Your search keyword '"Rezart Zhubi"' showing total 6 results

1. Comparative structural analyses of the NHL domains from the human E3 ligase TRIM–NHL family

Author

Apirat Chaikuad, Rezart Zhubi, Claudia Tredup, and Stefan Knapp

Subjects

trim nhls, nhl domains, trim e3 ligases, protein interaction domains, β-propeller protein modules, genetic mutations, Crystallography, QD901-999

Abstract

Tripartite motif (TRIM) proteins constitute one of the largest subfamilies of the RING-type E3 ubiquitin ligases that play a role in diverse processes from homeostasis and immune response to viral restriction. While TRIM proteins typically harbor an N-terminal RING finger, a B-box and a coiled-coil domain, a high degree of diversity lies in their C termini that contain diverse protein interaction modules, most of which, both structures and their roles in intermolecular interactions, remain unknown. Here, high-resolution crystal structures of the NHL domains of three of the four human TRIM–NHL proteins, namely TRIM2, TRIM3 and TRIM71, are presented. Comparative structural analyses revealed that, despite sharing an evolutionarily conserved six-bladed β-propeller architecture, the low sequence identities resulted in distinct properties of these interaction domains at their putative binding sites for macromolecules. Interestingly, residues lining the binding cavities represent a hotspot for genetic mutations linked to several diseases. Thus, high sequence diversity within the conserved NHL domains might be essential for differentiating binding partners among TRIM–NHL proteins.

Published

2022

2. Design of a Potent TLX Agonist by Rational Fragment Fusion

Author

Giuseppe Faudone, Rezart Zhubi, Fatih Celik, Stefan Knapp, Apirat Chaikuad, Jan Heering, Daniel Merk, and Publica

Subjects

Cell Survival, Ligands, Orphan Nuclear Receptors, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, HEK293 Cells, Drug Stability, Drug Design, Drug Discovery, Microsomes, Liver, Animals, Humans, Molecular Medicine, Piperazine, Protein Binding

Abstract

As a master regulator of neurogenesis, the orphan nuclear receptor tailless homologue (TLX, NR2E1) maintains neuronal stem cell homeostasis by acting as a transcriptional repressor of tumor suppressor genes. It is hence considered as an appealing target for the treatment of neurodegenerative diseases, but a lack of potent TLX modulators as tools to probe pharmacological TLX control hinders further validation of its promising potential. Here, we report the development of a potent TLX agonist based on fragment screening, pharmacophore modeling, and fragment fusion. Pharmacophore similarity of a fragment screening hit and the TLX ligand ccrp2 provided a rational basis for fragment linkage, which resulted in several TLX activator scaffolds. Among them, the fused compound 10 evolved as a valuable TLX agonist tool with submicromolar potency and high selectivity over related nuclear receptors, rendering it suitable for functional studies on TLX.

Published

2022

3. Shifting the selectivity of pyrido[2,3-d]pyrimidin-7(8H)-one inhibitors towards the salt-inducible kinase (SIK) subfamily

Author

Marcel Rak, Roberta Tesch, Lena M. Berger, Ekaterina Shevchenko, Monika Raab, Amelie Tjaden, Rezart Zhubi, Dimitrios-Ilias Balourdas, Andreas C. Joerger, Antti Poso, Andreas Krämer, Lewis Elson, Aleksandar Lučić, Thales Kronenberger, Thomas Hanke, Klaus Strebhardt, Mourad Sanhaji, and Stefan Knapp

Subjects

Pharmacology, Organic Chemistry, Drug Discovery, General Medicine

Abstract

Salt-inducible kinases 1-3 (SIK1-3) are key regulators of the LKB1-AMPK pathway and play an important role in cellular homeostasis. Dysregulation of any of the three isoforms has been associated with tumorigenesis in liver, breast, and ovarian cancers. We have recently developed the dual pan-SIK/group I p21-activated kinase (PAK) chemical probe MRIA9. However, inhibition of p21-activated kinases has been associated with cardiotoxicityin vivo, which complicates the use of MRIA9 as a tool compound. Here, we present a structure-based approach involving the back-pocket and gatekeeper residues, for narrowing the selectivity of pyrido[2,3-d]pyrimidin-7(8H)-one-based inhibitors towards SIK kinases, eliminating PAK activity. Optimization was guided by high-resolution crystal structure analysis and computational methods, resulting in a pan-SIK inhibitor, MR22, which no longer exhibited activity on STE group kinases and displayed excellent selectivity in a representative kinase panel. MR22-dependent SIK inhibition led to centrosome dissociation and subsequent cell-cycle arrest in ovarian cancer cells, as observed with MRIA9, conclusively linking these phenotypic effects to SIK inhibition. Taken together, MR22 represents a valuable tool compound for studying SIK kinase function in cells.

Published

2023

4. Fragment-based discovery of orphan nuclear receptor Nur77/NGFI-B ligands

Author

Silvia Arifi, Daniel Zaienne, Jan Heering, Thomas Wein, Rezart Zhubi, Apirat Chaikuad, Stefan Knapp, Julian A. Marschner, Daniel Merk, and Publica

Subjects

Virtual screening, Receptors, Steroid, Organic Chemistry, Apoptosis, NR4A, Ligands, Orphan Nuclear Receptors, Biochemistry, Neoplasms, Drug Discovery, Nuclear Receptor Subfamily 4, Group A, Member 1, Humans, Neurodegeneration, Transcription factor, Molecular Biology, Cancer

Abstract

The transcription factor nerve growth factor-induced clone B (NGFI-B, Nur77, NR4A1) is an orphan nuclear receptor playing a role in cell survival and apoptosis regulation. Pharmacological Nur77 modulation holds promise for cancer and (neuro-)inflammatory disease treatment. The available Nur77 ligand scaffolds based on highly lipophilic natural products cytosporone B, celastrol and isoalantolactone are inadequate for the development of potent Nur77 modulators with favorable properties as chemical tools and future drugs. By fragment library screening and subsequent modeling for fragment extension, we have obtained a set of new Nur77 ligands offering alternative chemotypes for the development of Nur77 agonists and inverse agonists. Computer-aided fragment extension in a second stage screening yielded a Nur77 agonist with significant activation efficacy and preference over the related NR4A receptors.

Published

2022

5. Propranolol Activates the Orphan Nuclear Receptor TLX to Counteract Proliferation and Migration of Glioblastoma Cells

Author

Rezart Zhubi, Jan Heering, Lea Rachor, Iris Bischoff-Kont, Astrid Kaiser, Apirat Chaikuad, Giuseppe Faudone, Daniel Merk, Robert Fürst, Stefan Knapp, and Sabine Willems

Subjects

Agonist, medicine.drug_class, Central nervous system, Regulator, Receptors, Cytoplasmic and Nuclear, 01 natural sciences, Structure-Activity Relationship, 03 medical and health sciences, Cell Movement, Cell Line, Tumor, Drug Discovery, Gene expression, medicine, Humans, Inverse agonist, Transcription factor, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Molecular Structure, Chemistry, Orphan Nuclear Receptors, Propranolol, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, HEK293 Cells, medicine.anatomical_structure, Nuclear receptor, Cancer research, Molecular Medicine, Glioblastoma, Homeostasis

Abstract

The ligand-sensing transcription factor tailless homologue (TLX, NR2E1) is an essential regulator of neuronal stem cell homeostasis with appealing therapeutic potential in neurodegenerative diseases and central nervous system tumors. However, knowledge on TLX ligands is scarce, providing an obstacle to target validation and medicinal chemistry. To discover TLX ligands, we have profiled a drug fragment collection for TLX modulation and identified several structurally diverse agonists and inverse agonists of the nuclear receptor. Propranolol evolved as the strongest TLX agonist and promoted TLX-regulated gene expression in human glioblastoma cells. Structure-activity relationship elucidation of propranolol as a TLX ligand yielded a structurally related negative control compound. In functional cellular experiments, we observed an ability of propranolol to counteract glioblastoma cell proliferation and migration, while the negative control had no effect. Our results provide a collection of TLX modulators as initial chemical tools and set of lead compounds and support therapeutic potential of TLX modulation in glioblastoma.

Published

2021

6. Kinase Domain Autophosphorylation Rewires the Activity and Substrate Specificity of CK1 Enzymes

Author

Sierra N. Cullati, Apirat Chaikuad, Jun-Song Chen, Jakob Gebel, Laura Tesmer, Rezart Zhubi, Jose Navarrete-Perea, Rodrigo X. Guillen, Steven P. Gygi, Gerhard Hummer, Volker Dötsch, Stefan Knapp, and Kathleen L. Gould

Subjects

Threonine, Cell Biology, Saccharomyces cerevisiae, Protein Serine-Threonine Kinases, Biochemistry, Article, Substrate Specificity, Casein Kinase Idelta, Genetics, Humans, Phosphorylation, Molecular Biology, Signal Transduction, Biotechnology

Abstract

CK1s are acidophilic serine/threonine kinases with multiple critical cellular functions; their misregulation contributes to cancer, neurodegenerative diseases, and sleep phase disorders. Here, we describe an evolutionarily conserved mechanism of CK1 activity: autophosphorylation of a threonine (T220 in human CK1δ) located at the N-terminus of helix αG, proximal to the substrate binding cleft. Crystal structures and molecular dynamics simulations uncovered inherent plasticity in αG that increased upon T220 autophosphorylation. The phosphorylation-induced structural changes significantly altered the conformation of the substrate binding cleft, affecting substrate specificity. In T220 phosphorylated yeast and human CK1s, activity toward many substrates was decreased, but we also identified a high-affinity substrate that was phosphorylated more rapidly, and quantitative phosphoproteomics revealed that disrupting T220 autophosphorylation rewired CK1 signaling in Schizosaccharomyces pombe. T220 is present exclusively in the CK1 family, thus its autophosphorylation may have evolved as a unique regulatory mechanism for this important family.

Published

2022