Your search keyword '"Matthias P Müller"' showing total 50 results

1. Targeting oncogenic KRasG13C with nucleotide-based covalent inhibitors

Author

Lisa Goebel, Tonia Kirschner, Sandra Koska, Amrita Rai, Petra Janning, Stefano Maffini, Helge Vatheuer, Paul Czodrowski, Roger S Goody, Matthias P Müller, and Daniel Rauh

Subjects

cancer, Ras, G13C, nucleotide analogues, covalent inhibitors, Medicine, Science, Biology (General), QH301-705.5

Abstract

Mutations within Ras proteins represent major drivers in human cancer. In this study, we report the structure-based design, synthesis, as well as biochemical and cellular evaluation of nucleotide-based covalent inhibitors for KRasG13C, an important oncogenic mutant of Ras that has not been successfully addressed in the past. Mass spectrometry experiments and kinetic studies reveal promising molecular properties of these covalent inhibitors, and X-ray crystallographic analysis has yielded the first reported crystal structures of KRasG13C covalently locked with these GDP analogues. Importantly, KRasG13C covalently modified with these inhibitors can no longer undergo SOS-catalysed nucleotide exchange. As a final proof-of-concept, we show that in contrast to KRasG13C, the covalently locked protein is unable to induce oncogenic signalling in cells, further highlighting the possibility of using nucleotide-based inhibitors with covalent warheads in KRasG13C-driven cancer.

Published

2023

2. Design and synthesis of Nrf2-derived hydrocarbon stapled peptides for the disruption of protein-DNA-interactions.

Author

Bianca Wiedemann, Dominic Kamps, Laura Depta, Jörn Weisner, Jana Cvetreznik, Stefano Tomassi, Sascha Gentz, Jan-Erik Hoffmann, Matthias P Müller, Oliver Koch, Leif Dehmelt, and Daniel Rauh

Subjects

Medicine, Science

Abstract

Misregulation and mutations of the transcription factor Nrf2 are involved in the development of a variety of human diseases. In this study, we employed the technology of stapled peptides to address a protein-DNA-complex and designed a set of Nrf2-based derivatives. Varying the length and position of the hydrocarbon staple, we chose the best peptide for further evaluation in both fixed and living cells. Peptide 4 revealed significant enrichment within the nucleus compared to its linear counterpart 5, indicating potent binding to DNA. Our studies suggest that these molecules offer an interesting strategy to target activated Nrf2 in cancer cells.

Published

2022

3. Structure-based design, synthesis and crystallization of 2-arylquinazolines as lipid pocket ligands of p38α MAPK.

Author

Mike Bührmann, Bianca M Wiedemann, Matthias P Müller, Julia Hardick, Maria Ecke, and Daniel Rauh

Subjects

Medicine, Science

Abstract

In protein kinase research, identifying and addressing small molecule binding sites other than the highly conserved ATP-pocket are of intense interest because this line of investigation extends our understanding of kinase function beyond the catalytic phosphotransfer. Such alternative binding sites may be involved in altering the activation state through subtle conformational changes, control cellular enzyme localization, or in mediating and disrupting protein-protein interactions. Small organic molecules that target these less conserved regions might serve as tools for chemical biology research and to probe alternative strategies in targeting protein kinases in disease settings. Here, we present the structure-based design and synthesis of a focused library of 2-arylquinazoline derivatives to target the lipophilic C-terminal binding pocket in p38α MAPK, for which a clear biological function has yet to be identified. The interactions of the ligands with p38α MAPK was analyzed by SPR measurements and validated by protein X-ray crystallography.

Published

2017

4. bMERB domains are bivalent Rab8 family effectors evolved by gene duplication

Author

Amrita Rai, Anastasia Oprisko, Jeremy Campos, Yangxue Fu, Timon Friese, Aymelt Itzen, Roger S Goody, Emerich Mihai Gazdag, and Matthias P Müller

Subjects

Rab effectors, Mical, EHBP, Medicine, Science, Biology (General), QH301-705.5

Abstract

In their active GTP-bound form, Rab proteins interact with proteins termed effector molecules. In this study, we have thoroughly characterized a Rab effector domain that is present in proteins of the Mical and EHBP families, both known to act in endosomal trafficking. Within our study, we show that these effectors display a preference for Rab8 family proteins (Rab8, 10, 13 and 15) and that some of the effector domains can bind two Rab proteins via separate binding sites. Structural analysis allowed us to explain the specificity towards Rab8 family members and the presence of two similar Rab binding sites that must have evolved via gene duplication. This study is the first to thoroughly characterize a Rab effector protein that contains two separate Rab binding sites within a single domain, allowing Micals and EHBPs to bind two Rabs simultaneously, thus suggesting previously unknown functions of these effector molecules in endosomal trafficking.

Published

2016

5. F<scp>ragtory</scp>: Pharmacophore-Focused Design, Synthesis, and Evaluation of an sp3-Enriched Fragment Library

Author

Mike Bührmann, Shivakrishna Kallepu, Jonas D. Warmuth, Jan N. Wiese, Christiane Ehrt, Helge Vatheuer, Wolf Hiller, Carina Seitz, Laura Levy, Paul Czodrowski, Sonja Sievers, Matthias P. Müller, and Daniel Rauh

Subjects

Drug Discovery, Molecular Medicine

Published

2023

6. Addressing the Osimertinib Resistance Mutation EGFR-L858R/C797S with Reversible Aminopyrimidines

Author

Tobias Grabe, Kirujan Jeyakumar, Janina Niggenaber, Tom Schulz, Sandra Koska, Silke Kleinbölting, Michael Edmund Beck, Matthias P. Müller, and Daniel Rauh

Subjects

Organic Chemistry, Drug Discovery, Biochemistry

Published

2023

7. Optimization of Covalent MKK7 Inhibitors via Crude Nanomole-Scale Libraries

Author

Paul Gehrtz, Shir Marom, Mike Bührmann, Julia Hardick, Silke Kleinbölting, Amit Shraga, Christian Dubiella, Ronen Gabizon, Jan N. Wiese, Matthias P. Müller, Galit Cohen, Ilana Babaev, Khriesto Shurrush, Liat Avram, Efrat Resnick, Haim Barr, Daniel Rauh, and Nir London

Subjects

Drug Discovery, Molecular Medicine

Published

2022

8. Insight into Targeting Exon20 Insertion Mutations of the Epidermal Growth Factor Receptor with Wild Type-Sparing Inhibitors

Author

Jonas Lategahn, Hannah L. Tumbrink, Carsten Schultz-Fademrecht, Alena Heimsoeth, Lisa Werr, Janina Niggenaber, Marina Keul, Fatma Parmaksiz, Matthias Baumann, Sascha Menninger, Eldar Zent, Ina Landel, Jörn Weisner, Kirujan Jeyakumar, Leonie Heyden, Nicole Russ, Fabienne Müller, Carina Lorenz, Johannes Brägelmann, Inga Spille, Tobias Grabe, Matthias P. Müller, Johannes M. Heuckmann, Bert M. Klebl, Peter Nussbaumer, Martin L. Sos, and Daniel Rauh

Subjects

Mice, Mutagenesis, Insertional, Lung Neoplasms, Carcinoma, Non-Small-Cell Lung, Mutation, Drug Discovery, Animals, Humans, Molecular Medicine, Protein Kinase Inhibitors

Abstract

Despite the clinical efficacy of epidermal growth factor receptor (EGFR) inhibitors, a subset of patients with non-small cell lung cancer displays insertion mutations in exon20 in EGFR and Her2 with limited treatment options. Here, we present the development and characterization of the novel covalent inhibitors LDC8201 and LDC0496 based on a 1

Published

2022

9. Author response: Targeting oncogenic KRasG13C with nucleotide-based covalent inhibitors

Author

Lisa Goebel, Tonia Kirschner, Sandra Koska, Amrita Rai, Petra Janning, Stefano Maffini, Helge Vatheuer, Paul Czodrowski, Roger S Goody, Matthias P Müller, and Daniel Rauh

Published

2023

10. Disturbance feedback-based model predictive control in uncertain dynamic environments

Author

Philipp, Buschermöhle, Taouba, Jouini, Torsten, Lilge, and Matthias, A. Müller

Abstract

This paper presents a robust MPC scheme for linear systems subject to time-varying, uncertain constraints that arise from uncertain environments. The predicted input sequence is parameterized over future environment states to guarantee constraint satisfaction despite an imprecise environment prediction and unknown evolution of the future constraints. We provide theoretical guarantees for recursive feasibility and asymptotic convergence. Finally a brief simulation example showcases our results.

Published

2024

11. Targeting oncogenic KRasG13C with nucleotide-based covalent inhibitors

Author

Lisa Goebel, Tonia Kirschner, Sandra Koska, Amrita Rai, Petra Janning, Stefano Maffini, Helge Vatheuer, Paul Czodrowski, Roger S. Goody, Matthias P. Müller, and Daniel Rauh

Subjects

General Immunology and Microbiology, General Neuroscience, General Medicine, General Biochemistry, Genetics and Molecular Biology

Abstract

Mutations within Ras proteins represent major drivers in human cancer. In this study, we report the structure-based design, synthesis, as well as biochemical and cellular evaluation of nucleotide-based covalent inhibitors for KRasG13C, an important oncogenic mutant of Ras that has not been successfully addressed in the past. Mass spectrometry experiments and kinetic studies reveal promising molecular properties of these covalent inhibitors, and X-ray crystallographic analysis has yielded the first reported crystal structures of KRasG13C covalently locked with these GDP analogues. Importantly, KRasG13C covalently modified with these inhibitors can no longer undergo SOS-catalysed nucleotide exchange. As a final proof-of-concept, we show that in contrast to KRasG13C, the covalently locked protein is unable to induce oncogenic signalling in cells, further highlighting the possibility of using nucleotide-based inhibitors with covalent warheads in KRasG13C-driven cancer., eLife;Vol. 12 2023, Artikel-ID: e82184

Published

2022

12. Complex Crystal Structures of EGFR with Third-Generation Kinase Inhibitors and Simultaneously Bound Allosteric Ligands

Author

Daniel Rauh, Matthias P. Müller, Jonas Lategahn, Tobias Grabe, Janina Niggenaber, and Leonie Heyden

Subjects

biology, 010405 organic chemistry, Chemistry, Kinase, medicine.drug_class, Organic Chemistry, Allosteric regulation, Resistance mutation, 01 natural sciences, Biochemistry, Tyrosine-kinase inhibitor, respiratory tract diseases, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Structural biology, Drug Discovery, medicine, Cancer research, biology.protein, Osimertinib, Epidermal growth factor receptor, Mode of action

Abstract

[Image: see text] Osimertinib is a third-generation tyrosine kinase inhibitor (TKI) and currently the gold-standard for the treatment of patients suffering from non-small cell lung cancer (NSCLC) harboring T790M-mutated epidermal growth factor receptor (EGFR). The outcome of the treatment, however, is limited by the emergence of the C797S resistance mutation. Allosteric inhibitors have a different mode of action and were developed to overcome this limitation. However, most of these innovative molecules are not effective as a single agent. Recently, mutated EGFR was successfully addressed with osimertinib combined with the allosteric inhibitor JBJ-04-125-02, but surprisingly, structural insights into their binding mode were lacking. Here, we present the first complex crystal structures of mutant EGFR in complex with third-generation inhibitors such as osimertinib and mavelertinib in the presence of simultaneously bound allosteric inhibitors. These structures highlight the possibility of further combinations targeting EGFR and lay the foundation for hybrid inhibitors as next-generation TKIs.

Published

2020

13. Targeting Her2-insYVMA with Covalent Inhibitors—A Focused Compound Screening and Structure-Based Design Approach

Author

Philip Klövekorn, Jonas Lategahn, Willem A. L. van Otterlo, Julia Hardick, Tobias Grabe, Daniel Rauh, Luke Hodson, Matthias P. Müller, Tonia Kirschner, Kirujan Jeyakumar, Matthias Baumann, Julia Ketzer, Sebastian Bauer, Susanne Terheyden, Janina Niggenaber, Christian Becker, Anke Unger, Hannah L. Tumbrink, Jörn Weisner, and Marina Keul

Subjects

Models, Molecular, Receptor, ErbB-2, Mutant, Drug Evaluation, Preclinical, Medizin, 01 natural sciences, Structure-Activity Relationship, 03 medical and health sciences, Western blot, Drug Discovery, Tumor Cells, Cultured, medicine, Humans, Structure–activity relationship, Pyrroles, Epidermal growth factor receptor, Binding site, Structural motif, Protein Kinase Inhibitors, 030304 developmental biology, 0303 health sciences, Dose-Response Relationship, Drug, Molecular Structure, medicine.diagnostic_test, biology, Chemistry, Receptor–ligand kinetics, 0104 chemical sciences, Kinetics, 010404 medicinal & biomolecular chemistry, Pyrimidines, Biochemistry, Drug Design, biology.protein, Molecular Medicine, Cysteine

Abstract

Mutated or amplified Her2 serves as a driver of non-small cell lung cancer or mediates resistance toward the inhibition of its family member epidermal growth factor receptor with small-molecule inhibitors. To date, small-molecule inhibitors targeting Her2 which can be used in clinical routine are lacking, and therefore, the development of novel inhibitors was undertaken. In this study, the well-established pyrrolopyrimidine scaffold was modified with structural motifs identified from a screening campaign with more than 1600 compounds, which were applied against wild-type Her2 and its mutant variant Her2-A775_G776insYVMA. The resulting inhibitors were designed to covalently target a reactive cysteine in the binding site of Her2 and were further optimized by means of structure-based drug design utilizing a set of obtained complex crystal structures. In addition, the analysis of binding kinetics and absorption, distribution, metabolism, and excretion parameters as well as mass spectrometry experiments and western blot analysis substantiated our approach.

Published

2020

14. Front Cover: Covalent Allosteric Inhibitors of Akt Generated Using a Click Fragment Approach (ChemMedChem 10/2022)

Author

Leandi Westhuizen, Jörn Weisner, Abu Taher, Ina Landel, Lena Quambusch, Marius Lindemann, Niklas Uhlenbrock, Matthias P. Müller, Ivan R. Green, Stephen C. Pelly, Daniel Rauh, and Willem A. L. Otterlo

Subjects

Pharmacology, Organic Chemistry, Drug Discovery, Molecular Medicine, General Pharmacology, Toxicology and Pharmaceutics, Biochemistry

Published

2022

15. Covalent Allosteric Inhibitors of Akt Generated Using a Click Fragment Approach

Author

Leandi Westhuizen, Jörn Weisner, Abu Taher, Ina Landel, Lena Quambusch, Marius Lindemann, Niklas Uhlenbrock, Matthias P. Müller, Ivan R. Green, Stephen C. Pelly, Daniel Rauh, and Willem A. L. Otterlo

Subjects

Pharmacology, Structure-Activity Relationship, Allosteric Regulation, Organic Chemistry, Drug Discovery, Molecular Medicine, General Pharmacology, Toxicology and Pharmaceutics, Biochemistry, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-akt

Abstract

Akt is a protein kinase that has been implicated in the progression of cancerous tumours. A number of covalent allosteric Akt inhibitors are known, and based on these scaffolds, a small library of novel potential covalent allosteric imidazopyridine-based inhibitors was designed. The envisaged compounds were synthesised, with click chemistry enabling a modular approach to a number of the target compounds. The binding modes, potencies and antiproliferative activities of these synthesised compounds were explored, thereby furthering the structure activity relationship knowledge of this class of Akt inhibitors. Three novel covalent inhibitors were identified, exhibiting moderate activity against Akt1 and various cancer cell lines, potentially paving the way for future covalent allosteric inhibitors with improved properties.

Published

2022

16. Covalent‐Allosteric Inhibitors to Achieve Akt Isoform‐Selectivity

Author

Niklas Uhlenbrock, Laura Depta, Jens T. Siveke, Jörn Weisner, Franziska Glanemann, Matthias P. Müller, Daniel Rauh, Lena Quambusch, Kristina Althoff, and Ina Landel

Subjects

Gene isoform, Allosteric regulation, Medizin, Isoform selectivity, 010402 general chemistry, 01 natural sciences, Catalysis, Covalent inhibitors, Structure-Activity Relationship, Allosteric Regulation, Akt isoforms, Transferase, Humans, Protein Isoforms, Protein kinase A, Allosteric sites, Protein kinase B, Cancer, 010405 organic chemistry, Chemistry, Cell growth, Kinase, Communication, General Chemistry, General Medicine, Small molecule, Communications, 0104 chemical sciences, Biochemistry, Drug Design, Proto-Oncogene Proteins c-akt, Allosteric Site

Abstract

Isoforms of protein kinase Akt are involved in essential processes including cell proliferation, survival, and metabolism. However, their individual roles in health and disease have not been thoroughly evaluated. Thus, there is an urgent need for perturbation studies, preferably mediated by highly selective bioactive small molecules. Herein, we present a structure‐guided approach for the design of structurally diverse and pharmacologically beneficial covalent‐allosteric modifiers, which enabled an investigation of the isoform‐specific preferences and the important residues within the allosteric site of the different isoforms. The biochemical, cellular, and structural evaluations revealed interactions responsible for the selective binding profiles. The isoform‐selective covalent‐allosteric Akt inhibitors that emerged from this approach showed a conclusive structure–activity relationship and broke ground in the development of selective probes to delineate the isoform‐specific functions of Akt kinases., Akt now! A structure and homology model guided approach for the design of diverse and pharmacologically beneficial covalent‐allosteric modifiers for protein kinase Akt is presented. The isoform‐selective Akt inhibitors show a conclusive structure–activity relationship and break ground for further development of selective probes for the dissection of Akt isoform‐specific functions.

Published

2019

17. Inhibition of osimertinib-resistant epidermal growth factor receptor EGFR-T790M/C797S

Author

Janina Niggenaber, Matthias Baumann, Sebastian Bauer, Heiko Muller, Tobias Grabe, Jan G. Hengstler, Marina Keul, Luke Hodson, Georgia Günther, Anke Unger, Bernhard Blank-Landeshammer, Daniel Rauh, Alena Heimsoeth, Hannah L. Tumbrink, Julia Ketzer, Christopher Golz, Matthias P. Müller, René P. Zahedi, Carsten Strohmann, Wolf Hiller, Julian Engel, Willem A. L. van Otterlo, Julia Hardick, Philip Klövekorn, Jonas Lategahn, Maren Flaßhoff, Laxmikanth Kollipara, Carsten Schultz-Fademrecht, and Thomas Mühlenberg

Subjects

biology, medicine.diagnostic_test, 010405 organic chemistry, Chemistry, Kinase, Mutant, Medizin, General Chemistry, Drug resistance, 010402 general chemistry, 01 natural sciences, Receptor–ligand kinetics, respiratory tract diseases, 0104 chemical sciences, T790M, Western blot, Cancer research, biology.protein, medicine, Osimertinib, Epidermal growth factor receptor

Abstract

We present inhibitors of drug resistant mutants of EGFR including T790M and C797S. In addition, we present the first X-ray crystal structures of covalent inhibitors in complex with C797S-mutated EGFR to gain insight into their binding mode., Precision medicine has revolutionized the treatment of patients in EGFR driven non-small cell lung cancer (NSCLC). Targeted drugs show high response rates in genetically defined subsets of cancer patients and markedly increase their progression-free survival as compared to conventional chemotherapy. However, recurrent acquired drug resistance limits the success of targeted drugs in long-term treatment and requires the constant development of novel efficient inhibitors of drug resistant cancer subtypes. Herein, we present covalent inhibitors of the drug resistant gatekeeper mutant EGFR-L858R/T790M based on the pyrrolopyrimidine scaffold. Biochemical and cellular characterization, as well as kinase selectivity profiling and western blot analysis, substantiate our approach. Moreover, the developed compounds possess high activity against multi drug resistant EGFR-L858R/T790M/C797S in biochemical assays due to their highly reversible binding character, that was revealed by characterization of the binding kinetics. In addition, we present the first X-ray crystal structures of covalent inhibitors in complex with C797S-mutated EGFR which provide detailed insight into their binding mode.

Published

2019

18. KRasG12C inhibitors in clinical trials: a short historical perspective

Author

Lisa Goebel, Daniel Rauh, Matthias P. Müller, and Roger S. Goody

Subjects

Pharmaceutical Science, medicine.disease_cause, Biochemistry, Approved drug, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, medicine, 030304 developmental biology, Pharmacology, 0303 health sciences, Ras oncogenes, Oncogene, business.industry, Organic Chemistry, Cancer, medicine.disease, Clinical trial, Chemistry, Direct targeting, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, KRAS, business, Human cancer

Abstract

Short historical perspective of the development of promising KRasG12C inhibitors that have recently entered clinical trials., KRas is the most frequently mutated oncogene in human cancer, and even 40 years after the initial discovery of Ras oncogenes in 1982, no approved drug directly targets Ras in Ras-driven cancer. New information and approaches for direct targeting of mutant Ras have fueled hope for the development of direct KRas inhibitors. In this review, we provide a comprehensive historical perspective of the development of promising KRasG12C inhibitors that covalently bind to the mutated cysteine residue in the switch-II pocket and trap the protein in the inactive GDP bound state. After decades of failure, three covalent G12C-specific inhibitors from three independent companies have recently entered clinical trials and therefore represent new hope for patients suffering from KRasG12C driven cancer.

Published

2020

19. Proximitäts-vermittelte kovalente Stabilisierung niedrig-affiner Proteinkomplexe in vitro und in vivo

Author

Aymelt Itzen, Kathrin Lang, Maximilian Fottner, Thorsten G. Müller, Roger S. Goody, Daniel Horn-Ghetko, Matthias P. Müller, Marko Cigler, and Marie-Kristin von Wrisberg

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Chemistry, General Medicine, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences

Published

2017

20. Proximity-Triggered Covalent Stabilization of Low-Affinity Protein Complexes In Vitro and In Vivo

Author

Marko Cigler, Matthias P. Müller, Kathrin Lang, Maximilian Fottner, Thorsten G. Müller, Roger S. Goody, Marie-Kristin von Wrisberg, Aymelt Itzen, and Daniel Horn-Ghetko

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, Green Fluorescent Proteins, Mutant, Catalysis, Protein–protein interaction, Amino Acyl-tRNA Synthetases, Nucleotide exchange factor, 03 medical and health sciences, GTP-Binding Protein Regulators, GTP-Binding Proteins, In vivo, Humans, Amino Acids, chemistry.chemical_classification, Protein Stability, Chemistry, General Chemistry, In vitro, Amino acid, HEK293 Cells, 030104 developmental biology, Covalent bond, Mutation, Transfer RNA, Protein Binding

Abstract

The characterization of low-affinity protein complexes is challenging due to their dynamic nature. Here, we present a method to stabilize transient protein complexes in vivo by generating a covalent and conformationally flexible bridge between the interaction partners. A highly active pyrrolysyl tRNA synthetase mutant directs the incorporation of unnatural amino acids bearing bromoalkyl moieties (BrCnK) into proteins. We demonstrate for the first time that low-affinity protein complexes between BrCnK-containing proteins and their binding partners can be stabilized in vivo in bacterial and mammalian cells. Using this approach, we determined the crystal structure of a transient GDP-bound complex between a small G-protein and its nucleotide exchange factor. We envision that this approach will prove valuable as a general tool for validating and characterizing protein-protein interactions in vitro and in vivo.

Published

2017

21. 2-Azo-, 2-diazocine-thiazols and 2-azo-imidazoles as photoswitchable kinase inhibitors: limitations and pitfalls of the photoswitchable inhibitor approach

Author

Miriam Schehr, Chiara Lanes, Jörn Weisner, Linda Heintze, Matthias P. Müller, Christian Pichlo, Julia Charl, Elena Brunstein, Julia Ewert, Marc Lehr, Ulrich Baumann, Daniel Rauh, Uwe Knippschild, Christian Peifer, and Rainer Herges

Subjects

Mitogen-Activated Protein Kinase 14, Models, Molecular, Structure-Activity Relationship, Thiazoles, Dose-Response Relationship, Drug, Molecular Structure, Casein Kinase Idelta, Imidazoles, Physical and Theoretical Chemistry, Ligands, Photochemical Processes, Azocines, Protein Kinase Inhibitors

Abstract

In photopharmacology, photoswitchable compounds including azobenzene or other diarylazo moieties exhibit bioactivity against a target protein typically in the slender E-configuration, whereas the rather bulky Z-configuration usually is pharmacologically less potent. Herein we report the design, synthesis and photochemical/inhibitory characterization of new photoswitchable kinase inhibitors targeting p38α MAPK and CK1δ. A well characterized inhibitor scaffold was used to attach arylazo- and diazocine moieties. When the isolated isomers, or the photostationary state (PSS) of isomers, were tested in commonly used in vitro kinase assays, however, only small differences in activity were observed. X-ray analyses of ligand-bound p38α MAPK and CK1δ complexes revealed dynamic conformational adaptations of the protein with respect to both isomers. More importantly, irreversible reduction of the azo group to the corresponding hydrazine was observed. Independent experiments revealed that reducing agents such as DTT (dithiothreitol) and GSH (glutathione) that are typically used for protein stabilization in biological assays were responsible. Two further sources of error are the concentration dependence of the E-Z-switching efficiency and artefacts due to incomplete exclusion of light during testing. Our findings may also apply to a number of previously investigated azobenzene-based photoswitchable inhibitors.

Published

2019

22. Mutant-Specific Targeting of Ras G12C Activity by Covalently Reacting Small Molecules

Author

Matthias P. Müller, Daniel Rauh, and Roger S. Goody

Subjects

GTP', Clinical Biochemistry, Mutant, GTPase, Guanosine triphosphate, Biology, 01 natural sciences, Biochemistry, Guanosine Diphosphate, Small Molecule Libraries, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Binding site, Molecular Biology, Pharmacology, Guanine binding, Binding Sites, 010405 organic chemistry, 0104 chemical sciences, chemistry, Guanosine diphosphate, ras Proteins, Molecular Medicine, Guanine nucleotide exchange factor, Guanosine Triphosphate

Abstract

In this review we discuss and compare recently introduced molecules that are able to react covalently with an oncogenic mutant of KRas, KRas G12C. Two different classes of compounds in question have been developed, both leading to the mutant being locked in the inactive (guanosine diphosphate [GDP]-bound) state. The first are compounds that interact reversibly with the switch-II pocket (S-IIP) before covalent interaction. The second class interact in a competitive manner with the GDP/guanosine triphosphate (GTP) binding site. The fundamental physico-chemical principles of the two inhibitor classes are evaluated. For GDP/GTP-competing molecules, we show that special attention must be paid to the influence of guanine nucleotide exchange factors (GEFs) and their elevated activity in cells harboring abnormally activated Ras mutants. A new approach is suggested involving compounds that interact with the guanine binding site of the GTPase, but in a manner that is independent of the interaction of the GTPase with its cognate GEF.

Published

2019

23. Molecular control of Rab activity by GEFs, GAPs and GDI

Author

Roger S. Goody and Matthias P. Müller

Subjects

0301 basic medicine, GTPase-activating protein, intracellular trafficking, GDI, Protein Prenylation, Review, Biology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Prenylation, GAPS, vesicular transport, Animals, Guanine Nucleotide Exchange Factors, Humans, Amino Acid Sequence, Guanine Nucleotide Dissociation Inhibitors, Effector, Cell Membrane, GTPase-Activating Proteins, fungi, GEFs, Cell Biology, Cell biology, Vesicular transport protein, 030104 developmental biology, Rab proteins, rab GTP-Binding Proteins, posttranslational modifications, Rab, Guanine nucleotide exchange factor, 030217 neurology & neurosurgery, Cysteine

Abstract

Rab proteins are the major regulators of vesicular trafficking in eukaryotic cells. Their activity can be tightly controlled within cells: Regulated by guanine nucleotide exchange factors (GEFs) and GTPase activating proteins (GAPs), they switch between an active GTP-bound state and an inactive GDP-bound state, interacting with downstream effector proteins only in the active state. Additionally, they can bind to membranes via C-terminal prenylated cysteine residues and they can be solubilized and shuttled between membranes by chaperone-like molecules called GDP dissociation inhibitors (GDIs). In this review we give an overview of Rab proteins with a focus on the current understanding of their regulation by GEFs, GAPs and GDI.

Published

2017

24. Multivalency in Rab effector interactions

Author

Amrita Rai, Matthias P. Müller, and Roger S. Goody

Subjects

Mini-Review - Commissioned, Protein Conformation, Biology, Biochemistry, Gcc185, 03 medical and health sciences, 0302 clinical medicine, Micals, Rab effectors, 030304 developmental biology, 0303 health sciences, Effector, EHBPs, fungi, MyoV, Cell Biology, multivalency, Rabenosyn-5, Cell biology, Vesicular transport protein, rab GTP-Binding Proteins, 030220 oncology & carcinogenesis, bMERB, Rab, RABENOSYN 5

Abstract

Rab proteins regulate vesicular transport in eukaryotic cells and establish connections to various cellular structures and processes by interacting with so-called effector molecules. Several of these effectors are known to not only bind a single Rab protein, but to be able to bind multiple different Rabs simultaneously. In this review we will give a short overview of effectors in general and (putative) functions of the aforementioned multivalent Rab:effector interactions.

Published

2017

25. Mechanisms of action of Rab proteins, key regulators of intracellular vesicular transport

Author

Roger S. Goody, Yao-Wen Wu, and Matthias P. Müller

Subjects

0301 basic medicine, Bacteria, Effector, Clinical Biochemistry, Cell, Chemical biology, GTPase, Biology, Biochemistry, Cell biology, Vesicular transport protein, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, rab GTP-Binding Proteins, medicine, Humans, Rab, Transport Vesicles, Molecular Biology, Intracellular

Abstract

Our understanding of the manner in which Rab proteins regulate intracellular vesicular transport has progressed remarkably in the last one or two decades by application of a wide spectrum of biochemical, biophysical and cell biological methods, augmented by the methods of chemical biology. Important additional insights have arisen from examination of the manner in which certain bacteria can manipulate vesicular transport mechanisms. The progress in these areas is summarized here.

Published

2016

26. Try Me: Promiscuous Inhibitors Still Allow for Selective Targeted Protein Degradation

Author

Matthias P. Müller and Daniel Rauh

Subjects

0301 basic medicine, Pharmacology, medicine.diagnostic_test, 010405 organic chemistry, Proteolysis, Clinical Biochemistry, Cell, Chemical biology, Proteins, Computational biology, Protein degradation, Biology, 01 natural sciences, Biochemistry, Article, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Drug Discovery, medicine, Molecular Medicine, Molecular Biology, Cellular proteins

Abstract

Inhibiting protein function selectively is a major goal of modern drug discovery. Here, we report a previously understudied benefit of small molecule Proteolysis Targeting Chimera (PROTACs) that recruit E3 ubiquitin ligases to target proteins for their ubiquitination and subsequent proteasome-mediated degradation. Using promiscuous CRBN- and VHL-recruiting PROTACs that bind >100 kinases, we show that only a subset of bound targets is degraded. The basis of this selectivity relies on protein-protein interactions between the E3 ubiquitin ligase and the target protein, as illustrated by engaged proteins that are not degraded as a result of unstable ternary complexes with PROTAC-recruited E3 ligases. In contrast, weak PROTAC:target protein affinity can be stabilized by high affinity target:PROTAC:ligase trimer interactions, leading to efficient degradation. This study highlights design guidelines for generating potent PROTACs as well as possibilities for degrading undruggable proteins immune to traditional small molecule inhibitors.

Published

2018

27. Preclinical Efficacy of Covalent-Allosteric AKT Inhibitor Borussertib in Combination with Trametinib in KRAS-Mutant Pancreatic and Colorectal Cancer

Author

Stephan A. Hahn, Niklas Dienstbier, Julia Hardick, Swetlana Ladigan, Anke Unger, Jan G. Hengstler, Heiner Wolters, Niklas Uhlenbrock, Heiko Muller, Rajesh Gontla, Daniel Rauh, Rebekka Scheinpflug, Richard Viebahn, Carsten Schultz-Fademrecht, Ina Landel, Lena Quambusch, Jens T. Siveke, Georgia Günther, Andrea Tannapfel, Jörn Weisner, Marius Lindemann, Marija Trajkovic-Arsic, Laura Depta, Matthias Baumann, Abdelouahid Maghnouj, Steven Smith, Christian Teschendorf, Michael Pohl, Matthias P. Müller, Christoph Reintjes, and Waldemar Uhl

Subjects

0301 basic medicine, Trametinib, Cancer Research, biology, Chemistry, MEK inhibitor, Medizin, Cancer, AKT1, medicine.disease, medicine.disease_cause, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, biology.protein, medicine, Cancer research, PTEN, KRAS, Protein kinase B, PI3K/AKT/mTOR pathway

Abstract

Aberrations within the PI3K/AKT signaling axis are frequently observed in numerous cancer types, highlighting the relevance of these pathways in cancer physiology and pathology. However, therapeutic interventions employing AKT inhibitors often suffer from limitations associated with target selectivity, efficacy, or dose-limiting effects. Here we present the first crystal structure of autoinhibited AKT1 in complex with the covalent-allosteric inhibitor borussertib, providing critical insights into the structural basis of AKT1 inhibition by this unique class of compounds. Comprehensive biological and preclinical evaluation of borussertib in cancer-related model systems demonstrated a strong antiproliferative activity in cancer cell lines harboring genetic alterations within the PTEN, PI3K, and RAS signaling pathways. Furthermore, borussertib displayed antitumor activity in combination with the MEK inhibitor trametinib in patient-derived xenograft models of mutant KRAS pancreatic and colon cancer. Significance: Borussertib, a first-in-class covalent-allosteric AKT inhibitor, displays antitumor activity in combination with the MEK inhibitor trametinib in patient-derived xenograft models and provides a starting point for further pharmacokinetic/dynamic optimization.

Published

2019

28. Structural and chemical insights into the covalent-allosteric inhibition of the protein kinase Akt

Author

Lena Quambusch, Daniel Rauh, Paul Czodrowski, Matthias P. Müller, Laura Depta, Jörn Weisner, Marius Lindemann, Bernd Engels, Steven Smith, Petra Janning, Ina Landel, Thien Anh Le, Rebekka Scheinpflug, Rajesh Gontla, Julia Hardick, and Niklas Uhlenbrock

Subjects

010405 organic chemistry, Kinase, Cell growth, Chemistry, Allosteric regulation, General Chemistry, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Cell biology, Pleckstrin homology domain, Protein kinase domain, Transferase, Protein kinase A, Protein kinase B

Abstract

Structure-based driven synthesis and biological evaluation provide innovative novel covalent-allosteric Akt inhibitors., The Ser/Thr kinase Akt (Protein Kinase B/PKB) is a master switch in cellular signal transduction pathways. Its downstream signaling influences cell proliferation, cell growth, and apoptosis, rendering Akt a prominent drug target. The unique activation mechanism of Akt involves a change of the relative orientation of its N-terminal pleckstrin homology (PH) and the kinase domain and makes this kinase suitable for highly specific allosteric modulation. Here we present a unique set of crystal structures of covalent-allosteric interdomain inhibitors in complex with full-length Akt and report the structure-based design, synthesis, biological and pharmacological evaluation of a focused library of these innovative inhibitors.

Published

2018

29. Preclinical Efficacy of Covalent-Allosteric AKT Inhibitor Borussertib in Combination with Trametinib in

Author

Jörn, Weisner, Ina, Landel, Christoph, Reintjes, Niklas, Uhlenbrock, Marija, Trajkovic-Arsic, Niklas, Dienstbier, Julia, Hardick, Swetlana, Ladigan, Marius, Lindemann, Steven, Smith, Lena, Quambusch, Rebekka, Scheinpflug, Laura, Depta, Rajesh, Gontla, Anke, Unger, Heiko, Müller, Matthias, Baumann, Carsten, Schultz-Fademrecht, Georgia, Günther, Abdelouahid, Maghnouj, Matthias P, Müller, Michael, Pohl, Christian, Teschendorf, Heiner, Wolters, Richard, Viebahn, Andrea, Tannapfel, Waldemar, Uhl, Jan G, Hengstler, Stephan A, Hahn, Jens T, Siveke, and Daniel, Rauh

Subjects

Pyridones, Cell Cycle, Mice, Nude, Antineoplastic Agents, Apoptosis, Pyrimidinones, Xenograft Model Antitumor Assays, Pancreatic Neoplasms, Proto-Oncogene Proteins p21(ras), Mice, Mutation, Tumor Cells, Cultured, Animals, Humans, Drug Therapy, Combination, Female, Colorectal Neoplasms, Proto-Oncogene Proteins c-akt, Cell Proliferation

Abstract

Aberrations within the PI3K/AKT signaling axis are frequently observed in numerous cancer types, highlighting the relevance of these pathways in cancer physiology and pathology. However, therapeutic interventions employing AKT inhibitors often suffer from limitations associated with target selectivity, efficacy, or dose-limiting effects. Here we present the first crystal structure of autoinhibited AKT1 in complex with the covalent-allosteric inhibitor borussertib, providing critical insights into the structural basis of AKT1 inhibition by this unique class of compounds. Comprehensive biological and preclinical evaluation of borussertib in cancer-related model systems demonstrated a strong antiproliferative activity in cancer cell lines harboring genetic alterations within the PTEN, PI3K, and RAS signaling pathways. Furthermore, borussertib displayed antitumor activity in combination with the MEK inhibitor trametinib in patient-derived xenograft models of mutant

Published

2018

30. Assays for Nucleotide Competitive Reversible and Irreversible Inhibitors of Ras GTPases

Author

Roger S. Goody, Matthias P. Müller, Sadasivam Jeganathan, and Imtiaz Ali

Subjects

0301 basic medicine, GTP', Mutant, GTPase, 01 natural sciences, Biochemistry, Guanosine Diphosphate, Adduct, 03 medical and health sciences, Animals, Humans, Nucleotide, chemistry.chemical_classification, 010405 organic chemistry, Nucleotides, Small molecule, Affinities, 0104 chemical sciences, Kinetics, 030104 developmental biology, Spectrometry, Fluorescence, chemistry, Covalent bond, ras Proteins, Biological Assay, Guanosine Triphosphate

Abstract

Although the Ras protein has been seen as a potential target for cancer therapy for the past 30 years, there was a tendency to consider it undruggable until recently. This has changed with the demonstration that small molecules with a specificity for (disease related mutants of) Ras can indeed be found, and some of these molecules form covalent adducts. A subgroup of these molecules can be characterized as competing with binding of the natural ligands GTP and GDP. Because of the distinct properties of Ras and related GTPases, in particular the very high nucleotide affinities and associated very low dissociation rates, assays for characterizing such molecules are not trivial. This is compounded by the fact that Ras family GTPases tend to be thermally unstable in the absence of a bound nucleotide. Here, we show that instead of using the unstable nucleotide-free Ras, the protein can be isolated as a 1:1 complex with a modified nucleotide (GDP-β-methyl ester) with low affinity to Ras. With this nucleotide analogue bound to the protein, testing of inhibitors is made experimentally more convenient and we present assays that allow the rapid assessment of the kinetic constants describing the inhibition process.

Published

2018

31. An Unusual Intramolecular Halogen Bond Guides Conformational Selection

Author

Christian Becker, Jonas Lategahn, Matthäus Getlik, Niklas Uhlenbrock, Matthias P. Müller, Michael Edmund Beck, Daniel Rauh, Marcelo Depólo Polêto, Hugo Verli, Daniel Alencar Rodrigues, Lena Quambusch, Fanny N. Costa, Roberta Tesch, Fabio Furlan Ferreira, Carlos Mauricio R. Sant'Anna, Pedro de Sena Murteira Pinheiro, and Carlos A. M. Fraga

Subjects

Halogen bond, biology, 010405 organic chemistry, Chemistry, Stereochemistry, Active site, General Chemistry, Crystal structure, 010402 general chemistry, 01 natural sciences, Catalysis, 0104 chemical sciences, Intramolecular force, Halogen, biology.protein, Molecule, Selection (genetic algorithm)

Abstract

PIK-75 is a phosphoinositide-3-kinase (PI3K) α-isoform-selective inhibitor with high potency. Although published structure-activity relationship data show the importance of the NO2 and the Br substituents in PIK-75, none of the published studies could correctly determine the underlying reason for their importance. In this publication, we report the first X-ray crystal structure of PIK-75 in complex with the kinase GSK-3β. The structure shows an unusual U-shaped conformation of PIK-75 within the active site of GSK-3β that is likely stabilized by an atypical intramolecular Br⋅⋅⋅NO2 halogen bond. NMR and MD simulations show that this conformation presumably also exists in solution and leads to a binding-competent preorganization of the PIK-75 molecule, thus explaining its high potency. We therefore suggest that the site-specific incorporation of halogen bonds could be generally used to design conformationally restricted bioactive substances with increased potencies.

Published

2018

32. Augmented Reality in Scientific Publications-Taking the Visualization of 3D Structures to the Next Level

Author

Daniel Rauh, Patrik Wolle, and Matthias P. Müller

Subjects

0301 basic medicine, Software visualization, 010405 organic chemistry, Computer science, Publications, Molecular Conformation, 3d model, General Medicine, 01 natural sciences, Biochemistry, 0104 chemical sciences, Visualization, World Wide Web, 03 medical and health sciences, 030104 developmental biology, General practice, Molecular Medicine, Humans, Augmented reality, Information Technology, Digital Revolution, Mobile device

Abstract

The examination of three-dimensional structural models in scientific publications allows the reader to validate or invalidate conclusions drawn by the authors. However, either due to a (temporary) lack of access to proper visualization software or a lack of proficiency, this information is not necessarily available to every reader. As the digital revolution is quickly progressing, technologies have become widely available that overcome the limitations and offer to all the opportunity to appreciate models not only in 2D, but also in 3D. Additionally, mobile devices such as smartphones and tablets allow access to this information almost anywhere, at any time. Since access to such information has only recently become standard practice, we want to outline straightforward ways to incorporate 3D models in augmented reality into scientific publications, books, posters, and presentations and suggest that this should become general practice.

Published

2018

33. Augmented Reality in Scientific Publications – Taking the Visualization of 3D Structures to the Next Level

Author

Patrik Wolle, Matthias P. Müller, and Daniel Rauh

Subjects

Molecular Medicine, General Medicine, Biochemistry

Published

2019

34. A pull-down procedure for the identification of unknown GEFs for small GTPases

Author

Petra Janning, Nathalie Bleimling, Timon Friese, Amrita Rai, Daniel Koch, Roger S. Goody, Matthias P. Müller, Aymelt Itzen, Andreas Brockmeyer, Imtiaz Ali, and Bruno Goud

Subjects

0301 basic medicine, enrichment, Saccharomyces cerevisiae Proteins, GTPase-activating protein, yeast two-hybrid, Two-hybrid screening, Saccharomyces cerevisiae, GTPase, Biology, Biochemistry, Nucleotide exchange factor, 03 medical and health sciences, 0302 clinical medicine, GTP-binding protein regulators, Two-Hybrid System Techniques, Guanine Nucleotide Exchange Factors, Small GTPase, GEF, pull-down, Cell Biology, in vitro transcription/translation, Cell biology, nucleotide exchange factor, 030104 developmental biology, rab GTP-Binding Proteins, small GTPase, Rab, Guanine nucleotide exchange factor, 030217 neurology & neurosurgery, Research Paper

Abstract

Members of the family of small GTPases regulate a variety of important cellular functions. In order to accomplish this, tight temporal and spatial regulation is absolutely necessary. The two most important factors for this regulation are GTPase activating proteins (GAPs) and guanine nucleotide exchange factors (GEFs), the latter being responsible for the activation of the GTPase downstream pathways at the correct location and time. Although a large number of exchange factors have been identified, it is likely that a similarly large number remains unidentified. We have therefore developed a procedure to specifically enrich GEF proteins from biological samples making use of the high affinity binding of GEFs to nucleotide-free GTPases. In order to verify the results of these pull-down experiments, we have additionally developed two simple validation procedures: An in vitro transcription/translation system coupled with a GEF activity assay and a yeast two-hybrid screen for detection of GEFs. Although the procedures were established and tested using the Rab protein Sec4, the similar basic principle of action of all nucleotide exchange factors will allow the method to be used for identification of unknown GEFs of small GTPases in general.

Published

2016

35. Structure of the tandem PX-PH domains of Bem3 from Saccharomyces cerevisiae

Author

Sungmin Eu, Nathalie Bleimling, Roger S. Goody, Daniel Koch, Matthias P. Müller, and Imtiaz Ali

Subjects

0301 basic medicine, Saccharomyces cerevisiae Proteins, Stereochemistry, Saccharomyces cerevisiae, Biophysics, Cooperativity, CDC42, PX domain, Biochemistry, Protein Structure, Secondary, Research Communications, 03 medical and health sciences, Structural Biology, Genetics, Protein Interaction Domains and Motifs, Amino Acid Sequence, phosphatidylinositol phosphates, biology, Tandem, Strain (chemistry), Bem3, Chemistry, PH domain, GTPase-Activating Proteins, PIP, pleckstrin homology, Condensed Matter Physics, biology.organism_classification, phox, Protein Structure, Tertiary, Pleckstrin homology domain, 030104 developmental biology, Membrane, Crystallization

Abstract

The structure of the putative membrane-binding tandem PX-PH domain module of the yeast protein Bem3 is reported., The structure of the tandem lipid-binding PX and pleckstrin-homology (PH) domains of the Cdc42 GTPase-activating protein Bem3 from Saccharomyces cerevisiae (strain S288c) has been determined to a resolution of 2.2 Å (R work = 21.1%, R free = 23.4%). It shows that the domains adopt a relative orientation that enables them to simultaneously bind to a membrane and suggests possible cooperativity in membrane binding.

Published

2018

36. Exploring Adenylylation and Phosphocholination as Post-Translational Modifications

Author

Christian Hedberg, Michael F. Albers, Aymelt Itzen, and Matthias P. Müller

Subjects

Adenosine, Bacteria, Chemistry, Phosphorylcholine, Organic Chemistry, Combined use, Pathogenic bacteria, Computational biology, medicine.disease_cause, Biochemistry, Antibodies, Enzymes, Specific antibody, medicine, Posttranslational modification, Molecular Medicine, Peptides, Protein Processing, Post-Translational, Molecular Biology, Adenylylation

Abstract

Editing the translations: Adenylylation and phosphocholination have recently been found as important post-translational modifications used by pathogenic bacteria during the infection process. This review discusses the combined use of chemical handles and specific antibodies for the identification of previously unknown substrates of these post-translational modifications in infected host cells.

Published

2013

37. Author response: bMERB domains are bivalent Rab8 family effectors evolved by gene duplication

Author

Roger S. Goody, Anastasia Oprisko, Amrita Rai, Aymelt Itzen, Timon Friese, Emerich Mihai Gazdag, Matthias P. Müller, Jeremy Campos, and Yangxue Fu

Subjects

Genetics, Effector, Gene duplication, Biology, Bivalent (genetics)

Published

2016

38. bMERB domains are bivalent Rab8 family effectors evolved by gene duplication

Author

Roger S. Goody, Yangxue Fu, Amrita Rai, Emerich Mihai Gazdag, Jeremy Campos, Anastasia Oprisko, Timon Friese, Aymelt Itzen, and Matthias P. Müller

Subjects

0301 basic medicine, QH301-705.5, Endosome, Science, EHBP, Biology, Endocytosis, Biochemistry, General Biochemistry, Genetics and Molecular Biology, Bivalent (genetics), Mixed Function Oxygenases, Evolution, Molecular, 03 medical and health sciences, Protein Domains, Gene Duplication, Gene duplication, Biology (General), Binding site, Rab effectors, Adaptor Proteins, Signal Transducing, General Immunology and Microbiology, Effector, General Neuroscience, fungi, Microfilament Proteins, General Medicine, LIM Domain Proteins, Biophysics and Structural Biology, Cell biology, Cytoskeletal Proteins, 030104 developmental biology, Structural biology, rab GTP-Binding Proteins, Mical, Medicine, Rab, Carrier Proteins, Research Article, Human

Abstract

In their active GTP-bound form, Rab proteins interact with proteins termed effector molecules. In this study, we have thoroughly characterized a Rab effector domain that is present in proteins of the Mical and EHBP families, both known to act in endosomal trafficking. Within our study, we show that these effectors display a preference for Rab8 family proteins (Rab8, 10, 13 and 15) and that some of the effector domains can bind two Rab proteins via separate binding sites. Structural analysis allowed us to explain the specificity towards Rab8 family members and the presence of two similar Rab binding sites that must have evolved via gene duplication. This study is the first to thoroughly characterize a Rab effector protein that contains two separate Rab binding sites within a single domain, allowing Micals and EHBPs to bind two Rabs simultaneously, thus suggesting previously unknown functions of these effector molecules in endosomal trafficking. DOI: http://dx.doi.org/10.7554/eLife.18675.001

Published

2016

39. Characterization of Enzymes from Legionella pneumophila Involved in Reversible Adenylylation of Rab1 Protein

Author

Roger S. Goody, Aymelt Itzen, Alexander V. Shkumatov, Philip Roger Goody, Stefan Schoebel, Matthias P. Müller, and Lena K. Oesterlin

Subjects

G protein, RAB1, Cell Biology, Vacuole, Biology, biology.organism_classification, Biochemistry, Legionella pneumophila, rab1 GTP-Binding Proteins, Secretory protein, Bacterial Proteins, SIDD, Enzymology, Guanine Nucleotide Exchange Factors, Humans, Rab, Legionnaires' Disease, Protein Processing, Post-Translational, Molecular Biology, Adenylylation

Abstract

After the pathogenic bacterium Legionella pneumophila is phagocytosed, it injects more than 250 different proteins into the cytoplasm of host cells to evade lysosomal digestion and to replicate inside the host cell. Among these secreted proteins is the protein DrrA/SidM, which has been shown to modify Rab1b, a main regulator of vesicular trafficking in eukaryotic cells, by transfer of adenosine monophosphate (AMP) to Tyr(77). In addition, Legionella provides the protein SidD that hydrolytically reverses the covalent modification, suggesting a tight spatial and temporal control of Rab1 function by Legionella during infection. Small angle x-ray scattering experiments of DrrA allowed us to validate a tentative complex model built by combining available crystallographic data. We have established the effects of adenylylation on Rab1 interactions and properties in a quantitative way. In addition, we have characterized the kinetics of DrrA-catalyzed adenylylation as well as SidD-catalyzed deadenylylation toward Rab1 and have determined the nucleotide specificities of both enzymes. This study enhances our knowledge of proteins subverting Rab1 function at the Legionella-containing vacuole.

Published

2012

40. Bacterial Pathogens Commandeer Rab GTPases to Establish Intracellular Niches

Author

Angela Wandinger-Ness, Matthias P. Müller, and Mary-Pat Stein

Subjects

Effector, Endocytic cycle, Chlamydiae, Cell Biology, GTPase, Biology, Endocytosis, biology.organism_classification, Biochemistry, Cell biology, Transport protein, Microbiology, Structural Biology, Genetics, Rab, Molecular Biology, Intracellular

Abstract

Intracellular bacterial pathogens deploy virulence factors termed effectors to inhibit degradation by host cells and to establish intracellular niches where growth and differentiation take place. Here, we describe mechanisms by which human bacterial pathogens (including Chlamydiae; Coxiella burnetii; Helicobacter pylori; Legionella pneumophila; Listeria monocytogenes; Mycobacteria; Pseudomonas aeruginosa, Salmonella enterica) modulate endocytic and exocytic Rab GTPases in order to thrive in host cells. Host cell Rab GTPases are critical for intracellular transport following pathogen phagocytosis or endocytosis. At the molecular level bacterial effectors hijack Rab protein function to: evade degradation, direct transport to particular intracellular locations and monopolize host vesicles carrying molecules that are needed for a stable niche and/or bacterial growth and differentiation. Bacterial effectors may serve as specific receptors for Rab GTPases or as enzymes that post-translationally modify Rab proteins or endosomal membrane lipids required for Rab function. Emerging data indicate that bacterial effector expression is temporally and spatially regulated and multiple virulence factors may act concertedly to usurp Rab GTPase function, alter signaling and ensure niche establishment and intracellular bacterial growth, making this field an exciting area for further study.

Published

2012

41. Reversible phosphocholination of Rab proteins byLegionella pneumophilaeffector proteins

Author

Katharina Heller, Matthias P. Müller, Roger S. Goody, Aymelt Itzen, Lena K. Oesterlin, and Philip Roger Goody

Subjects

General Immunology and Microbiology, GTPase-activating protein, GTP', General Neuroscience, RAB1, GTPase, Biology, General Biochemistry, Genetics and Molecular Biology, Cell biology, GTP-binding protein regulators, Biochemistry, GTP Phosphohydrolases, Rab, Guanine nucleotide exchange factor, Molecular Biology

Abstract

The Legionella pneumophila protein AnkX that is injected into infected cells by a Type IV secretion system transfers a phosphocholine group from CDP-choline to a serine in the Rab1 and Rab35 GTPase Switch II regions. We show here that the consequences of phosphocholination on the interaction of Rab1/Rab35 with various partner proteins are quite distinct. Activation of phosphocholinated Rabs by GTP/GDP exchange factors (GEFs) and binding to the GDP dissociation inhibitor (GDI) are strongly inhibited, whereas deactivation by GTPase activating proteins (GAPs) and interactions with Rab-effector proteins (such as LidA and MICAL-3) are only slightly inhibited. We show that the Legionella protein lpg0696 has the ability to remove the phosphocholine group from Rab1. We present a model in which the action of AnkX occurs as an alternative to GTP/GDP exchange, stabilizing phosphocholinated Rabs in membranes in the GDP form because of loss of GDI binding ability, preventing interactions with cellular GTPase effectors, which require the GTP-bound form. Generation of the GTP form of phosphocholinated Rab proteins cannot occur due to loss of interaction with cellular GEFs.

Published

2012

42. Effiziente Synthese und Anwendung von Peptiden mit adenylylierten Tyrosinresten

Author

Roger S. Goody, Martijn F. Erland, Cornelis Smit, Matthias P. Müller, Aymelt Itzen, Julia Blümer, Christian Hedberg, and Michael F. Albers

Subjects

Chemistry, General Medicine

Published

2011

43. Efficient Synthesis and Applications of Peptides containing Adenylylated Tyrosine Residues

Author

Martijn F. Eerland, Cornelis Smit, Julia Blümer, Michael F. Albers, Christian Hedberg, Matthias P. Müller, Aymelt Itzen, and Roger S. Goody

Subjects

Effector, Chemistry, Blotting, Western, General Chemistry, GTPase, Small molecule, Adenosine Monophosphate, Catalysis, Legionella pneumophila, rab1 GTP-Binding Proteins, Bacterial Proteins, Biochemistry, Cdc42 GTP-Binding Protein, COS Cells, Chlorocebus aethiops, Animals, Tyrosine, Small GTPase, Rab, Peptides, cdc42 GTP-Binding Protein, Antibodies, Immobilized, Protein Processing, Post-Translational, Adenylylation

Abstract

During infections, bacterial microorganisms initiate profound interactions with mammalian host cells. Usually defense mechanisms of the host destroy intruding bacteria in rapid manner. However, many bacterial pathogens have evolved in a way to avoid these mechanisms. By use of effector molecules, which can be small organic molecules or proteins with enzymatic activity, the host is manipulated on a molecular level. Effectors mediating post-translational modifications (PTMs) are employed by many pathogens to influence the biological activity of host proteins. In the presented thesis, two related PTMs are investigated in detail: Adenylylation, the covalent transfer of an adenosine monophosphate group from adenosine triphosphate onto proteins, and phosphocholination, the covalent transfer of a phosphocholine moiety onto proteins. Over the past years, enzymes mediating these modifications have been discovered in several pathogens, especially as a mechanism to influence the signaling of eukaryotic cells by adenylylating or phosphocholinating small GTPases. However, the development of reliable methods for the isolation and identification of adenylylated and phosphocholinated proteins remains a vehement challenge in this field of research. This thesis presents general procedures for the synthesis of peptides carrying adenylylated or phosphocholinated tyrosine, threonine and serine residues. From the resulting peptides, mono-selective polyclonal antibodies against adenylylated tyrosine and threonine have been raised. The antibodies were used as tools for proteomic research to isolate unknown substrates of adenylyl transferases from eukaryotic cells. Mass spectrometric fragmentation techniques have been investigated to ease the identification of adenylylated proteins. Furthermore, this work presents a new strategy to identify adenylylated proteins. Additionally, small effector molecules are involved in the regulation of infection mechanisms. In this work, the small molecule LAI-1 (Legionella autoinducer 1) from the pathogen Legionella pneumophila, the causative agent of the Legionnaire’s disease, was synthesised together with its amino-derivatives. LAI-1 showed are a clear pharmacological effect on the regulation of the life cycle of L. pneumophila, initiating transmissive traits like motility and virulence. Furthermore, LAI-1 was shown to have an effect on eukaryotic cells as well. Directed motility of the eukaryotic cells was significantly reduced and the cytoskeletal architecture was reorganised, probably by interfering with the small GTPase Cdc42.

Published

2011

44. Locking GTPases covalently in their functional states

Author

Fu Li, Frank Hofmann, Matthias P. Müller, Roger S. Goody, Aymelt Itzen, Daniel Koch, Sophie Vieweg, David Wiegandt, and Yao-Wen Wu

Subjects

GTP', General Physics and Astronomy, Plasma protein binding, GTPase, Guanosine triphosphate, Biology, Crystallography, X-Ray, Guanosine Diphosphate, General Biochemistry, Genetics and Molecular Biology, Article, GTP Phosphohydrolases, Fungal Proteins, chemistry.chemical_compound, GTP-binding protein regulators, Escherichia coli, Fungal protein, Multidisciplinary, Binding Sites, Escherichia coli Proteins, General Chemistry, ddc, Biochemistry, chemistry, rab GTP-Binding Proteins, Biophysics, Rab, Guanosine Triphosphate, Protein Binding

Abstract

GTPases act as key regulators of many cellular processes by switching between active (GTP-bound) and inactive (GDP-bound) states. In many cases, understanding their mode of action has been aided by artificially stabilizing one of these states either by designing mutant proteins or by complexation with non-hydrolysable GTP analogues. Because of inherent disadvantages in these approaches, we have developed acryl-bearing GTP and GDP derivatives that can be covalently linked with strategically placed cysteines within the GTPase of interest. Binding studies with GTPase-interacting proteins and X-ray crystallography analysis demonstrate that the molecular properties of the covalent GTPase–acryl–nucleotide adducts are a faithful reflection of those of the corresponding native states and are advantageously permanently locked in a defined nucleotide (that is active or inactive) state. In a first application, in vivo experiments using covalently locked Rab5 variants provide new insights into the mechanism of correct intracellular localization of Rab proteins., The cellular function of small GTPases is regulated by switching between active (GTP-bound) and inactive (GDP-bound) states. Here the authors develop nucleotide analogues that can be covalently linked to GTPases via a strategically placed cysteine residue to lock the target GTPase in defined activation states.

Published

2015

45. Reversible phosphocholination of Rab proteins by Legionella pneumophila effector proteins

Author

Philip R, Goody, Katharina, Heller, Lena K, Oesterlin, Matthias P, Müller, Aymelt, Itzen, and Roger S, Goody

Subjects

Bacterial Proteins, rab GTP-Binding Proteins, Phosphorylcholine, fungi, GTPase-Activating Proteins, Guanine Nucleotide Exchange Factors, Article, GTP Phosphohydrolases, Legionella pneumophila

Abstract

The Legionella pneumophila protein AnkX that is injected into infected cells by a Type IV secretion system transfers a phosphocholine group from CDP-choline to a serine in the Rab1 and Rab35 GTPase Switch II regions. We show here that the consequences of phosphocholination on the interaction of Rab1/Rab35 with various partner proteins are quite distinct. Activation of phosphocholinated Rabs by GTP/GDP exchange factors (GEFs) and binding to the GDP dissociation inhibitor (GDI) are strongly inhibited, whereas deactivation by GTPase activating proteins (GAPs) and interactions with Rab-effector proteins (such as LidA and MICAL-3) are only slightly inhibited. We show that the Legionella protein lpg0696 has the ability to remove the phosphocholine group from Rab1. We present a model in which the action of AnkX occurs as an alternative to GTP/GDP exchange, stabilizing phosphocholinated Rabs in membranes in the GDP form because of loss of GDI binding ability, preventing interactions with cellular GTPase effectors, which require the GTP-bound form. Generation of the GTP form of phosphocholinated Rab proteins cannot occur due to loss of interaction with cellular GEFs.

Published

2011

46. The versatile Legionella effector protein DrrA

Author

Roger S. Goody, Matthias P. Müller, Stefan Schoebel, Lena K. Oesterlin, Julia Blümer, Heide Peters, Wulf Blankenfeldt, and Aymelt Itzen

Subjects

General Agricultural and Biological Sciences, Article Addendum

Abstract

The human pathogen Legionella pneumophila is a bacterium that infects human cells and interferes with intracellular signaling. The Legionella protein DrrA is one of the numerous effectors that the bacterium translocates into the host cytosol. DrrA binds to the Legionella containing vacuole (LCV), an organelle in which Legionella survives and replicates, and recruits and activates the vesicular trafficking regulator Rab1 to redirect vesicular trafficking between the endoplasmatic reticulum and the Golgi. After depositing Rab1 at the LCV, DrrA covalently modifies Rab1 with an AMP moiety at a specific tyrosine residue (Tyr77), which is centrally located in the functionally important switch II region. This adenylylation reaction interferes with the deactivation of Rab1 by GTPase activating proteins (GAPs), thereby presumably prolonging the active state of the protein at the LCV. Here, we summarize the versatile properties of DrrA and speculate on the effects of Rab1-adenylylation.

Published

2011

47. The Legionella effector protein DrrA AMPylates the membrane traffic regulator Rab1b

Author

Roger S. Goody, Heide Peters, Wulf Blankenfeldt, Julia Blümer, Aymelt Itzen, and Matthias P. Müller

Subjects

Models, Molecular, GTPase-activating protein, Guanosine, GTPase, Guanosine triphosphate, Legionella pneumophila, Mass Spectrometry, chemistry.chemical_compound, Bacterial Proteins, Chlorocebus aethiops, Animals, Guanine Nucleotide Exchange Factors, Adenylylation, Multidisciplinary, Crystallography, biology, RAB1, biology.organism_classification, Adenosine Monophosphate, Cell biology, Protein Structure, Tertiary, rab1 GTP-Binding Proteins, chemistry, Biochemistry, Guanosine diphosphate, rab GTP-Binding Proteins, COS Cells

Abstract

Legionella Hijacks Rab Legionella pneumophila can infect eukaryotic cells and takes up residence within intracellular vacuoles, where it multiplies. In order to produce and maintain this intracellular niche, the pathogen must manipulate membrane trafficking within the host cell. Now, Müller et al. (p. 946 , published online 22 July) describe the ability of Legionella pneumophila to manipulate vesicular trafficking by the covalent modification of the small guanosine triphosphatase (GTPase) Rab1, which normally regulates the transport of endoplasmic reticulum–derived vesicles in eukaryotic cells. The Legionella protein DrrA is released into the cytosol of infected cells, where it specifically AMPylates a tyrosine residue of one of the regulating regions of Rab1. The modification renders the Rab protein inaccessible to GTPase-activating proteins and thus locks it in its active guanosine triphosphate–bound state.

Published

2010

48. Cellular model system to dissect the isoform-selectivity of Akt inhibitors

Author

Lena Quambusch, Laura Depta, Ina Landel, Melissa Lubeck, Tonia Kirschner, Jonas Nabert, Niklas Uhlenbrock, Jörn Weisner, Michael Kostka, Laura M. Levy, Carsten Schultz-Fademrecht, Franziska Glanemann, Kristina Althoff, Matthias P. Müller, Jens T. Siveke, and Daniel Rauh

Subjects

Science

Abstract

Elucidating specific effects of protein kinase Akt isoforms remains challenging. Here, the authors establish an Akt isoform-dependent cellular model system and use it, together with X-ray crystallography and structure-based ligand design, to develop isoform-selective covalent-allosteric Akt inhibitors

Published

2021

49. Hair Loss Associated with Fluoxetine but not with Citalopram

Author

Seifritz, Erich, Hatzinger, Martin, Matthias, J Müller, Hemmeter, Ulrich, and Holsboer-Trachsler, Edith

Published

1995

50. Nucleotide based covalent inhibitors of KRas can only be efficient in vivo if they bind reversibly with GTP-like affinity

Author

Matthias P. Müller, Sadasivam Jeganathan, Angelika Heidrich, Jeremy Campos, and Roger S. Goody

Subjects

Medicine, Science

Abstract

Abstract Simple reversible competitive inhibition of nucleotide binding of GTP to Ras family GTPases has long been recognized as an unlikely approach to manipulating the activity of such proteins for experimental or therapeutic purposes. This is due to the high affinity of GTP to GTPases coupled with high cellular GTP concentrations, but also to problems of specificity for the highly conserved binding sites in GTPases. A recent approach suggested that these problems might be overcome by using GDP derivatives that can undergo a covalent reaction with disease specific mutants, in particular addressing inhibition of KRasG12C using GDP equipped with an electrophilic group at the β-phosphate. We show here that a major drawback to this approach is a loss of reversible affinity of such β-modified derivatives for Ras of at least 104 compared to GTP and GDP. With the help of a thorough kinetic characterization, we show that this leads to covalent reaction times that are too slow to make the compounds attractive for intracellular use, but that generation of a hypothetical reactive GDP derivative that retains the high reversible affinity of GDP/GTP to Ras might be a viable alternative.

Published

2017