Effects of the novel compound aniracetam (Ro 13-5057) upon impaired learning and memory in rodents

Cumin, R.; Bandle, E.; Gamzu, Elkan; Haefely, W.

doi:10.1007/bf00432244

Cited by 222 publications

(73 citation statements)

References 40 publications

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“…According to Olpe et al (1986) 1 mm oxiracetam is ineffective on the evoked responses in CAI. Since other in vitro studies with similar compounds (Satoh et al, 1986; and behavioural work (Cumin et al, 1982) showed a bell-shaped dose-effect relation, our findings may indicate the need to avoid unduly large concentrations of nootropics as their actions tend to dissipate following high doses.…”

Section: Discussionmentioning

confidence: 60%

“…In spite of the fact that differences in the action of piracetam and related nootropic drugs in many behavioural tests are seemingly related only to the doses used (Cumin et al, 1982;Schindler et al, 1984), the few data available for the electrophysiological effects of these drugs on the hippocampus suggest a different site and/or mechanism of action for each compound. Piracetam, for instance, has been found to increase reversibly the amplitude of the population spike, without any effect on the dentritic field e.p.s.p.…”

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confidence: 99%

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Effect of the nootropic drug oxiracetam on field potentials of rat hippocampal slices

Pugliese

Corradetti

Ballerini

et al. 1990

British J Pharmacology

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1 The effect of the nootropic drug oxiracetam on hippocampal neurotransmission was investigated in the CAI region of the rat hippocampal slice in vitro by use of extracellular recordings.2 Superfusion of oxiracetam (0.1-1001iM) produced a concentration-dependent, wash-resistant (>90 min), increase in initial slope and amplitude of the dendritic field excitatory postsynaptic potential (e.p.s.p.). This increase was maximal at a concentration of 1 YM (70%). 3 Input-output curves relating the initial slope to the amplitude of the afferent volley were significantly (P < 0.05) steeper and showed a greater maximal response in the presence of 1 gM oxiracetam than in control conditions. 4 Two trains of high frequency stimulation (100 Hz, 0.4 s, 5 min apart) delivered in the stratum radiatum 30min after washout of oxiracetam (1 yM) still elicited a long-term potentiation (LTP) of the field e.p.s.p.However, the absolute magnitude of the LTP produced did not differ from that obtained in untreated slices.5 After induction and establishment of LTP, oxiracetam (1 yM) had a smaller (27%) and reversible effect on the evoked field e.p.s.p.6 D-2-Amino-5-phosphonopentanoic acid (AP-5), at the same concentration (50pM) which in our conditions prevented the induction of LTP, blocked the action of 1 yM oxiracetam and strongly depressed the effect of higher concentrations of the nootropic drug. 7 It is concluded that oxiracetam provokes an enduring increase of neurotransmission in the CAl rat hippocampal region. This action appears to share some features with LTP as indicated by its persistence, sensitivity to AP-5 and lack of additivity with electrically-induced LTP.

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Section: Discussionmentioning

confidence: 60%

mentioning

confidence: 99%

Effect of the nootropic drug oxiracetam on field potentials of rat hippocampal slices

Pugliese

Corradetti

Ballerini

et al. 1990

British J Pharmacology

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“…Although some differences exist for training to test (retention test) intervals among the three PAR-failure models except for scopolamine PAR-failure in rats, these pro cedures may be considered to cause re trograde amnesia by impairing the memory consolidation process (8) For comparison, Ca-hopantenate which has been claimed to be effective for senile mental disorders (9), cholinomimetic agents (physostigmine and choline chloride) and nootropic agents (piracetam and aniracetam), which have also been reported to have beneficial effects on memory or cerebral impairment disorders (10-13), were also examined. In the ECS-PAR failure test, the retention test was performed at either 3 or 24 hr after the training.…”

Section: Discussionmentioning

confidence: 99%

Effects of Bifemelane Hydrochloride (MCI-2016) on Experimental Amnesia (Passive Avoidance Failure) in Rodents

Tobe

Yamaguchi

Nagai

et al. 1985

Japanese Journal of Pharmacology

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“…This modification is induced via the aniracetam ability to bind to a putative allosteric site located in the extracellular loop between the TM3 and TM4 regions ofvarious molecular forms of AMPA receptors (18,19). It has been reported that aniracetam administered to rodents (20) and monkeys (16) antagonizes the cognition deficit induced by scopolamine, an acetylcholine muscarinic antagonist. Since aniracetam neither binds to nicotinic or muscarinic receptors nor inhibits acetylcholinesterases or high-affinity choline uptake, it has been considered an indirect cholinomimetic (21).…”

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confidence: 99%

“…However, in light of aniracetam's action on AMPA receptors, its reduction of scopolamine-induced amnesia could be attributed to the strengthening of the excitatory synaptic function linked to regulation of the cholinergic neurons that innervate neocortical and limbic structures (10). Although aniracetam and its congeners did not achieve a strong clinical endorsement because their action is weak and short lasting (22), these pyrrolidinone derivatives might nevertheless be viewed as prototypes of cognition enhancers that allosterically facilitate glutamatergic transmission without producing excitotoxicity or other adverse effects (5,23 (19,20,24), thereby allosterically facilitating AMPA receptor activity by inhibiting desensitization of glutamate-mediated synaptic transmission in hippocampus; the potency of IDRA 21 was found to be severalfold higher than that of aniracetam (24). Among various 1,2,4-benzothiadiazine derivatives that allosterically modulate AMPA cationic current in primary hippocampal neuronal cultures or in hippocampal slices (24,25), IDRA 21 given orally is the only known compound enhancing cognition in normal rats and potently antagonizing the cognition deficit elicited by the AMPA receptor antagonist 2,3-dihydro-6-nitro-7-sulfamoylbenzo(f)quinoxaline (NBQX) (10).…”

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confidence: 99%

7-Chloro-3-methyl-3,4-dihydro-2H-1,2,4-benzothiadiazine S,S-dioxide (IDRA 21), a congener of aniracetam, potently abates pharmacologically induced cognitive impairments in patas monkeys.

Thompson

Guidotti

Dibella

et al. 1995

Proc. Natl. Acad. Sci. U.S.A.

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We report here on the ability of IDRA 21 and aniracetam, two negative allosteric modulators of glutamateinduced DL-a-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptor desensitization, to attenuate alprazolam-induced learning deficit in patas monkeys working in a complex behavioral task. In one component of a multiple schedule (repeated acquisition or "learning"), patas monkeys acquired a different four-response chain each session by responding sequentially on three keys in the presence of four discriminative stimuli (geometric forms or numerals). In the other component (performance) the four-response chain was the same each session. In the central nervous system, y-aminobutyric acid (GABA) is the most important and abundant inhibitory neurotransmitter, acting at GABAA and GABAB receptors (1, 2). Glutamate is the most potent and abundant excitatory neurotransmitter, acting at ionotropic DL-a-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA)/kainate, N-methyl-Daspartate receptors, and on metabotropic receptors (3). Together these two neurotransmitters maintain a fragile balance between neuronal excitation and inhibition. Regulation of such balance establishes a time-related association of functional neuronal assemblies and changes the strength of neuronal circuits (i.e., long-term potentiation) underlying various forms of learning and memory processes (4, 5), thereby establishing functional neuronal maps in the neocortex and the limbic system attending cognitive and sensory-motor function expression (6-8). Drugs that up-regulate GABAergic or downregulate glutamatergic transmission in neocortical and limbic brain areas produce dramatic sensory-motor and learning impairments (9-13). For example, a facilitation of GABAergic transmission elicited at specific GABA receptors by benzodiazepines acting as full or selective positive allosteric modulators (i.e., alprazolam, triazolam, or diazepam) or an inhibition of glutamatergic transmission elicited by competitive and noncompetitive inhibitors of glutamate action at N-methyl-Daspartate receptors (phencyclidine, dizocilpine, etc.) reduces acquisition and retention in rodents and in human and nonhuman primates (9-13). These considerations are central to the working model that neuropharmacologists have recently adopted in order to develop animal models to evaluate potency and efficacy of cognition-enhancing drugs acting through neocortical or limbic glutamatergic or GABAergic neurons (5, 9, 10, 13).In the past several years in our and others' laboratories, attention has been focused on allosteric modulatory sites located on GABAergic and glutamatergic receptors that might be targets for the action of drugs (i.e., partial allosteric modulators) improving neurological or neuropsychiatric disorders, including learning and memory abnormalities, without or with minimal adverse side effects (1,5,9,(10)(11)(12)14).A role for the negative allosteric modulation of glutamateinduced AMPA receptor desensitization in long-term potentiation and cognition ...

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Effects of the novel compound aniracetam (Ro 13-5057) upon impaired learning and memory in rodents

Cited by 222 publications

References 40 publications

Effect of the nootropic drug oxiracetam on field potentials of rat hippocampal slices

Effect of the nootropic drug oxiracetam on field potentials of rat hippocampal slices

Effects of Bifemelane Hydrochloride (MCI-2016) on Experimental Amnesia (Passive Avoidance Failure) in Rodents

7-Chloro-3-methyl-3,4-dihydro-2H-1,2,4-benzothiadiazine S,S-dioxide (IDRA 21), a congener of aniracetam, potently abates pharmacologically induced cognitive impairments in patas monkeys.

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