A novel derivative of xanomeline improved memory function in aged mice

Cui, Yihui; Wen, Shi Wu; Yin, Lei; An, Shuming; Jin, Jing; Deng, Shining; Cao, Xiaohua

doi:10.1007/s12264-008-0204-5

Cited by 11 publications

(7 citation statements)

References 23 publications

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“…Although there is substantial evidence that enhancing mAChR signaling can benefit recognition memory [17], the relative efficacy of VU0364572, BQCA and VU0152100 to improve recognition memory performance has yet to be investigated. The task to evaluate drug effects on memory was based on the rats' spontaneous preference for novel objects [18], involved little in terms of rule learning, and permitted each rat to be tested on all drug conditions.…”

Section: Introductionmentioning

confidence: 99%

Effects of Selective Activation of M1 and M4 Muscarinic Receptors on Object Recognition Memory Performance in Rats

Galloway¹,

Lebois

Shagarabi³

et al. 2014

Pharmacology

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Acetylcholine signaling through muscarinic receptors has been shown to benefit memory performance in some conditions, but pan-muscarinic activation also frequently leads to peripheral side effects. Drug therapies that selectively target M₁ or M₄ muscarinic receptors could potentially improve memory while minimizing side effects mediated by the other muscarinic receptor subtypes. The ability of three recently developed drugs that selectively activate M₁ or M₄ receptors to improve recognition memory was tested by giving Long-Evans rats subcutaneous injections of three different doses of the M₁ agonist VU0364572, the M₁ positive allosteric modulator BQCA or the M₄ positive allosteric modulator VU0152100 before performing an object recognition memory task. VU0364572 at 0.1 mg/kg, BQCA at 1.0 mg/kg and VU0152100 at 3.0 and 30.0 mg/kg improved the memory performance of rats that performed poorly at baseline, yet the improvements in memory performance were the most statistically robust for VU0152100 at 3.0 mg/kg. The results suggested that selective M₁ and M₄ receptor activation each improved memory but that the likelihood of obtaining behavioral efficacy at a given dose might vary between subjects even in healthy groups depending on baseline performance. These results also highlighted the potential of drug therapies that selectively target M₁ or M₄ receptors to improve memory performance in individuals with impaired memory.

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Section: Introductionmentioning

confidence: 99%

Effects of Selective Activation of M1 and M4 Muscarinic Receptors on Object Recognition Memory Performance in Rats

Galloway¹,

Lebois

Shagarabi³

et al. 2014

Pharmacology

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“…Xanomeline is a functionally-selective M1 and M4 muscarinic agonist that has been investigated as a potential pro-cognitive cholinergic stimulant in Alzheimer disease (Avery et al, 1997;Bodick et al, 1997;Cui et al, 2008;Si et al, 2010;Wang et al, 2011), as well as a putative antipsychotic agent, based on the hypothesis that the muscarinic system is involved in the pathogenesis of schizophrenia (Hyde and Crook, 2001;Lucas-Meunier et al, 2003;Mirza et al, 2003;NR et al, 2003;Sarter, 2005;Raedler et al, 2006;Lisman et al, 2008). The primary original contributions of this report are the demonstration that xanomeline acutely reduces functional connectivity in a widespread set of mouse brain networks and reverses the hyperconnectivity induced by PCP, but focally increasing connectivity in terminals of the mesolimbic pathway in both conditions.…”

Section: Discussionmentioning

confidence: 99%

“…An increasing body of preclinical and clinical evidence has highlighted a potential beneficial effect of cholinergic stimulation on brain disorders characterized by cognitive dysfunction or psychosis, including neurodegenerative conditions such as Alzheimer disease or neuropsychiatric diseases such as schizophrenia (Felder et al, 2018;Verma et al, 2018;Erskine et al, 2019). These properties have prompted clinical investigations into the use of this drug to improve cognitive function and behavioral disturbance in Alzheimer's disease patients, with encouraging results but dose-limiting peripheral cholinergic side effects (Avery et al, 1997;NC et al, 1997;Cui et al, 2008;Si et al, 2010;Wang et al, 2011;Melancon et al, 2013). Interestingly, a parallel set of clinical observations have linked recreational use of betel nut with fewer positive and negative symptoms in schizophrenia (Sullivan et al, 2000), a finding that has been linked to the observation of decreased M1/M4 mAChR density in the brains of schizophrenia patients (for review, see Scarr & Dean 2008).…”

Section: Introductionmentioning

confidence: 99%

The M1/M4 agonist xanomeline modulates functional connectivity and NMDAR antagonist-induced changes in the mouse brain

Montani

Canella

Schwarz

et al. 2020

Preprint

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Cholinergic drugs acting at M1/M4 muscarinic receptors hold promise for the treatment of symptoms associated with brain disorders characterized by cognitive impairment, mood disturbances or psychosis, such as Alzheimer's disease or schizophrenia. However, the brain-wide functional substrates engaged by muscarinic agonists remain poorly understood. Here we used a combination of pharmacological fMRI (phMRI), resting-state fMRI (rsfMRI) and resting-state quantitative EEG (qEEG) to investigate the effects of a behaviorally-active dose of M1/M4 agonist xanomeline on brain functional activity in the rodent brain. We investigated both the effects of xanomeline per se and its modulatory effects on signals elicited by the NMDA-receptor antagonists phencyclidine (PCP) and ketamine. We found that xanomeline induces robust and widespread BOLD signal phMRI amplitude increases and decreased high frequency qEEG spectral activity. rsfMRI mapping in the mouse revealed that xanomeline robustly decreased neocortical and striatal connectivity but induces focal increases in functional connectivity within the nucleus accumbens and basal forebrain. Notably, xanomeline pre-administration robustly attenuated both the cortico-limbic phMRI response and the fronto-hippocampal hyper-connectivity induced by PCP, enhanced PCP-modulated functional connectivity locally within the nucleus accumbens and basal forebrain, and reversed the gamma and high frequency qEEG power increases induced by ketamine. Collectively, these results show that xanomeline robustly induces both cholinergic-like neocortical activation and desynchronization of functional networks in the mammalian brain. These effects could serve as a translatable biomarker for future clinical investigations of muscarinic agents, and bear mechanistic relevance for the putative therapeutic effect of these class of compounds in brain disorders.

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“…In tests with rodents, it showed an improvement in memory and cognition;h owever,i tf ailed phase II clinical trials due to an umber of side effects generally of gastrointestinal nature.T hese effectsw ere possibly due to the simultaneous activation of both receptor subtypes. [96][97][98][99] In fact, this is an example of ac ase that has raised doubts about the importance of the quest for selectivity.T his is because Alt et al [100] have shown, in anotheri nvivo study,t hat selectivec ompounds,s pecifically those for the M1 receptor, also elicit the same side effects. That is, even compounds that interacts electively with the M1 receptor were found to show side effects similar to those of xanomeline, which interacts with the M1 andM 3r eceptors.…”

Section: M1 Muscarinic Receptorsmentioning

confidence: 99%

Allosteric Modulators of Potential Targets Related to Alzheimer's Disease: a Review

et al. 2019

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Among neurodegenerative disorders, Alzheimer's disease (AD) is the most common type of dementia, and there is an urgent need to discover new and efficacious forms of treatment for it. Pathological patterns of AD include cholinergic dysfunction, increased β‐amyloid (Aβ) peptide concentration, the appearance of neurofibrillary tangles, among others, all of which are strongly associated with specific biological targets. Interactions observed between these targets and potential drug candidates in AD most often occur by competitive mechanisms driven by orthosteric ligands that sometimes result in the production of side effects. In this context, the allosteric mechanism represents a key strategy; this can be regarded as the selective modulation of such targets by allosteric modulators in an advantageous manner, as this may decrease the likelihood of side effects. The purpose of this review is to present an overview of compounds that act as allosteric modulators of the main biological targets related to AD.

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A novel derivative of xanomeline improved memory function in aged mice

Cited by 11 publications

References 23 publications

Effects of Selective Activation of M<sub>1</sub> and M<sub>4</sub> Muscarinic Receptors on Object Recognition Memory Performance in Rats

Effects of Selective Activation of M<sub>1</sub> and M<sub>4</sub> Muscarinic Receptors on Object Recognition Memory Performance in Rats

The M1/M4 agonist xanomeline modulates functional connectivity and NMDAR antagonist-induced changes in the mouse brain

Allosteric Modulators of Potential Targets Related to Alzheimer's Disease: a Review

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