Drug Derived Fluorescent Probes for the Specific Visualization of Cannabinoid Type 2 Receptor - A Toolbox Approach

Gazzi, Thais; Brennecke, Benjamin; Atz, Kenneth; Korn, Claudia; Sykes, David A.; Sarott, Roman C.; Westphal, Matthias V.; Pfaff, Patrick; Weise, Marie; Mostinski, Yelena; Hoare, Bradley L.; Miljuš, Tamara; Mexi, Maira; Guba, Wolfgang; Anker, André; Rufer, Arne C.; Kusznir, Eric A.; Huber, Sylwia; Raposo, Catarina; Zirwes, Elisabeth A.; Osterwald, Anja; Pavlovic, Anto; Moes, Svenja; Beck, Jennifer; Benito-Cuesta, Irene; Grande, Teresa; Drawnel, Faye; Widmer, Gabriella; Holzer, Daniela; Wel, Tom van der; Mandhair, Harpreet; Saroz, Yurii; Grimsey, Natasha L.; Honer, Michael; Fingerle, Jürgen; Gawrisch, Klaus; Romero, Julián; Hillard, Cecilia J.; McCormick, Peter J.; Varga, Zoltán V.; Stelt, Mario van der; Pacher, Pál; Gertsch, Jürg; Ullmer, Christoph; Oddi, Sergio; Maccarrone, Mauro; Veprintsev, Dmitry B.; Carreira, Erick M.; Grether, Uwe; Nazaré, Marc

doi:10.26434/chemrxiv.10283027.v1

Cited by 2 publications

(7 citation statements)

References 16 publications

(27 reference statements)

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“…In this study, we emulate a real‐time experiment described by Thais et al (2019). In their work, they explore ligand receptor binding for SiR‐6 at the cannabinoid 2 receptor (CB 2 ).…”

Section: Methodsmentioning

confidence: 99%

“…The workflow of this approach is shown in Figure 2. First, we chose a set of parameter values and random effects that reflect those from the real‐world experiment referred to above (Thais et al, 2019). Second, we propose several experimental designs to be tested, each with varying characteristics, including group sizes ( n ).…”

Section: Methodsmentioning

confidence: 99%

“…We use the parameters derived from the binding experiments of the CB 2 receptor as the template (Thais et al, 2019), shown in Table 1. In addition, we included random error associated with the observations that represents error from sources such as operator error and measurement error.…”

Section: Methodsmentioning

confidence: 99%

“…The right panel is the classical equilibrium concentration–effect curve, which only use the last time points of the real‐time assay, which are then fitted with an E max model. The data presented here are simulated and are based on the study of Thais et al (2019). The error bar in figure here is the standard error of the simulated data (10% proportional error and 1 additive error as stated in Table 1)…”

Section: Introductionmentioning

confidence: 99%

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Exploring group size for statistical analysis of real‐time signalling experiments

Yang

Zhu

Finlay

et al. 2021

British J Pharmacology

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Background and Purpose Classical pharmacological bioassays generally use observed effects from a concentration series, at a single equilibrium time point to construct a concentration–effect curve, representing one experiment. However, if the full kinetic profile of the effect data for each concentration was evaluated simultaneously, then the analysis would be more powerful. In this work, we explore if more precise parameters can be achieved by using the full kinetic method. Experimental Approach We used a simulation estimation study to explore the influence of kinetic analysis on the precision of the Emax model parameter estimates (Emax and C50). We compared a full kinetic approach in which all effect versus time data from a theoretical real‐time signalling experiment were analysed simultaneously with a ‘reference’ approach. The theoretical real‐time signalling experiment was based on a previously published CB2 receptor‐binding experiment. Key Results The reference method with a group size (n) of 5 provided highly precise parameter estimates (coefficient of variation [CV] 3.4% for Emax and 0.72% for C50). A full kinetic method provided more precise estimates than the reference with equal or smaller group sizes. Note that group size ‘n’ here refers to the number of technical replicates rather than the number of biological replicates. Conclusion and Implications A full kinetic method can yield more precise parameter estimates than the equilibrium method. Such an approach may be more useful for researchers.

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“…In this study, we emulate a real‐time experiment described by Thais et al (2019). In their work, they explore ligand receptor binding for SiR‐6 at the cannabinoid 2 receptor (CB 2 ).…”

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Exploring group size for statistical analysis of real‐time signalling experiments

Yang

Zhu

Finlay

et al. 2021

British J Pharmacology

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“…The Carreira group focussed on modifying pyrazine and pyridine scaffolds, in which no previous cannabinoid fluorescent probes have been published. [139] With parent compounds RO6839251 (K i (hCB 2 R) ¼ 0.2 nM) and RO6852763 (K i (hCB 2 R) ¼ 0.2 nM), displaying good affinity and selectivity to CB 2 R, fluorescent moieties NBD, AttoThio12, Silicon Rhodamine (SiR), and Cy5.5 were linked via variations on PEG or C-6 alkyl chains. NBD (59) and AttoThio12 (60) linked compounds displayed the highest affinity to CB 2 R but maintained moderate affinity to CB 1 R. In flow cytometry experiments, AttoThio12 and SiR (61) bound compounds labelled mouse and human CB 2 R, CHO cells overexpressing cannabinoid receptors, as well as WT CHO cells.…”

Section: Fluorescent Pyrazine/pyridine Cannabinoidsmentioning

confidence: 99%

Imaging Cannabinoid Receptors: A Brief Collection of Covalent and Fluorescent Probes for CB

Hamilton¹,

Payne²,

Mocerino³

et al. 2021

Aust. J. Chem.

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There has been an expanding public interest towards the notion that modulation of the sophisticated endocannabinoid system can lead to various therapeutic benefits that are yet to be fully explored. In recent years, the drug discovery paradigm in this field has been largely based on the development of selective CB 2 receptor agonists, avoiding the unwanted CB 1 receptor-mediated psychoactive side effects. Mechanistically, target engagement studies are crucial for confirming the ligand-receptor interaction and the subsequent biological cascades that lead to the observed therapeutic effects. Concurrently, imaging techniques for visualisation of cannabinoid receptors are increasingly reported in the literature. Small molecule imaging tools ranging from phytocannabinoids such as tetrahydrocannabinol (THC) and cannabidiol (CBD) to the endocannabinoids as well as the purely synthetic cannabimimetics, have been explored to date with varying degrees of success. This Review will cover currently known photoactivatable, electrophilic, and fluorescent ligands for both the CB 1 and CB 2 receptors. Structural insights from techniques such as ligand-assisted protein structure (LAPS) and the discovery of novel allosteric modulators are significant additions for better understanding of the endocannabinoid system. There has also been a plethora of fluorescent conjugates that have been assessed for their binding to cannabinoid receptors as well as their potential for cellular imaging. More recently, bifunctional probes containing either fluorophores or electrophilic tags are becoming more prevalent in the literature. Collectively, these molecular tools are invaluable in demonstrating target engagement within the human endocannabinoid system.

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Drug Derived Fluorescent Probes for the Specific Visualization of Cannabinoid Type 2 Receptor - A Toolbox Approach

Cited by 2 publications

References 16 publications

Exploring group size for statistical analysis of real‐time signalling experiments

Exploring group size for statistical analysis of real‐time signalling experiments

Imaging Cannabinoid Receptors: A Brief Collection of Covalent and Fluorescent Probes for CB

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