Gs-DREADD Knock-In Mice for Tissue-Specific, Temporal Stimulation of Cyclic AMP Signaling

Akhmedov, Dmitry; Mendoza-Rodriguez, Maria G.; Rajendran, Kavitha; Rossi, Mario; Wess, Jürgen; Berdeaux, Rebecca

doi:10.1128/mcb.00584-16

Cited by 30 publications

(38 citation statements)

References 70 publications

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“…DREADD (designer receptors solely activated by designer drugs) technology overcomes these limitations by using a combined genetic/ chemical approach. [8][9][10][11][12] These genetically modified designer GPCRs are unable to bind endogenous ligands, but can be activated by otherwise inert small molecules. 13 The most commonly used DREADDs represent mutant muscarinic receptors that can be specifically activated by the DREADD agonist clozapine-N-oxide (CNO) but not by their natural ligand acetylcholine.…”

Section: Introductionmentioning

confidence: 99%

“…13 The most commonly used DREADDs represent mutant muscarinic receptors that can be specifically activated by the DREADD agonist clozapine-N-oxide (CNO) but not by their natural ligand acetylcholine. 14 DREADDs show only minimal constitutive activity even at high levels of expression and no noteworthy response to acetylcholine, 14,15 Up to now, DREADD technology has been mostly used by neuroscientists, but DREADDs have also been expressed in pancreatic b-cells 15,16 , hepatocytes, 12 and cancer cells. 17 Here, we present the first transgenic mouse line expressing a functional Gq-coupled designer receptor, M3Dq (Dq) 15 under the transcriptional control of the muscle creatine kinase (MCK) promoter.…”

Section: Introductionmentioning

confidence: 99%

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DREADD technology reveals major impact of Gq signalling on cardiac electrophysiology

Kaiser

Tian

Wagner

et al. 2018

Cardiovascular Research

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Aims Signalling via Gq-coupled receptors is of profound importance in many cardiac diseases such as hypertrophy and arrhythmia. Nevertheless, owing to their widespread expression and the inability to selectively stimulate such receptors in vivo, their relevance for cardiac function is not well understood. We here use DREADD technology to understand the role of Gq-coupled signalling in vivo in cardiac function. Methods and results We generated a novel transgenic mouse line that expresses a Gq-coupled DREADD (Dq) in striated muscle under the control of the muscle creatine kinase promotor. In vivo injection of the DREADD agonist clozapine-N-oxide (CNO) resulted in a dose-dependent, rapid mortality of the animals. In vivo electrocardiogram data revealed severe cardiac arrhythmias including lack of P waves, atrioventricular block, and ventricular tachycardia. Following Dq activation, electrophysiological malfunction of the heart could be recapitulated in the isolated heart ex vivo. Individual ventricular and atrial myocytes displayed a positive inotropic response and arrhythmogenic events in the absence of altered action potentials. Ventricular tissue sections revealed a strong co-localization of Dq with the principal cardiac connexin CX43. Western blot analysis with phosphor-specific antibodies revealed strong phosphorylation of a PKC-dependent CX43 phosphorylation site following CNO application in vivo. Conclusion Activation of Gq-coupled signalling has a major impact on impulse generation, impulse propagation, and coordinated impulse delivery in the heart. Thus, Gq-coupled signalling does not only modulate the myocytes’ Ca2+ handling but also directly alters the heart’s electrophysiological properties such as intercellular communication. This study greatly advances our understanding of the plethora of modulatory influences of Gq signalling on the heart in vivo.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

DREADD technology reveals major impact of Gq signalling on cardiac electrophysiology

Kaiser

Tian

Wagner

et al. 2018

Cardiovascular Research

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“…DREADDs represent mutant GPCRs that are no longer activated by any endogenous ligands but can be selectively activated by clozapine-N-oxide (CNO), a synthetic ligand that is otherwise pharmacologically inert (10,11). During the past few years, we and other investigators have successfully used DREADD technology to study the in vivo metabolic effects of activating distinct functional classes of GPCRs in several metabolically relevant cell types, including pancreatic b-cells (12,13), hepatocytes (14)(15)(16), and adipocytes (17).…”

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confidence: 99%

Skeletal Muscle–Specific Activation of Gq Signaling Maintains Glucose Homeostasis

et al. 2019

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Skeletal muscle (SKM) insulin resistance plays a central role in the pathogenesis of type 2 diabetes. Because G-protein–coupled receptors (GPCRs) represent excellent drug targets, we hypothesized that activation of specific functional classes of SKM GPCRs might lead to improved glucose homeostasis in type 2 diabetes. At present, little is known about the in vivo metabolic roles of the various distinct GPCR signaling pathways operative in SKM. In this study, we tested the hypothesis that selective activation of SKM Gq signaling can improve SKM glucose uptake and whole-body glucose homeostasis under physiological and pathophysiological conditions. Studies with transgenic mice expressing a Gq-linked designer GPCR selectively in SKM cells demonstrated that receptor-mediated activation of SKM Gq signaling greatly promoted glucose uptake into SKM and significantly improved glucose homeostasis in obese, glucose-intolerant mice. These beneficial metabolic effects required the activity of SKM AMPK. In contrast, obese mutant mice that lacked both Gαq and Gα11 selectively in SKM showed severe deficits in glucose homeostasis. Moreover, GPCR-mediated activation of Gq signaling also stimulated glucose uptake in primary human SKM cells. Taken together, these findings strongly suggest that agents capable of enhancing SKM Gq signaling may prove useful as novel antidiabetic drugs.

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“…Mice lacking all 3 β-ARs (β-less) were on FVB background and provided by Bradford Lowell of Harvard Medical School (Boston, Massachusetts, USA) (13). Conditional Gs-DREADD mice (27) and EpoR-Cre mice (28,29) were obtained from Rebecca Berdeaux and Yang Xia of the University of Texas Medical School at Houston. The mice were crossed to generate rbc-GsD.…”

Section: Methodsmentioning

confidence: 99%

“…DREADDs are mutated muscarinic GPCRs with selectivity for individual G protein effector pathways (Gs, Gi, or Gq) and only respond to the otherwise inert ligand clozapine N-oxide (CNO) (26). ROSA26-LSL-Gs-DREADD animals enable temporal control of cAMP signaling in selective cell types using cell type-specific Cre drivers (27). EpoR-Cre mice were used to achieve rbc-specific expression of Cre (28,29).…”

Section: Activation Of Camp Signaling In Rbc Increases Hfd-induced Eementioning

confidence: 99%

Red blood cell β-adrenergic receptors contribute to diet-induced energy expenditure by increasing O2 supply

Kim

Fan

Akhmedov³

et al. 2017

JCI Insight

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Gs-DREADD Knock-In Mice for Tissue-Specific, Temporal Stimulation of Cyclic AMP Signaling

Cited by 30 publications

References 70 publications

DREADD technology reveals major impact of Gq signalling on cardiac electrophysiology

DREADD technology reveals major impact of Gq signalling on cardiac electrophysiology

Skeletal Muscle–Specific Activation of Gq Signaling Maintains Glucose Homeostasis

Red blood cell β-adrenergic receptors contribute to diet-induced energy expenditure by increasing O2 supply

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