The Chemerin Receptor CMKLR1 Requires Full‐Length Chemerin for High Affinity in Contrast to GPR1 as Demonstrated by a New Nanoluciferase‐Based Binding Assay

Czerniak, Anne Sophie; Kretschmer, Kevin; Weiss, Th.; Beck‐Sickinger, Annette G.

doi:10.1002/cmdc.202200413

Cited by 5 publications

(23 citation statements)

References 62 publications

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“…Here, C9 is sufficient for high affinity and full activation as confirmed by binding experiments using a bioluminescence resonance energy transfer (BRET) based assay set-up with nano-luciferase (Nluc) modified receptors. [21] Thus, in addition to the already known interaction of the C-terminal segment of ChemS157 with the transmembrane orthosteric binding pocket we hypothesize an additional interaction of ChemS157 at the CMKLR1.…”

Section: Introductionmentioning

confidence: 69%

“…Here, the activity of ChemS157 drops to values comparable to C9 at the CMKLR1 wt (227 nM and 1042 nM; Table 1). N-terminal receptor deletions have little impact on the interaction of C9 with a maximal 3-fold loss of receptor activation for the CMKLR1[ΔNterm [4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22] ] variant (Table 1).…”

Section: The Cmklr1 N Terminus Shows a High Influence On Stable Chems...mentioning

confidence: 99%

“…All assays were performed at least three times in duplicate using transiently transfected COS-7 cells. [13][14][15][16][17] , YPDYL [18][19][20][21][22] and the full N terminus (E 4 À L 22 ), respectively. Aspartic acid and glutamic acid residues are highlighted in red.…”

Section: The Negatively Charged N Terminus Of Cmklr1 Is Important For...mentioning

confidence: 99%

“…To get detailed kinetic information about the negatively charged patches of the CMKLR1 N terminus, Nluc-based bioluminescence resonance energy transfer (NanoBRET) binding assays were performed as previously described. [21] First, the CMKLR1 alanine variants (CMKLR1[EDED 4-7 AAAA] and CMKLR1 [DED 16,17,20 AAA]) were N-terminally fused to Nluc (Figure 5A). All Nluc-labeled receptor constructs showed wt-like membrane localization (Figure S4).…”

Section: Investigation Of Binding Kinetics For the Distinct Negativel...mentioning

confidence: 99%

“…[17a,20] The C-terminal nonapeptide chemerin-9 (C9) is able to display full activity at the CMKLR1 receptor in non-equilibrium Ca 2 + flux assays, [8a] whereas full-length ChemS157 is required for strong interactions as determined by equilibrium assays such as IP accumulation and competition binding studies. [21] Interestingly, this is different for GPR1. Here, C9 is sufficient for high affinity and full activation as confirmed by binding experiments using a bioluminescence resonance energy transfer (BRET) based assay set-up with nano-luciferase (Nluc) modified receptors.…”

Section: Introductionmentioning

confidence: 95%

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Stable Binding of Full‐Length Chemerin Is Driven by Negative Charges in the CMKLR1 N Terminus

et al. 2023

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The adipokine chemerin is the endogenous ligand of the chemokine‐like receptor 1 (CMKLR1), a member of the family of G protein‐coupled receptors (GPCRs). This protein ligand plays an important role in obesity and inflammatory processes. Stable receptor–ligand interactions are highly relevant for its different physiological effects such as the migration of immune cells towards sites of inflammation. Here, we demonstrate that negative charges in the CMKLR1 N terminus are involved in the formation of strong contacts with a specific positively charged patch at the surface of full‐length chemerin, which is absent in the short nonapeptide agonist chemerin‐9, thus explaining its reduced affinity. Using receptor chimera of G protein‐coupled receptor 1 (GPR1) and CMKLR1, we were able to identify the residues of this interaction and its relevance for stable full‐length chemerin binding. This could help to develop more potent ligands for the treatment of inflammation‐related diseases.

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Section: Introductionmentioning

confidence: 69%

Section: The Cmklr1 N Terminus Shows a High Influence On Stable Chems...mentioning

confidence: 99%

Section: The Negatively Charged N Terminus Of Cmklr1 Is Important For...mentioning

confidence: 99%

Section: Investigation Of Binding Kinetics For the Distinct Negativel...mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 95%

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Stable Binding of Full‐Length Chemerin Is Driven by Negative Charges in the CMKLR1 N Terminus

et al. 2023

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Binding Mode of Cyclic Chemerin‐9 Peptide and ChemerinS157 Protein at CMKLR1

Schermeng,

Liessmann,

Katharina Ambrosius

et al. 2024

ChemBioChem

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The chemokine‐like receptor 1 (CMKLR1) is activated by the adipokine and chemoattractant protein chemerin. Cryo‐EM structures of chemerin‐9‐CMKLR1‐Gi have been published, where chemerin‐9 is the nonapeptide of the C terminus of chemerinS157. Chemerin‐9 is as active as the full‐length protein in Ca2+‐release but shows differences in equilibrium read‐outs. An equally potent cyclic chemerin‐9 variant (cC9) was reported previously. Now, we have built a computational model of CMKLR1 to investigate the binding mode of cC9 and chemerinS157 in comparison to chemerin‐9. Differences were investigated using CMKLR1 variants. Double‐mutant cycle analysis identified CMKLR1‐F2.53 as the relevant position for Phe8‐binding of cC9. Energy contribution revealed slight differences in Phe8‐binding to CMKLR1‐F2.53 and space for larger residues. This was confirmed as the chemerin‐9 variant with 1‐naphthyl‐L‐alanine at position 8 showed a 4‐fold increased potency of 2 nM (pEC50=8.6±0.15). While chemerin‐9 and cC9 share their interactions at the CMKLR1, chemerinS157 tolerates most mutations of CMKLR1 in the deep binding site. The computational model of chemerinS157 suggests a β‐sheet interaction between the N‐terminal CMKLR1‐segment I25VVL28 and the β‐sheet D108KVLGRLVH116 of ChemS157, which was confirmed experimentally. Our data expand the knowledge by identifying the binding mode of chemerinS157 and cC9 at CMKLR1 facilitating future structure‐based drug design.

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The Chemerin Receptor CMKLR1 Requires Full‐Length Chemerin for High Affinity in Contrast to GPR1 as Demonstrated by a New Nanoluciferase‐Based Binding Assay

et al. 2022

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To study the binding mode of the adipokine chemerin as well as the short peptide agonist chemerin‐9 (C9) to its two receptors chemokine‐like receptor 1 (CMKLR1) and G protein‐coupled receptor 1 (GPR1), we generated 5‐carboxytetramethylrhodamine (TAMRA) modified variants of both ligands. In addition, we labeled GPR1 and CMKLR1 with a nanoluciferase at the N‐terminus to perform NanoBRET binding assays. For GPR1, both ligands show high affinity and comparable binding. Significant differences were found for CMKLR1, whereby only full‐length chemerin binds with high affinity in saturation and displacement assays. For TAMRA‐C9 a biphasic binding consisting of two binding states has been found and no displacement studies could be performed. Thus, we conclude that CMKLR1 requires full‐length chemerin for stable binding in contrast to GPR1. This work demonstrates the NanoBRET binding assay as a new tool for binding studies at chemerin receptors and it enables deeper insights into the ligand binding parameters.

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The Chemerin Receptor CMKLR1 Requires Full‐Length Chemerin for High Affinity in Contrast to GPR1 as Demonstrated by a New Nanoluciferase‐Based Binding Assay

Cited by 5 publications

References 62 publications

Stable Binding of Full‐Length Chemerin Is Driven by Negative Charges in the CMKLR1 N Terminus

Stable Binding of Full‐Length Chemerin Is Driven by Negative Charges in the CMKLR1 N Terminus

Binding Mode of Cyclic Chemerin‐9 Peptide and ChemerinS157 Protein at CMKLR1

The Chemerin Receptor CMKLR1 Requires Full‐Length Chemerin for High Affinity in Contrast to GPR1 as Demonstrated by a New Nanoluciferase‐Based Binding Assay

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