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Meeting ReportBasic and Translational Neurosciences

Identification and Preclinical Development of a Radiofluorinated Probe for Imaging the Muscarinic Acetylcholine Receptor M4 by Positron Emission Tomography

Ahmed Haider, Xiaoyun Deng, Olivia Mastromihalis, Stefanie Pfister, Troels Jeppesen, Zhiwei Xiao, Vi Pham, Jian Rong, Chunyu Zhao, Jiahui Chen, Yinlong Li, Tessa Connors, April Davenport, James Daunais, Wenqing Ran, Arthur Christopoulos, Lu Wang, Celine Valant and Steven Liang
Journal of Nuclear Medicine August 2022, 63 (supplement 2) 2968;
Ahmed Haider
1Harvard Medical School
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Xiaoyun Deng
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Olivia Mastromihalis
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Stefanie Pfister
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Troels Jeppesen
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Zhiwei Xiao
2Massachusetts General Hospital
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Vi Pham
3Monash University
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Jian Rong
2Massachusetts General Hospital
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Chunyu Zhao
2Massachusetts General Hospital
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Jiahui Chen
2Massachusetts General Hospital
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Yinlong Li
2Massachusetts General Hospital
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Tessa Connors
2Massachusetts General Hospital
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April Davenport
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James Daunais
4Wake Forest School of Medicine
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Wenqing Ran
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Arthur Christopoulos
3Monash University
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Lu Wang
5The first affiliated hospital of Jinan University
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Celine Valant
6Drug Discovery Biology
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Steven Liang
7Harvard Medical School and Mass General Hospital
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Abstract

2968

Introduction: An accumulating body of evidence suggests that the muscarinic acetylcholine receptor 4 (M4) is implicated in schizophrenia and dementia with Lewy body. Of note, previous studies revealed that M4 is markedly expressed in the brain, with high abundancies in the striatum and thalamus. Strenuous research efforts prompted the discovery of several M4 agonists, however, they have not yet reached advanced clinical stages, at least in part, due to the lack of a clinically validated M4-targeted probe. As such, we envisioned the development of a suitable M4 PET ligand that allows the visualization of M4 in vitro and in vivo.

Methods: Structure-activity relationship studies of pyrazol-4-yl-pyridine derivates prompted the discovery of target compound 2, a positive allosteric modulator (PAM) of M4. The radiofluorinated analogue, [18F]2, was challenged by in vitro autoradiography on mouse, rat, non-human primate (NHP) and human brain sections. To assess the effect of orthosteric ligand binding on the binding attributes of [18F]2, we performed all autoradiographic studies either in the presence or in the absence of the commercially available orthosteric agonist, carbachol. PET imaging was conducted in NHPs.

Results: Initial in vitro autoradiograms on rodent brain sections were performed in the absence of carbachol and showed only marginal specificity and a low selectivity of [18F]2 for the M4-expressing striatum. Nonetheless, upon addition of carbachol, a substantially higher tracer binding was observed in the rat striatum, which was significantly reduced under blocking conditions (Figure 1), suggesting that orthosteric ligand interaction is essential for efficient binding of [18F]2 to the allosteric binding site. Similar observations were made on autoradiograms of mouse brain sections. Notably, the presence of carbachol did not further improve the specificity and selectivity of [18F]2 in brain sections of NHPs and humans. In conclusion, these findings revealed significant species-differences with regard to the effects of orthosteric ligand binding on the tracer performance characteristics and paved the way for a preliminary PET study in NHPs, where brain uptake of [18F]2 was highest in the putamen and in cortical regions with known M4 expression.

Conclusions: We report on the identification and preclinical development of the first radiofluorinated M4 PET radioligand with promising in vitro and in vivo performance characteristics. Indeed, specificity and selectivity were demonstrated across different species by in vitro autoradiography on mouse, rat, NHP and human brain sections. PET imaging in NHP showed highest tracer uptake in brain regions with known M4 expression. The availability of a clinically validated M4 PET radioligand holds promise to provide a useful diagnostic tool for non-invasive imaging, thereby facilitating the clinical development of M4-targeted drugs in the pipeline.

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Journal of Nuclear Medicine
Vol. 63, Issue supplement 2
August 1, 2022
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Identification and Preclinical Development of a Radiofluorinated Probe for Imaging the Muscarinic Acetylcholine Receptor M4 by Positron Emission Tomography
Ahmed Haider, Xiaoyun Deng, Olivia Mastromihalis, Stefanie Pfister, Troels Jeppesen, Zhiwei Xiao, Vi Pham, Jian Rong, Chunyu Zhao, Jiahui Chen, Yinlong Li, Tessa Connors, April Davenport, James Daunais, Wenqing Ran, Arthur Christopoulos, Lu Wang, Celine Valant, Steven Liang
Journal of Nuclear Medicine Aug 2022, 63 (supplement 2) 2968;

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Identification and Preclinical Development of a Radiofluorinated Probe for Imaging the Muscarinic Acetylcholine Receptor M4 by Positron Emission Tomography
Ahmed Haider, Xiaoyun Deng, Olivia Mastromihalis, Stefanie Pfister, Troels Jeppesen, Zhiwei Xiao, Vi Pham, Jian Rong, Chunyu Zhao, Jiahui Chen, Yinlong Li, Tessa Connors, April Davenport, James Daunais, Wenqing Ran, Arthur Christopoulos, Lu Wang, Celine Valant, Steven Liang
Journal of Nuclear Medicine Aug 2022, 63 (supplement 2) 2968;
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