Divergent acute <i>versus</i> prolonged pharmacological GLP-1R responses in adult beta cell-selective β-arrestin 2 knockout mice

Bitsi, Stavroula; Manchanda, Yusman; Eleid, Liliane; Mohamed, Nimco; Hansen, Ben; Suba, Kinga; Rutter, Guy A.; Salem, Victoria; Jones, Ben; Tomás, Alejandra

doi:10.1101/2022.04.21.489075

Cited by 7 publications

(12 citation statements)

References 76 publications

(172 reference statements)

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“…However, β-cellspecific conditional knockout studies of β-arrestin-1 and -2 in mice showed no acute insulin secretory deficit in response to GLP-1R agonists, 41,42 although we recently found that loss of β-arrestin-2 may lead to reduced GLP-1R agonist-induced insulin secretion in female mice and DIO male mice, omitted from earlier studies. 43 With this in mind, we aimed to test whether partial or complete loss of GLP-1R agonist-induced β-arrestin recruitment is optimal for enhancing insulin secretion using SRB106 and SRB107 The rapid expansion of next-generation sequencing technology has highlighted extensive genomic coding variation in drug targets. 17 Current GLP-1R agonists are effective for many patients, but a significant minority fail to achieve treatment targets.…”

Section: Discussionmentioning

confidence: 99%

Abolishing β‐arrestin recruitment is necessary for the full metabolic benefits of G protein‐biased glucagon‐like peptide‐1 receptor agonists

Hinds,

Peace,

Chen

et al. 2023

Diabetes Obesity Metabolism

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AimEarlier studies have shown that peptide glucagon‐like peptide‐1 receptor (GLP‐1R) agonists with reduced β‐arrestin recruitment show enhanced anti‐hyperglycaemic efficacy through avoidance of GLP‐1R desensitization. However, the ligand modifications needed to decrease β‐arrestin recruitment usually also reduces GLP‐1R affinity, therefore higher doses are needed. Here we aimed to develop new, long‐acting, G protein‐biased GLP‐1R agonists with acute signalling potency comparable with semaglutide, to provide insights into specific experimental and therapeutic scenarios.Materials and MethodsNew GLP‐1R agonist peptides were assessed using a variety of in vitro and in vivo assays.ResultsFirst, we show that very substantial reductions in β‐arrestin recruitment efficacy are required to realize fully the benefits of GLP‐1R agonism on blood glucose lowering in mice, with more moderate reductions being less effective. Secondly, our lead compound (SRB107) performs substantially better than semaglutide for effects on blood glucose and weight loss, which may be jointly attributable to its biased agonist action and protracted pharmacokinetics. Thirdly, we show that biased agonist‐specific GLP‐1R internalization profiles occur at clinically relevant pharmacological concentrations. Finally, we show that SRB107 cAMP signalling is differentially modulated by single and double GLP1R coding variants seen in human populations, with implications for GLP‐1R agonist pharmacogenomics.ConclusionsCompletely abolishing β‐arrestin recruitment improves the anti‐hyperglycaemic effects of GLP‐1R agonists in mice.

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Section: Discussionmentioning

confidence: 99%

Abolishing β‐arrestin recruitment is necessary for the full metabolic benefits of G protein‐biased glucagon‐like peptide‐1 receptor agonists

Hinds,

Peace,

Chen

et al. 2023

Diabetes Obesity Metabolism

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“…Here, we again observe reduced propensity for b-arrestin 2 recruitment by the GIPR, this time in a beta cell context. The role of b-arrestins on incretin receptor trafficking and signaling has previously been investigated by us from several angles, for example by the use of biased agonists with different capabilities for b-arrestin recruitment [8,26], using in vivo conditional b-arrestin 2 knockout mouse models [21], or with in vitro cell systems with deleted b-arrestin 1/2 expression [13,26]. In all these instances, b-arrestin recruitment closely correlated with the degree of incretin receptor internalization, but alterations in b-arrestin expression levels or complete b-arrestin deletion did not lead to .…”

Section: Discussionmentioning

confidence: 99%

“…Here, we again observe reduced propensity for β-arrestin 2 recruitment by the GIPR, this time in a beta cell context. The role of β-arrestins on incretin receptor trafficking and signaling has previously been investigated by us from several angles, for example by the use of biased agonists with different capabilities for β-arrestin recruitment [8, 26], using in vivo conditional β-arrestin 2 knockout mouse models [21], or with in vitro cell systems with deleted β-arrestin 1/2 expression [13, 26]. In all these instances, β-arrestin recruitment closely correlated with the degree of incretin receptor internalization, but alterations in β-arrestin expression levels or complete β-arrestin deletion did not lead to significant effects in receptor endocytosis, but rather resulted in the prolongation of cAMP/PKA signaling duration, suggesting that the main effect of this important signaling mediator lies in the steric hindrance caused by its binding to the receptor, leading to reduced access of Gα S to its binding pocket and promoting homologous receptor desensitization [30].…”

Section: Discussionmentioning

confidence: 99%

“…Of note, similar reduced GIPR versus GLP-1R β-arrestin recruitment and internalization into a Rab5-positive endosomal compartment were also apparent in a separate study [31], although in this instance the authors focused on the comparison between responses from single and dual agonists such as tirzepatide or MAR709 for each receptor rather than performing a direct comparison of both receptor responses. Also interestingly, we previously observed that in vivo GIPR responses were less affected by β-arrestin 2 deletion specifically from pancreatic beta cells [21], suggesting a reduced reliance on β-arrestin 2 to regulate GIPR signaling effects in the pancreas.…”

Section: Discussionmentioning

confidence: 99%

“…Imaging of INS-1 832/3 cells or whole-islet Ca 2+ dynamics was performed as previously described [21]. Cells or Matrigel-encased islets from individual animals were loaded with the Ca 2+ responsive dye Cal-520 AM (AAT Bioquest), pre-incubated for 1 hr in KRBH G6, and imaged in MatTek glass bottom dishes every 6 sec at 488 nm using a Nikon Eclipse Ti microscope with an ORCA-Flash 4.0 camera (Hamamatsu) and Metamorph software (Molecular Devices) while maintained at 37°C on a heated stage.…”

Section: Calcium Assaysmentioning

confidence: 99%

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An examination of the divergent spatiotemporal signaling of GLP-1R versus GIPR in pancreatic beta cells

Manchanda

Bitsi

Chen

et al. 2022

Preprint

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The incretin receptors, glucagon-like peptide-1 receptor (GLP-1R) and glucose-dependent insulinotropic polypeptide receptor (GIPR), are class B GPCRs and prime therapeutic targets for the treatment of type 2 diabetes (T2D) and obesity. They are expressed in pancreatic beta cells where they potentiate insulin release in response to food intake. Despite GIP being the main incretin in healthy individuals, GLP-1R has been favoured versus GIPR as a therapeutic target due to GIPR responses being blunted in T2D patients and the conflicting effects of GIPR agonists and antagonists in improving glucose tolerance and preventing weight gain. There is, however, a recently renewed interest in GIPR biology following the realisation that GIPR responses can be restored after an initial period of blood glucose normalization and the recent development of dual GLP-1R-GIPR agonists with superior capacity for the control of blood glucose levels and weight. The importance of GLP-1R trafficking and subcellular signaling in the control of receptor outputs is well established, but little is known about the pattern of spatiotemporal signaling from the GIPR in beta cells. Here we have directly compared the main trafficking and signaling characteristics of both receptors in pancreatic beta cells, finding striking differences in their propensities for internalization, recycling, and degradation, as well as plasma membrane versus endosomal activity, with potential implications for receptor-specific control of beta cell function.

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Biased agonism and polymorphic variation at the GLP-1 receptor: Implications for the development of personalised therapeutics

Eid

Reynolds²,

Tomás³

et al. 2022

Pharmacological Research

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Divergent acute versus prolonged pharmacological GLP-1R responses in adult beta cell-selective β-arrestin 2 knockout mice

Cited by 7 publications

References 76 publications

Abolishing β‐arrestin recruitment is necessary for the full metabolic benefits of G protein‐biased glucagon‐like peptide‐1 receptor agonists

Abolishing β‐arrestin recruitment is necessary for the full metabolic benefits of G protein‐biased glucagon‐like peptide‐1 receptor agonists

An examination of the divergent spatiotemporal signaling of GLP-1R versus GIPR in pancreatic beta cells

Biased agonism and polymorphic variation at the GLP-1 receptor: Implications for the development of personalised therapeutics

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