The influence of manipulations to alter ambient GABA concentrations on the hypnotic and immobilizing actions produced by sevoflurane, propofol, and midazolam
-
Add time:07/26/2019 Source:sciencedirect.com
Recent studies have suggested that extrasynaptic GABAA receptors, which contribute tonic conductance, are important targets for general anesthetics. We tested the hypothesis that manipulations designed to alter ambient GABA concentrations (tonic conductance) would affect hypnotic (as indicated by loss of righting reflex, LORR) and immobilizing (as indicated by loss of tail-pinch withdrawal reflex, LTWR) actions of sevoflurane, propofol, and midazolam. Two manipulations studied were 1) the genetic absence of glutamate decarboxylase (GAD) 65 gene (GAD65−/−), which purportedly reduced ambient GABA concentrations, and 2) the pharmacological manipulation of GABA uptake using GABA transporter inhibitor (NO-711). The influence of these manipulations on cellular and behavioral responses to the anesthetics was studied using behavioral and electrophysiological assays. HPLC revealed that GABA levels in GAD65−/− mice were reduced in the brain (76.7% of WT) and spinal cord (68.5% of WT). GAD65−/− mice showed a significant reduction in the duration of LORR and LTWR produced by propofol and midazolam, but not sevoflurane. NO-711 (3 mg/kg, ip) enhanced the duration of LORR and LTWR by propofol and midazolam, but not sevoflurane. Patch-clamp recordings revealed that sevoflurane (0.23 mM) slightly enhanced the amplitude of tonic GABA current in the frontal cortical neurons; however, these effects were not strong enough to alter discharge properties of cortical neurons. These results demonstrate that ambient GABA concentration is an important determinant of the hypnotic and immobilizing actions of propofol and midazolam in mice, whereas manipulations of ambient GABA concentrations minimally alter cellular and behavioral responses to sevoflurane.
We also recommend Trading Suppliers and Manufacturers of 4-Amino Propofol Hydrochloride (cas 100251-91-0). Pls Click Website Link as below: cas 100251-91-0 suppliers
Prev:α Subunit isoform influences GABAA receptor modulation by propofol
Next:Structure–activity relationships of novel P2-receptor antagonists structurally related to Reactive Blue 2) - 【Back】【Close 】【Print】【Add to favorite 】
- Related Information
- α Subunit isoform influences GABAA receptor modulation by propofol07/25/2019
- Effects of ketamine and propofol on inflammatory responses of primary glial cell cultures stimulated with lipopolysaccharide07/24/2019
- Interactions between opioid drugs and propofol in laboratory models of seizures07/23/2019
- Highly water-soluble derivatives of the anesthetic agent propofol: in vitro and in vivo evaluation of cyclic amino acid esters07/22/2019
- Distinct actions of etomidate and propofol at β3-containing γ-aminobutyric acid type A receptors07/20/2019
- Reduced emergence agitation with proparacaine hydrochloride eye drops after general anaesthesia for paediatric strabismus surgery07/21/2019
- Propofol Protects Rat Hypoglossal Motoneurons in an In Vitro Model of Excitotoxicity by Boosting GABAergic Inhibition and Reducing Oxidative Stress07/19/2019
- Effects of propofol and sevoflurane on aquaporin-4 and aquaporin-9 expression in patients performed gliomas resection07/18/2019
- Neurotoxicity of propofol on rat hypoglossal motoneurons in vitro07/17/2019
