Effects of acute subcutaneous nicotine on attention, information processing and short-term memory in alzheimer's disease

Jones, Gemma M. M.; Sahakian, Barbara J.; Levy, Raymond; Warburton, David M.; Gray, Jeffrey A.

doi:10.1007/bf02247426

Cited by 443 publications

(234 citation statements)

References 33 publications

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“…Although substantial loss of cholinergic neurons has been demonstrated in AD (Francis et al, 1999), post-mortem studies have shown that some functional nAChRs remain, even at a late stage of the disease (Shimohama et al, 1986;Whitehouse et al, 1986;Schroder et al, 1991;Court et al, 2001;Perry et al, 2001). In agreement with this observation, nicotine, the nonselective prototypical ligand for nAChRs, improves certain cognitive functions in AD patients (Jones et al, 1992;Wilson et al, 1995;White and Levin, 1999;Newhouse et al, 2001;Rezvani and Levin, 2001). Unfortunately, nicotine also exhibits a broad spectrum of undesirable side effects (Benowitz, 1986;Watkins et al, 2000), which limits its use as a therapy.…”

Section: Introductionmentioning

confidence: 95%

Cognitive Enhancing Properties and Tolerability of Cholinergic Agents in Mice: A Comparative Study of Nicotine, Donepezil, and SIB-1553A, a Subtype-Selective Ligand for Nicotinic Acetylcholine Receptors

Bontempi¹,

Whelan²,

Risbrough³

et al. 2003

Neuropsychopharmacol

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Several studies have demonstrated the importance of nicotinic mechanisms in the pathophysiology of neurodegenerative and cognitive disorders, warranting the search and development of novel nicotinic ligands as potential therapeutic agents. The present study was designed to assess whether the subtype-selective nicotinic acetylcholine receptor (nAChR) ligand SIB-1553A [( 7 )-4-{[2-(1-methyl-2-pyrrolidinyl)ethyl]thio}phenol hydrochloride], with predominant agonist activity at b4 subunit-containing human nAChRs, and no activity at muscle nAChR subtypes, could enhance cognitive performance in rodents with a more desirable safety/tolerability profile as compared to the nonselective prototypic nAChR ligand nicotine. SIB-1553A was equi-efficacious to nicotine in improving working memory performance in scopolamine-treated mice as measured by increased alternation in a T-maze, and was more efficacious than nicotine in improving the baseline cognitive performance of aged mice. This effect on working memory was confirmed in a delayed nonmatching to place task using the eight-arm radial maze. SIB-1553A produced dose-dependent side effects (ie motor deficits and seizures), although these effects were observed at doses 12 to 640-fold above those required to increase cognitive performance. Overall, SIB-1553A was significantly less potent than nicotine in eliciting these undesirable effects. Thus, the subtype-selective profile of SIB-1553A appears to translate into a more efficacious and better tolerated nAChR ligand as compared to nicotine. In the present studies, cognitive enhancement induced by SIB-1553A was similar in magnitude to that produced by the clinically efficacious acetylcholinesterase inhibitor donepezil. Taken together, the present data confirm the importance of nAChR subtypes in modulating cognitive processes, and suggest that activation of nAChR subtypes by selective nAChR ligands may be a viable approach to enhance cognitive performance.

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Section: Introductionmentioning

confidence: 95%

Cognitive Enhancing Properties and Tolerability of Cholinergic Agents in Mice: A Comparative Study of Nicotine, Donepezil, and SIB-1553A, a Subtype-Selective Ligand for Nicotinic Acetylcholine Receptors

Bontempi¹,

Whelan²,

Risbrough³

et al. 2003

Neuropsychopharmacol

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“…Nicotine administration may just be relieving withdrawal and correcting those deficits. However, if low-dose nicotine is administered to normal nonsmokers, thereby avoiding the confound of withdrawal, there is enhanced performance on the continuous performance test with decreased errors of omission without an increase in errors of commission [62] In Alzheimer's disease, where nicotinic cholinergic receptors are known to be decreased in the cortex and hippocampus [63,64], nicotine injections or nicotine skin patches significantly improve attention, learning and memory [65,66,67,68,69,70]. Similarly, in adults with attention deficit disorder, nicotine skin patch reduces clinical symptoms and increases reaction time, but does not improve errors of omission in the Continuous Performance Test [71].…”

Section: α7 In Learning and Memorymentioning

confidence: 99%

Treating schizophrenia symptoms with an α7 nicotinic agonist, from mice to men

Olincy

Stevens

2007

Biochemical Pharmacology

125

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Current antipsychotic treatments fail to fully address the range of symptoms of schizophrenia, particularly with respect to social and occupational dysfunctions. Recent work has highlighted the role of nicotinic in both cognitive and attentional deficits as well as deficient processing of repetitive sensory information. The predilection for schizophrenia patients to be extremely heavy cigarette smokers may be related to their attempt to compensate for a reduction in hippocampal α7 nicotinic cholinergic receptors by delivering exogenous ligand to the remaining receptors. Studies in rodent models of both learning and memory deficits and deficits in sensory inhibition have confirmed a role for α7 subtype of the nicotinic cholinergic receptors in these processes. Rodent studies also demonstrated the efficacy of a selective partial α7 nicotinic agonist, DMXBA, to improve these deficits. Subsequent human clinical trials demonstrated improved sensory inhibition in 12 schizophrenia patients and showed improvement in several subtests of the RBANS learning and memory assessment instrument. These data suggest that therapeutic agents selected for α7 nicotinic activity may have utility in treating certain symptoms of schizophrenia. KeywordsSchizophrenia; nicotinic receptors; DMXBA; P50 auditory evoked potential; cognitive deficits; nicotine Although the positive symptoms such as hallucinations and delusions of schizophrenia are partially treated with the available antipsychotic medications, social and occupational dysfunction remains a major issue in treating this disorder. Cognitive deficits have been identified as more closely related to ability to adequately function [1]. In the search for new and more effective therapeutic agents for schizophrenia, recent attention has turned the nicotinic cholinergic receptors system. α7 and P50 Auditory GatingPeople with schizophrenia, in addition to the cardinal symptoms of hallucinations and delusions, suffer from the inability to focus attention. This may stem from being overwhelmed

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“…The results of most studies reveal that smokers report alleviation of negative affect by smoking, (Brandon and Baker 1991) and increased anxiety during withdrawal. Nicotine also has a stimulant effect on cognitive processes, improving vigilance, enhancing selective attention, and promoting response inhibition to irrelevant stimuli (Jones et al 1992). …”

Section: Introductionmentioning

confidence: 99%

Fear-Potentiated Startle to Threat, and Prepulse Inhibition Among Young Adult Nonsmokers, Abstinent Smokers, and Nonabstinent Smokers

Grillon

Avenevoli

Daurignac

et al. 2007

Biological Psychiatry

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Effects of acute subcutaneous nicotine on attention, information processing and short-term memory in alzheimer's disease

Cited by 443 publications

References 33 publications

Cognitive Enhancing Properties and Tolerability of Cholinergic Agents in Mice: A Comparative Study of Nicotine, Donepezil, and SIB-1553A, a Subtype-Selective Ligand for Nicotinic Acetylcholine Receptors

Cognitive Enhancing Properties and Tolerability of Cholinergic Agents in Mice: A Comparative Study of Nicotine, Donepezil, and SIB-1553A, a Subtype-Selective Ligand for Nicotinic Acetylcholine Receptors

Treating schizophrenia symptoms with an α7 nicotinic agonist, from mice to men

Fear-Potentiated Startle to Threat, and Prepulse Inhibition Among Young Adult Nonsmokers, Abstinent Smokers, and Nonabstinent Smokers

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