Different GABA
            <sub>A</sub>
            receptor subtypes mediate the anxiolytic, abuse-related, and motor effects of benzodiazepine-like drugs in primates

Rowlett, James K.; Platt, Donna M.; Lelas, Snjezana; Atack, John; Dawson, Gerard R.

doi:10.1073/pnas.0405621102

Cited by 189 publications

(219 citation statements)

References 15 publications

Supporting

Mentioning

192

Contrasting

Unclassified

Order By: Relevance

“…Expanding on our previous findings with the a1-sparing compound L-838,417 (Rowlett et al, 2005), we show that a1-sparing compounds with varying pharmacodynamic and pharmacokinetic profiles can have reinforcing effects in rhesus monkeys. However, self-administration of a1-sparing compounds appears to depend critically on baseline conditions, as all compounds tested had reinforcing effects in monkeys experienced primarily with midazolam, but not in monkeys experienced primarily with cocaine.…”

Section: Discussionsupporting

confidence: 73%

“…Moreover, mice with point mutations rendering the a1GABA A receptor insensitive to benzodiazepines did not show a preference for oral midazolam vs sucrose solutions, in contrast to wild-type mice (Tan et al, 2010). We have shown, however, that the a1-sparing compound, L-838,417, was reliably self-administered by rhesus monkeys (Rowlett et al, 2005), a finding clearly inconsistent with the hypothesis that a1GABA A receptors mediate the reinforcing effects of benzodiazepines.…”

Section: Introductioncontrasting

confidence: 76%

“…drug injection (Rowlett et al, 2005;Rowlett and Lelas, 2007). Previously, the monkeys in the midazolam baseline group had received single-day tests with other benzodiazepines (clonazepam, diazepam, alprazolam, triazolam) over an approximately 6-month period (unpublished).…”

Section: Subjects Surgery and Designmentioning

confidence: 99%

“…A possibility is the differences in the pharmacological profiles of the two compounds: TPA023 has notably lower intrinsic efficacy in vitro (measured via Cl-conductance in cloned human receptor subtypes) than L-838,417, with the highest efficacy for TPA023 at a3GABA A receptors whereas L-838 417 is equi-effective at a2GABA A , a3 GABA A , and a5GABA A receptors, raising the possibility that differences in levels of intrinsic efficacy could be key factors mediating selfadministration (for reviews, see Licata and Rowlett, 2008;Atack, 2011). Moreover, TPA023 likely has a relatively long duration of action (Atack et al, 2006Ator et al, 2010) while that of L-838 417 is shorter (Rowlett et al, 2005;Licata et al, 2010;J.R. Atack, unpublished data).…”

Section: Introductionmentioning

confidence: 99%

“…Although there are several differences between the studies of Ator et al (2010) and Rowlett et al (2005), one potentially important difference is training/maintenance drug (cocaine vs methohexital). Drug history, including the type of drug used for self-administration training, has been shown to be a major determinant of the reinforcing effects of benzodiazepines (Nelson et al, 1983;Bergman and Johanson, 1985;Falk and Tang, 1989).…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Shinday

Sawyer

Fischer

et al. 2012

Neuropsychopharmacol

View full text Add to dashboard Cite

Benzodiazepines are prescribed widely but their utility is limited by unwanted side effects, including abuse potential. The mechanisms underlying the abuse-related effects of benzodiazepines are not well understood, although a1 subunit-containing GABA A receptors have been proposed to have a critical role. Here, we examine the reinforcing effects of several compounds that vary with respect to intrinsic efficacy at a2, a3, and a5 subunit-containing GABA A receptors but lack efficacy at a1 subunit-containing GABA A receptors ('a1-sparing compounds'): MRK-623 (functional selectivity for a2/a3 subunit-containing receptors), TPA023B (functional selectivity for a2/a3/a5 subunit-containing receptors), and TP003 (functional selectivity for a3 subunit-containing receptors). The reinforcing effects of the a1-sparing compounds were compared with those of the non-selective benzodiazepine receptor partial agonist MRK-696, and non-selective benzodiazepine receptor full agonists, midazolam and lorazepam, in rhesus monkeys trained to self-administer midazolam or cocaine, under a progressive-ratio schedule of intravenous (i.v.) drug injection. The a1-sparing compounds were self-administered significantly above vehicle levels in monkeys maintained under a midazolam baseline, but not under a cocaine baseline over the dose ranges tested. Importantly, TP003 had significant reinforcing effects, albeit at lower levels of self-administration than non-selective benzodiazepine receptor agonists. Together, these results suggest that a1 subunit-containing GABA A receptors may have a role in the reinforcing effects of benzodiazepine-type compounds in monkeys with a history of stimulant self-administration, whereas a3 subunit-containing GABA A receptors may be important mediators of the reinforcing effects of benzodiazepine-type compounds in animals with a history of sedative-anxiolytic/benzodiazepine self-administration.

show abstract

Section: Discussionsupporting

confidence: 73%

Section: Introductioncontrasting

confidence: 76%

Section: Subjects Surgery and Designmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Shinday

Sawyer

Fischer

et al. 2012

Neuropsychopharmacol

View full text Add to dashboard Cite

show abstract

Neurobiology of Anxiety

Tóth

Zupan

2007

Handbook of Contemporary Neuropharmacology

View full text Add to dashboard Cite

Anxiety/fear is a normal reaction to threatening situations and it represents a physiologically protective function. Anxiety/fear is often manifested as avoidance and is also characterized by overt sympathetic reactions. Pathological anxiety is a level of anxiety that is disproportionate to the threat and can be manifested even in the absence of threat. In clinical practice, categorical systems set the boundary at which a particular level of anxiety becomes an anxiety disorder. Although a genetic contribution to anxiety disorders has long been suspected, it is only recently that genetic polymorphisms in various neurotransmitter and neuromodulatory systems have been linked to anxiety disorders. Still, the contribution of these factors is relatively small to the overall disease phenotype and the complex interaction between genetic factors and the environment will ultimately explain the development of susceptibility to anxiety. Genetic and biochemical studies, combined with the analysis of mouse strains with induced genetic mutations implicate multiple neurobiological processes in anxiety disorders. Although the association of neurotransmitters and their receptors with anxiety‐like behavior is not surprising, cytokines and cell adhesion molecules were also identified as modulators of anxiety. Furthermore, intracellular signaling pathways and their target genes were linked to anxiety allowing the assembly of specific “anxiety” pathways. It is apparent that anxiety‐related pathways and processes involve communication between various neurons that, via signaling pathways, eventually converge onto regulation of transcription and/or translation. The proper function of these pathways is especially crucial during early postnatal development and one can hypothesize that abnormalities in these pathways at any level lead to, via altered gene expression, to changes in neuronal morphology and/or function. Importantly, all commonly used anxiolytic drugs can be integrated into this model implying that anxiolytic drugs target and modulate the molecular and cellular pathways which establish and/or control the level of anxiety.

show abstract

Dopaminergic and GABAergic Regulation of Alcohol‐Motivated Behaviors: Novel Neuroanatomical Substrates

June

Eiler

2007

Handbook of Contemporary Neuropharmacology

View full text Add to dashboard Cite

show abstract

Different GABA _A receptor subtypes mediate the anxiolytic, abuse-related, and motor effects of benzodiazepine-like drugs in primates

Cited by 189 publications

References 15 publications

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Neurobiology of Anxiety

Dopaminergic and GABAergic Regulation of Alcohol‐Motivated Behaviors: Novel Neuroanatomical Substrates

Contact Info

Product

Resources

About

Different GABA A receptor subtypes mediate the anxiolytic, abuse-related, and motor effects of benzodiazepine-like drugs in primates

Cited by 189 publications

References 15 publications

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Reinforcing Effects Of Compounds Lacking Intrinsic Efficacy At α1 Subunit-Containing GABAA Receptor Subtypes in Midazolam- But Not Cocaine-Experienced Rhesus Monkeys

Neurobiology of Anxiety

Dopaminergic and GABAergic Regulation of Alcohol‐Motivated Behaviors: Novel Neuroanatomical Substrates

Contact Info

Product

Resources

About

Different GABA _A receptor subtypes mediate the anxiolytic, abuse-related, and motor effects of benzodiazepine-like drugs in primates