Galantamine is an allosterically potentiating ligand of the human α4/β2 nAChR

Samochocki, Marek; Zerlin, Marion; Jostock, Ruth; Kormelink, Paul J Groot; Luyten, Walter; Albuquerque, Edson X.; Maelicke, Alfred

doi:10.1034/j.1600-0404.2000.00310.x

Cited by 130 publications

(116 citation statements)

References 30 publications

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“…al., 1985) was the finding that physostigmine-induced inhibition of ␣4␤4 and ␣4␤2 nAChR activity was voltage dependent . As we have shown previously for galantamine (Schrattenholz et al, 1996;Samochocki et al, 2000), physostigmineinduced potentiation of nAChR activity was only evident at subsaturating concentrations of classical agonists . Based on the finding that the potentiating effect of physostigmine faded away as the agonist concentration was increased and that physostigmine displaced the binding of the classical nicotinic agonist epibatidine from ␣4␤4 nAChRs ectopically expressed in oocytes, Zwart and collaborators (2000) concluded that the potentiating action of physostigmine is the result of its interaction with the ACh-recognition sites on the nAChRs.…”

Section: Exogenous Unconventional Nachr Ligands That Modulate Receptsupporting

confidence: 80%

“…These effects can be detected as early as 30 s after beginning the perfusion of the slices with galantamine-containing artificial cerebrospinal fluid (ACSF). In contrast, cholinesterase inhibitors devoid of nicotinic APL action, including methamidophos, donepezil, and rivastigimine (Samochocki et al, 2000), cause no significant changes in evoked EPSCs or IPSCs in hippocampal slices (Santos et al, 2002). Numerous lines of evidence demonstrated that facilitation of glutamatergic and GABAergic transmissions by galantamine cannot be accounted for by changes in the electrical properties of the neurons or in the activity of postsynaptic glutamate or GABA A receptors.…”

Section: Therapeutic Significance Of Nicotinic Aplsmentioning

confidence: 99%

“…Although the exact mechanism by which nicotinic APLs sensitize nAChRs to activation by classical agonists is still unclear, studies from our laboratories have indicated that nicotinic APLs can increase the probability of nAChR channel openings induced by ACh in outside-out patches excised from PC12 cells and enhance the apparent potency, but not the efficacy of nicotinic agonists in activating different nAChR subtypes (Storch et al, 1995;Samochocki et al, 2000). These results support the notion that APLs enhance the binding affinity of agonists and/or frequency of channel openings for a given level of receptor occupancy as long as receptor activation is still submaximal.…”

Section: Exogenous Unconventional Nachr Ligands That Modulate Receptmentioning

confidence: 99%

“…In fact, the highly potent cholinesterase inhibitors donepezil and rivastigmine are devoid of the nicotinic APL action (Samochocki et al, 2000). Some structural requirements seem to be essential in a compound that acts as a nicotinic APL.…”

Section: Exogenous Unconventional Nachr Ligands That Modulate Receptmentioning

confidence: 99%

“…In both conditions, there is a bell-shaped concentration/ dose-response relationship that may be due to the fact that galantamine up to 1 M increases agonist-induced nAChR activation and reduces/prevents agonist-induced nAChR desensitization, whereas at higher concentrations it inhibits nAChR activation (Pereira et al, 1993;Schrattenholz et al, 1996;Samochocki et al, 2000). In addition, the brain concentration of galantamine achieved after treatment of rats with the most behaviorally active dose (2.5 mg/kg, p.o.)…”

Section: Therapeutic Significance Of Nicotinic Aplsmentioning

confidence: 99%

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Unconventional ligands and modulators of nicotinic receptors

et al. 2002

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ABSTRACT:Evidence gathered from epidemiologic and behavioral studies have indicated that neuronal nicotinic receptors (nAChRs) are intimately involved in the pathogenesis of a number of neurologic disorders, including Alzheimer's disease, Parkinson's disease, and schizophrenia. In the mammalian brain, neuronal nAChRs, in addition to mediating fast synaptic transmission, modulate fast synaptic transmission mediated by the major excitatory and inhibitory neurotransmitters glutamate and GABA, respectively. Of major interest, however, is the fact that the activity of the different subtypes of neuronal nAChR is also subject to modulation by substances of endogenous origin such as choline, the tryptophan metabolite kynurenic acid, neurosteroids, and ␤-amyloid peptides and by exogenous substances, including the so-called nicotinic allosteric potentiating ligands, of which galantamine is the prototype, and psychotomimetic drugs such as phencyclidine and ketamine. The present article reviews and discusses the effects of unconventional ligands on nAChR activity and briefly describes the potential benefits of using some of these compounds in the treatment of neuropathologic conditions in which nAChR function/expression is known to be altered.

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Section: Exogenous Unconventional Nachr Ligands That Modulate Receptsupporting

confidence: 80%

Section: Therapeutic Significance Of Nicotinic Aplsmentioning

confidence: 99%

Section: Exogenous Unconventional Nachr Ligands That Modulate Receptmentioning

confidence: 99%

Section: Exogenous Unconventional Nachr Ligands That Modulate Receptmentioning

confidence: 99%

Section: Therapeutic Significance Of Nicotinic Aplsmentioning

confidence: 99%

See 3 more Smart Citations

Unconventional ligands and modulators of nicotinic receptors

et al. 2002

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The Cognitive Benefits of Galantamine Are Sustained for at Least 36 Months

Raskind¹,

Peskind²,

Truyen³

et al. 2004

Arch Neurol

148

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Galantamin und die nikotinisch-cholinerge Neurotransmission: Neue Theorien!

Maelicke

Weichel

2002

Pharmazie in unserer Zeit

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Eines der klarsten neurochemischen Kennzeichen für die Alzheimer'sche Demenz ist die verringerte Zahl an nikotinischen Acetylcholinrezeptoren in Cortex und Hippokampus. Der Verlust an nAChRs ist dabei eng korreliert mit dem Verlust an kognitiver Hirnleistung und bietet sich daher als Ziel für eine Arzneimitteltherapie an. Von den möglichen Therapieansätzen haben sich weder eine Förderung der Synthese von Acetylcholin noch eine Behandlung mit nikotinischen oder muskarinischen Agonisten bewährt. Die Behandlung mit schwachen Hemmern der ersten Generation hat sich über kürzere Zeiträume bewährt, wobei die klinischen Verbesserungen jedoch nur moderater Art sind. Über längere Zeiträume verliert diese Therapie an Wirkung, möglicherweise, weil sie im wesentlichen symptomatischer und nicht ursächlicher Natur ist und die neurodegenerative Grunderkrankung nicht berührt. Ein neuer Ansatz, um direkt das nikotinisch‐cholinerge Defizit zu bekämpfen, ist die Verwendung von „allosterisch potenzierenden Liganden (APL)”︁ nikotinischer Rezeptoren. Die APL sensibilisieren sowohl die postsynaptischen wie auch die prä‐ und perisynaptischen nikotinischen Rezeptoren gegenüber dem natürlichen Transmitter Acetylcholin und bewirken so neben erhöhten elektrischen Reizantworten (Membrandepolarisation) auch erhöhte präsynaptische Transmitterausschüttung und Veränderungen der Genregulation, wobei sich letztere günstig auf die Zahl der nikotinischen Rezeptoren auswirken kann. Die Wirkungen auf prä‐ und perisynaptische nikotinische Rezeptoren ist dabei vermutlich von besonders großer Bedeutung, da diese Rezeptoren modulierend nicht nur auf die cholinerge, sondern auch auf andere Neurotransmissionssysteme wirken und so neben Lern‐ und Gedächtnisprozessen auch andere psychologische Verhaltensmuster bei der AD beeinflussen können. Galantamin ist ein besonders wirksamer nikotinischer APL. Außerdem wirkt es als schwacher reversibler Inhibitor der Acetylcholinesterase und hat somit einen dualen Wirkmechanismus. Zusammen mit seinen günstigen pharmakokinetischen Eigenschaften und sehr günstigem Nebenwirkungsprofil bietet sich Galantamin daher für die gezielte, auf Maximierung der Wirkung ausgelegte Behandlung des nikotinisch‐cholinergen Defizits bei der Alzheimer'schen Demenz an.

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Galantamine is an allosterically potentiating ligand of the human α4/β2 nAChR

Cited by 130 publications

References 30 publications

Unconventional ligands and modulators of nicotinic receptors

Unconventional ligands and modulators of nicotinic receptors

The Cognitive Benefits of Galantamine Are Sustained for at Least 36 Months

Galantamin und die nikotinisch-cholinerge Neurotransmission: Neue Theorien!

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