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10 results on '"Katja Spiess"'

1. Viral GPCR US28 can signal in response to chemokine agonists of nearly unlimited structural degeneracy

Author

Timothy F Miles, Katja Spiess, Kevin M Jude, Naotaka Tsutsumi, John S Burg, Jessica R Ingram, Deepa Waghray, Gertrud M Hjorto, Olav Larsen, Hidde L Ploegh, Mette M Rosenkilde, and K Christopher Garcia

Subjects
G protein-coupled receptor, chemokine, biased signaling, membrane protein crystallography, yeast surface display, Medicine, Science, Biology (General), QH301-705.5
Abstract

Human cytomegalovirus has hijacked and evolved a human G-protein-coupled receptor into US28, which functions as a promiscuous chemokine 'sink’ to facilitate evasion of host immune responses. To probe the molecular basis of US28’s unique ligand cross-reactivity, we deep-sequenced CX3CL1 chemokine libraries selected on ‘molecular casts’ of the US28 active-state and find that US28 can engage thousands of distinct chemokine sequences, many of which elicit diverse signaling outcomes. The structure of a G-protein-biased CX3CL1-variant in complex with US28 revealed an entirely unique chemokine amino terminal peptide conformation and remodeled constellation of receptor-ligand interactions. Receptor signaling, however, is remarkably robust to mutational disruption of these interactions. Thus, US28 accommodates and functionally discriminates amongst highly degenerate chemokine sequences by sensing the steric bulk of the ligands, which distort both receptor extracellular loops and the walls of the ligand binding pocket to varying degrees, rather than requiring sequence-specific bonding chemistries for recognition and signaling.

Published
2018
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2. A guide to adhesion GPCR research

Author

Cheng-Chih Hsiao, Katarina Trajkovic, Orkun Cevheroğlu, Ines Liebscher, Katja Spiess, André F. Maia, Nicole Scholz, Hannes Schihada, Simone Prömel, Mickey Kosloff, Mark Soave, and Experimental Immunology

Subjects
STRUCTURAL BASIS, structure–function, Computer science, GPR56 ADGRG1, Adhesion GPCRs, TETHERED AGONIST, Biochemistry, structure-function, ANGIOGENESIS, MEMORY T-CELLS, INHIBITORY RECEPTOR, Molecular Biology, G protein-coupled receptor, Cognitive science, Structure function, Cell Biology, PROTEIN-COUPLED-RECEPTOR, GENE, Bench to bedside, clinical application, physiology, signaling, NEURAL-TUBE DEFECTS, CD97
Abstract

Adhesion G protein-coupled receptors (aGPCRs) are a class of structurally and functionally highly intriguing cell surface receptors with essential functions in health and disease. Thus, they display a vastly unexploited pharmacological potential. Our current understanding of the physiological functions and signaling mechanisms of aGPCRs form the basis for elucidating further molecular aspects. Combining these with novel tools and methodologies from different fields tailored for studying these unusual receptors yields a powerful potential for pushing aGPCR research from singular approaches toward building up an in-depth knowledge that will facilitate its translation to applied science. In this review, we summarize the state-of-the-art knowledge on aGPCRs in respect to structure-function relations, physiology, and clinical aspects, as well as the latest advances in the field. We highlight the upcoming most pressing topics in aGPCR research and identify strategies to tackle them. Furthermore, we discuss approaches how to promote, stimulate, and translate research on aGPCRs 'from bench to bedside' in the future.

Published
2021

3. Methods for studying endocytotic pathways of herpesvirus encoded G protein-coupled receptors

Author

Mette M. Rosenkilde, Valentina Kubale, Milka Vrecl, Catrin S. Rutland, Maša Mavri, and Katja Spiess

Subjects
Endocytic cycle, Cell, Pharmaceutical Science, Cellular homeostasis, Cytomegalovirus, Review, Biology, Endocytosis, Analytical Chemistry, Receptors, G-Protein-Coupled, methods, lcsh:QD241-441, 03 medical and health sciences, Viral Proteins, 0302 clinical medicine, lcsh:Organic chemistry, herpesvirus, Drug Discovery, medicine, Animals, Humans, endocytosis, Physical and Theoretical Chemistry, Receptor, Herpesviridae, 030304 developmental biology, G protein-coupled receptor, 0303 health sciences, Organic Chemistry, Cell Membrane, Transmembrane protein, Cell biology, Eukaryotic Linear Motif resource, medicine.anatomical_structure, udc:636.09:616, G-protein coupled receptors, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, Molecular Medicine, Receptors, Chemokine, Signal Transduction
Abstract

Endocytosis is a fundamental process involved in trafficking of various extracellular and transmembrane molecules from the cell surface to its interior. This enables cells to communicate and respond to external environments, maintain cellular homeostasis, and transduce signals. G protein-coupled receptors (GPCRs) constitute a family of receptors with seven transmembrane alpha-helical domains (7TM receptors) expressed at the cell surface, where they regulate physiological and pathological cellular processes. Several herpesviruses encode receptors (vGPCRs) which benefits the virus by avoiding host immune surveillance, supporting viral dissemination, and thereby establishing widespread and lifelong infection, processes where receptor signaling and/or endocytosis seem central. vGPCRs are rising as potential drug targets as exemplified by the cytomegalovirus-encoded receptor US28, where its constitutive internalization has been exploited for selective drug delivery in virus infected cells. Therefore, studying GPCR trafficking is of great importance. This review provides an overview of the current knowledge of endocytic and cell localization properties of vGPCRs and methodological approaches used for studying receptor internalization. Using such novel approaches, we show constitutive internalization of the BILF1 receptor from human and porcine γ-1 herpesviruses and present motifs from the eukaryotic linear motif (ELM) resources with importance for vGPCR endocytosis.

Published
2021

4. Distinct Roles of Extracellular Domains in the Epstein-Barr Virus-Encoded BILF1 Receptor for Signaling and Major Histocompatibility Complex Class I Downregulation

Author

Mark R. Wills, Jianmin Zuo, Mette M. Rosenkilde, Suzan Fares, Emma T. B. Olesen, Sarah E. Jackson, Thomas N Kledal, Katja Spiess, Jackson, Sarah [0000-0002-4230-9220], Wills, Mark [0000-0001-8548-5729], and Apollo - University of Cambridge Repository

Subjects
Herpesvirus 4, Human, Molecular Biology and Physiology, Major histocompatibility complex, DNA Mutational Analysis, Down-Regulation, Microbiology, Receptors, G-Protein-Coupled, 03 medical and health sciences, Chemokine receptor, Viral Proteins, 0302 clinical medicine, GPCR, Downregulation and upregulation, Genes, Reporter, Virology, MHC class I, Extracellular, Humans, Epstein-Barr virus, tumor immunology, Receptor, Luciferases, 030304 developmental biology, G protein-coupled receptor, 0303 health sciences, biology, Chemistry, Histocompatibility Antigens Class I, EBV-BILF1, Flow Cytometry, Signaling, major histocompatibility complex, QR1-502, Cell biology, Transmembrane domain, HEK293 Cells, Host-Pathogen Interactions, biology.protein, Tumor immunology, Mutant Proteins, signaling, 030215 immunology, Signal Transduction, Research Article
Abstract

G protein-coupled receptors constitute the largest family of membrane proteins. As targets of >30% of the FDA-approved drugs, they are valuable for drug discovery. The receptor is composed of seven membrane-spanning helices and intracellular and extracellular domains. BILF1 is a receptor encoded by Epstein-Barr virus (EBV), which evades the host immune system by various strategies. BILF1 facilitates the virus immune evasion by downregulating MHC class I and is capable of inducing signaling-mediated tumorigenesis. BILF1 homologs from primate viruses show highly conserved extracellular domains. Here, we show that conserved residues in the extracellular domains of EBV-BILF1 are important for downregulating MHC class I and that the receptor signaling and immune evasion can be inhibited by drug-like small molecules. This suggests that BILF1 could be a target to inhibit the signaling-mediated tumorigenesis and interfere with the MHC class I downregulation, thereby facilitating virus recognition by the immune system., The Epstein-Barr virus (EBV) BILF1 gene encodes a constitutively active G protein-coupled receptor (GPCR) that downregulates major histocompatibility complex (MHC) class I and induces signaling-dependent tumorigenesis. Different BILF1 homologs display highly conserved extracellular loops (ECLs) including the conserved cysteine residues involved in disulfide bridges present in class A GPCRs (GPCR bridge between transmembrane helix 3 [TM-3] and ECL-2) and in chemokine receptors (CKR bridge between the N terminus and ECL-3). In order to investigate the roles of the conserved residues in the receptor functions, 25 mutations were created in the extracellular domains. Luciferase reporter assays and flow cytometry were used to investigate the G protein signaling and MHC class I downregulation in HEK293 cells. We find that the cysteine residues involved in the GPCR bridge are important for both signaling and MHC class I downregulation, whereas the cysteine residues in the N terminus and ECL-3 are dispensable for signaling but important for MHC class I downregulation. Multiple conserved residues in the extracellular regions are important for the receptor-induced MHC class I downregulation, but not for signaling, indicating distinct structural requirements for these two functions. In an engineered receptor containing a binding site for Zn+2 ions in a complex with an aromatic chelator (phenanthroline or bipyridine), a ligand-driven inhibition of both the receptor signaling and MHC class I downregulation was observed. Taken together, this suggests that distinct regions in EBV-BILF1 can be pharmacologically targeted to inhibit the signaling-mediated tumorigenesis and interfere with the MHC class I downregulation.

Published
2019

5. Viral GPCR US28 can signal in response to chemokine agonists of nearly unlimited structural degeneracy

Author

Olav Larsen, Jessica R. Ingram, Hidde L. Ploegh, Katja Spiess, John S Burg, K. Christopher Garcia, Timothy F Miles, Kevin Jude, Naotaka Tsutsumi, Gertrud Malene Hjortø, Deepa Waghray, and Mette M. Rosenkilde

Subjects
Models, Molecular, 0301 basic medicine, Chemokine, yeast surface display, Protein Conformation, Structural Biology and Molecular Biophysics, S. cerevisiae, Cytomegalovirus, Ligands, Receptors, G-Protein-Coupled, membrane protein crystallography, Degeneracy (biology), Biology (General), biased signaling, biology, Chemistry, General Neuroscience, High-Throughput Nucleotide Sequencing, General Medicine, Ligand (biochemistry), 3. Good health, Peptide Conformation, Cell biology, Medicine, Receptors, Chemokine, Research Article, Human, Protein Binding, Signal Transduction, QH301-705.5, Science, Chemical biology, General Biochemistry, Genetics and Molecular Biology, Viral Proteins, 03 medical and health sciences, Biochemistry and Chemical Biology, GTP-Binding Proteins, Animals, Humans, G protein-coupled receptor, CX3CL1, General Immunology and Microbiology, Chemokine CX3CL1, chemokine, E. coli, HEK293 Cells, 030104 developmental biology, Structural biology, Mutation, biology.protein
Abstract

Human cytomegalovirus has hijacked and evolved a human G-protein-coupled receptor into US28, which functions as a promiscuous chemokine 'sink’ to facilitate evasion of host immune responses. To probe the molecular basis of US28’s unique ligand cross-reactivity, we deep-sequenced CX3CL1 chemokine libraries selected on ‘molecular casts’ of the US28 active-state and find that US28 can engage thousands of distinct chemokine sequences, many of which elicit diverse signaling outcomes. The structure of a G-protein-biased CX3CL1-variant in complex with US28 revealed an entirely unique chemokine amino terminal peptide conformation and remodeled constellation of receptor-ligand interactions. Receptor signaling, however, is remarkably robust to mutational disruption of these interactions. Thus, US28 accommodates and functionally discriminates amongst highly degenerate chemokine sequences by sensing the steric bulk of the ligands, which distort both receptor extracellular loops and the walls of the ligand binding pocket to varying degrees, rather than requiring sequence-specific bonding chemistries for recognition and signaling.

Published
2018

7. Rationally designed chemokine-based toxin targeting the viral G protein-coupled receptor US28 potently inhibits cytomegalovirus infection in vivo

Author

K. Christopher Garcia, Tong Cheng, Hua Zhu, Katja Spiess, Olav Larsen, Gertrud Malene Hjortø, Mikkel Malmgaard-Clausen, Karen Krzywkowski, Michael A. Jarvis, John S Burg, Thomas N Kledal, Mads G. Jeppesen, Kalpana Dulal, and Mette M. Rosenkilde

Subjects
Human cytomegalovirus, Chemokine, Time Factors, Cell Survival, medicine.drug_class, Recombinant Fusion Proteins, viruses, Cytomegalovirus, Microbiology, Cell Line, Viral Proteins, Bacterial Proteins, SDG 3 - Good Health and Well-being, Fusion Toxin, In vivo, medicine, Humans, Viral G-Protein Coupled Receptor, Receptor, Lung, G protein-coupled receptor, Multidisciplinary, Dose-Response Relationship, Drug, biology, Chemokine CX3CL1, Fibroblasts, Biological Sciences, medicine.disease, Virology, HEK293 Cells, Drug Design, Cytomegalovirus Infections, Host-Pathogen Interactions, biology.protein, Receptors, Chemokine, Antiviral drug, Protein Binding
Abstract

The use of receptor-ligand interactions to direct toxins to kill diseased cells selectively has shown considerable promise for treatment of a number of cancers and, more recently, autoimmune disease. Here we move the fusion toxin protein (FTP) technology beyond cancer/autoimmune therapeutics to target the human viral pathogen, human cytomegalovirus (HCMV), on the basis of its expression of the 7TM G protein-coupled chemokine receptor US28. The virus origin of US28 provides an exceptional chemokine-binding profile with high selectivity and improved binding for the CX3C chemokine, CX3CL1. Moreover, US28 is constitutively internalizing by nature, providing highly effective FTP delivery. We designed a synthetic CX3CL1 variant engineered to have ultra-high affinity for US28 and greater specificity for US28 than the natural sole receptor for CX3CL1, CX3CR1, and we fused the synthetic variant with the cytotoxic domain of Pseudomonas Exotoxin A. This novel strategy of a rationally designed FTP provided unparalleled anti-HCMV efficacy and potency in vitro and in vivo.

Published
2015

8. Identification and Functional Comparison of Seven-Transmembrane G-Protein-Coupled BILF1 Receptors in Recently Discovered Nonhuman Primate Lymphocryptoviruses

Author

Alexander Hovard Sparre-Ulrich, Suzan Fares, Bernhard Ehlers, Mette M. Rosenkilde, Ellen Hilgenberg, Michael A. Jarvis, and Katja Spiess

Subjects
Primates, Genotype, Immunology, Major histocompatibility complex, Microbiology, Lymphocryptovirus, Receptors, G-Protein-Coupled, Virology, Animals, Cluster Analysis, Humans, Receptor, Phylogeny, Cellular localization, G protein-coupled receptor, Genetics, NFATC Transcription Factors, Sequence Homology, Amino Acid, biology, NF-kappa B, Genetic Variation, NFAT, biology.organism_classification, Genetic Diversity and Evolution, Insect Science, biology.protein, Signal transduction, Oncovirus, Signal Transduction
Abstract

Coevolution of herpesviruses with their respective host has resulted in a delicate balance between virus-encoded immune evasion mechanisms and host antiviral immunity. BILF1 encoded by human Epstein-Barr virus (EBV) is a 7-transmembrane (7TM) G-protein-coupled receptor (GPCR) with multiple immunomodulatory functions, including attenuation of PKR phosphorylation, activation of G-protein signaling, and downregulation of major histocompatibility complex (MHC) class I surface expression. In this study, we explored the evolutionary and functional relationships between BILF1 receptor family members from EBV and 12 previously uncharacterized nonhuman primate (NHP) lymphocryptoviruses (LCVs). Phylogenetic analysis defined 3 BILF1 clades, corresponding to LCVs of New World monkeys (clade A) or Old World monkeys and great apes (clades B and C). Common functional properties were suggested by a high degree of sequence conservation in functionally important regions of the BILF1 molecules. A subset of BILF1 receptors from EBV and LCVs from NHPs (chimpanzee, orangutan, marmoset, and siamang) were selected for multifunctional analysis. All receptors exhibited constitutive signaling activity via G protein Gαi and induced activation of the NF-κB transcription factor. In contrast, only 3 of 5 were able to activate NFAT (nuclear factor of activated T cells); chimpanzee and orangutan BILF1 molecules were unable to activate NFAT. Similarly, although all receptors were internalized, BILF1 from the chimpanzee and orangutan displayed an altered cellular localization pattern with predominant cell surface expression. This study shows how biochemical characterization of functionally important orthologous viral proteins can be used to complement phylogenetic analysis to provide further insight into diverse microbial evolutionary relationships and immune evasion function. IMPORTANCE Epstein-Barr virus (EBV), known as an oncovirus, is the only human herpesvirus in the genus Lymphocryptovirus (LCV). EBV uses multiple strategies to hijack infected host cells, establish persistent infection in B cells, and evade antiviral immune responses. As part of EBV's immune evasion strategy, the virus encodes a multifunctional 7-transmembrane (7TM) G-protein-coupled receptor (GPCR), EBV BILF1. In addition to multiple immune evasion-associated functions, EBV BILF1 has transforming properties, which are linked to its high constitutive activity. We identified BILF1 receptor orthologues in 12 previously uncharacterized LCVs from nonhuman primates (NHPs) of Old and New World origin. As 7TM receptors are excellent drug targets, our unique insight into the molecular mechanism of action of the BILF1 family and into the evolution of primate LCVs may enable validation of EBV BILF1 as a drug target for EBV-mediated diseases, as well as facilitating the design of drugs targeting EBV BILF1.

Published
2015

10. Arrestin‐independent constitutive endocytosis of GPR125/ADGRA3

Author

Riia Karoliina Junnila, Kristian H. R. Jensen, Sofie O. Bagger, Mette M. Rosenkilde, Lola Torz, Anna L. Walser, Gertrud Malene Hjortø, Katja Spiess, Jone M. Kvam, Ann-Sofie K. Møgelmose, and Viktorija Daugvilaite

Subjects
0301 basic medicine, media_common.quotation_subject, Transferrin receptor, ADGRA3, Endocytosis, Biochemistry, General Biochemistry, Genetics and Molecular Biology, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, History and Philosophy of Science, Genetics, Arrestin, Humans, GPR125, endocytosis, Internalization, Molecular Biology, media_common, G protein-coupled receptor, Orphan receptor, beta-arrestin, Chemistry, General Neuroscience, Wnt signaling pathway, Cell Biology, Original Articles, adhesion GPCR, Cell biology, internalization, HEK293 Cells, 030104 developmental biology, Original Article, Signal transduction, β‐arrestin, 030217 neurology & neurosurgery, Protein Binding, Signal Transduction
Abstract

The orphan receptor GPR125 (ADGRA3) belongs to subgroup III of the adhesion G protein−coupled receptor (aGPCR) family. aGPCRs, also known as class B2 GPCRs, share basic structural and functional properties with other GPCRs. Many of them couple to G proteins and activate G protein−dependent and −independent signaling pathways, but little is known about aGPCR internalization and β‐arrestin recruitment. GPR125 was originally described as a spermatogonial stem cell marker and studied for its role in Wnt signaling and cell polarity. Here, using cell‐based assays and confocal microscopy, we show that GPR125 is expressed on the cell surface and undergoes constitutive endocytosis in a β‐arrestin−independent, but clathrin‐dependent manner, as indicated by colocalization with transferrin receptor 1, an early endosome marker. These data support that the constitutive internalization of GPR125 contributes to its biological functions by controlling receptor surface expression and accessibility for ligands. Our study sheds light on a new property of aGPCRs, namely internalization; a property described to be important for signal propagation, signal termination, and desensitization of class A (rhodopsin‐like) and B1 (VIP/secretin) GPCRs., Here, using cell‐based assays and confocal microscopy, we show that GPR125 is expressed on the cell surface and undergoes constitutive endocytosis in a β‐arrestin−independent, but clathrin‐dependent manner, as indicated by colocalization with transferrin receptor 1, an early endosome marker. These data support that the constitutive internalization of GPR125 contributes to its biological functions by controlling receptor surface expression and accessibility for ligands.

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