Your search keyword '"Ebenhoch R"' showing total 7 results

1. Crystal structure of mKHK in complex with compound-4

Author

Ebenhoch, R., primary and Pautsch, A., additional

Published

2023

2. Cryo-EM Map of the latTGF-beta 28G11 Fab complex

Author

Ebenhoch, R., primary and Nar, H., additional

Published

2023

3. Isoquinoline small molecule ligands are agonists and probe-dependent allosteric modulators of the glucagon subfamily of GPCRs.

Author

Yuliantie E, Nh Trinh P, Hick C, Ebenhoch R, Nar H, Weichert D, Christopoulos A, M Sexton P, and Wootten D

Subjects

Humans, Ligands, Allosteric Regulation drug effects, Allosteric Regulation physiology, Glucagon-Like Peptide-1 Receptor agonists, Glucagon-Like Peptide-1 Receptor metabolism, HEK293 Cells, Animals, Cricetulus, Receptors, Gastrointestinal Hormone agonists, Receptors, Gastrointestinal Hormone metabolism, Receptors, Gastrointestinal Hormone chemistry, Small Molecule Libraries pharmacology, Small Molecule Libraries chemistry, CHO Cells, Receptors, Calcitonin agonists, Receptors, Calcitonin metabolism, Receptors, Calcitonin chemistry, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled metabolism, Receptors, G-Protein-Coupled chemistry, Glucagon metabolism, Glucagon agonists, Glucagon chemistry, Molecular Probes chemistry, Molecular Probes pharmacology, Isoquinolines pharmacology, Isoquinolines chemistry, Receptors, Glucagon agonists, Receptors, Glucagon metabolism

Abstract

Class B1 G protein-coupled receptors (GPCRs) are peptide hormone receptors and well validated therapeutic targets, however development of non-peptide drugs targeting this class of receptors is challenging. Recently, a series of isoquinoline-based derivates were reported in the patent literature as allosteric ligands for the glucagon receptor subfamily, and two compounds, LSN3451217 and LSN3556672, were used to facilitate structural studies with the glucagon-like peptide-1 receptor (GLP-1R) and glucose dependent insulinotropic peptide receptor (GIPR) bound to orthosteric agonists. Here we pharmacologically characterized stereoisomers of LSN3451217 and LSN3556672, across the class B1 GPCR family. This revealed LSN3556672 isomers are agonists for the glucagon receptor (GCGR), GLP-1R, GIPR and the calcitonin receptor (CTR), albeit the degree of agonism varied at each receptor. In contrast, LSN3451217 isomers were more selective agonists at the GLP-1R, with lower potency at the GCGR and CTR and no activity at the GIPR. All compounds also modulated peptide-mediated cyclic adenosine monophosphate (cAMP) signaling at the GIPR, and to a lesser extent the GLP-1R, in a probe-dependent manner, with modest positive allosteric modulation observed for some peptides, and negligible effects observed with other peptides. In contrast neutral or weak negative/positive allosteric modulation was observed with peptides assessed at the GCGR and CTR. This study expands our knowledge on class B1 GPCR allosteric modulation and may have implications for future structural and drug discovery efforts targeting the class B1 GPCR subfamily., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: D.Wootten, P.M.S and A.C are co-founders of DACRA therapeutics. P.M.S and A.C are co-founders and scientific advisors, and D.W is a scientific advisory board member for Septerna Inc. R.E., H.N., D. Weichert are employees of Boehringer Ingelheim., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

4. Discovery of BI-9787, a potent zwitterionic ketohexokinase inhibitor with oral bioavailability.

Author

Heine N, Weber A, Pautsch A, Gottschling D, Uphues I, Bauer M, Ebenhoch R, Magarkar A, Nosse B, and Kley JT

Subjects

Animals, Rats, Administration, Oral, Humans, Structure-Activity Relationship, Drug Discovery, Molecular Structure, Dose-Response Relationship, Drug, Fructokinases antagonists & inhibitors, Fructokinases metabolism, Biological Availability, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics

Abstract

Fructose metabolism by ketohexokinase (KHK) is implicated in a variety of metabolic disorders. KHK inhibition is a potential therapeutic strategy for the treatment of diseases including diabetes, non-alcoholic fatty liver disease, and non-alcoholic steatohepatitis. The first small-molecule KHK-inhibitors have entered clinical trials, but it remains unclear if systemic inhibition of KHK by small-molecules will eventually benefit patients. Here we report the discovery of BI-9787, a potent, zwitterionic KHK inhibitor characterized by high permeability and favorable oral rat pharmacokinetics. BI-9787 was identified by optimizing chemical starting points generated via a ligand-based virtual screening of Boehringer's virtual library of synthetically accessible compounds (BICLAIM). It serves as a high-quality in vitro and in vivo tool compound for investigating the role of fructose metabolism in disease., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Bernd Nosse is an employee of Boehringer Ingelheim International. All other authors are employees of Boehringer Ingelheim Pharma GmbH & Co KG, which funded the research., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

5. Crystal structures of human and mouse ketohexokinase provide a structural basis for species- and isoform-selective inhibitor design.

Author

Ebenhoch R, Bauer M, Romig H, Gottschling D, Kley JT, Heine N, Weber A, Uphues I, Nar H, and Pautsch A

Abstract

A molecular understanding of the proteins involved in fructose metabolism is essential for controlling the current spread of fructose-related obesity, diabetes and related adverse metabolic states in Western populations. Fructose catabolism starts with the phosphorylation of D-fructose to fructose 1-phosphate by ketohexokinase (KHK). KHK exists in two alternatively spliced isoforms: the hepatic and intestinal isoform KHK-C and the peripheral isoform KHK-A. Here, the structure of apo murine KHK (mKHK), which differs from structures of human KHK in overall conformation, is reported. An isoform-selective ligand, which offers a 50-fold higher potency on mKHK and human KHK-A compared with KHK-C, is further characterized. In mKHK, large-scale conformational changes are observed upon ligand binding. The structures suggest a combined strategy for the design of species- and isoform-selective KHK inhibitors.

Published

2023

6. Anti-GARP Antibodies Inhibit Release of TGF-β by Regulatory T Cells via Different Modes of Action, but Do Not Influence Their Function In Vitro.

Author

Igney FH, Ebenhoch R, Schiele F, and Nar H

Subjects

Humans, Membrane Proteins immunology, Receptors, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta1 metabolism, T-Lymphocytes, Regulatory, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta pharmacology, Antibodies pharmacology

Abstract

Regulatory T cells (Treg) play a critical role in controlling immune responses in diseases such as cancer or autoimmunity. Activated Treg express the membrane protein GARP (LRRC32) in complex with the latent form of the immunosuppressive cytokine TGF-β (L-TGF-β). In this study, we confirmed that active TGF-β was generated from its latent form in an integrin-dependent manner and induced TGF-β receptor signaling in activated human Treg. We studied a series of Abs targeting the L-TGF-β/GARP complex with distinct binding modes. We found that TGF-β receptor signaling could be inhibited by anti-TGF-β and by some, but not all, Abs against the L-TGF-β/GARP complex. Cryogenic electron microscopy structures of three L-TGF-β/GARP complex-targeting Abs revealed their distinct epitopes and allowed us to elucidate how they achieve blockade of TGF-β activation. Three different modes of action were identified, including a novel unusual mechanism of a GARP-binding Ab. However, blockade of GARP or TGF-β by Abs did not influence the suppressive activity of human Treg in vitro. We were also not able to confirm a prominent role of GARP in other functions of human Treg, such as FOXP3 induction and Treg stability. These data show that the GARP/TGF-β axis can be targeted pharmacologically in different ways, but further studies are necessary to understand its complexity and to unleash its therapeutic potential., (Copyright © 2023 The Authors.)

Published

2023

7. Crystallization and preliminary X-ray analysis of the C-type lectin domain of the spicule matrix protein SM50 from Strongylocentrotus purpuratus. Corrigendum.

Author

Ebenhoch R, Juneja P, Rao A, Cölfen H, Diederichs K, and Welte W

Abstract

The identity of the crystallized protein in the article by Juneja et al. [(2014), Acta Cryst. F70, 260-262] is corrected.

Published

2022