Receptor Activity-modifying Protein-directed G Protein Signaling Specificity for the Calcitonin Gene-related Peptide Family of Receptors

Weston, Cathryn; Winfield, Ian J.; Harris, Matthew; Hodgson, Rose; Shah, Archna; Dowell, Simon J.; Mobarec, Juan Carlos; Woodlock, David A.; Reynolds, Christopher A.; Poyner, David R.; Watkins, Harriet A.; Ladds, Graham

doi:10.1074/jbc.m116.751362

Cited by 84 publications

(97 citation statements)

References 71 publications

(116 reference statements)

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“…Gα s is the main signal pathway activated by CRLR‐ and CTR‐based receptors (Hong et al , ), but RAMPs influence the biased activation of CRLR and CTR in a ligand‐dependent manner. In HEK‐293 cells treated with ADM2/IMD 1–47 , the CGRP receptors display a bias toward Gα s signalling; AM 1 receptors shows a bias toward Gα q signalling; and AM 2 receptors show bias toward Gα s signalling (Weston et al , ) (Figure ).…”

Section: Adm2 and Adm2 Receptorsmentioning

confidence: 99%

“…However, when HEK‐293 cells are treated with CGRP, ADM or ADM2, the G protein selectivity of CRLR is also changed. Now, CGRP receptors displays a bias toward Gα s signalling in response to CGRP and change to a Gα i bias, in response to ADM. AM 1 receptors shows a bias toward Gα s when treated with CGRP and ADM. AM 2 receptors show bias toward Gα s in response to ADM and change to Gα q in response to CGRP (Weston et al , ). Therefore, the biased activation of CRLR by different peptides is another mechanism underlying the differences in effects between ADM2, CGRP and ADM.…”

Section: Adm2 and Adm2 Receptorsmentioning

confidence: 99%

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Adrenomedullin 2/intermedin: a putative drug candidate for treatment of cardiometabolic diseases

Zhang

Wang

2017

British J Pharmacology

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Adrenomedullin (ADM) 2/intermedin (IMD) is a short peptide that belongs to the CGRP superfamily. Although it shares receptors with CGRP, ADM and amylin, ADM2 has significant and unique functions in the cardiovascular system. In the past decade, the cardiovascular effect of ADM2 has been carefully analysed. In this review, progress in understanding the effects of ADM2 on the cardiovascular system and its protective role in cardiometabolic diseases are summarized. LINKED ARTICLESThis article is part of a themed section on Spotlight on Small Molecules in Cardiovascular Diseases. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v175.8/issuetoc Abbreviations AAC, abdominal aortic constriction; ACS, acute coronary syndrome; ADM, adrenomedullin; AMPK, AMP-activated protein kinase; AMY, amylin; CRLR, calcitonin receptor-like receptor; ER, endoplasmic reticulum; I/R, ischaemia/reperfusion; RAMP, receptor activity-modifying protein; SHR, spontaneously hypertensive rat; TAC, transverse aortic contraction; VSMC, vascular smooth muscle cell Takei et al., 2004). It is one of the members of the ADM family which are all found in fish but, in mammals, only three peptides -ADM, ADM2 and ADM5 -have been found (Takei et al., 2008). These ADM peptides are themselves a part of the CGRP superfamily. ADM2 is also called intermedin (IMD), owing to its high expression in the intermediate lobe of the pituitary. Both terms, 'ADM2' and 'IMD', are widely used in the literature. However, because IMD was used as the former name for α-melanocyte stimulating hormone, we will use the terms ADM2, ADM2/IMD 1-53 , ADM2/IMD 1-47 and ADM2/IMD 1-40 in this review to avoid confusion. ADM2 shares receptors with CGRP, ADM and amylin (AMY) (Hay et al., 2005) and is widely expressed throughout the body. Recently, progress has been made on the physiological roles of ADM2 in cardiovascular homeostasis and as a protective agent against cardiometabolic diseases. In this review, the structure and expression of ADM2 and the pharmacology of ADM2, in the context of the cardiovascular system and cardiometabolic diseases, are summarized. ADM2 and ADM2 receptorsThe structure of ADM2The Adm2 gene is located on the distal arm of human chromosome 22q13.33 and encodes a pre-pro-peptide containing 148 amino acid residues with a signal sequence at the N terminus . ADM2 belongs to the CGRP superfamily, which includes α-CGRP, β-CGRP, calcitonin receptor-stimulating peptide, AMY, ADM and ADM5 (Hong et al., 2012). ADM2 shares the same structural characteristics with the other family members, including an intramolecular ring of six amino acids residues flanked by a disulfide bond and a putative amidation signal at the C terminus .Sequence alignment has shown that ADM2 shares only 28% sequence identity with its closest paralogue, ADM.However, ADM2 is highly conserved in the orthologues of different species. The mature human ADM2 shares over 60% similarity with fish and 87% identity with the rodent peptides . The property of high con...

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Section: Adm2 and Adm2 Receptorsmentioning

confidence: 99%

Section: Adm2 and Adm2 Receptorsmentioning

confidence: 99%

Adrenomedullin 2/intermedin: a putative drug candidate for treatment of cardiometabolic diseases

Zhang

Wang

2017

British J Pharmacology

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“…Thus, perhaps small molecules that: 1) act as non-selective antagonists at both CRF subtypes, 2) exhibit inverse agonist activity, or 3) also modulate activities of other CRF system molecules, such as CRF-BP or receptor activity modifying protein-2 (RAMP2) (Wooten et al 2013; Weston et al 2016; Gingell et al 2016) would have greater therapeutic activity than the many selective CRF 1 neutral antagonists tested to date. Similarly, the structural manner of binding the receptor may be important; perhaps small molecules that bind differentially to certain residues of the atypical allosteric binding site (e.g., compare MTIP vs. CP-376395; Xu et al 2015) may slow the antagonist’s escape kinetics (Bai et al 2014) or direct its anti-signaling pathway bias (Suen et al 2014; Zhang et al 2016).…”

Section: Targeting and Validating Drug Action In Humansmentioning

confidence: 99%

Don’t stress about CRF: assessing the translational failures of CRF1antagonists

2017

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BACKGROUND Dr. Athina Markou sought treatments for a common neural substrate shared by depression and drug dependence. Antagonists of corticotropin-releasing factor (CRF) receptors, a target of interest to her, have not reached the clinic despite strong preclinical rationale and sustained translational efforts. METHODS We explore potential causes for the failure of CRF1 antagonists and review recent findings concerning CRF-CRF1 systems in psychopathology. RESULTS Potential causes for negative outcomes include: 1) poor safety and efficacy of initial drug candidates due to bad pharmacokinetic and physicochemical properties 2) specificity problems with preclinical screens, 3) the acute nature of screens vs late-presenting patients, 4.) positive preclinical results were limited to certain models and conditions with dynamic CRF-CRF1 activation not homologous to tested patients, 5) repeated CRF1 activation-induced plasticity that reduces the importance of ongoing CRF1 agonist stimulation, 6) therapeutic silencing may need to address CRF2 receptor or CRF-BP molecules, constitutive CRF1 activity, or molecules that influence agonist-independent activity or to target structural regions other than the allosteric site bound by all drug candidates We describe potential markers of activation towards individualized treatment, human genetic and functional data that still implicate CRF1 systems in emotional disturbance, sex differences, and suggestive clinical findings for CRF1 antagonists in food craving and CRF-driven HPA-axis overactivation. CONCLUSION The therapeutic scope of selective CRF1 antagonists now appears narrower than had been hoped. Yet, much remains to be learned about CRF’s role in the neurobiology of dysphoria and addiction and the potential for novel anti-CRF therapies therein.

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“…Islets were isolated as previously described (59) and dispersed to single cell suspension using Enzyme Free Dissociation Buffer (Gibco). Islets were seeded in a 384-well Optiplate (PerkinElmer) (4000 cells per well) and stimulated with either GLP-1 or GIP for 30 minutes prior to measurement of cAMP accumulation using a LANCE® Ultra cAMP Detection Kit (PerkinElmer) in accordance with the manufacturer's instructions and as described previously (61,62). Results are presented as % of total stimulation with 10 µM forskolin (a direct activator of adenylyl cyclase).…”

Section: Cyclic Amp Assaymentioning

confidence: 99%

GLP-1R is downregulated in beta cells of NOD mice and T1D patients

Recino

Barkan

Schmidt-Christensen

et al. 2019

Preprint

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Glucagon-like peptide 1 (GLP-1) is produced by L cells in the small intestine in response to ingested glucose and increases insulin release from pancreatic beta cells by activation of its cognate receptor (GLP-1R). Stimulation of this receptor also contributes to increased beta cell survival and regeneration. We have found that pancreatic beta cells from Non Obese Diabetic (NOD) mice express significantly lower levels of GLP-1R than C57BL/6 mice, leaving the NOD beta cells with an impaired response to GLP-1 stimulation. The lower expression appears to be caused by accelerated degradation of GLP-1R in the beta cells, a process that can be reversed by inhibiting trafficking to the lysosome. Importantly, our results appear to translate to the human disease since we also observed significantly lower expression of the GLP-1R in pancreatic islets from donors with type 1 diabetes. These results suggest that beta cell physiology may play a role in susceptibility to autoimmune inflammation.

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Receptor Activity-modifying Protein-directed G Protein Signaling Specificity for the Calcitonin Gene-related Peptide Family of Receptors

Cited by 84 publications

References 71 publications

Adrenomedullin 2/intermedin: a putative drug candidate for treatment of cardiometabolic diseases

Adrenomedullin 2/intermedin: a putative drug candidate for treatment of cardiometabolic diseases

Don’t stress about CRF: assessing the translational failures of CRF1antagonists

GLP-1R is downregulated in beta cells of NOD mice and T1D patients

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