Characterization of a CNS penetrant, selective M<sub>1</sub>muscarinic receptor agonist, 77‐LH‐28‐1

Langmead, Christopher J.; Austin, Nigel; Branch, Clive L.; Brown, Jon T.; Buchanan, Katherine A.; Davies, Ceri H.; Forbes, Ian J.; Fry, Victoria A. H.; Hagan, Jim J.; Herdon, Hugh J.; Jones, Gareth; Jeggo, Ross; Kew, James N.C.; Mazzali, Angelica; Melarange, R.A.; Patel, Nisha; Pardoe, Joanne; Randall, Andrew D.; Roberts, Claire; Roopun, Anita K.; Starr, Kathryn R.; Teriakidis, Adrianna; Wood, Martyn; Whittington, Miles A.; Wu, Zining; Watson, Jeannette M.

doi:10.1038/bjp.2008.152

Cited by 121 publications

(147 citation statements)

References 39 publications

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“…The apparent binding affinity (pK B ) for each agonist is summarized in Table 1. Consistent with previous reports, both AC-42 and 77-LH-28-1 are able to displace specific [ 3 H]NMS binding from M 2 and M 3 mACh receptors (Spalding et al, 2002;May et al, 2007;Langmead et al, 2008a) with 77-LH-28-1 and AC-42 apparent affinities at the M 2 subtype being comparable with those observed at the M 1 mACh receptor (Table 1).…”

supporting

confidence: 91%

“…Recent studies have reported actions of AC-42 and 77-LH-28-1 at non-M 1 mACh receptor subtypes (May et al, 2007;Langmead et al, 2008a). Here, we have shown that both allosteric agonists can displace specific [ 3 H]NMS binding to the M 2 and M 3 mACh receptors (Table 1).…”

Section: Determination Of Agonistsupporting

confidence: 59%

“…Here, we have shown that both allosteric agonists can displace specific [ 3 H]NMS binding to the M 2 and M 3 mACh receptors (Table 1). AC-42 and 77-LH-28-1 have been reported to act allosterically at the M 2 mACh receptor (May et al, 2007), but a similar mechanism of action has not been reported at the M 3 receptor (Langmead et al, 2008a). Oxo-M stimulated significant increases ERK1/2 phosphorylation (P Ͻ 0.001) via human M 1 , M 2 , and M 3 mACh receptor subtypes stably expressed in CHO cells (Fig.…”

Section: Determination Of Agonistmentioning

confidence: 78%

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Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Thomas¹,

Langmead²,

Wood³

et al. 2009

J Pharmacol Exp Ther

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A new class of subtype-selective muscarinic acetylcholine (mACh) receptor agonist that activates the receptor through interaction at a site distinct from the orthosteric acetylcholine binding site has been reported recently. Here, we have compared the effects of orthosteric (oxotremorine-M, arecoline, pilocarpine) and allostericagonists on M 1 mACh receptor internalization and downregulation, as well as functional coupling in a Chinese hamster ovary (CHO) cell line. In contrast to full and partial orthosteric agonists, which cause significant receptor internalization and down-regulation, prolonged exposure to AC-42 did not significantly alter either cell-surface or total cellular M 1 mACh receptor expression. 77-LH-28-1, an AC-42 homolog, did cause some receptor internalization, but not down-regulation. The presence of atropine completely prevented the orthosteric agonist-induced adaptive changes in receptor populations; however, in contrast, the copresence of atropine and AC-42 significantly increased both cell-surface receptor and total M 1 mACh receptor expression. Maximal phosphoinositide hydrolysis responses to the partial agonist arecoline were similar in CHO-M 1 cells pretreated for 24 h with either AC-42 or vehicle; in contrast, these responses were markedly reduced when cells were pretreated with oxotremorine-M or pilocarpine. These data indicate that, whereas AC-42 binding to the M 1 mACh receptor can initiate signal transduction, the AC-42-liganded receptor is resistant to the usual mechanisms regulating receptor internalization and down-regulation. In addition, our data suggest unusual interactions between allosteric agonists and orthosteric antagonists to regulate cell-surface and total cellular receptor expression. proteins and inhibition of adenylyl cyclase activity (Caulfield and Birdsall, 1998). The mACh receptors are widely distributed throughout the periphery and central nervous system, and have been implicated as potential therapeutic targets in an array of diseases, including chronic obstructive pulmonary disease, irritable bowel syndrome, Alzheimer's disease, and schizophrenia (see Eglen et al., 1999;Felder et al., 2000;Langmead et al., 2008b).A major obstacle in the development of successful cholinergic therapies has been the lack of mACh receptor subtypespecific ligands, and the potentially serious side-effect profile of agents that interact with multiple mACh receptor subtypes (Bymaster et al., 1998;Eglen et al., 1999;Bartolomeo

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supporting

confidence: 91%

Section: Determination Of Agonistsupporting

confidence: 59%

Section: Determination Of Agonistmentioning

confidence: 78%

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Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Thomas¹,

Langmead²,

Wood³

et al. 2009

J Pharmacol Exp Ther

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“…117 77-LH-28-1 (34, Figure 23), an M 1 mAChR-selective compound closely structurally related to the AC compounds, demonstrated agonistic behavior at rat hippocampal M 1 mAChRs in vitro and CNS penetration leading to the stimulation of rat hippocampal cell firing in vivo. 124 Furthermore, activation of M1 mAChRs by 77-LH-28-1 enhanced NMDA receptor activation in vitro, facilitating long-term potentiation. 125 Consistent with the interactions of AC-42, the mAChR orthosteric antagonists pirenzepine and scopolamine both produced a dextral displacement of the 77-LH-28-1 CRC; 124 however, 77-LH-28-1 has also been shown to compete with the prototypical muscarinic negative allosteric modulator C 7 /3-phth (at the NMS-occupied receptor), 115 adding weight to the theory that this scaffold interacts with portions of both orthosteric and allosteric sites on the M 1 mAChR.…”

Section: ■ M 1 Machr-selective Ligandsmentioning

confidence: 98%

Development of M₁ mAChR Allosteric and Bitopic Ligands: Prospective Therapeutics for the Treatment of Cognitive Deficits

Davie

Christopoulos

Scammells

2013

ACS Chem. Neurosci.

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Since the cholinergic hypothesis of memory dysfunction was first reported, extensive research efforts have focused on elucidating the mechanisms by which this intricate system contributes to the regulation of processes such as learning, memory, and higher executive function. Several cholinergic therapeutic targets for the treatment of cognitive deficits, psychotic symptoms, and the underlying pathophysiology of neurodegenerative disorders, such as Alzheimer's disease and schizophrenia, have since emerged. Clinically approved drugs now exist for some of these targets; however, they all may be considered suboptimal therapeutics in that they produce undesirable off-target activity leading to side effects, fail to address the wide variety of symptoms and underlying pathophysiology that characterize these disorders, and/or afford little to no therapeutic effect in subsets of patient populations. A promising target for which there are presently no approved therapies is the M 1 muscarinic acetylcholine receptor (M 1 mAChR). Despite avid investigation, development of agents that selectively activate this receptor via the orthosteric site has been hampered by the high sequence homology of the binding site between the five muscarinic receptor subtypes and the wide distribution of this receptor family in both the central nervous system (CNS) and the periphery. Hence, a plethora of ligands targeting less structurally conserved allosteric sites of the M 1 mAChR have been investigated. This Review aims to explain the rationale behind allosterically targeting the M 1 mAChR, comprehensively summarize and critically evaluate the M 1 mAChR allosteric ligand literature to date, highlight the challenges inherent in allosteric ligand investigation that are impeding their clinical advancement, and discuss potential methods for resolving these issues. KEYWORDS: M 1 mAChR, allosteric ligands, Alzheimer's disease, schizophrenia, cognitive deficits, memory T he muscarinic acetylcholine receptor (mAChR) family is a group of rhodopsin-like (Family A) G protein-coupled receptors (GPCRs) consisting of five distinct subtypes M 1 −M 5 . Activation of the M 1 , M 3 , and M 5 receptor subtypes primarily results in coupling to the G q/11 family of G proteins, activation of phospholipase C (PLC), release of inositol-1,4,5-trisphosphate (IP 3 ), and subsequent mobilization of intracellular calcium Ca 2+ . Activation of the M 2 and M 4 receptor subtypes primarily results in coupling to the G i/o family of G proteins, inhibition of adenylate cyclase (AC), reduction in cyclic AMP (cAMP), and a decrease in neurotransmitter release via the blockage of voltage-gated calcium channels (Figure 1). These pathways represent a generalized view of each receptor's coupling capacity, as all five subtypes couple to a broader range of G protein-and non-G protein-mediated signaling and regulatory pathways, 1 ultimately leading to the regulation of enzymes and neurotransmitters critical for intercellular chemical communication and biological function. In a ...

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“…TBPB promotes the processing of APP towards the non-amyloidogenic pathway, decreases Aβ production in vitro, and has been shown to improve cognition in animal models (122). 77-LH-28-1 is another potent, selective and CNS penetrant allosteric M1 agonist which was a structural analog of AC-42 that was reported to improve cognition in animal models (123) as did AC-260584 (124). However, it is unclear if any of these agents are being pursued for clinical development.…”

Section: Neurotransmitter-based Therapies Muscarinic Agonistsmentioning

confidence: 99%

Alzheimer’s Disease: Dawn of a New Era?

et al. 2017

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Alzheimer’s disease (AD) is an irreversible neurodegenerative disease characterized by a progressive decline in cognition and memory, leading to significant impairment in daily activities and ultimately death. It is the most common cause of dementia, the prevalence of which increases with age; however, age is not the only predisposing factor. The pathology of this cognitive impairing disease is still not completely understood, which has limited the development of valid therapeutic options. Recent years have witnessed a wide range of novel approaches to combat this disease, so that they greatly increased our understanding of the disease and of the unique drug development issues associated with this disease. In this paper, we provide a brief overview of the history, the clinical presentation and diagnosis, and we undertake a comprehensive review of the various approaches that have been brought to clinical trials in recent years, including immunotherapeutic approaches, tau-targeted strategies, neurotransmitter-based therapies, neurotropic and hematopoietic growth factors, and antioxidant therapies, trying to highlight the lessons learned from these approaches. This article is open to POST-PUBLICATION REVIEW. Registered readers (see “For Readers”) may comment by clicking on ABSTRACT on the issue’s contents page.

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Characterization of a CNS penetrant, selective M₁muscarinic receptor agonist, 77‐LH‐28‐1

Cited by 121 publications

References 39 publications

Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Development of M₁ mAChR Allosteric and Bitopic Ligands: Prospective Therapeutics for the Treatment of Cognitive Deficits

Alzheimer’s Disease: Dawn of a New Era?

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Characterization of a CNS penetrant, selective M1muscarinic receptor agonist, 77‐LH‐28‐1

Cited by 121 publications

References 39 publications

Contrasting Effects of Allosteric and Orthosteric Agonists on M1Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Contrasting Effects of Allosteric and Orthosteric Agonists on M1Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Development of M1 mAChR Allosteric and Bitopic Ligands: Prospective Therapeutics for the Treatment of Cognitive Deficits

Alzheimer’s Disease: Dawn of a New Era?

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Product

Resources

About

Characterization of a CNS penetrant, selective M₁muscarinic receptor agonist, 77‐LH‐28‐1

Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Contrasting Effects of Allosteric and Orthosteric Agonists on M₁Muscarinic Acetylcholine Receptor Internalization and Down-regulation

Development of M₁ mAChR Allosteric and Bitopic Ligands: Prospective Therapeutics for the Treatment of Cognitive Deficits