated neuronal membranes, suggesting it entails activation of cytoplasmic cyclases (Enna, 2000). The physiological relevance of these effects on cAMP production has been confirmed by in vivo microdialysis experiments in the cerebral cortex of freely moving rats (Hashimoto and Kuriyama, 1997). Both baclofen and GABA reduced the increase in cAMP generated by an infusion of forskolin, and this was blocked by CGP54626, a selective GABA_B receptor antagonist, substantiating the role of GABA_B receptors in this response. Baclofen was also able to potentiate the increase in cAMP produced by isoprenaline in this in vivo preparation.

A direct GABA_B-mediated increase in basal adenylate cyclase activity has been detected in membranes of rat olfactory bulb (Olianas and Onali, 1999). Interestingly, this effect is blocked by pertussis toxin, suggesting an involvement of G_i/G_o rather than G_s protein.

B. Ion Channels

When activated, GABA_B receptors decrease Ca²⁺ and increase K⁺conductance in neuronal membranes. The effect on Ca²⁺ conductance appears to be primarily associated with presynaptic P/Q- and N-type currents (Santos et al., 1995; Lambert and Wilson, 1996; Chen and van den Pol, 1998; Takahashi et al., 1998; Bussieres and El Manira, 1999; Barral et al., 2000), although facilitation of an L-type current in non-mammalian retina has also been described (Shen and Slaughter, 1999).

Modulation of K⁺ conductance appears to be linked primarily with postsynaptic GABA_B sites and with perhaps multiple types of K⁺ channels (Wagner and Dekin, 1993, 1997; Lüscher et al., 1997; Harayama et al., 1998). Whereas a K⁺(A) current is thought to be coupled to GABA_B receptors on presynaptic terminals in hippocampal cultures, changes in membrane K⁺ flux appear to be due to postsynaptic GABA_B receptor activation (Saint et al., 1990).

Although suppression of Ca²⁺ influx is probably the most frequently observed response associated with presynaptic GABA_B receptors (Doze et al., 1995; Wu and Saggau, 1995; Isaacson, 1997, 1998; Isaacson and Hille, 1997), a process independent of Ca²⁺ or K⁺ channels but perhaps linked with protein kinase C activation, has been reported in rodent CA1 hippocampal pyramidal cells (Jarolimek and Misgeld, 1997). This had been demonstrated previously but was then only apparent in rat hippocampal slices obtained in early postnatal life (Tremblay et al., 1995).

Low threshold Ca²⁺ T-currents, which are inactivated at normal resting membrane potentials, may also be involved in the response to GABA_B receptor activation, at least within the thalamus (Scott et al., 1990). This postsynaptic hyperpolarization of long duration, which initiates Ca²⁺ spiking activity in thalamocortical cells, could contribute to the generation of spike and wave discharges associated with absence seizures (Crunelli and Leresche, 1991).

IV. γ-Aminobutyric Acid_B Receptor Subtypes

Although GABA_B receptors appear structurally heterogenous in the sense that several splice variants exist for the two subunits known, evidence for functionally distinct receptor subtypes is limited. Transmitter release studies with native and rat brain GABA_B receptors suggest pharmacological differences between autoreceptors and heteroreceptors and even within heteroreceptors (Bonanno and Raiteri, 1993a; Banerjee and Snead, 1995;Teoh et al., 1996; Bonanno et al., 1997; Ong et al., 1998b; Phelan, 1999). Similarly, the dual action of GABA_Bagonists on adenylate cyclase in brain slices would support the concept of receptor subtypes (Cunningham and Enna, 1996). The existence of pharmacologically distinct subtypes of a native receptor has traditionally been considered likely when the affinities of one antagonist for the hypothetical subtypes differed by at least one order of magnitude. In the case of GABA_B receptors sited on terminals releasing GABA, glutamate, cholecystokinin, or somatostatin, not only do the antagonist affinities differ in some cases by more than two orders of magnitude but the orders of potency of some antagonists differ between receptors. Qualitatively similar results were obtained when GABA_B receptor antagonists were tested on nerve endings isolated from human cerebrocortex (Fassio et al., 1994; Bonanno et al., 1996, 1997, 1999;Raiteri et al., 1996). The results with rat and human nerve endings are summarized in Table 2. Pharmacological differences also seem to exist between GABA_Bautoreceptors inhibiting GABA release in rat cerebral cortex and spinal cord (Raiteri et al., 1989; Bonanno and Raiteri, 1992, 1993b; Bonanno et al., 1998). Thus, the evidence for pharmacologically distinct subtypes of the GABA_B receptor derived from release studies appears to at least equate with some other receptor systems, which can boast the chrism of molecular biology. Also it would be quite surprising if the GABA_Breceptor was the only example of a metabotropic receptor without subtypes. Comparative data obtained with wild-type GABA_B receptors and recombinant GABA_Bl(b)/B2 receptors expressed in CHO cells indicate that the recombinant receptor, unlike the wild-type, is insensitive to the antagonists, phaclofen, saclofen, and CGP35348 (Wood et al., 2000). However, a comparison of GABA_Breceptors containing different isoforms of GABA_B1in combination with GABA_B2 in CHO cells indicate that these heterodimers are pharmacologically indistinguishable (Kaupmann et al., 1998a; Green et al., 2000).

View this table:

Table 2

GABA_Breceptor subtypes IC₅₀values of antagonists (μM). The drugs were tested against (−)-baclofen.

In a recent report, Ng et al. (2001) presented data suggesting gabapentin, an anticonvulsant/analgesic agent, is a selective agonist at the GABA_B1(a)/GABA_B2site, compared with the GABA_B1(b)/B2 receptors, expressed in oocytes. A similar conclusion was drawn from studies on wild-type GABA_B receptors in mIL-tsA58 cells (Bertrand et al., 2001). Questions remain, however, whether this selectivity is generally detectable when testing wild-type receptors in nontransformed mammalian central nervous system tissue. In fact, the possible relationship between gabapentin and GABA_b receptors has been examined independently by Lanneau et al. (2001). These authors believe that gabapentin is not a GABA_B receptor agonist. In another study the antihyperalgesic effects of the GABA_B agonists, baclofen and CGP35024, but not those produced by gabapentin, were blocked by CGP56433A, a GABA_B receptor antagonist (Patel et al., 2001). Thus, the extent to which the actions of gabapentin are mediated in vivo by effects on GABA_B receptors, remains to be conclusively demonstrated. Nevertheless, the possibility that under certain conditions gabapentin can activate a particular form of the GABA_B receptor is an interesting observation.

Electrophysiological studies in mammalian brain suggest subtle distinctions between pre- and postsynaptic receptors (Colmers and Williams, 1988; Dutar and Nicoll, 1988b; Harrison et al., 1990;Thompson and Gähwiler, 1992; Deisz et al., 1997; Chan et al., 1998; Yamada et al., 1999). For example, the GABA_B receptor agonist CGP44533 failed to induce an increase in postsynaptic membrane conductance whereas (−)-baclofen and CGP35024 did (Yamada et al., 1999) and, on comparing the effects of six GABA_B receptor antagonists, it was found that 5- to 10-fold higher concentrations were required to block presynaptic as opposed to postsynaptic receptors in the rat hippocampus (Pozza et al., 1999). However, in general, the receptor ligands currently available do not reliably distinguish between potential subtypes. Unfortunately, studies in GABA_B1 null-mice have also failed to provide any positive evidence for subtyping of the GABA_B receptors (Prosser et al., 2001; Schuler et al., 2001).

V. γ-Aminobutyric Acid_B Receptor Distribution

A. Central Nervous System

Within the mammalian brain, the highest density of GABA_B binding sites is in the thalamic nuclei, the molecular layer of the cerebellum, the cerebral cortex, the interpeduncular nucleus, and the dorsal horn of the spinal cord (Bowery et al., 1987; Chu et al., 1990). In situ hybridization studies of mRNA for the GABA_B1(a) and GABA_B1(b) splice variants reveal they are distributed differentially in brain (Liang et al., 2000). Studies with rat and human cerebellum and spinal cord indicate that GABA_B1(a) is associated with presynaptic receptors, whereas GABA_B1b is located predominantly at postsynaptic sites, at least in cerebellum (Kaupmann et al., 1998b; Billinton et al., 1999; Bischoff et al., 1999;Princivalle et al., 2000; Towers et al., 2000). Elsewhere in the brain, however, the GABA_B1(b) protein is in presynaptic terminals and the GABA_B1(a) at postsynaptic sites (Benke et al., 1999; Princivalle et al., 2001). In the dorsal horn of the rat spinal cord, the density of GABA_B1(a) is low, whereas in the dorsal root ganglia, which contain cell bodies of the primary afferent fibers, >90% of the GABA_B1subunit mRNA is GABA_B1(a), with GABA_B1(b) comprising less than 10% of the total GABA_B1 mRNA (Towers et al., 2000). Immunocytochemical studies provide support for this in revealing that the level of GABA_B1(a) protein appears to be higher than of GABA_B1(b) in the dorsal horn of the rat spinal cord (A. P. Princivalle and N. G. Bowery, unpublished observation). Similarly, in rat and human cerebellum, GABA_B1(a) mRNA is detected over the granule cells, which send their excitatory fibers into the molecular layer to innervate the Purkinje cell dendrites (Kaupmann et al., 1998b;Billinton et al., 1999; Bischoff et al., 1999). Presumably, the GABA_B receptors on the granule cell terminals modulate the output of the excitatory transmitter. In contrast, GABA_B1(b) mRNA is associated with the Purkinje cell bodies, which express GABA_B receptors on their dendrites in the molecular layer postsynaptic to the GABA-ergic stellate cells. However, the contrary arrangement has also been observed elsewhere in the brain. For example, GABA_B1(a) subunits appear to be postsynaptic on cell bodies in the thalamocortical circuits (Princivalle et al., 2001). Thus, it would seem that a functional role, or cellular location, cannot be generally assigned to specific GABA_Breceptor subunit splice variants (Poorkhalkali et al., 2000;Princivalle et al., 2001).

The regional distribution of individual GABA_B1and GABA_B2 protein subunits is similar to that of the wild-type receptor, but in some brain areas such as the caudate-putamen, GABA_B2 is not detectable, even though GABA_B1 and the native receptor are present (Durkin et al., 1999; Margeta-Mitrovic et al., 1999; Clark et al., 2000). In addition, there appears to be very little GABA_B2 mRNA, relative to GABA_B1 mRNA, in the hypothalamus (Jones et al., 1998; Clark et al., 2000). These findings, along with those suggesting that GABA_B1 and GABA_B2subunit expression is not regulated in tandem (McCarson and Enna, 1999), support the existence of additional, as yet unidentified, GABA_B receptor subunits.

B. Peripheral Organs and Tissues

Functional GABA_B receptors are not restricted to the central nervous system. Thus, GABA has been known for some time to play an important role in modulating autonomic inputs to the intestine, and GABA_B receptors are capable of mediating responses in other organs (Ong and Kerr, 1990). Moreover, GABA_B receptor agonists inhibit relaxation of the lower esophageal sphincter in dogs, ferrets, and humans, and attenuate esophageal reflux by an inhibitory action on the vagus nerve (Blackshaw et al., 1999, 2000; Lehmann et al., 1999, 2000; Lidums et al., 2000;Smid and Blackshaw, 2000).

Studies monitoring functional GABA_B responses suggest their presence in peripheral organs (see Bowery, 1993). More recently, Northern blot analysis and receptor protein immunoblotting has provided direct evidence for GABA_B1 isoforms and GABA_B receptors throughout the periphery of the rat (Castelli et al., 1999; Calver et al., 2000). However, the GABA_B2 subunit was not always present with GABA_B1, such as in uterus and spleen (Calver et al., 2000).

Western blotting revealed the presence of GABA_B1and GABA_B2 proteins in rat heart myocytes, supporting the observation that baclofen influences inwardly rectifying K⁺ currents in these cells (Lorente et al., 2000). Moreover, photoaffinity-labeling studies suggest that GABA_B1(a) and GABA_B1(b) are differentially distributed in the periphery as well as in the central nervous system (Belley et al., 1999). Thus, GABA_B1(a) is present in the adrenals, pituitary, spleen, and prostate, whereas GABA_B1(b), but not GABA_B1(a), is found in the rat kidney and liver.

VI. γ-Aminobutyric Acid_B Receptor-Mediated Responses

A. γ-Aminobutyric Acid_B Receptor Agonists

The observation that β-[4-chorophenyl] GABA (baclofen; Fig.1), is a stereospecifically active agonist at the GABA_B receptor (Bowery et al., 1980, 1981) provided part of the original evidence for the existence of a distinct receptor. Since then 3-aminopropyl-phosphinic acid (3-APPA, CGP27492; Bittiger et al., 1988) and its methyl homolog (3-APMPA, CGP35024 identical with SK&F 97541; Froestl et al., 1992, 1993; Howson et al., 1993) have emerged and are reported to be 3- to 7-fold more potent than the active isomer of baclofen [IC₅₀values, i.e., inhibition of binding of [³H]CGP27492 to GABA_Breceptors on rat cerebral cortex membranes: baclofen: 107 nM, (R)-(−)-baclofen: 32 nM, 3-APPA (CGP27492): 5 nM, 3-APMPA (CGP35024): 16 nM]. The latter compounds are also available as tritiated radioligands (Bittiger et al., 1988; Hall et al., 1995). Other methyl phosphinic acid-based agonists have been produced (Froestl et al., 1995a), such as CGP44532 (IC₅₀ = 45 nM) and its (R)-(+)-enantiomer CGP44533 (IC₅₀ = 152 nM; racemate CGP34938: IC₅₀ = 77 nM; Fig. 1), which differ only by a factor of 3 in binding to GABA_B receptors and show comparative activities in biochemical paradigms (Ong et al., 2001) but show significant differences in electrophysiological experiments (Yamada et al., 1999).

Figure 1

Structures of high-affinity GABA_Breceptor agonists.

Interestingly, ethyl (and higher homolog) phosphinic acids derivatives (e.g., CGP36216, IC₅₀ = 2 μM; Fig.2) show effects of GABA_B receptor antagonists (Froestl et al., 1995b). The difluoromethyl phosphinic acid derivative CGP47656 (IC₅₀ = 89 nM; Fig. 1) with a substituent, the size of which is between a methyl and an ethyl group, showed properties of a partial GABA_B receptor agonist (Froestl et al., 1995a). GABA_B receptor agonists display a number of pharmacological effects, including central muscle relaxation, antitussive action, bronchiolar relaxation, inhibition of urinary bladder contraction, an increase in gastrointestinal motility, epileptogenesis, suppression of cocaine, nicotine, and opioid self-administration, antinociception, yawning, hypotension, brown fat thermogenesis, cognitive impairment, inhibition of gastric acid secretion, and inhibition of hormone release.

Figure 2

Structures of low-affinity GABA_Breceptor antagonists.

1. Antispasticity.

The centrally mediated muscle relaxant effect of baclofen is the most widely exploited clinical response to this agent. This action appears due to a baclofen-induced reduction in neurotransmitter release onto motoneurons in the ventral horn of the spinal cord. There is also a suggestion that the antispastic effect is due to post- rather than presynaptic action on motoneurons (Orsnes et al., 2000a). Regardless of the site of action, the efficacy of baclofen in alleviating spasticity has made it a drug of choice for this condition, although side effects, principally sedation, limit its utility. Baclofen is effective in treating spasticity associated with tardive dystonia, brain and spinal cord injury, cerebral palsy, tetanus, multiple sclerosis, and stiff-man syndrome (Ochs et al., 1989,1999; Penn et al., 1989; Penn and Mangieri, 1993; Becker et al., 1995,1997, 2000; Campbell et al., 1995; Seitz et al., 1995; Albright et al., 1996; Azouvi et al., 1996; Dressnandt and Conrad, 1996; Ford et al., 1996; Paret et al., 1996; Armstrong et al., 1997; Dressler et al., 1997; Dressnandt et al., 1997; François et al., 1997, 2001;Meythaler et al., 1997; Gerszten et al., 1998; Auer et al., 1999;Orsnes et al., 2000b; Trampitsch et al., 2000; Krach, 2001).

2. Antinociceptive.

Even though baclofen is used to treat migraine headache, musculoskeletal pain, and the pain associated with trigeminal neuralgia, stroke, and spinal cord injury, its general effectiveness as an analgesic is limited (Fromm, 1994; Taira et al., 1995; Hansson and Kinnman, 1996; Loubser and Akman, 1996; Hering-Hanit, 1999; Idänpään-Heikkilä and Guilbaud, 1999;Becker et al., 2000). Although the reason for this is unknown, it may be due to a rapid desensitization of GABA_Breceptors.

Laboratory animal studies have established the antinociceptive action of GABA_B receptor agonists and suggest it is mediated by effects in both spinal cord and brain (Cutting and Jordan, 1975; Levy and Proudfit, 1979; Liebman and Pastor, 1980; Kendall et al., 1982; Sawynok and Dickson, 1985; Vaught et al., 1985; Serrano et al., 1992; Hammond and Washington, 1993; Smith et al., 1994; Dirig and Yaksh, 1995; Thomas et al., 1995; McCarson and Enna, 1996; Thomas et al., 1996; Wiesenfeld-Hallin et al., 1997; Cui et al., 1998; Przesmycki et al., 1998). Further evidence supporting the analgesic potential of GABA_B agonists is provided by the finding that tiagabine, a GABA uptake inhibitor, displays antinociceptive activity in rodents that is blocked by CGP35348, a GABA_Breceptor antagonist (Ipponi et al., 1999). Inasmuch as intrathecal administration of a GABA-producing neuronal cell line permanently reverses neuropathic pain, it has been suggested that altered spinal GABA levels may contribute to the induction phase of chronic pain (Eaton et al., 1999).

In the dorsal horn of the rat spinal cord, GABA_Breceptors are located on small diameter afferent fiber terminals, with activation of these sites decreasing the evoked release of sensory transmitters, such as substance P and glutamate (Price et al., 1987;Malcangio and Bowery, 1996; Ataka et al., 2000; Iyadomi et al., 2000;Riley et al., 2001). It has also been suggested that modulation of voltage-dependent, nifedipine-sensitive calcium channels in dorsal horn neurons may contribute to the antinociceptive effects of GABA_B agonists (Voisin and Nagy, 2001).

Baclofen and CGP35024 reversed neuropathic mechanical hyperalgesia following single s.c. or intrathecal administration but did not affect inflammatory mechanical hyperalgesia (Patel et al., 2001). GABA_B receptor agonists, such as baclofen and CGP44532, inhibit the formalin-induced increase of the expression of neurokinin-1 receptor mRNA (Enna et al., 1998).

The hot-plate, tail-flick as well as the paw pressure techniques were used to characterize acute pain behaviors in GABA_B1 null-mutant mice (Schuler et al., 2001). The tail-flick is a reflex response to a noxious thermal stimulus applied to the tail and is generally taken to represent a spinal reflex response, whereas the hot-plate response to a noxious thermal stimulus to the plantar surface of the paws is thought to involve supraspinal sites. In these nociceptive tests, GABA_B1null-mutant mice showed pronounced hyperalgesia to noxious heat in the hot-plate and tail-flick tests and reduced paw withdrawal thresholds to mechanical pressure. From these data it is likely that GABA_B-mediated effects do indeed exert a tonic control of nociceptive processes in the naive animal. The sites for this action are expected to be both spinal and supraspinal, although further experiments are needed to confirm this.

3. Suppression of Drug Craving.

Preliminary data suggest that baclofen reduces the craving for cocaine in humans (Ling et al., 1998). In rats, baclofen suppresses cocaine self-administration at doses that do not affect responding for food reinforcement (Roberts and Andrews, 1997; Shoaib et al., 1998; Campbell et al., 1999; Munzar et al., 2000). Moreover, the selective GABA_B receptor agonist CGP44532 mimics this action of baclofen without disrupting the response for food (Brebner et al., 1999, 2000a,b). Similar results are obtained whether laboratory animals are administered the GABA_B agonist either systemically or directly into select brain regions (Corrigall et al., 2000).

The importance of these observations in the possible treatment of drug abuse is reinforced by the finding that baclofen reduces craving for a host of addictive substances, including heroin, alcohol, and nicotine (Xi and Stein, 1999; Corrigall et al., 2000; Lobina et al., 2000). Thus, elevation of endogenous GABA levels in the mesolimbic area by administration of vigabatrin, an inhibitor of GABA metabolism, or the GABA uptake inhibitor NO-711, attenuates heroin and cocaine self-administration in rats and prevents cocaine-induced increases in dopamine in this brain region (Ashby et al., 1999; Xi and Stein, 2000). It has also been reported that gabapentin, a putative GABA_B receptor agonist (Bertrand et al., 2001; Ng et al., 2001), reduces the craving for cocaine in dependent adults (Myrick et al., 2001).

There is preclinical and preliminary clinical evidence that baclofen is effective in reducing alcohol craving and intake (Addolorato et al., 2000; Colombo et al., 2000). Baclofen blocks the rapid tolerance to ethanol, an effect that can be blocked by GABA_Bantagonists such as CGP36742 and CGP56433A (Zaleski et al., 2001).

4. Miscellaneous Actions.

GABA_Breceptors in the hypothalamus and nucleus tractus solitarius modulate sympathetic nerve activity, resulting in an elevation in blood pressure (Takenaka et al., 1995). GABA_B receptor activation in the hypothalamus also leads to an increase in metabolic rate and brown fat thermogenesis (Addae et al., 1986). In addition to the above, other centrally mediated effects of GABA_B agonists include alterations in epileptogenesis, cognition (Tang and Hasselmo, 1996), yawning (Doger et al., 1989), and micturition (Kontani et al., 1988).

Baclofen has been shown to have anti-bronchoconstrictor activity through activation of presynaptic receptors on parasympathetic nerve terminals (Chapman et al., 1991). In addition, through an action on sensory nerves in the lung, baclofen is reported to inhibit nonadrenergic, noncholinergic bronchoconstriction (Belvisi et al., 1989).

Baclofen has also displayed antitussive activity in humans and laboratory animals (Bolser et al., 1993, 1994; Dicpinigaitis and Dobkin, 1997). This effect is mediated through both a direct action on peripheral nerves in the lung as well as receptors in the brain stem controlling the cough reflex. Through a similar mechanism, possibly involving GABA-ergic inputs from the nucleus raphe magnus (Oshima et al., 1998), baclofen is effective in the management of intractable hiccoughs (Guelaud et al., 1995; Nickerson et al., 1997; Kumar and Dromerick, 1998; Marino, 1998). Baclofen has also been reported to inhibit the growth of mammary cancer cells in mice and humans, and there appears to be a correlation between glandular GABA levels and mammary pathology (Opolski et al., 2000).

B. γ-Aminobutyric Acid_B Receptor Antagonists

The design and development of selective, high-affinity GABA_B receptor antagonists have been important in establishing the significance and isolation of the GABA_B receptor genes. Kerr, Ong and their colleagues (1987, 1988; Fig. 2) described phaclofen, saclofen, and 2-hydroxysaclofen, the first selective antagonists. Although these agents have low affinities (IC₅₀ values, i.e., inhibition of binding of [³H]CGP27492 to GABA_B receptors on rat cerebral cortex membranes: 130, 26, and 11 μM, respectively) for GABA_Bbinding sites in rat brain membranes, as the first antagonists they were important tools for defining the pharmacological and physiological relevance of GABA_B receptors (Dutar and Nicoll, 1988a; Karlsson et al., 1988).

Subsequent discoveries of antagonists were derived largely by a group at Novartis in Basel, Switzerland (Froestl and Mickel, 1997). They developed the first GABA_B receptor antagonist able to cross the blood-brain barrier, CGP35348, and the first orally active agents, CGP36742 (Olpe et al., 1990, 1993a) and CGP51176 (Froestl et al., 1995b). However, these compounds, and others in this chemical series, have affinities for the GABA_Breceptor in the same range as 2-hydroxysaclofen (IC₅₀ values: 27, 38, and 6 μM, respectively). The same is true for SCH 50911 (IC₅₀ = 3 μM; Fig. 2), a chemically distinct agent that is effective following systemic administration but which has a relatively low affinity for the receptor (Bolser et al., 1995; Frydenvang et al., 1997). The most crucial breakthrough in the discovery of antagonists came with the development of compounds with affinities about 10,000 times higher than previous antagonists. This major advance stemmed from the attachment of 3,4-dichlorobenzyl or 3-carboxybenzyl substituents to the existing molecules. This produced a profusion of compounds with affinities in the low nanomolar range (Froestl et al., 1996; Froestl and Mickel, 1997). Numerous investigations have been carried out with CGP52432 (IC₅₀ = 55 nM), CGP54626A (IC₅₀ = 4 nM), CGP55845A (IC₅₀ = 6 nM), CGP56433A (IC₅₀ = 80 nM), CGP56999A (IC₅₀ = 2 nM), CGP61334 (IC₅₀ = 36 nM), and CGP62349 (IC₅₀ = 2 nM; Fig.3). Several compounds are also available as radioligands, such as [³H]CGP54626 (Bittiger et al., 1992; Green et al., 2000), [³H]CGP56999, and [³H]CGP62349 (Bittiger et al., 1996a;Ambardekar et al., 1999; Keir et al., 1999; Sloviter et al., 1999;Billinton et al., 2000). From the latter compound a radioligand containing the positron-emitting isotope ¹¹C was prepared as a potential positron emission tomography ligand (Todde et al., 2000).

Figure 3

Structures of high-affinity GABA_Breceptor antagonists.

Introducing the phosphinic acid moiety into the Schering compound SCH 50911 led to a new class of very potent GABA_Breceptor antagonists, such as CGP76290A (Ong et al., 1998a; IC₅₀ = 2 nM, enantiomer CGP76291: IC₅₀ = 69 nM, racemate CGP71982, IC₅₀ = 8 nM; Fig. 3).

Finally, two iodinated high-affinity antagonists, i.e., [¹²⁵I]CGP64213 (IC₅₀ = 1.6 nM, i.e., inhibition of binding of [¹²⁵I]CGP64213 to GABA_Breceptors on rat cerebral cortex membranes) and [¹²⁵I]CGP71872 (IC₅₀ = 2.4 nM), a photoaffinity ligand, both with high specific radioactivities of >2000 Ci/mmol were developed, which were used for the elucidation of the structure of GABA_B1(Kaupmann et al., 1997; Belley et al., 1999; Calon et al., 2000;Froestl et al., 2001; Fig. 4). The ligand [¹²⁵I]CGP84963 (IC₅₀ = 6 nM, i.e., inhibition of binding of [¹²⁵I]CGP64213 to GABA_Breceptors on rat cerebral cortex membranes; Fig. 4) combines in one molecule a GABA_B receptor-binding part, an azidosalicylic acid as a photoaffinity moiety separated by a spacer of three GABA molecules from 2-iminobiotin, which binds to avidin in a reversible, pH dependent fashion. This compound was prepared to facilitate isolation and purification of the extracellular N-terminal GABA_B1 receptor fragment for crystallization and X-ray studies of the GABA_B1 binding site (Froestl et al., 1999).

Figure 4

Structures of high-affinity¹²⁵I-labeled GABA_B receptor antagonist.

Although GABA_B receptor antagonists have yet to be studied in humans, results of animal studies suggest that they may have clinical utility. Thus, GABA_B receptor antagonists suppress absence seizures in a variety of animal models (Marescaux et al., 1992). When administered either systemically or directly into the thalamus, GABA_B receptor antagonists prevent spike and wave discharges in the electroencephalograms of genetic absence rats. Similar results are obtained with the lethargic mouse and in rats injected with γ-hydroxybutyrate (GHB), which produces absence-like seizure activity (Hosford et al., 1992; Snead, 1992). In all cases, GABA_B receptor antagonists dose dependently reduce seizure activity. In the genetic absence rats, the spontaneous seizures are blocked by bilateral administration of pertussis toxin, supporting the involvement of G_i/G_o coupling in generating and maintaining the seizures (Bowery et al., 1999). These results suggest that GABA_B receptor activation may contribute to the absence syndrome, possibly through Ca²⁺ spike generation in the thalamus (Crunelli and Leresche, 1991; Charpier et al., 1999).

At high doses, GABA_B receptor antagonists induce convulsions in rats (Vergnes et al., 1997). Although the mechanism(s) underlying this action is unknown, the response is blocked by GABA_B receptor agonists. Importantly, not all GABA_B receptor antagonists cause seizures. For example, SCH 50911 fails to cause convulsions at doses 10- to 100-fold higher than those that completely block seizures in the genetic absence rat (Richards and Bowery, 1996).

The GHB-induced absence-like seizures in rats appear due, at least in part, to a weak partial agonist action at GABA_Breceptors (Bernasconi et al., 1999; Lingenhoehl et al., 1999). However, GHB also acts through sites distinct from GABA_Breceptors (Snead, 2000).

Several GABA_B receptor antagonists have been found to improve cognitive performance in a variety of animal paradigms, such as the low-affinity compounds, CGP35348 (Bianchi and Panerai, 1993; Castellano et al., 1993; Saha et al., 1993;Stäubli et al., 1999) and CGP36742 (Carletti et al., 1993;Mondadori et al., 1993, 1994, 1996a,b; Nakagawa and Takashima, 1997; Yu et al., 1997; Bonanno et al., 1999; Genkova-Papazova et al., 2000; Farr et al., 2000; Pittaluga et al., 2001), or the high-affinity compounds CGP55845A, CGP56433A, CGP61334, CGP62349, and CGP71872 (Getova et al., 1997; Getova and Bowery, 1998). Olpe et al. (1993b) observed a very pronounced facilitation of long-term potentiation in vivo with doses of 100 mg/kg i.v. CGP35348 on eliciting long-term potentiation by nonprimed tetanic stimulation in the CA1 region of the hippocampus of rats. Brucato et al. (1996) reported a suppression of long-term potentiation with CGP46381 using θ-like stimulus trains to the dentate gyrus. However, the latter GABA_B receptor antagonist did not show effects on working memory in the radial maze in rats (Brucato et al., 1996) nor did it improve learning and memory in mice in a step-down passive avoidance paradigm (C. Mondadori and W. Froestl, unpublished observations).

Perhaps not surprisingly, therefore, GABA_Bagonists impair learning behavior in animal models (Soubrie et al., 1976; Swartzwelder et al., 1987; Nabeshima et al., 1988a,b; Sidel et al., 1988; Castellano et al., 1989; Sharma and Kulkarni, 1990 and 1993;Castellano and McGaugh, 1991; Saha et al., 1993; DeSousa et al., 1994;Stackman and Walsh, 1994; Nakagawa et al., 1995; McNamara and Skelton, 1996; Tang and Hasselmo, 1996; Arolfo et al., 1998). This induced amnesia appears to be mediated via G protein-linked receptors because the impairment produced by baclofen in mice can be blocked by pertussis toxin administered intracerebroventricularly (Galeotti et al., 1998). Baclofen has occasionally produced memory deficits in patients (Sandyk and Gillman, 1985).

GABA_B receptor antagonists improve cognitive performance in a variety of animal models (Carletti et al., 1993;Mondadori et al., 1993; Brucato et al., 1996; Getova et al., 1997;Nakagawa and Takashima, 1997; Yu et al., 1997; Getova and Bowery, 1998;Stäubli et al., 1999; Genkova-Papazova et al., 2000; Farr et al., 2000). Conversely, GABA_B receptor agonists impair learning, an action that is blocked by pertussis toxin, supporting the involvement of G_i/G_o in the action of these agents (Nakagawa et al., 1995; McNamara and Skelton, 1996; Tang and Hasselmo, 1996; Arolfo et al., 1998; Galeotti et al., 1998). In studies with mice lacking the GABA_B1receptor subunit, a clear impairment of passive avoidance performance was observed, which was related to gene dosage (Schuler et al., 2001). These passive avoidance deficits are a reflection of impaired memory processes further linking GABA_B receptors to memory performance. Reports suggest that both GABA_B receptor antagonists and agonists are neuroprotective. Although baclofen is neuroprotective in a gerbil cerebral ischemia model, very high doses are required (Lal et al., 1995). Moreover, baclofen attenuates the neurotoxic effect of quinolinic acid on CA1 cells in rat hippocampus (Beskid et al., 1999). In contrast, studies with mouse cultured striatal neurons reveal that GABA_B receptor activation enhances the neurotoxic effects of N-methyl-d-aspartate, reinforcing the concept that GABA_B antagonists are more likely to be neuroprotective than agonists (Lafon-Cazal et al., 1999). In support of this, low doses of GABA_B receptor antagonists increase levels of nerve growth factor and brain-derived neurotrophic factor in rat brain hippocampus, neocortex, and spinal cord, which could attenuate neurodegenerative processes (Heese et al., 2000).

The potential significance GABA_B receptor mechanisms in depression was first suggested by Lloyd and colleagues (Pilc and Lloyd, 1984; Lloyd et al., 1985, 1989), but this was challenged by other groups. More recently, however, further suggestions that GABA_B antagonists, e.g. CGP36742, are effective in animal models of depression have emerged (Nakagawa et al., 1999). Clear antidepressant effects were seen after 4 weeks of oral treatment with CGP51176 in the chronic mild stress model (Bittiger et al., 1996b). This might be supported in due course by the observations of Heese et al. (2000) who showed that GABA_Bantagonists produce a rapid increase in nerve growth factor and brain-derived neurotrophic factor levels. Interestingly, antidepressants have been shown to produce the same increase in those growth factors but only after 2 to 3 weeks (Nibuya et al., 1995; Duman et al., 1997). Could there be a link between these phenomena?

VII. Conclusions

The G protein-coupled GABA_B receptor was first described over 20 years ago but only recently has the site been cloned and with this has come the identification of its unique heterodimeric structure. Even though much is known about the formation and characteristics of this receptor, many important questions remain. Thus, it is crucial to determine whether GABA_Breceptor subtypes exist that can be exploited pharmacologically, to determine whether other proteins can link with GABA_B1 to form a functional receptor, to establish whether GABA_B receptor subunits serve other functions in the cell, and to assess the clinical value of GABA_B receptor agonists and antagonists. Given the pace of discovery in this field, answers to these questions will be forthcoming. These results will not only have significant implications with regard to understanding the GABA_B receptor system in particular but may allow novel drugs acting at this receptor to be developed.

It is evident that the presence of two distinct proteins (or a protein and an essential accessory protein), coupled to G proteins, forming a receptor for GABA, poses certain problems for nomenclature. The subcommittee considers that there is little evidence for distinct functional types of the receptor, but this is a rare, and usually short-lived, situation in pharmacology. The present proposition is to continue to call the receptor the GABA_B receptor, and when distinct splice variants are studied, i.e. GABA_B1(a)/2(a), using the NC-IUPHAR designation for splice variants. This nomenclature is provisional and may be changed when there is evidence of distinct functional GABA_B receptor types or if NC-IUPHAR issues general guidelines for ligand-gated ion channels, which modify the GABA_A/B terminology.

Footnotes

Address correspondence to: Dr. Norman Bowery, University of Birmingham Medical School, Edgbaston, Birmingham, B15 2TT UK. E-mail:n.g.bowery{at}bham.ac.uk

Abbreviations

GABA_B: γ-aminobutyric acid_B
3-APPA: 3-aminopropyl-phosphinic acid
3-APMPA: methyl homolog of 3-APPA
GHB: γ-hydroxybutyrate
NC-IUPHAR: International Union of Pharmacology Committee on Receptor Nomenclature and Drug Classification
CHO: Chinese hamster ovary

U.S. Government

References

↵
1. Addae JI,
2. Rothwell NJ,
3. Stock MJ, and
4. Stone TW
(1986) Activation of thermogenesis of brown fat in rats by baclofen. Neuropharmacology 25:627–631.
OpenUrl CrossRef PubMed
↵
1. Addolorato G,
2. Caputo F,
3. Capristo E,
4. Colombo G,
5. Gessa GL, and
6. Gasbarrini G
(2000) Ability of baclofen in reducing alcohol craving and intake: II—preliminary clinical evidence. Alcohol Clin Exp Res 24:67–71.
OpenUrl CrossRef PubMed
↵
1. Albright AL,
2. Barry MJ,
3. Fasick P,
4. Barron W, and
5. Shultz B
(1996) Continuous intrathecal baclofen infusion for symptomatic generalized dystonia. Neurosurgery 38:934–939.
OpenUrl CrossRef PubMed
↵
1. Ambardekar AV,
2. Ilinsky IA,
3. Froestl W,
4. Bowery NG, and
5. Kultas-Ilinsky K
(1999) Distribution and properties of GABA_B antagonist [³H]CGP62349 binding in the Rhesus monkey thalamus and basal ganglia and the influence of lesions in the reticular thalamic nucleus. Neuroscience 93:1339–1347.
OpenUrl CrossRef PubMed
↵
1. Andrade R,
2. Malenka RC, and
3. Nicoll RA
(1986) A G protein couples serotonin and GABA_B receptors to the same channels in hippocampus. Science (Wash DC) 234:1261–1265.
OpenUrl Abstract/FREE Full Text
↵
1. Armstrong RW,
2. Steinbok P,
3. Cochrane DD,
4. Kube SD,
5. Fife SE, and
6. Farrell K
(1997) Intrathecally administered baclofen for treatment of children with spasticity of cerebral origin. J Neurosurg 87:409–414.
OpenUrl CrossRef PubMed
↵
1. Arolfo MP,
2. Zanudio MA, and
3. Ramirez OA
(1998) Baclofen infused in rat hippocampal formation impairs spatial learning. Hippocampus 8:109–113.
OpenUrl CrossRef PubMed
↵
1. Ashby CR,
2. Rohatgi R,
3. Ngosuwan J,
4. Borda T,
5. Gerasimov MR,
6. Morgan AE,
7. Kushner S,
8. Brodie JD, and
9. Dewey SL
(1999) Implication of the GABA_B receptor in gamma vinyl-GABA's inhibition of cocaine-induced increases in nucleus accumbens dopamine. Synapse 31:151–153.
OpenUrl CrossRef PubMed
↵
1. Ataka T,
2. Kumamoto E,
3. Shimoji K, and
4. Yoshimura M
(2000) Baclofen inhibits more effectively C-afferent than A delta-afferent glutamatergic transmission in substantia gelatinosa neurons of adult rat spinal cord slices. Pain 86:273–282.
OpenUrl CrossRef PubMed
↵
1. Auer C,
2. Siebner HR,
3. Dressnandt J, and
4. Conrad B
(1999) Intrathecal baclofen increases corticospinal output to hand muscles in multiple sclerosis. Neurology 52:1298–1299.
OpenUrl FREE Full Text
↵
1. Azouvi P,
2. Mane M,
3. Thiebaut JB,
4. Denys P,
5. Remy-Neris O, and
6. Bussel B
(1996) Intrathecal baclofen administration for control of severe spinal spasticity: functional improvement and long-term follow-up. Arch Phys Med Rehab 77:35–39.
OpenUrl CrossRef PubMed
↵
1. Banerjee PK and
2. Snead OC
(1995) Presynaptic gamma-hydroxybutyric acid (GHB) and gamma-aminobutyric acid_B (GABA_B) receptor-mediated release of GABA and glutamate (Glu) in rat thalamic ventrobasal nucleus (VB): a possible mechanism for the generation of absence-like seizures induced by GHB. J Pharmacol Exp Ther 273:1534–1543.
OpenUrl Abstract/FREE Full Text
↵
1. Barral J,
2. Toro S,
3. Galarraga E, and
4. Bargas J
(2000) GABAergic presynaptic inhibition of rat neostriatal afferents is mediated by Q-type Ca²⁺ channels. Neurosci Lett 283:33–36.
OpenUrl CrossRef PubMed
↵
1. Becker R,
2. Alberti O, and
3. Bauer BL
(1997) Continuous intrathecal baclofen infusion in severe spasticity after traumatic or hypoxic brain injury. J Neurol 244:160–166.
OpenUrl CrossRef PubMed
↵
1. Becker R,
2. Benes L,
3. Sure U,
4. Hellwig D, and
5. Bertalanffy H
(2000) Intrathecal baclofen alleviates autonomic dysfunction in severe brain injury. J Clin Neurosci 7:316–319.
OpenUrl CrossRef PubMed
↵
1. Becker WJ,
2. Harris CJ,
3. Long ML,
4. Ablett DP,
5. Klein GM, and
6. DeForge DA
(1995) Long-term intrathecal baclofen therapy in patients with intractable spasticity. Can J Neurol Sci 22:208–217.
OpenUrl PubMed
↵
1. Birkmayer W
1. Bein HJ
(1972) Pharmacological differentiations of muscle relaxants. in Spasticity: A Topical Survey, ed Birkmayer W (Hans Huber, Vienna), pp 76–89.
↵
1. Belley M,
2. Sullivan R,
3. Reeves A,
4. Evans J,
5. O'Neill G, and
6. Ng GYK
(1999) Synthesis of the nanomolar photoaffinity GABA_B receptor ligand CGP 71872 reveals diversity in the tissue distribution of GABA_B receptor forms. Bioorg Med Chem 7:2697–2704.
OpenUrl CrossRef PubMed
↵
1. Belvisi MG,
2. Ichinose M, and
3. Barnes PJ
(1989) Modulation of non-adrenergic, non-cholinergic neural bronchoconstriction in guinea-pig airways via GABA_B receptors. Br J Pharmacol 97:1225–1231.
OpenUrl PubMed
↵
1. Benke D,
2. Honer M,
3. Michel C,
4. Bettler B, and
5. Mohler H
(1999) Gamma-aminobutyric acid type B receptor splice variant proteins GBR1a and GBR1b are both associated with GBR2 in situ and display differential regional and subcellular distribution. J Biol Chem 274:27323–27330.
OpenUrl Abstract/FREE Full Text
↵
1. Bernasconi R,
2. Mathivet P,
3. Bischoff S, and
4. Marescaux C
(1999) Gamma-hydroxybutyric acid: an endogenous neuromodulator with abuse potential. Trends Pharmacol Sci 20:135–141.
OpenUrl CrossRef PubMed
↵
1. Bertrand S,
2. Ng GYK,
3. Purisai MG,
4. Wolfe SE,
5. Severidt MW,
6. Nouel D,
7. Robitaille R,
8. Low MJ,
9. O'Neill GP,
10. Metters K,
11. et al.
(2001) The anticonvulsant, antihyperalgesic agent gabapentin is an agonist at brain gamma-aminobutyric acid type B receptors negatively coupled to voltage-dependent calcium channels. J Pharmacol Exp Ther 298:15–24.
OpenUrl Abstract/FREE Full Text
↵
1. Beskid M,
2. Rozycka Z, and
3. Taraszewska A
(1999) Quinolinic acid and GABA-B receptor ligand: effect on pyramidal neurons of the CA1 sector of rat's dorsal hippocampus following peripheral administration. Folia Neuropathol 37:99–106.
OpenUrl PubMed
↵
1. Bianchi M and
2. Panerai AE
(1993) Reversal of scopolamine-induced amnesia by the GABA_B receptor antagonist CGP 35348 in the mouse. Cognit Brain Res 1:135–136.
OpenUrl CrossRef PubMed
↵
1. Billinton A,
2. Stean TO,
3. Bowery NG, and
4. Upton N
(2000) GABA_B(I) splice variant mRNAs are differentially affected by electroshock induced seizure in rats. Neuroreport 11:3817–3822.
OpenUrl PubMed
↵
1. Billinton A,
2. Upton N, and
3. Bowery NG
(1999) GABA_B receptor isoforms GBR1a and GBR1b, appear to be associated with pre- and post-synaptic elements respectively in rat and human cerebellum. Br J Pharmacol 126:1387–1392.
OpenUrl CrossRef PubMed
↵
1. Bindokas VP and
2. Ishida AT
(1991) (−)-Baclofen and gamma-aminobutyric acid inhibit calcium currents in isolated retinal ganglion cells. Proc Natl Acad Sci USA 88:10759–10763.
OpenUrl Abstract/FREE Full Text
↵
1. Bischoff S,
2. Leonhard S,
3. Reymann N,
4. Schuler V,
5. Shigemoto R,
6. Kaupmann K, and
7. Bettler B
(1999) Spatial distribution of GABA_BR1 receptor mRNA and binding sites in the rat brain. J Comp Neurol 412:1–16.
OpenUrl CrossRef PubMed
↵
1. Bittiger H,
2. Bellouin C,
3. Froestl W,
4. Heid J,
5. Schmutz M, and
6. Stampf P
(1996a) [³H]CGP 62349: a new potent GABA_B receptor antagonist radioligand. Pharmacol Rev Commun 8:97–98.
OpenUrl
↵
1. Tanaka C and
2. Bowery NG
1. Bittiger H,
2. Froestl W,
3. Gentsch C,
4. Jaekel J,
5. Mickel SJ,
6. Mondadori C,
7. Olpe HR, and
8. Schmutz M
(1996b) GABA_B receptor antagonists: potential therapeutic applications. in GABA: Receptors, Transporters and Metabolism, eds Tanaka C and Bowery NG (Birkhaeuser Verlag, Basel), pp 297–305.
↵
1. Bittiger H,
2. Reymann N,
3. Froestl W, and
4. Mickel SJ
(1992) ³H-CGP54626: a potent antagonist radioligand for GABA_B receptors. Pharmacol Commun 2:23.
OpenUrl
↵
1. Bittiger H,
2. Reymann N,
3. Hall R, and
4. Kane P
(1988) CGP27492, a new potent and selective radioligand for GABA_B receptors (Abstract). Eur J Neurosci 16 (Suppl):10.
OpenUrl
↵
1. Blackshaw LA,
2. Smid SD,
3. O'Donnell TA, and
4. Dent J
(2000) GABA_B receptor-mediated effects on vagal pathways to the lower oesophageal sphincter and heart. Br J Pharmacol 130:279–288.
OpenUrl CrossRef PubMed
↵
1. Blackshaw LA,
2. Staunton E,
3. Lehmann A, and
4. Dent J
(1999) Inhibition of transient lower esophageal sphincter relaxations and reflux in ferrets by GABA receptor agonists. Am J Physiol 277:G867–G874.
OpenUrl PubMed
↵
1. Bolser DC,
2. Aziz SM,
3. DeGennaro FC,
4. Kreutner W,
5. Egan RW,
6. Siegel MI, and
7. Chapman RW
(1993) Antitussive effects of GABA_B agonists in the cat and guinea-pig. Br J Pharmacol 110:491–495.
OpenUrl CrossRef PubMed
↵
1. Bolser DC,
2. Blythin DJ,
3. Chapman RW,
4. Egan RW,
5. Hey JA,
6. Rizzo C,
7. Kuo SC, and
8. Kreutner W
(1995) The pharmacology of SCH 50911: a novel, orally-active GABA-B receptor antagonist. J Pharmacol Exp Ther 274:1393–1398.
OpenUrl Abstract/FREE Full Text
↵
1. Bolser DC,
2. DeGennaro FC,
3. O'Reilly S,
4. Chapman RW,
5. Kreutner W,
6. Egan RW, and
7. Hey JA
(1994) Peripheral and central sites of action of GABA-B agonists to inhibit the cough reflex in the cat and guinea pig. Br J Pharmacol 113:1344–1348.
OpenUrl CrossRef PubMed
↵
1. Bonanno G,
2. Carita F,
3. Cavazzani P,
4. Munari C, and
5. Raiteri M
(1999) Selective block of rat and human neocortex GABA_B receptors regulating somatostatin release by a GABA_B antagonist endowed with cognition enhancing activity. Neuropharmacology 38:1789–1795.
OpenUrl CrossRef PubMed
↵
1. Bonanno G,
2. Fassio A,
3. Sala R,
4. Schmid G, and
5. Raiteri M
(1998) GABA_B receptors as potential targets for drugs able to prevent excitatory amino acid transmission in the spinal cord. Eur J Pharmacol 362:143–148.
OpenUrl CrossRef PubMed
↵
1. Bonanno G,
2. Fassio A,
3. Schmid G,
4. Severi P,
5. Sala R, and
6. Raiteri M
(1997) Pharmacologically distinct GABA_B receptors that mediate inhibition of GABA and glutamate release in human neocortex. Br J Pharmacol 120:60–64.
OpenUrl CrossRef PubMed
↵
1. Bonanno G,
2. Gemignani A,
3. Schmid G,
4. Severi P,
5. Cavazzani P, and
6. Raiteri M
(1996) Human brain somatostatin release from isolated cortical nerve endings and its modulation through GABA_B receptors. Br J Pharmacol 118:1441–1446.
OpenUrl PubMed
↵
1. Bonanno G and
2. Raiteri M
(1992) Functional evidence for multiple GABA_B receptor subtypes in the rat cerebral cortex. J Pharmacol Exp Ther 262:114–118.
OpenUrl Abstract/FREE Full Text
↵
1. Bonanno G and
2. Raiteri M
(1993a) Multiple GABA_B receptors. Trends Pharmacol Sci 14:259–261.
OpenUrl CrossRef PubMed
↵
1. Bonanno G and
2. Raiteri M
(1993b) Gamma-aminobutyric (GABA) autoreceptors in rat cerebral cortex and spinal cord represent pharmacologically distinct subtypes of the GABA_B receptor. J Pharmacol Exp Ther 265:765–770.
OpenUrl Abstract/FREE Full Text
↵
1. Bouvier M
(2001) Oligomerization of G-protein-coupled transmitter receptors. Nat Rev Neurosci 2:274–286.
OpenUrl CrossRef PubMed
↵
1. Bowery NG
(1993) GABA_B receptor pharmacology. Annu Rev Pharmacol Toxicol 33:109–147.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Doble A,
3. Hill DR,
4. Hudson AL,
5. Shaw JS,
6. Turnbull MJ, and
7. Warrington R
(1981) Bicuculline-insensitive GABA receptors on peripheral autonomic nerve terminals. Eur J Pharmacol 71:53–70.
OpenUrl CrossRef PubMed
↵
1. Bowery NG and
2. Enna SJ
(2000) Gamma-aminobutyric acid (B) receptors: first of the functional metabotropic heterodimers. J Pharmacol Exp Ther 292:2–7.
OpenUrl Abstract/FREE Full Text
1. Bowery NG,
2. Hill DR, and
3. Hudson AL
(1983) Characteristics of GABA_B receptor sites on rat whole brain synaptic membranes. Br J Pharmacol 78:191–206.
OpenUrl CrossRef PubMed
1. Bowery NG,
2. Hill DR, and
3. Hudson AL
(1985) [³H](−)Baclofen: an improved ligand for GABA_B sites. Neuropharmacology 24:207–210.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Hill DR,
3. Hudson AL,
4. Doble A,
5. Middlemiss DN,
6. Shaw J, and
7. Turnbull M
(1980) (−)Baclofen decreases neurotransmitter release in the mammalian CNS by an action at a novel GABA receptor. Nature (Lond) 283:92–94.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Hudson AL, and
3. Price GW
(1987) GABA_A and GABA_B receptor site distribution in the rat central nervous system. Neuroscience 20:365–383.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Parry K,
3. Boehrer A,
4. Mathivet P,
5. Marescaux C, and
6. Bernasconi R
(1999) Pertussis toxin decreases absence seizures and GABA_B receptor binding in thalamus of a genetically prone rat (GAERS). Neuropharmacology 38:1691–1697.
OpenUrl CrossRef PubMed
↵
1. Brebner K,
2. Froestl W,
3. Andrews M,
4. Phelan R, and
5. Roberts DCS
(1999) The GABA_B agonist CGP44532 decreases cocaine self-administration in rats: demonstration using a progressive ratio and a discrete trials procedure. Neuropharmacology 38:1797–1804.
OpenUrl CrossRef PubMed
↵
1. Brebner K,
2. Phelan R, and
3. Roberts DCS
(2000a) Effect of baclofen on cocaine self-administration in rats reinforced under fixed-ratio 1 and progressive-ratio schedules. Psychopharmacology 148:314–321.
OpenUrl CrossRef PubMed
↵
1. Brebner K,
2. Phelan R, and
3. Roberts DCS
(2000b) Intra-VTA baclofen attenuates cocaine self-administration on a progressive ratio schedule of reinforcement. Pharmacol Biochem Behav 66:857–862.
OpenUrl CrossRef PubMed
↵
1. Brucato FH,
2. Levin ED,
3. Mott DD,
4. Lewis DV,
5. Wilson WA, and
6. Swartzwelder HS
(1996) Hippocampal long-term potentiation and spatial learning in the rat: effects of GABA_B receptor blockade. Neuroscience 74:331–339.
OpenUrl CrossRef PubMed
↵
1. Bussieres N and
2. El Manira A
(1999) GABA_B receptor activation inhibits N- and P/Q-type calcium channels in cultured lamprey sensory neurons. Brain Res 847:175–185.
OpenUrl CrossRef PubMed
↵
1. Calon F,
2. Morissette M,
3. Goulet M,
4. Grondin R,
5. Blanchet PJ,
6. Bedard PJ, and
7. Di Paolo T
(2000) ¹²⁵I-CGP 64213 binding to GABA_B receptors in the brain of monkeys: effect of MPTP and dopaminomimetic treatments. Exp Neurol 163:191–199.
OpenUrl CrossRef PubMed
↵
1. Calver AR,
2. Medhurst AD,
3. Robbins MJ,
4. Charles KJ,
5. Evans ML,
6. Harrison DC,
7. Stammers M,
8. Hughes SA,
9. Hervieu G,
10. Couve A,
11. et al.
(2000) The expression of GABA_B1 and GABA_B2 receptor subunits in the CNS differs from that in peripheral tissues. Neuroscience 100:155–170.
OpenUrl CrossRef PubMed
↵
1. Calver AR,
2. Robbins MJ,
3. Cosio C,
4. Rice SQJ,
5. Babbs AJ,
6. Hirst WD,
7. Boyfield I,
8. Wood MD,
9. Russell RB,
10. Price GW,
11. et al.
(2001) The C-terminal domains of the GABA_B receptor subunits mediate intracellular trafficking but are not required for receptor signaling. Neuroscience 21:1203–1210.
OpenUrl Abstract/FREE Full Text
↵
1. Campbell SK,
2. Almeida GL,
3. Penn RD, and
4. Corcos DM
(1995) The effects of intrathecally administered baclofen on function in patients with spasticity. Phys Ther 75:352–362.
OpenUrl Abstract/FREE Full Text
↵
1. Campbell UC,
2. Lac ST, and
3. Carroll ME
(1999) Effects of baclofen on maintenance and reinstatement of intravenous cocaine self-administration in rats. Psychopharmacology 143:209–214.
OpenUrl CrossRef PubMed
↵
1. Carletti R,
2. Libri V, and
3. Bowery NG
(1993) The GABA_B antagonist CGP 36742 enhances spatial learning performance and antagonises baclofen-induced amnesia in mice. Br J Pharmacol 109:74P.
OpenUrl
↵
1. Castellano C,
2. Brioni JD,
3. Nagahara AH, and
4. McGaugh JL
(1989) Post-training systemic and intra-amygdala administration of the GABA-B agonist baclofen impairs retention. Behav Neural Biol 52:170–179.
OpenUrl CrossRef PubMed
↵
1. Castellano C,
2. Cestari V,
3. Cabib S, and
4. Puglisi-Allegra S
(1993) Strain-dependent effects of post-training GABA receptor agonists and antagonists on memory storage in mice. Psychopharmacology 111:134–138.
OpenUrl CrossRef PubMed
↵
1. Castellano C and
2. McGaugh JL
(1991) Oxotremorine attenuates retrograde amnesia induced by post-training administration of the GABAergic agonists muscimol and baclofen. Behav Neural Biol 56:25–31.
OpenUrl CrossRef PubMed
↵
1. Castelli MP,
2. Ingianni A,
3. Stefanini E, and
4. Gessa GL
(1999) Distribution of GABA_B receptor mRNAs in the rat brain and peripheral organs. Life Sci 64:1321–1328.
OpenUrl CrossRef PubMed
↵
1. Chan PKY,
2. Leung CKS, and
3. Yung WH
(1998) Differential expression of pre- and postsynaptic GABA_B receptors in rat substantia nigra pars reticulata neurones. Eur J Pharmacol 349:187–197.
OpenUrl CrossRef PubMed
↵
1. Chapman RW,
2. Danko G,
3. Rizzo C,
4. Egan RW,
5. Mauser PJ, and
6. Kreutner W
(1991) Prejunctional GABA-B inhibition of cholinergic, neurally-mediated airway contractions in guinea-pigs. Pulm Pharmacol 4:218–224.
OpenUrl CrossRef PubMed
↵
1. Charpier S,
2. Leresche N,
3. Deniau JM,
4. Mahon S,
5. Hughes SW, and
6. Crunelli V
(1999) On the putative contribution of GABA_B receptors to the electrical events occurring during spontaneous spike and wave discharges. Neuropharmacology 38:1699–1706.
OpenUrl CrossRef PubMed
↵
1. Chen G and
2. van den Pol AN
(1998) Presynaptic GABA_B autoreceptor modulation of P/Q-type calcium channels and GABA release in rat suprachiasmatic nucleus neurons. J Neurosci 18:1913–1922.
OpenUrl Abstract/FREE Full Text
↵
1. Chronwall BM,
2. Davis TD,
3. Severidt MW,
4. Wolfe SE,
5. McCarson KE,
6. Beatty DM,
7. Low MJ,
8. Morris SJ, and
9. Enna SJ
(2001) Constitutive expression of functional GABA_B receptors in mIL-tsA58 cells requires both GABA_B(1) and GABA_B2(2) genes. J Neurochem 77:1237–1247.
OpenUrl CrossRef PubMed
↵
1. Chu DCM,
2. Albin RL,
3. Young AB, and
4. Penney JB
(1990) Distribution and kinetics of GABA_B binding sites in rat central nervous system: a quantitative autoradiographic study. Neuroscience 34:341–357.
OpenUrl CrossRef PubMed
↵
1. Clark JA,
2. Mezey E,
3. Lam AS, and
4. Bonner TI
(2000) Distribution of the GABA_B receptor subunit gb2 in rat CNS. Brain Res 860:41–52.
OpenUrl CrossRef PubMed
↵
1. Colmers WF and
2. Williams JT
(1988) Pertussis toxin pretreatment discriminates between pre- and postsynaptic actions of baclofen in rat dorsal raphe nucleus in vitro. Neurosci Lett 93:300–306.
OpenUrl CrossRef PubMed
↵
1. Colombo G,
2. Agabio R,
3. Carai MAM,
4. Lobina C,
5. Pani M,
6. Reali R,
7. Addolorato G, and
8. Gessa GL
(2000) Ability of baclofen in reducing alcohol intake and withdrawal severity: I—preclinical evidence. Alcohol Clin Exp Res 24:58–66.
OpenUrl CrossRef PubMed
↵
1. Corrigall WA,
2. Coen KM,
3. Adamson KL,
4. Chow BLC, and
5. Zhang J
(2000) Response of nicotine self-administration in the rat to manipulations of mu-opioid and gamma-aminobutyric acid receptors in the ventral tegmental area. Psychopharmacology 149:107–114.
OpenUrl CrossRef PubMed
↵
1. Couve A,
2. Filippov AK,
3. Connolly CN,
4. Bettler B,
5. Brown DA, and
6. Moss SJ
(1998) Intracellular retention of GABA_B receptors. J Biol Chem 273:26361–26367.
OpenUrl Abstract/FREE Full Text
↵
1. Couve A,
2. Kittler JT,
3. Uren JM,
4. Calver AR,
5. Pangalos MN,
6. Walsh FS, and
7. Moss SJ
(2001) Association of GABA_B receptors and members of the 14–3-3 family of signaling proteins. Mol Cell Neurosci 17:317–328.
OpenUrl CrossRef PubMed
↵
1. Crunelli V and
2. Leresche N
(1991) A role for GABA_B receptors in excitation and inhibition of thalamocortical cells. Trends Neurosci 14:16–21.
OpenUrl CrossRef PubMed
↵
1. Cui JG,
2. Meyerson BA,
3. Sollevi A, and
4. Linderoth B
(1998) Effect of spinal cord stimulation on tactile hypersensitivity in mononeuropathic rats is potentiated by simultaneous GABA_B and adenosine receptor activation. Neurosci Lett 247:183–186.
OpenUrl CrossRef PubMed
↵
1. Cui LN,
2. Coderre E, and
3. Renaud LP
(2000) GABA_B presynaptically modulates suprachiasmatic input to hypothalamic paraventricular magnocellular neurons. Am J Physiol Regul Integr Comp Physiol 278:R1210–R1216.
OpenUrl PubMed
↵
1. Cunningham MD and
2. Enna SJ
(1996) Evidence for pharmacologically distinct GABA_B receptors associated with cAMP production in rat brain. Brain Res 720:220–224.
OpenUrl CrossRef PubMed
↵
1. Cutting DA and
2. Jordan CC
(1975) Alternative approaches to analgesia: baclofen as a model compound. Br J Pharmacol 54:171–179.
OpenUrl PubMed
↵
1. Deisz RA,
2. Billard JM, and
3. Zieglgänsberger W
(1997) Presynaptic and postsynaptic GABA_B receptors of neocortical neurons of the rat in vitro: differences in pharmacology and ionic mechanisms. Synapse 25:62–72.
OpenUrl CrossRef PubMed
↵
1. DeSousa NJ,
2. Beninger RJ,
3. Jhamandas K, and
4. Boegman RJ
(1994) Stimulation of GABA_B receptors in the basal forebrain selectively impairs working memory of rats in the double Y-maze. Brain Res 641:29–38.
OpenUrl CrossRef PubMed
↵
1. Dicpinigaitis PV and
2. Dobkin JB
(1997) Antitussive effect of the GABA-agonist baclofen. Chest 111:996–999.
OpenUrl CrossRef PubMed
↵
1. Dirig DM and
2. Yaksh TL
(1995) Intrathecal baclofen and muscimol, but not midazolam, are antinociceptive using the rat-formalin model. J Pharmacol Exp Ther 275:219–227.
OpenUrl Abstract/FREE Full Text
↵
1. Doger E,
2. Urba-Holmgren R,
3. Eguibar JR, and
4. Holmgren B
(1989) GABAergic modulation of yawning behavior. Pharmacol Biochem Behav 34:237–240.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Bittiger H, and
3. Olpe H-R
1. Dolphin AC,
2. Huston E, and
3. Scott RH
(1990) GABA_B-mediated inhibition of calcium currents: a possible role in presynaptic inhibition. in GABA_B Receptors in Mammalian Function, eds Bowery NG, Bittiger H, and Olpe H-R (Wiley, Chichester), pp 259–271.
↵
1. Doze VA,
2. Cohen GA, and
3. Madison DV
(1995) Calcium channel involvement in GABA_B receptor-mediated inhibition of GABA release in area CA1 of the rat hippocampus. J Neurophysiol 74:43–53.
OpenUrl CrossRef PubMed
↵
1. Dressler D,
2. Oeljeschläger RO, and
3. Rüther E
(1997) Severe tardive dystonia: treatment with continuous intrathecal baclofen administration. Movement Disorders 12:585–587.
OpenUrl CrossRef PubMed
↵
1. Dressnandt J and
2. Conrad B
(1996) Lasting reduction of severe spasticity after ending chronic treatment with intrathecal baclofen. J Neurol Neurosurg Psychiatry 2:168–173.
OpenUrl
↵
1. Dressnandt J,
2. Konstanzer A,
3. Weinzierl FX,
4. Pfab R, and
5. Klingelhöfer J
(1997) Intrathecal baclofen in tetanus: four cases and a review of reported cases. Intensive Care Med 23:896–902.
OpenUrl CrossRef PubMed
↵
1. Duman RS,
2. Heninger GR, and
3. Nestler EJ
(1997) A molecular and cellular theory of depression. Arch Gen Psychiatry 54:597–606.
OpenUrl CrossRef PubMed
↵
1. Durkin MM,
2. Gunwaldsen CA,
3. Borowsky B,
4. Jones KA, and
5. Branchek TA
(1999) An in situ hybridization study of the distribution of the GABA_B2 protein mRNA in the rat CNS. Mol Brain Res 71:185–200.
OpenUrl CrossRef PubMed
↵
1. Dutar P and
2. Nicoll RA
(1988a) A physiological role for GABA_B receptors in the central nervous system. Nature (Lond) 332:156–158.
OpenUrl CrossRef PubMed
↵
1. Dutar P and
2. Nicoll RA
(1988b) Pre- and postsynaptic GABA_B receptors in the hippocampus have different pharmacological properties. Neuron 1:585–591.
OpenUrl CrossRef PubMed
↵
1. Eaton MJ,
2. Martinez MA, and
3. Karmally S
(1999) A single intrathecal injection of GABA permanently reverses neuropathic pain after nerve injury. Brain Res 835:334–339.
OpenUrl CrossRef PubMed
↵
1. Enna SJ
(1997) GABA_B receptor agonists and antagonists: pharmacological properties and therapeutic possibilities. Exp Opin Invest Drugs 6:1319–1325.
OpenUrl CrossRef
↵
1. Möhler H
1. Enna SJ
(2000) GABA_B receptor signaling pathways. in Pharmacology of GABA and Glycine Neurotransmission, ed Möhler H (Springer-Verlag, Berlin), pp 329–342.
↵
1. Enna SJ and
2. Bowery NG
(1997) The GABA Receptors (Humana Press, Totowa, NJ), 2nd ed.
↵
1. Enna SJ,
2. Harstad EB, and
3. McCarson KE
(1998) Regulation of neurokinin-1 receptor expression by GABA_B receptor agonists. Life Sci 62:1525–1530.
OpenUrl CrossRef PubMed
↵
1. Farr SA,
2. Uezu K,
3. Creonte TA,
4. Flood JF, and
5. Morley JE
(2000) Modulation of memory processing in the cingulate cortex of mice. Pharmacol Biochem Behav 65:363–368.
OpenUrl CrossRef PubMed
↵
1. Fassio A,
2. Bonanno G,
3. Cavazzani P, and
4. Raiteri M
(1994) Characterization of the GABA autoreceptor in human neocortex as a pharmacological subtype of the GABA_B receptor. Eur J Pharmacol 263:311–314.
OpenUrl CrossRef PubMed
↵
1. Filippov AK,
2. Couve A,
3. Pangalos MN,
4. Walsh FS,
5. Brown DA, and
6. Moss SJ
(2000) Heteromeric assembly of GABA_BR1 and GABA_BR2 receptor subunits inhibits Ca²⁺ current in sympathetic neurons. J Neurosci 20:2867–2874.
OpenUrl Abstract/FREE Full Text
↵
1. Ford B,
2. Greene P,
3. Louis ED,
4. Petzinger G,
5. Bressman SB,
6. Goodman R,
7. Brin MF,
8. Sadiq S, and
9. Fahn S
(1996) Use of intrathecal baclofen in the treatment of patients with dystonia. Arch Neurol 53:1241–1246.
OpenUrl CrossRef PubMed
↵
1. François B,
2. Clavel M,
3. Desachy A,
4. Vignon P,
5. Salle JY, and
6. Gastinne H
(1997) Continuous intrathecal baclofen in tetanus. A therapeutic alternative. Presse Med 26:1045–1047.
OpenUrl PubMed
↵
1. François B,
2. Vacher P,
3. Roustan J,
4. Salle JY,
5. Vidal J,
6. Moreau JJ, and
7. Vignon P
(2001) Intrathecal baclofen after traumatic brain injury: early treatment using a new technique to prevent spasticity. J Trauma Inj Infect Crit Care 50:158–161.
OpenUrl CrossRef
↵
1. Fritschy JM,
2. Meskenaite V,
3. Weinmann O,
4. Honer M,
5. Benke D, and
6. Mohler H
(1999) GABA_B-receptor splice variants GB1a and GB1b in rat brain: developmental regulation, cellular distribution and extrasynaptic localization. Eur J Neurosci 11:761–768.
OpenUrl CrossRef PubMed
↵
1. Froestl W,
2. Bettler B,
3. Bittiger H,
4. Heid J,
5. Kaupmann K,
6. Mickel SJ, and
7. Strub D
(1999) Ligands for the isolation of GABA_B receptors. Neuropharmacology 38:1641–1646.
OpenUrl CrossRef PubMed
↵
1. Froestl W,
2. Bettler B,
3. Bittiger H,
4. Heid J,
5. Kaupmann K,
6. Mickel SJ, and
7. Strub D
(2001) Ligands for expression cloning and isolation of GABA_B receptors. Farmaco 56:101–105.
OpenUrl CrossRef PubMed
↵
1. Enna SJ and
2. Bowery NG
1. Froestl W and
2. Mickel SJ
(1997) Chemistry of GABA_B modulators. in The GABA Receptors, eds Enna SJ and Bowery NG (Humana Press, Totowa, NJ), pp 271–296.
↵
1. Froestl W,
2. Mickel SJ, and
3. Bittiger H
(1993) Potent GABA_B agonists and antagonists. Curr Opin Therap Patents 3:561–567.
OpenUrl
↵
1. Froestl W,
2. Mickel SJ,
3. Hall RG,
4. von Sprecher G,
5. Strub D,
6. Baumann PA,
7. Brugger F,
8. Gentsch C,
9. Jaekel J,
10. Olpe H-R,
11. Rihs G,
12. Vassout A,
13. Waldmeier PC, and
14. Bittiger H
(1995a) Phosphinic acid analogues of GABA. 1. New potent and selective GABA_B agonists. J Med Chem 38:3297–3312.
OpenUrl CrossRef PubMed
↵
1. Froestl W,
2. Mickel SJ,
3. Schmutz M, and
4. Bittiger H
(1996) Potent, orally active GABA_B receptor antagonists. Pharmacol Rev Commun 8:127–133.
OpenUrl
↵
1. Froestl W,
2. Mickel SJ,
3. von Sprecher G,
4. Bittiger H, and
5. Olpe HR
(1992) Chemistry of new GABA_B antagonists. Pharmacol Commun 2:52–56.
OpenUrl
↵
1. Froestl W,
2. Mickel SJ,
3. von Sprecher G,
4. Diel PJ,
5. Hall RG,
6. Maier L,
7. Strub D,
8. Melillo V,
9. Baumann PA,
10. Bernasconi R,
11. et al.
(1995b) Phosphinic acid analogues of GABA. 2. Selective, orally active GABA_B antagonists. J Med Chem 38:3313–3331.
OpenUrl CrossRef PubMed
↵
1. Fromm GH
(1994) Baclofen as an adjuvant analgesic. J Pain Symptom Manage 9:500–509.
OpenUrl CrossRef PubMed
↵
1. Frydenvang K,
2. Enna SJ, and
3. Krogsgaard-Larsen P
(1997) (−) (R)-5,5-Dimethylmorpholinyl-2-acetic acid ethyl ester hydrochloride. Acta Crystallogr C53:1088–1091.
OpenUrl
↵
1. Gage PW
(1992) Activation and modulation of neuronal K⁺ channels by GABA. Trends Neurosci 15:46–51.
OpenUrl CrossRef PubMed
↵
1. Galeotti N,
2. Ghelardini C, and
3. Bartolini A
(1998) Effect of pertussis toxin on baclofen- and diphenhydramine-induced amnesia. Psychopharmacology 136:328–334.
OpenUrl CrossRef PubMed
↵
1. Galvez T,
2. Duthey B,
3. Kniazeff J,
4. Blahos J,
5. Rovelli G,
6. Bettler B,
7. Prezeau L, and
8. Pin JP
(2001) Allosteric interactions between GB1 and GB2 subunits are required for optimal GABA_B receptor function. EMBO J 20:2152–2159.
OpenUrl Abstract
1. Gemignani A,
2. Paudice P,
3. Bonanno G, and
4. Raiteri M
(1994) Pharmacological discrimination between gamma-aminobutyric acid type B receptors regulating cholecystokinin and somatostatin release from rat neocortex synaptosomes. Mol Pharmacol 46:558–562.
OpenUrl Abstract
↵
1. Genkova-Papazova MG,
2. Petkova B,
3. Shishkova N, and
4. Lazarova-Bakarova M
(2000) The GABA-B antagonist CGP 36742 prevent PTZ-kindling-provoked amnesia in rats. Eur Neuropsychopharmacol 10:273–278.
OpenUrl PubMed
↵
1. Gerszten PC,
2. Albright AL, and
3. Johnstone GF
(1998) Intrathecal baclofen infusion and subsequent orthopedic surgery in patients with spastic cerebral palsy. J Neurosurg 88:1009–1013.
OpenUrl PubMed
↵
1. Getova D and
2. Bowery NG
(1998) The modulatory effects of high affinity GABA_B receptor antagonists in an active avoidance learning paradigm in rats. Psychopharmacology 137:369–373.
OpenUrl CrossRef PubMed
↵
1. Getova D,
2. Bowery NG, and
3. Spassov V
(1997) Effects of GABA_B receptor antagonists on learning and memory retention in a rat model of absence epilepsy. Eur J Pharmacol 320:9–13.
OpenUrl CrossRef PubMed
↵
1. Green A,
2. Walls S,
3. Wise A,
4. Green RH,
5. Martin AK, and
6. Marshall FH
(2000) Characterization of [³H]-CGP54626A binding to heterodimeric GABA_B receptors stably expressed in mammalian cells. Br J Pharmacol 131:1766–1774.
OpenUrl CrossRef PubMed
↵
1. Guelaud C,
2. Similowski T,
3. Bizec JL,
4. Cabane J,
5. Whitelaw WA, and
6. Derenne JP
(1995) Baclofen therapy for chronic hiccup. Eur Respir J 8:235–237.
OpenUrl Abstract
↵
1. Hall RG,
2. Kane PD,
3. Bittiger H, and
4. Froestl W
(1995) Phosphinic acid analogues of gamma-aminobutyric acid (GABA). Synthesis of a new radioligand. J Label Compd Radiopharm 36:129–135.
OpenUrl
↵
1. Hammond DL and
2. Washington JD
(1993) Antagonism of L-baclofen-induced antinociception by CGP 35348 in the spinal cord of the rat. Eur J Pharmacol 234:255–262.
OpenUrl CrossRef PubMed
↵
1. Hansson P and
2. Kinnman E
(1996) Unmasking mechanisms of peripheral neuropathic pain in a clinical perspective. Pain Rev 3:272–292.
OpenUrl
↵
1. Harayama N,
2. Shibuya I,
3. Tanaka K,
4. Kabashima N,
5. Ueta Y, and
6. Yamashita H
(1998) Inhibition of N- and P/Q-type calcium channels by postsynaptic GABA_B receptor activation in rat supraoptic neurones. J Physiol 509:371–383.
OpenUrl CrossRef PubMed
↵
1. Bowery NG,
2. Bittiger H, and
3. Olpe H-R
1. Harrison NL,
2. Lambert NA, and
3. Lovinger DM
(1990) Presynaptic GABA_B receptors on rat hippocampal neurons. in GABA_B Receptors in Mammalian Function, eds Bowery NG, Bittiger H, and Olpe H-R (Wiley, Chichester), pp 207–221.
↵
1. Hashimoto T and
2. Kuriyama K
(1997) In vivo evidence that GABA_B receptors are negatively coupled to adenylate cyclase in rat striatum. J Neurochem 69:365–370.
OpenUrl PubMed
↵
1. Heese K,
2. Otten U,
3. Mathivet P,
4. Raiteri M,
5. Marescaux C, and
6. Bernasconi R
(2000) GABA_B receptor antagonists elevate both mRNA and protein levels of the neurotrophins nerve growth factor (NGF) and brain-derived neurotrophic factor (BDNF) but not neurotrophin-3 (NT-3) in brain and spinal cord of rats. Neuropharmacology 39:449–462.
OpenUrl CrossRef PubMed
↵
1. Hering-Hanit R
(1999) Baclofen for prevention of migraine. Cephalalgia 19:589–591.
OpenUrl CrossRef PubMed
↵
1. Hill DR
(1985) GABA_B receptor modulation of adenylate cyclase activity in rat brain slices. Br J Pharmacol 84:249–257.
OpenUrl PubMed
↵
1. Hill DR and
2. Bowery NG
(1981) ³H-baclofen and ³H-GABA bind to bicuculline-insensitive GABA_B sites in rat brain. Nature (Lond) 290:149–152.
OpenUrl CrossRef PubMed
↵
1. Hill DR,
2. Bowery NG, and
3. Hudson AL
(1984) Inhibition of GABA_B receptor binding by guanyl nucleotides. J Neurochem 42:652–657.
OpenUrl PubMed
1. Hirst WD,
2. Rice SQJ,
3. Minton JAL,
4. Calver AR,
5. Pangalos MN,
6. Jenkins O, and
7. Price GW
(2000) Characterisation of a CHO cell line stably co-expressing GABA_BR1b and GABA_BR2 receptors. Br J Pharmacol 129:80P.
OpenUrl CrossRef
↵
1. Hosford DA,
2. Clark S,
3. Cao Z,
4. Wilson WA,
5. Lin F,
6. Morrisett RA, and
7. Huin A
(1992) The role of GABA_B receptor activation in absence seizures of lethargic (lh/lh) mice. Science (Wash DC) 257:398–401.
OpenUrl Abstract/FREE Full Text
↵
1. Howson W,
2. Mistry J,
3. Broekman M, and
4. Hills JM
(1993) Biological activity of 3-aminopropyl (methyl) phosphinic acid, a potent and selective GABA_B agonist with CNS activity. Bioorg Med Chem Lett 3:515–518.
OpenUrl CrossRef
↵
1. Idänpään-Heikkilä JJ and
2. Guilbaud G
(1999) Pharmacological studies on a rat model of trigeminal neuropathic pain: baclofen, but not carbamazepine, morphine or tricyclic antidepressants, attenuate the allodynia-like behaviour. Pain 79:281–290.
OpenUrl CrossRef PubMed
↵
1. Inoue M,
2. Matsuo T, and
3. Ogata N
(1985) Possible involvement of K⁺-conductance in the action of gamma-aminobutyric acid in the guinea-pig hippocampus. Br J Pharmacol 86:515–524.
OpenUrl PubMed
↵
1. Ipponi A,
2. Lamberti C,
3. Medica A,
4. Bartolini A, and
5. Malmberg-Aiello P
(1999) Tiagabine antinociception in rodents depends on GABA_B receptor activation: parallel antinociception testing and medial thalamus GABA microdialysis. Eur J Pharmacol 368:205–211.
OpenUrl CrossRef PubMed
↵
1. Isaacson JS
(1997) GABA receptor-mediated modulation of presynaptic currents and excitatory transmission at a fast central synapse. Soc Neurosci Abstr 23:366.
OpenUrl
↵
1. Isaacson JS
(1998) GABA_B receptor-mediated modulation of presynaptic currents and excitatory transmission at a fast central synapse. J Neurophysiol 80:1571–1576.
OpenUrl PubMed
↵
1. Isaacson JS and
2. Hille B
(1997) GABA_B-mediated presynaptic inhibition of excitatory transmission and synaptic vesicle dynamics in cultured hippocampal neurons. Neuron 18:143–152.
OpenUrl CrossRef PubMed
↵
1. Isomoto S,
2. Kaibara M,
3. Sakurai-Yamashita Y,
4. Nagayama Y,
5. Uezono Y,
6. Yano K, and
7. Taniyama K
(1998) Cloning and tissue distribution of novel splice variants of the rat GABA_B receptor. Biochem Biophys Res Commun 253:10–15.
OpenUrl CrossRef PubMed
↵
1. Iyadomi M,
2. Iyadomi I,
3. Kumamoto E,
4. Tomokuni K, and
5. Yoshimura M
(2000) Presynaptic inhibition by baclofen of miniature EPSCs and IPSCs in substantia gelatinosa neurons of the adult rat spinal dorsal horn. Pain 85:385–393.
OpenUrl CrossRef PubMed
↵
1. Jarolimek W and
2. Misgeld U
(1997) GABA_B receptor-mediated inhibition of tetrodotoxin-resistant GABA release in rodent hippocampal CA1 pyramidal cells. J Neurosci 17:1025–1032.
OpenUrl Abstract/FREE Full Text
↵
1. Jones KA,
2. Borowsky B,
3. Tamm JA,
4. Craig DA,
5. Durkin MM,
6. Dai M,
7. Yao WJ,
8. Johnson M,
9. Gunwaldsen C,
10. Huang LY,
11. et al.
(1998) GABA_B receptors function as a heteromeric assembly of the subunits GABA_BR1 and GABA_BR2. Nature (Lond) 396:674–679.
OpenUrl CrossRef PubMed
↵
1. Karbon EW,
2. Duman RS, and
3. Enna SJ
(1984) GABA_B receptors and norepinephrine-stimulated cAMP production in rat brain cortex. Brain Res 306:327–332.
OpenUrl CrossRef PubMed
↵
1. Karbon EW and
2. Enna SJ
(1985) Characterization of the relationship between gamma-aminobutyric acid B agonists and transmitter-coupled cyclic nucleotide-generating systems in rat brain. Mol Pharmacol 27:53–59.
OpenUrl Abstract
↵
1. Karlsson G,
2. Pozza M, and
3. Olpe HR
(1988) Phaclofen: a GABA_B blocker reduces long-duration inhibition in the neocortex. Eur J Pharmacol 148:485–486.
OpenUrl CrossRef PubMed
↵
1. Kaupmann K,
2. Huggel K,
3. Heid J,
4. Flor PJ,
5. Bischoff S,
6. Mickel SJ,
7. McMaster G,
8. Angst C,
9. Bittiger H,
10. Froestl W, and
11. Bettler B
(1997) Expression cloning of GABA_B receptors uncovers similarity to metabotropic glutamate receptors. Nature (Lond) 386:239–246.
OpenUrl CrossRef PubMed
↵
1. Kaupmann K,
2. Malitschek B,
3. Schuler V,
4. Heid J,
5. Froestl W,
6. Beck P,
7. Mosbacher J,
8. Bischoff S,
9. Kulik A,
10. Shigemoto R,
11. et al.
(1998a) GABA_B-receptor subtypes assemble into functional heteromeric complexes. Nature (Lond) 396:683–687.
OpenUrl CrossRef PubMed
↵
1. Kaupmann K,
2. Schuler V,
3. Mosbacher J,
4. Bischoff S,
5. Bittiger H,
6. Heid J,
7. Froestl W,
8. Leonhard S,
9. Pfaff T,
10. Karschin A, and
11. Bettler B
(1998b) Human gamma-aminobutyric acid type B receptors are differentially expressed and regulate inwardly rectifying K⁺ channels. Proc Natl Acad Sci USA 95:14991–14996.
OpenUrl Abstract/FREE Full Text
↵
1. Birkmayer W
1. Keberle H and
2. Faigle JW
(1972) Synthesis and structure-activity relationship of the gamma-aminobutyric acid derivatives. in Spasticity: A Topical Survey, ed Birkmayer W (Hans Huber, Vienna), pp 90–100.
↵
1. Keir MJ,
2. Barakat MJ,
3. Dev KK,
4. Bittiger H,
5. Bettler B, and
6. Henley JM
(1999) Characterisation and partial purification of the GABA_B receptor from the rat cerebellum using the novel antagonist [³H]CGP 62349. Mol Brain Res 71:279–289.
OpenUrl PubMed
↵
1. Kendall DA,
2. Browner M, and
3. Enna SJ
(1982) Comparison of the antinociceptive effect of gamma-aminobutyric acid (GABA) agonists: evidence for a cholinergic involvement. J Pharmacol Exp Ther 220:482–487.
OpenUrl Abstract/FREE Full Text
↵
1. Kerr DIB,
2. Ong J,
3. Johnston GAR,
4. Abbenante J, and
5. Prager RH
(1988) 2-Hydroxy-saclofen: an improved antagonist at central and peripheral GABA_B receptors. Neurosci Lett 92:92–96.
OpenUrl CrossRef PubMed
↵
1. Kerr DIB,
2. Ong J,
3. Prager RH,
4. Gynther BD, and
5. Curtis DR
(1987) Phaclofen: a peripheral and central baclofen antagonist. Brain Res 405:150–154.
OpenUrl CrossRef PubMed
↵
1. Knight AR and
2. Bowery NG
(1996) The pharmacology of adenylyl cyclase modulation by GABA_B receptors in rat brain slices. Neuropharmacology 35:703–712.
OpenUrl CrossRef PubMed
↵
1. Kontani H,
2. Kawabata Y, and
3. Koshiura R
(1988) The effect of baclofen on the urinary bladder contraction accompanying micturition in anesthetized rats. Jpn J Pharmacol 46:7–15.
OpenUrl PubMed
↵
1. Krach LE
(2001) Pharmacotherapy of spasticity: oral medications and intrathecal baclofen. J Child Neurol 16:31–36.
OpenUrl CrossRef PubMed
↵
1. Kumar A and
2. Dromerick AW
(1998) Intractable hiccups during stroke rehabilitation. Arch Phys Med Rehab 79:697–699.
OpenUrl CrossRef PubMed
↵
1. Kuner R,
2. Köhr G,
3. Grünewald S,
4. Eisenhardt G,
5. Bach A, and
6. Kornau HC
(1999) Role of heteromer formation in GABA_B receptor function. Science (Wash DC) 283:74–77.
OpenUrl Abstract/FREE Full Text
↵
1. Lafon-Cazal M,
2. Viennois G,
3. Kuhn R,
4. Malitschek B,
5. Pin JP,
6. Shigemoto R, and
7. Bockaert J
(1999) mGluR7-like receptor and GABA_B receptor activation enhance neurotoxic effects of N-methyl-D-aspartate in cultured mouse striatal GABAergic neurones. Neuropharmacology 38:1631–1640.
OpenUrl CrossRef PubMed
↵
1. Lal S,
2. Shuaib A, and
3. Ijaz S
(1995) Baclofen is cytoprotective to cerebral ischemia in gerbils. Neurochem Res 20:115–119.
OpenUrl CrossRef PubMed
↵
1. Lambert NA and
2. Wilson WA
(1996) High-threshold Ca²⁺ currents in rat hippocampal interneurones and their selective inhibition by activation of GABA_B receptors. J Physiol 492:115–127.
OpenUrl CrossRef PubMed
↵
1. Lanneau C,
2. Green A,
3. Hirst WD,
4. Wise A,
5. Brown J,
6. Donnier E,
7. Charles KJ,
8. Wood M,
9. Davies CH, and
10. Pangalos MN
(2001) Gabapentin is not a GABA_B receptor agonist. Neuropharmacology 41:965–975.
OpenUrl CrossRef PubMed
↵
1. Lehmann A,
2. Antonsson M,
3. Bremner-Danielsen M,
4. Flärdh M,
5. Hansson-Bränden L, and
6. Kärrberg L
(1999) Activation of the GABA(B) receptor inhibits transient lower esophageal sphincter relaxations in dogs. Gastroenterology 117:1147–1154.
OpenUrl CrossRef PubMed
↵
1. Lehmann A,
2. Hansson-Bränden L, and
3. Kärrberg L
(2000) Effects of repeated administration of baclofen on transient lower esophageal sphincter relaxation in the dog. Eur J Pharmacol 403:163–167.
OpenUrl CrossRef PubMed
↵
1. Levy RA and
2. Proudfit HK
(1979) Analgesia produced by microinjection of baclofen and morphine at brain stem sites. Eur J Pharmacol 57:43–55.
OpenUrl CrossRef PubMed
↵
1. Liang F,
2. Hatanaka Y,
3. Saito H,
4. Yamamori T, and
5. Hashikawa T
(2000) Differential expression of gamma-aminobutyric acid type B receptor-1a and -1b mRNA variants in GABA and non-GABAergic neurons of the rat brain. J Comp Neurol 416:475–495.
OpenUrl CrossRef PubMed
↵
1. Lidums I,
2. Lehmann A,
3. Checklin H,
4. Dent J, and
5. Holloway RH
(2000) Control of transient lower esophageal sphincter relaxations and reflux by the GABA_B agonist baclofen in normal subjects. Gastroenterology 118:7–13.
OpenUrl CrossRef PubMed
↵
1. Liebman JM and
2. Pastor G
(1980) Antinociceptive effects of baclofen and muscimol upon intraventricular administration. Eur J Pharmacol 61:225–230.
OpenUrl CrossRef PubMed
↵
1. Ling W,
2. Shoptaw S, and
3. Majewska D
(1998) Baclofen as a cocaine anti-craving medication: a preliminary clinical study. Neuropsychopharmacology 18:403–404.
OpenUrl CrossRef PubMed
↵
1. Lingenhoehl K,
2. Brom R,
3. Heid J,
4. Beck P,
5. Froestl W,
6. Kaupmann K,
7. Bettler B, and
8. Mosbacher J
(1999) Gamma-hydroxybutyrate is a weak agonist at recombinant GABA_B receptors. Neuropharmacology 38:1667–1673.
OpenUrl CrossRef PubMed
↵
1. Lloyd KG,
2. Thuret F, and
3. Pilc A
(1985) Upregulation of gamma-aminobutyric acid (GABA) B binding sites in rat frontal cortex: a common action of repeated administration of different classes of antidepressants and electroshock. J Pharmacol Exp Ther 235:191–199.
OpenUrl Abstract/FREE Full Text
↵
1. Lloyd KG,
2. Zivkovic B,
3. Scatton B,
4. Morselli PL, and
5. Bartholini G
(1989) The GABAergic hypothesis of depression. Prog Neuro-Psychopharmacol Biol Psychiatry 13:341–351.
OpenUrl CrossRef PubMed
↵
1. Lobina C,
2. Pani M,
3. Reali R,
4. Addolarato G, and
5. Gessa GL
(2000) Ability of baclofen in reducing alcohol intake and withdrawal severity: I—preclinical evidence. Alcohol Clin Exp Res 24:58–66.
OpenUrl CrossRef PubMed
↵
1. Lorente P,
2. Lacampagne A,
3. Pouzeratte Y,
4. Richards S,
5. Malitschek B,
6. Kuhn R,
7. Bettler B, and
8. Vassort G
(2000) Gamma-aminobutyric acid type B receptors are expressed and functional in mammalian cardiomyocytes. Proc Natl Acad Sci USA 97:8664–8669.
OpenUrl Abstract/FREE Full Text
↵
1. Loubser PG and
2. Akman NM
(1996) Effects of intrathecal baclofen on chronic spinal cord injury pain. J Pain Symptom Manage 12:241–247.
OpenUrl CrossRef PubMed
↵
1. Lüscher C,
2. Jan LY,
3. Stoffel M,
4. Malenka RC, and
5. Nicoll RA
(1997) G protein-coupled inwardly rectifying K⁺ channels (GIRKs) mediate postsynaptic but not presynaptic transmitter actions in hippocampal neurons. Neuron 19:687–695.
OpenUrl CrossRef PubMed
↵
1. Malcangio M and
2. Bowery NG
(1996) GABA and its receptors in the spinal cord. Trends Pharmacol Sci 17:457–462.
OpenUrl CrossRef PubMed
↵
1. Marescaux C,
2. Vergnes M, and
3. Bernasconi R
(1992) GABA_B receptor antagonists: potential new anti-absence drugs. J Neural Transm 35:179–188.
OpenUrl CrossRef
↵
1. Margeta-Mitrovic M,
2. Jan YN, and
3. Jan LY
(2000) A trafficking checkpoint controls GABA_B receptor heterodimerization. Neuron 27:97–106.
OpenUrl CrossRef PubMed
↵
1. Margeta-Mitrovic M,
2. Mitrovic I,
3. Riley RC,
4. Jan LY, and
5. Basbaum AI
(1999) Immunohistochemical localization of GABA_B receptors in the rat central nervous system. J Comp Neurol 405:299–321.
OpenUrl CrossRef PubMed
↵
1. Marino RA
(1998) Baclofen therapy for intractable hiccups in pancreatic carcinoma. Am J Gastroenterol 93:2000.
OpenUrl PubMed
↵
1. Marshall FH,
2. Jones KA,
3. Kaupmann K, and
4. Bettler B
(1999a) GABA_B receptors—the first 7TM heterodimers. Trends Pharmacol Sci 20:396–399.
OpenUrl CrossRef PubMed
↵
1. Marshall FH,
2. White J,
3. Main M,
4. Green A, and
5. Wise A
(1999b) GABA_B receptors function as heterodimers. Biochem Soc Trans 27:530–535.
OpenUrl FREE Full Text
↵
1. Martin SC,
2. Russek SJ, and
3. Farb DH
(1999) Molecular identification of the human GABA_B R2: cell surface expression and coupling to adenylyl cyclase in the absence of GABA_B R1. Mol Cell Neurosci 13:180–191.
OpenUrl CrossRef PubMed
↵
1. Martin SC,
2. Russek SJ, and
3. Farb DH
(2001) Human GAGA_BR genomic structure: evidence for splice variants in GABA_BR1 but not GABA_BR2. Gene 278:63–79.
OpenUrl CrossRef PubMed
↵
1. McCarson KE and
2. Enna SJ
(1996) Relationship between GABA_B receptor activation and neurokinin receptor expression in spinal cord. Pharmacol Rev Commun 8:191–194.
OpenUrl
↵
1. McCarson KE and
2. Enna SJ
(1999) Nociceptive regulation of GABA_B receptor gene expression in rat spinal cord. Neuropharmacology 38:1767–1773.
OpenUrl CrossRef PubMed
↵
1. McLatchie LM,
2. Fraser NJ,
3. Main MJ,
4. Wise A,
5. Brown J,
6. Thompson N,
7. Solari R,
8. Lee MG, and
9. Foord SM
(1998) RAMPs regulate the transport and ligand specificity of the calcitonin-receptor-like receptor. Nature (Lond) 393:333–339.
OpenUrl CrossRef PubMed
↵
1. McNamara RK and
2. Skelton RW
(1996) Baclofen, a selective GABA_B receptor agonist, dose-dependently impairs spatial learning in rats. Pharmacol Biochem Behav 53:303–308.
OpenUrl CrossRef PubMed
↵
1. Meythaler JM,
2. McCary A, and
3. Hadley MN
(1997) Prospective assessment of continuous intrathecal infusion of baclofen for spasticity caused by acquired brain injury: a preliminary report. J Neurosurg 87:415–419.
OpenUrl CrossRef PubMed
↵
1. Mondadori C,
2. Hengerer B,
3. Ducret T, and
4. Borkowski J
(1994) Delayed emergence of effects on memory-enhancing drugs: implications for the dynamics of long-term memory. Proc Natl Acad Sci USA 91:2041–2045.
OpenUrl Abstract/FREE Full Text
↵
1. Mondadori C,
2. Jaekel J, and
3. Preiswerk G
(1993) CGP 36742: the first orally active GABA_B blocker improves the cognitive performance of mice, rats and rhesus monkeys. Behav Neural Biol 60:62–68.
OpenUrl CrossRef PubMed
↵
1. Mondadori C,
2. Moebius HJ, and
3. Borkowski J
(1996a) The GABA_B receptor antagonist CGP36742 and the nootropic oxiracetam facilitate the formation of long-term memory. Behav Brain Res 77:223–225.
OpenUrl CrossRef PubMed
↵
1. Mondadori C,
2. Moebius HJ, and
3. Zingg M
(1996b) CGP36742, an orally active GABA_B receptor antagonist, facilitates memory in a social recognition test in rats. Behav Brain Res 77:227–229.
OpenUrl CrossRef PubMed
↵
1. Moran JM,
2. Enna SJ, and
3. McCarson KE
(2001) Developmental regulation of GABA_B receptor function in rat spinal cord. Life Sci 68:2287–2295.
OpenUrl CrossRef PubMed
1. Muhyaddin M,
2. Roberts PJ, and
3. Woodruff GN
(1982) Presynaptic gamma-aminobutyric acid receptors in the rat anococcygeus muscle and their antagonism by 5-aminovaleric acid. Br J Pharmacol 77:163–168.
OpenUrl PubMed
↵
1. Munzar P,
2. Kutkat SW,
3. Miller CR, and
4. Goldberg SR
(2000) Failure of baclofen to modulate discriminative-stimulus effects of cocaine or methamphetamine in rats. Eur J Pharmacol 408:169–174.
OpenUrl CrossRef PubMed
↵
1. Myrick H,
2. Henderson S,
3. Brady KT, and
4. Malcolm R
(2001) Gabapentin in the treatment of cocaine dependence: a case series. J Clin Psychiatry 62:19–23.
OpenUrl CrossRef PubMed
↵
1. Nabeshima T,
2. Noda Y,
3. Itoh K, and
4. Kameyama T
(1988a) Role of cholinergic and GABAergic neuronal systems in cycloheximide-induced amnesia in mice. Pharmacol Biochem Behav 31:405–409.
OpenUrl CrossRef PubMed
↵
1. Nabeshima T,
2. Noda Y, and
3. Kameyama T
(1988b) GABAergic modulation of memory with regard to passive avoidance and conditioned suppression tasks in mice. Psychopharmacology 94:69–73.
OpenUrl CrossRef PubMed
↵
1. Nakagawa Y,
2. Ishibashi Y,
3. Yoshii T, and
4. Tagashira E
(1995) Involvement of cholinergic systems in the deficit of place learning in Morris water maze task induced by baclofen in rats. Brain Res 683:209–214.
OpenUrl CrossRef PubMed
↵
1. Nakagawa Y,
2. Sasaki A, and
3. Takashima T
(1999) The GABA_B receptor antagonist CGP36742 improves learned helplessness in rats. Eur J Pharmacol 381:1–7.
OpenUrl CrossRef PubMed
↵
1. Nakagawa Y and
2. Takashima T
(1997) The GABA_B receptor antagonist CGP36742 attenuates the baclofen-and scopolamine-induced deficit in Morris water maze task in rats. Brain Res 766:101–106.
OpenUrl CrossRef PubMed
↵
1. Nehring RB,
2. Horikawa HPM,
3. El Far O,
4. Kneussel M,
5. Brandstätter JH,
6. Stamm S,
7. Wischmeyer E,
8. Betz H, and
9. Karschin A
(2000) The metabotropic GABA_B receptor directly interacts with the activating transcription factor 4. J Biol Chem 275:35185–35191.
OpenUrl Abstract/FREE Full Text
1. Newberry NR and
2. Nicoll RA
(1984) Direct hyperpolarizing action of baclofen on hippocampal pyramidal cells. Nature (Lond) 308:450–452.
OpenUrl CrossRef PubMed
↵
1. Ng GYK,
2. Bertrand S,
3. Sullivan R,
4. Ethier N,
5. Wang J,
6. Yergey J,
7. Belley M,
8. Trimble L,
9. Bateman K,
10. Alder L,
11. et al.
(2001) Gamma-aminobutyric acid type B receptors with specific heterodimer composition and postsynaptic actions in hippocampal neurons are targets of anticonvulsant gabapentin action. Mol Pharmacol 59:144–152.
OpenUrl Abstract/FREE Full Text
↵
1. Ng GYK,
2. Clark J,
3. Coulombe N,
4. Ethier N,
5. Hebert TE,
6. Sullivan R,
7. Kargman S,
8. Chateauneuf A,
9. Tsukamoto N,
10. McDonald T,
11. et al.
(1999) Identification of a GABA_B receptor subunit, gb2, required for functional GABA_B receptor activity. J Biol Chem 274:7607–7610.
OpenUrl Abstract/FREE Full Text
↵
1. Nibuya M,
2. Morinobu S, and
3. Duman RS
(1995) Regulation of BDNF and trkB mRNA in rat brain by chronic electroconvulsive seizure and antidepressant drug treatments. J Neurosci 15:7539–7547.
OpenUrl Abstract/FREE Full Text
↵
1. Nickerson RB,
2. Atchison JW,
3. Van Hoose JD, and
4. Hayes D
(1997) Hiccups associated with lateral medullary syndrome. A case report. Am J Phys Med Rehabil 76:144–146.
OpenUrl CrossRef PubMed
↵
1. Noguchi J and
2. Yamashita H
(1999) Baclofen inhibits postsynaptic voltage-dependent calcium currents of supraoptic nucleus neurons isolated from young rats. Biomed Res (Tokyo) 20:239–247.
OpenUrl
↵
1. Ochs G,
2. Naumann C,
3. Dimitrijevic M, and
4. Sindou M
(1999) Intrathecal baclofen therapy for spinal origin spasticity: spinal cord injury, spinal cord disease and multiple sclerosis. Neuromodulation 2:108–119.
OpenUrl CrossRef PubMed
↵
1. Ochs G,
2. Struppler A,
3. Meyerson BA,
4. Linderoth G,
5. Gybels J,
6. Gardner BP,
7. Teddy P,
8. Jamous A, and
9. Weinmann P
(1989) Intrathecal baclofen for long-term treatment of spasticity: a multi-centre study. J Neurol Neurosurg Psychiatry 52:933–939.
OpenUrl Abstract/FREE Full Text
↵
1. Odagaki Y and
2. Koyama T
(2001) Identification of G alpha subtype(s) involved in gamma-aminobutyric acid_B receptor-mediated high-affinity guanosine triphosphatase activity in rat cerebral cortical membranes. Neurosci Lett 297:137–141.
OpenUrl CrossRef PubMed
↵
1. Odagaki Y,
2. Nishi N, and
3. Koyama T
(2000) Functional coupling of GABA_B receptors with G proteins that are sensitive to N-ethylmaleimide treatment, suramin and benzalkonium chloride in rat cerebral cortical membranes. J Neural Transm 107:1101–1116.
OpenUrl CrossRef PubMed
↵
1. Olianas MC and
2. Onali P
(1999) GABA_B receptor-mediated stimulation of adenylyl cyclase activity in membranes of rat olfactory bulb. Br J Pharmacol 126:657–664.
OpenUrl CrossRef PubMed
↵
1. Olpe HR,
2. Karlsson G,
3. Pozza MF,
4. Brugger F,
5. Steinmann M,
6. Van Riezen H,
7. Fagg G,
8. Hall RG,
9. Froestl W, and
10. Bittiger H
(1990) CGP 35348: a centrally active blocker of GABA_B receptors. Eur J Pharmacol 187:27–38.
OpenUrl CrossRef PubMed
↵
1. Olpe HR,
2. Steinmann MW,
3. Ferrat T,
4. Pozza MF,
5. Greiner K,
6. Brugger F,
7. Froestl W,
8. Mickel SJ, and
9. Bittiger H
(1993a) The actions of orally active GABA_B receptor antagonists on GABAergic transmission in vivo and in vitro. Eur J Pharmacol 233:179–186.
OpenUrl CrossRef PubMed
↵
1. Olpe HR,
2. Woerner W, and
3. Ferrat T
(1993b) Stimulation parameter determine role of GABA_B receptors in long-term potentiation. Experientia (Basel) 49:542–546.
OpenUrl
↵
1. Ong J,
2. Bexis S,
3. Marino V,
4. Parker DAS,
5. Kerr DIB, and
6. Froestl W
(2001) Comparative activities of the enantiomeric GABA_B receptor agonists CGP 44532 and 44533 in central and peripheral tissues. Eur J Pharmacol 412:27–37.
OpenUrl CrossRef PubMed
↵
1. Ong J and
2. Kerr DIB
(1990) GABA-receptors in peripheral tissues. Life Sci 46:1489–1501.
OpenUrl CrossRef PubMed
↵
1. Ong J,
2. Kerr DIB,
3. Bittiger H,
4. Waldmeier PC,
5. Baumann PA,
6. Cooke NG,
7. Mickel SJ, and
8. Froestl W
(1998a) Morpholin-2-yl-phosphinic acids are potent GABA_B receptor antagonists in rat brain. Eur J Pharmacol 362:27–34.
OpenUrl CrossRef PubMed
↵
1. Ong J,
2. Marino V,
3. Parker DAS, and
4. Kerr DIB
(1998b) Differential effects of phosphonic analogues of GABA on GABA_B autoreceptors in rat neocortical slices. Naunyn-Schmiedeberg's Arch Pharmacol 357:408–412.
OpenUrl CrossRef PubMed
↵
1. Opolski A,
2. Mazurkiewicz M,
3. Wietrayk J,
4. Kleinrok Z, and
5. Radzikowski C
(2000) The role of GABA-ergic system in human mammary gland pathology and in growth of transplantable murine mammary cancer. J Exp Clin Cancer Res 19:383–390.
OpenUrl PubMed
↵
1. Orsnes G,
2. Crone C,
3. Krarup C,
4. Petersen N, and
5. Nielsen J
(2000a) The effect of baclofen on the transmission in spinal pathways in spastic multiple sclerosis patients. Clin Neurophysiol 111:1372–1379.
OpenUrl CrossRef PubMed
↵
1. Orsnes GB,
2. Sorensen PS,
3. Larsen TK, and
4. Ravnborg M
(2000b) Effect of baclofen on gait in spastic MS patients. Acta Neurol Scand 101:244–248.
OpenUrl CrossRef PubMed
↵
1. Oshima T,
2. Sakamoto M,
3. Tatsuta H, and
4. Arita H
(1998) GABAergic inhibition of hiccup-like reflex induced by electrical stimulation in medulla of cats. Neurosci Res 30:287–293.
OpenUrl CrossRef PubMed
↵
1. Pagano A,
2. Rovelli G,
3. Mosbacher J,
4. Lohmann T,
5. Duthey B,
6. Stauffer D,
7. Ristig D,
8. Schuler V,
9. Meigel I,
10. Lampert C,
11. et al.
(2001) C-terminal interaction is essential for surface trafficking but not for heteromeric assembly of GABA_B receptors. J Neurosci 21:1189–1202.
OpenUrl Abstract/FREE Full Text
↵
1. Paret G,
2. Tirosh R,
3. Ben Zeev B,
4. Vardi A,
5. Brandt N, and
6. Barzilay Z
(1996) Intrathecal baclofen for severe torsion dystonia in a child. Acta Paediatr 85:635–637.
OpenUrl PubMed
↵
1. Patel S,
2. Naeem S,
3. Kesingland A,
4. Froestl W,
5. Capogna M,
6. Urban L, and
7. Fox A
(2001) The effects of GABA_B agonists and gabapentin on mechanical hyperalgesia in models of neuropathic and inflammatory pain in the rat. Pain 90:217–226.
OpenUrl CrossRef PubMed
↵
1. Penn RD and
2. Mangieri EA
(1993) Stiff-man syndrome treated with intrathecal baclofen. Neurology 43:2412.
OpenUrl FREE Full Text
↵
1. Penn RD,
2. Savoy SM,
3. Corcos D,
4. Latash M,
5. Gottlieb G,
6. Parke B, and
7. Kroin JS
(1989) Intrathecal baclofen for severe spinal spasticity. N Engl J Med 320:1517–1521.
OpenUrl CrossRef PubMed
↵
1. Pfaff T,
2. Malitschek B,
3. Kaupmann K,
4. Prezeau L,
5. Pin JP,
6. Bettler B, and
7. Karschin A
(1999) Alternative splicing generates a novel isoform of the rat metabotropic GABA_BR1 receptor. Eur J Neurosci 11:2874–2882.
OpenUrl CrossRef PubMed
↵
1. Phelan KD
(1999) N-Ethylmaleimide selectively blocks presynaptic GABA-B autoreceptor but not heteroreceptor-mediated inhibition in adult rat striatal slices. Brain Res 847:308–313.
OpenUrl CrossRef PubMed
↵
1. Pilc A and
2. Lloyd KG
(1984) Chronic antidepressants and GABA “B” receptors: a GABA hypothesis of antidepressant drug action. Life Sci 35:2149–2154.
OpenUrl CrossRef PubMed
↵
1. Pittaluga A,
2. Feligioni M,
3. Ghersi C,
4. Gemignani A, and
5. Raiteri M
(2001) Potentiation of NMDA receptor function through somatostatin release: a possible mechanism for the cognition-enhancing activity of GABA_B receptor antagonists. Neuropharmacology 41:301–310.
OpenUrl CrossRef PubMed
↵
1. Poorkhalkali N,
2. Juneblad K,
3. Jönsson AC,
4. Lindberg M,
5. Karlsson O,
6. Wallbrandt P,
7. Ekstrand J, and
8. Lehmann A
(2000) Immunocytochemical distribution of the GABA_B receptor splice variants GABA_BR1a and R1b in the rat CNS and dorsal root ganglia. Anat Embryol 201:1–13.
OpenUrl CrossRef PubMed
↵
1. Pozza MF,
2. Manuel NA,
3. Steinmann M,
4. Froestl W, and
5. Davies CH
(1999) Comparison of antagonist potencies at pre- and post-synaptic GABA_B receptors at inhibitory synapses in the CA1 region of the rat hippocampus. Br J Pharmacol 127:211–219.
OpenUrl CrossRef PubMed
↵
1. Price GW,
2. Kelly JS, and
3. Bowery NG
(1987) The location of GABA_B receptor binding sites in mammalian spinal cord. Synapse 1:530–538.
OpenUrl CrossRef PubMed
↵
1. Princivalle A,
2. Spreafico R,
3. Bowery N, and
4. de Curtis M
(2000) Layer-specific immunocytochemical localization of GABA_BR1a and GABA_BR1b receptors in the rat piriform cortex. Eur J Neurosci 12:1516–1520.
OpenUrl CrossRef PubMed
↵
1. Princivalle AP,
2. Pangalos MN,
3. Bowery NG, and
4. Spreafico R
(2001) Distribution of GABA_B(1a), GABA_B(1b) and GABA_B2 receptor protein in cerebral cortex and thalamus of adult rats. Neuroreport 12:591–595.
OpenUrl CrossRef PubMed
↵
1. Prosser HM,
2. Gill CH,
3. Hirst WD,
4. Grau E,
5. Robbins M,
6. Calver A,
7. Soffin EM,
8. Farmer CE,
9. Lanneau C,
10. Gray J,
11. et al.
(2001) Epileptogenesis and enhanced prepulse inhibition in GABA_B1-deficient mice. Mol Cell Neurosci 10:1–10.
OpenUrl CrossRef
↵
1. Przesmycki K,
2. Dzieciuch JA,
3. Czuczwar SJ, and
4. Kleinrok Z
(1998) An isobolographic analysis of drug interaction between intrathecal clonidine and baclofen in the formalin test in rats. Neuropharmacology 37:207–214.
OpenUrl CrossRef PubMed
↵
1. Raiteri M,
2. Bonanno G,
3. Paudice P,
4. Cavazzini P, and
5. Schmid G
(1996) Human brain cholecystokinin release of cholecystokinin-like immunoreactivity (CCK-LI) from isolated cortical nerve endings and its modulation through GABA_B receptors. J Pharmacol Exp Ther 228:747–751.
OpenUrl
↵
1. Raiteri M,
2. Pellegrini G,
3. Cantoni C, and
4. Bonanno G
(1989) A novel type of GABA receptor in rat spinal cord. Naunyn-Schmiedeberg's Arch Pharmacol 340:666–670.
OpenUrl CrossRef PubMed
↵
1. Richards DA and
2. Bowery NG
(1996) Anti-seizure effects of the GABA_B antagonist, SCH-50911, in the genetic absence epilepsy rat from Strasbourg (GAERS). Pharmacol Rev Commun 8:227–230.
OpenUrl
↵
1. Riley RC,
2. Trafton JA,
3. Chi SI, and
4. Basbaum AI
(2001) Presynaptic regulation of spinal cord tachykinin signaling via GABA_B but not GABA_A receptor activation. Neuroscience 103:725–737.
OpenUrl CrossRef PubMed
↵
1. Roberts DCS and
2. Andrews MM
(1997) Baclofen suppression of cocaine self-administration: demonstration using a discrete trials procedure. Psychopharmacology 131:271–277.
OpenUrl CrossRef PubMed
↵
1. Saha N,
2. Chugh Y,
3. Sankaranaryanan A, and
4. Sharma PL
(1993) Effects of post-training administration of (−)-baclofen and chlordiazepoxide on memory retention in ICRC Swiss mice: interactions with GABA_A and GABA_B receptor antagonists. Pharmacol Toxicol 72:159–162.
OpenUrl PubMed
↵
1. Saint DA,
2. Thomas T, and
3. Gage PW
(1990) GABA_B agonists modulate a transient potassium current in cultured mammalian hippocampal neurons. Neurosci Lett 118:9–13.
OpenUrl CrossRef PubMed
↵
1. Sandyk R and
2. Gillman MA
(1985) Baclofen-induced memory impairment. Clin Neuropharmacol 8:294–295.
OpenUrl CrossRef PubMed
↵
1. Santos AE,
2. Carvalho CM,
3. Macedo TA, and
4. Carvalho AP
(1995) Regulation of intracellular [Ca²⁺] and GABA release by presynaptic GABA_B receptors in rat cerebrocortical synaptosomes. Neurochem Int 27:397–406.
OpenUrl CrossRef PubMed
↵
1. Sawynok J and
2. Dickson C
(1985) D-Baclofen is an antagonist at baclofen receptors mediating antinociception in the spinal cord. Pharmacology 31:248–259.
OpenUrl PubMed
↵
1. Schuler V,
2. Lüscher C,
3. Blanchet C,
4. Klix N,
5. Sansig G,
6. Klebs K,
7. Schmutz M,
8. Heid J,
9. Gentry C,
10. Urban L,
11. et al.
(2001) Epilepsy, hyperalgesia, impaired memory and loss of pre-and postsynaptic GABA_B responses in mice lacking GABA_B(1). Neuron 31:47–58.
OpenUrl CrossRef PubMed
1. Schulz S and
2. Hollt V
(1998) Opioid withdrawal activates MAPkinase in locus coeruleus neurons in morphine dependent rats in vivo. Eur J Neurosci 10:1196–1201.
OpenUrl CrossRef PubMed
↵
1. Schwarz DA,
2. Barry G,
3. Eliasof SD,
4. Petroski RE,
5. Conlon PJ, and
6. Maki RA
(2000) Characterization of gamma-aminobutyric acid receptor GABA_B(1e), a GABA_B(1) splice variant encoding a truncated receptor. J Biol Chem 275:32174–32181.
OpenUrl Abstract/FREE Full Text
↵
1. Scott RH,
2. Wootton JF, and
3. Dolphin AC
(1990) Modulation of neuronal T-type calcium channel currents by photoactivation of intracellular guanosine 5′-O(3-thio) triphosphate. Neuroscience 38:285–294.
OpenUrl CrossRef PubMed
↵
1. Seitz RJ,
2. Blank B,
3. Kiwit JCW, and
4. Benecke R
(1995) Stiff-person syndrome with anti-glutamic acid decarboxylase autoantibodies: complete remission of symptoms after intrathecal baclofen administration. J Neurol 242:618–622.
OpenUrl CrossRef PubMed
↵
1. Serrano I,
2. Ruiz RM,
3. Serrano JS, and
4. Fernandez A
(1992) GABAergic and cholinergic mediation in the antinociceptive action of homotaurine. Gen Pharmacol 23:421–426.
OpenUrl PubMed
↵
1. Sharma AC and
2. Kulkarni SK
(1990) Evidence for GABA-BZ receptor modulation in short-term memory passive avoidance task paradigm in mice. Meth Find Exp Clin Pharmacol 12:175–180.
OpenUrl PubMed
↵
1. Sharma AC and
2. Kulkarni SK
(1993) (±)Baclofen sensitive scopolamine-induced short-term memory deficits in mice. Indian J Exp Biol 31:348–352.
OpenUrl PubMed
↵
1. Shen W and
2. Slaughter MM
(1999) Metabotropic GABA receptors facilitate L-type and inhibit N-type calcium channels in single salamander retinal neurons. J Physiol 516:711–718.
OpenUrl CrossRef PubMed
↵
1. Shoaib M,
2. Swanner LS,
3. Beyer CE,
4. Goldberg SR, and
5. Schindler CW
(1998) The GABA_B agonist baclofen modifies cocaine self-administration in rats. Behav Pharmacol 9:195–206.
OpenUrl PubMed
↵
1. Sidel ES,
2. Tilson HA,
3. McLamb RL,
4. Wilson WA, and
5. Swartzwelder HS
(1988) Potential interactions between GABAb and cholinergic systems: baclofen augments scopolamine-induced performance deficits in the eight-arm radial maze. Psychopharmacology 96:116–120.
OpenUrl CrossRef PubMed
↵
1. Sloviter RS,
2. Ali-Akbarian L,
3. Elliott RC,
4. Bowery BJ, and
5. Bowery NG
(1999) Localization of GABA_B (R1) receptors in the rat hippocampus by immunocytochemistry and high resolution autoradiography, with specific reference to its localization in identified hippocampal interneuron subpopulations. Neuropharmacology 38:1707–1721.
OpenUrl CrossRef PubMed
↵
1. Smid SD and
2. Blackshaw LA
(2000) Vagal neurotransmission to the ferret lower oesophageal sphincter: inhibition via GABA_B receptors. Br J Pharmacol 131:624–630.
OpenUrl CrossRef PubMed
↵
1. Smith GD,
2. Harrison SM,
3. Birch PJ,
4. Elliott PJ,
5. Malcangio M, and
6. Bowery NG
(1994) Increased sensitivity to the antinociceptive activity of (±)-baclofen in an animal model of chronic neuropathic, but not chronic inflammatory hyperalgesia. Neuropharmacology 33:1103–1108.
OpenUrl CrossRef PubMed
↵
1. Snead OC
(1992) Evidence for GABA_B-mediated mechanisms in experimental generalized absence seizures.