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834 results on '"Chaikuad A."'

255. Structure-based identification of inhibitory fragments targeting the p300/CBP-associated factor bromodomain

Author

Chaikuad, Apirat, Lang, Steffen, Brennan, Paul E., Temperini, Claudia, Fedorov, Oleg, Hollander, Johan, Nachane, Ruta, Abell, Chris, Müller, Susanne, Siegal, Gregg, and Knapp, Stefan

Subjects
Models, Molecular, Molecular Docking Simulation, Small Molecule Libraries, Brief Article, ddc:570, Drug Discovery, Humans, p300-CBP Transcription Factors, ddc:610, Ligands, Protein Binding, Protein Structure, Tertiary
Abstract

The P300/CBP-associated factor plays a central role in retroviral infection and cancer development, and the C-terminal bromodomain provides an opportunity for selective targeting. Here, we report several new classes of acetyl-lysine mimetic ligands ranging from mM to low micromolar affinity that were identified using fragment screening approaches. The binding modes of the most attractive fragments were determined using high resolution crystal structures providing chemical starting points and structural models for the development of potent and selective PCAF inhibitors.

Published
2016

257. Isoform-Selective ATAD2 Chemical Probe with Novel Chemical Structure and Unusual Mode of Action

Author

Fernández-Montalván, Amaury E., primary, Berger, Markus, additional, Kuropka, Benno, additional, Koo, Seong Joo, additional, Badock, Volker, additional, Weiske, Joerg, additional, Puetter, Vera, additional, Holton, Simon J., additional, Stöckigt, Detlef, additional, ter Laak, Antonius, additional, Centrella, Paolo A., additional, Clark, Matthew A., additional, Dumelin, Christoph E., additional, Sigel, Eric A., additional, Soutter, Holly H., additional, Troast, Dawn M., additional, Zhang, Ying, additional, Cuozzo, John W., additional, Keefe, Anthony D., additional, Roche, Didier, additional, Rodeschini, Vincent, additional, Chaikuad, Apirat, additional, Díaz-Sáez, Laura, additional, Bennett, James M., additional, Fedorov, Oleg, additional, Huber, Kilian V. M., additional, Hübner, Jan, additional, Weinmann, Hilmar, additional, Hartung, Ingo V., additional, and Gorjánácz, Mátyás, additional

Published
2017
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260. Abstract 5084: Potent and isoform-selective ATAD2 bromodomain inhibitor with unprecedented chemical structure and mode of action

Author

Fernández-Montalván, Amaury E., primary, Berger, Markus, additional, Kuropka, Benno, additional, Koo, Seong Joo, additional, Badock, Volker, additional, Weiske, Joerg, additional, Holton, Simon J., additional, Chaikuad, Apirat, additional, Díaz-Sáez, Laura, additional, Bennett, James, additional, Federov, Oleg, additional, Huber, Kilian, additional, Centrella, Paolo, additional, Clark, Matthew A., additional, Dumelin, Christoph E., additional, Sigel, Eric A., additional, Soutter, Holly S., additional, Troast, Dawn M., additional, Zhang, Ying, additional, Cuozzo, John W., additional, Keefe, Anthony D., additional, Roche, Didier, additional, Rodeschini, Vincent, additional, Hübner, Jan, additional, Weinmann, Hilmar, additional, Hartung, Ingo V., additional, and Gorjanacz, Matyas, additional

Published
2017
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263. The ins and outs of selective kinase inhibitor development

Author

Stefan Knapp, Nathanael S. Gray, Susanne Müller, and Apirat Chaikuad

Subjects
Genetics, Kinase, Protein Conformation, United States Food and Drug Administration, Quantitative Structure-Activity Relationship, Cell Biology, Computational biology, Biology, Crystallography, X-Ray, United States, Small Molecule Libraries, Catalytic Domain, Drug Design, Drug Discovery, Humans, Kinome, Molecular Biology, Drug Approval, Protein Kinase Inhibitors, Protein Kinases, Allosteric Site
Abstract

Protein kinases have emerged as one of the most successful families of drug targets. To date, most selective kinase inhibitors have been discovered serendipitously either through broad selectivity screening or through the discovery of unique binding modes. Here we discuss design strategies that could lead to a broader coverage of the kinome with selective inhibitors and to a more rational approach for developing them.

Published
2015

264. Combined Cardioprotective and Adipocyte Browning Effects Promoted by the Eutomer of Dual sEH/PPARγ Modulator

Author

Hartmann, Markus, Bibli, Sofia-Iris, Tews, Daniel, Ni, Xiaomin, Kircher, Theresa, Kramer, Jan S., Kilu, Whitney, Heering, Jan, Hernandez-Olmos, Victor, Weizel, Lilia, Scriba, Gerhard K. E., Krait, Sulaiman, Knapp, Stefan, Chaikuad, Apirat, Merk, Daniel, Fleming, Ingrid, Fischer-Posovszky, Pamela, and Proschak, Ewgenij

Abstract

The metabolic syndrome (MetS) is a constellation of cardiovascular and metabolic symptoms involving insulin resistance, steatohepatitis, obesity, hypertension, and heart disease, and patients suffering from MetS often require polypharmaceutical treatment. PPARγ agonists are highly effective oral antidiabetics with great potential in MetS, which promote adipocyte browning and insulin sensitization. However, the application of PPARγ agonists in clinics is restricted by potential cardiovascular adverse events. We have previously demonstrated that the racemic dual sEH/PPARγ modulator RB394 (3) simultaneously improves all risk factors of MetS in vivo. In this study, we identify and characterize the eutomer of 3. We provide structural rationale for molecular recognition of the eutomer. Furthermore, we could show that the dual sEH/PPARγ modulator is able to promote adipocyte browning and simultaneously exhibits cardioprotective activity which underlines its exciting potential in treatment of MetS.

Published
2021
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265. A core of kinase-regulated interactomes defines the neoplastic MDSC lineage

Author

Noelia Casares, David Guerrero-Setas, Idoia Blanco-Luquin, Isabel Zudaire, Stefan Knapp, Teresa Lozano, Grazyna Kochan, Apirat Chaikuad, David Escors, Enrique Santamaría, Maria Gato-Cañas, Hugo Arasanz, Xabier Martínez de Morentin, Therese Liechtenstein, and Joaquín Fernández-Irigoyen

Subjects
MAPK/ERK pathway, Proteomics, Proteasome Endopeptidase Complex, Myeloid, Cell Survival, Cellular differentiation, MDSC, Melanoma, Experimental, Bone Marrow Cells, Biology, therapeutic targets, interactomes, 03 medical and health sciences, Inhibitory Concentration 50, Mice, Phosphatidylinositol 3-Kinases, 0302 clinical medicine, Neoplasms, medicine, Electric Impedance, Animals, Humans, Cell Lineage, Myeloid Cells, Cancer epigenetics, RNA, Small Interfering, Extracellular Signal-Regulated MAP Kinases, Protein kinase B, 030304 developmental biology, 0303 health sciences, Kinase, Gene Expression Profiling, Cell Differentiation, Dendritic Cells, 3. Good health, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, medicine.anatomical_structure, HEK293 Cells, kinases, Oncology, 030220 oncology & carcinogenesis, Immunology, Proto-Oncogene Proteins c-akt, Proto-oncogene tyrosine-protein kinase Src, Signal Transduction, Research Paper
Abstract

// Maria Gato-Canas 1, 2, * , Xabier Martinez de Morentin 3, * , Idoia Blanco-Luquin 1, 2, * , Joaquin Fernandez-Irigoyen 3, * , Isabel Zudaire 1 , Therese Liechtenstein 1, 2 , Hugo Arasanz 1, 4 , Teresa Lozano 5 , Noelia Casares 5 , Apirat Chaikuad 6 , Stefan Knapp 6, 7 , David Guerrero-Setas 8 , David Escors 1, 2 , Grazyna Kochan 9 , Enrique Santamaria 3 1 Immunomodulation group, Navarrabiomed-FMS, IdiSNA, Pamplona, Spain 2 Immunomodulation group, Division of Infection and Immunity, University College London, UK 3 Proteomics Unit, Navarrabiomed-FMS, Proteored-ISCIII IdiSNA, Pamplona, Spain 4 Hospital de Navarra, Department of Oncology, IdiSNA, Pamplona, Spain 5 Immunology and Immunotherapy Program, Center for Applied Medical Research, University of Navarra, IdiSNA, Pamplona, Spain 6 Structural Genomics Consortium (SGC), University of Oxford, Headington, UK 7 Institute for Pharmaceutical Chemistry, Johann Wolfgang Goethe-University, Frankfurt, Germany 8 Cancer Epigenetics group, Navarrabiomed-FMS, IdiSNA, Pamplona, Spain 9 Protein Production Unit, Navarrabiomed-FMS, IdiSNA, Pamplona, Spain * These authors have contributed equally to this work Correspondence to: David Escors, e-mail: descorsm@navarra.es Grazyna Kochan, e-mail: grazyna.kochan@navarra.es Enrique Santamaria, e-mail: esantamma@navarra.es Keywords: MDSC, proteomics, interactomes, kinases, therapeutic targets Received: May 25, 2015 Accepted: July 13, 2015 Published: July 23, 2015 ABSTRACT Myeloid-derived suppressor cells (MDSCs) differentiate from bone marrow precursors, expand in cancer-bearing hosts and accelerate tumor progression. MDSCs have become attractive therapeutic targets, as their elimination strongly enhances anti-neoplastic treatments. Here, immature myeloid dendritic cells (DCs), MDSCs modeling tumor-infiltrating subsets or modeling non-cancerous (NC)-MDSCs were compared by in-depth quantitative proteomics. We found that neoplastic MDSCs differentially expressed a core of kinases which controlled lineage-specific (PI3K-AKT and SRC kinases) and cancer-induced (ERK and PKC kinases) protein interaction networks (interactomes). These kinases contributed to some extent to myeloid differentiation. However, only AKT and ERK specifically drove MDSC differentiation from myeloid precursors. Interfering with AKT and ERK with selective small molecule inhibitors or shRNAs selectively hampered MDSC differentiation and viability. Thus, we provide compelling evidence that MDSCs constitute a distinct myeloid lineage distinguished by a “kinase signature” and well-defined interactomes. Our results define new opportunities for the development of anti-cancer treatments targeting these tumor-promoting immune cells.

Published
2015

266. Selective inhibitors of Cyclin-G associated kinase (GAK) as anti-HCV agents

Author

Kovackova, Sona, Chang, Lei, Bekerman, Elena, Neveu, Gregory, Barouch-Bentov, Rina, Chaikuad, Apirat, Heroven, Christina, Šála, Michal, De Jonghe, Steven, Knapp, Stefan, Einav, Shirit, and Herdewijn, Piet

Subjects
Models, Molecular, Pyridines, Intracellular Signaling Peptides and Proteins, Hepacivirus, Protein Serine-Threonine Kinases, Virus Internalization, Crystallography, X-Ray, Antiviral Agents, Hepatitis C, Article, Cell Line, Thiazoles, Humans, Protein Kinase Inhibitors
Abstract

Cyclin G associated kinase (GAK) emerged as a promising drug target for the treatment of viral infections. However, no potent and selective GAK inhibitors have been reported in the literature to date. This paper describes the discovery of isothiazolo[5,4-b]pyridines as selective GAK inhibitors, with the most potent congeners displaying low nanomolar binding affinity for GAK. Cocrystallization experiments revealed that these compounds behaved as classic type I ATP-competitive kinase inhibitors. In addition, we have demonstrated that these compounds exhibit a potent activity against hepatitis C virus (HCV) by inhibiting two temporally distinct steps in the HCV life cycle (i.e., viral entry and assembly). Hence, these GAK inhibitors represent chemical probes to study GAK function in different disease areas where GAK has been implicated (including viral infection, cancer, and Parkinson's disease).

Published
2015

267. A Chemical Probe for Dark Kinase STK17B Derives Its Potency and High Selectivity through a Unique P-Loop Conformation

Author

Picado, Alfredo, Chaikuad, Apirat, Wells, Carrow I., Shrestha, Safal, Zuercher, William J., Pickett, Julie E., Kwarcinski, Frank E., Sinha, Parvathi, de Silva, Chandi S., Zutshi, Reena, Liu, Shubin, Kannan, Natarajan, Knapp, Stefan, Drewry, David H., and Willson, Timothy M.

Abstract

STK17B is a member of the death-associated protein kinase family and has been genetically linked to the development of diverse diseases. However, the role of STK17B in normal and disease pathology is poorly defined. Here, we present the discovery of thieno[3,2-d] pyrimidine SGC-STK17B-1(11s), a high-quality chemical probe for this understudied “dark” kinase. 11sis an ATP-competitive inhibitor that showed remarkable selectivity over other kinases including the closely related STK17A. X-ray crystallography of 11sand related thieno[3,2-d]pyrimidines bound to STK17B revealed a unique P-loop conformation characterized by a salt bridge between R41 and the carboxylic acid of the inhibitor. Molecular dynamic simulations of STK17B revealed the flexibility of the P-loop and a wide range of R41 conformations available to the apo-protein. The isomeric thieno[2,3-d]pyrimidine SGC-STK17B-1N(19g) was identified as a negative control compound. The >100-fold lower activity of 19gon STK17B was attributed to the reduced basicity of its pyrimidine N1.

Published
2020
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268. Design, Synthesis, and Characterization of an Orally Active Dual-Specific ULK1/2 Autophagy Inhibitor that Synergizes with the PARP Inhibitor Olaparib for the Treatment of Triple-Negative Breast Cancer

Author

Ren, Huiyu, Bakas, Nicole A., Vamos, Mitchell, Chaikuad, Apirat, Limpert, Allison S., Wimer, Carina D., Brun, Sonja N., Lambert, Lester J., Tautz, Lutz, Celeridad, Maria, Sheffler, Douglas J., Knapp, Stefan, Shaw, Reuben J., and Cosford, Nicholas D. P.

Abstract

Inhibition of autophagy, the major cellular recycling pathway in mammalian cells, is a promising strategy for the treatment of triple-negative breast cancer (TNBC). We previously reported SBI-0206965, a small molecule inhibitor of unc-51-like autophagy activating kinase 1 (ULK1), which is a key regulator of autophagy initiation. Herein, we describe the design, synthesis, and characterization of new dual inhibitors of ULK1 and ULK2 (ULK1/2). One inhibitor, SBP-7455 (compound 26), displayed improved binding affinity for ULK1/2 compared with SBI-0206965, potently inhibited ULK1/2 enzymatic activity in vitro and in cells, reduced the viability of TNBC cells and had oral bioavailability in mice. SBP-7455 inhibited starvation-induced autophagic flux in TNBC cells that were dependent on autophagy for survival and displayed synergistic cytotoxicity with the poly (ADP-ribose) polymerase (PARP) inhibitor olaparib against TNBC cells. These data suggest that combining ULK1/2 and PARP inhibition may have clinical utility for the treatment of TNBC.

Published
2020
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269. p63 uses a switch-like mechanism to set the threshold for induction of apoptosis

Author

Gebel, Jakob, Tuppi, Marcel, Chaikuad, Apirat, Hötte, Katharina, Schröder, Martin, Schulz, Laura, Löhr, Frank, Gutfreund, Niklas, Finke, Franziska, Henrich, Erik, Mezhyrova, Julija, Lehnert, Ralf, Pampaloni, Francesco, Hummer, Gerhard, Stelzer, Ernst H. K., Knapp, Stefan, and Dötsch, Volker

Abstract

The p53 homolog TAp63a is the transcriptional key regulator of genome integrity in oocytes. After DNA damage, TAp63a is activated by multistep phosphorylation involving multiple phosphorylation events by the kinase CK1, which triggers the transition from a dimeric and inactive conformation to an open and active tetramer that initiates apoptosis. By measuring activation kinetics in ovaries and single-site phosphorylation kinetics in vitro with peptides and full-length protein, we show that TAp63a phosphorylation follows a biphasic behavior. Although the first two CK1 phosphorylation events are fast, the third one, which constitutes the decisive step to form the active conformation, is slow. Structure determination of CK1 in complex with differently phosphorylated peptides reveals the structural mechanism for the difference in the kinetic behavior based on an unusual CK1/TAp63a substrate interaction in which the product of one phosphorylation step acts as an inhibitor for the following one.

Published
2020
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270. Discovery of the First in Vivo Active Inhibitors of the Soluble Epoxide Hydrolase Phosphatase Domain.

Author

Kramer, Jan S., Woltersdorf, Stefano, Duflot, Thomas, Hiesinger, Kerstin, Lillich, Felix F., Knöll, Felix, Wittmann, Sandra K., Klingler, Franca-M., Brunst, Steffen, Chaikuad, Apirat, Morisseau, Christophe, Hammock, Bruce D., Buccellati, Carola, Sala, Angelo, Rovati, G. Enrico, Leuillier, Matthieu, Fraineau, Sylvain, Rondeaux, Julie, Hernandez-Olmos, Victor, and Heering, Jan

Published
2019
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271. Development of Potent, Selective SRPK1 Inhibitors as Potential Topical Therapeutics for Neovascular Eye Disease

Author

Batson, J, Toop, HD ; https://orcid.org/0000-0003-4637-4764, Redondo, C, Babaei-Jadidi, R, Chaikuad, A, Wearmouth, SF, Gibbons, B, Allen, C, Tallant, C, Zhang, J, Du, C, Hancox, JC, Hawtrey, T, Da Rocha, J, Griffith, R ; https://orcid.org/0000-0001-7739-5686, Knapp, S, Bates, DO, Morris, JC ; https://orcid.org/0000-0002-5109-9069, Batson, J, Toop, HD ; https://orcid.org/0000-0003-4637-4764, Redondo, C, Babaei-Jadidi, R, Chaikuad, A, Wearmouth, SF, Gibbons, B, Allen, C, Tallant, C, Zhang, J, Du, C, Hancox, JC, Hawtrey, T, Da Rocha, J, Griffith, R ; https://orcid.org/0000-0001-7739-5686, Knapp, S, Bates, DO, and Morris, JC ; https://orcid.org/0000-0002-5109-9069

Abstract

Serine/arginine-protein kinase 1 (SRPK1) regulates alternative splicing of VEGF-A to pro-angiogenic isoforms and SRPK1 inhibition can restore the balance of pro/antiangiogenic isoforms to normal physiological levels. The lack of potency and selectivity of available compounds has limited development of SRPK1 inhibitors, with the control of alternative splicing by splicing factor-specific kinases yet to be translated. We present here compounds that occupy a binding pocket created by the unique helical insert of SRPK1, and trigger a backbone flip in the hinge region, that results in potent (<10 nM) and selective inhibition of SRPK1 kinase activity. Treatment with these inhibitors inhibited SRPK1 activity and phosphorylation of serine/arginine splicing factor 1 (SRSF1), resulting in alternative splicing of VEGF-A from pro-angiogenic to antiangiogenic isoforms. This property resulted in potent inhibition of blood vessel growth in models of choroidal angiogenesis in vivo. This work identifies tool compounds for splice isoform selective targeting of pro-angiogenic VEGF, which may lead to new therapeutic strategies for a diversity of diseases where dysfunctional splicing drives disease development.

Published
2017

272. Development of potent, selective SRPK1 inhibitors as potential topical therapeutics for neovascular eye disease

Author

Batson, Jennifer, Toop, Hamish D., Redondo, Clara, Babaei-Jadid, Roya, Chaikuad, Apirat, Wearmouth, Stephen F., Gibbons, Brian, Allen, Claire, Tallant, Cynthia, Zhang, Jingxue, Du, Chunyun, Hancox, Jules C., Hawtrey, Tom, Rocha, Joana Pinto da, Griffith, Renate, Knapp, Stefan, Bates, David O., Morris, Jonathan C., Batson, Jennifer, Toop, Hamish D., Redondo, Clara, Babaei-Jadid, Roya, Chaikuad, Apirat, Wearmouth, Stephen F., Gibbons, Brian, Allen, Claire, Tallant, Cynthia, Zhang, Jingxue, Du, Chunyun, Hancox, Jules C., Hawtrey, Tom, Rocha, Joana Pinto da, Griffith, Renate, Knapp, Stefan, Bates, David O., and Morris, Jonathan C.

Abstract

Serine/arginine-protein kinase 1 (SRPK1) regulates alternative splicing of VEGF-A to pro-angiogenic isoforms and SRPK1 inhibition can restore the balance of pro/antiangiogenic isoforms to normal physiological levels. The lack of potency and selectivity of available compounds has limited development of SRPK1 inhibitors, with the control of alternative splicing by splicing factor-specific kinases yet to be translated. We present here compounds that occupy a binding pocket created by the unique helical insert of SRPK1, and trigger a backbone flip in the hinge region, that results in potent (<10 nM) and selective inhibition of SRPK1 kinase activity. Treatment with these inhibitors inhibited SRPK1 activity and phosphorylation of serine/arginine splicing factor 1 (SRSF1), resulting in alternative splicing of VEGF-A from pro-angiogenic to antiangiogenic isoforms. This property resulted in potent inhibition of blood vessel growth in models of choroidal angiogenesis in vivo. This work identifies tool compounds for splice isoform selective targeting of pro-angiogenic VEGF, which may lead to new therapeutic strategies for a diversity of diseases where dysfunctional splicing drives disease development.

Published
2017

276. Bisubstrate inhibitor approach for targeting mitotic kinase Haspin

Author

Apirat Chaikuad, Gerda Raidaru, Darja Lavogina, Asko Uri, Katrin Kestav, and Stefan Knapp

Subjects
Models, Molecular, Biomedical Engineering, Pharmaceutical Science, Mitosis, Bioengineering, Protein Serine-Threonine Kinases, Histones, chemistry.chemical_compound, Histone H3, Adenosine Triphosphate, Humans, Amino Acid Sequence, Binding site, Protein kinase A, Protein Kinase Inhibitors, Pharmacology, Protein-Serine-Threonine Kinases, Binding Sites, biology, Kinase, Chemistry, Organic Chemistry, Intracellular Signaling Peptides and Proteins, Recombinant Proteins, Histone, Biochemistry, biology.protein, Phosphorylation, Peptides, Adenosine triphosphate, Biotechnology
Abstract

During the past decade, the basophilic atypical kinase Haspin has emerged as a key player in mitosis responsible for phosphorylation of Thr3 residue of histone H3. Here, we report the construction of conjugates comprising an aromatic fragment targeted to the ATP-site of Haspin and a peptide mimicking the N-terminus of histone H3. The combination of effective solid phase synthesis procedures and a high throughput binding/displacement assay with fluorescence anisotropy readout afforded the development of inhibitors with remarkable subnanomolar affinity toward Haspin. The selectivity profiles of novel conjugates were established by affinity studies with a model basophilic kinase (catalytic subunit of cAMP-dependent protein kinase) and by a commercial 1-point inhibition assay with 43 protein kinases.

Published
2015

277. Abstract 5084: Potent and isoform-selective ATAD2 bromodomain inhibitor with unprecedented chemical structure and mode of action

Author

L. Diaz-Saez, Hilmar Weinmann, Christoph E. Dumelin, Dawn M. Troast, Joerg Weiske, John W. Cuozzo, Ingo Hartung, Ying Zhang, James M. Bennett, Anthony D. Keefe, Didier M. Roche, Seong Joo Koo, Kilian Huber, Benno Kuropka, Oleg Federov, Matthew A. Clark, Markus Berger, Eric A. Sigel, Paolo A. Centrella, Mátyás Gorjánácz, Volker Badock, Apirat Chaikuad, Jan Hübner, Simon Holton, Holly S. Soutter, Amaury Ernesto Fernandez-Montalvan, and Vincent Rodeschini

Subjects
Cancer Research, biology, Protein family, Chemistry, Bromodomain, Chromatin, Histone H4, Histone, Oncology, Biochemistry, biology.protein, Mode of action, E2F, Transcription factor
Abstract

ATAD2 (ATPase family AAA-domain containing protein 2, also called ANCCA) is an epigenetic regulator that binds to chromatin through its bromodomain (BD), a motif specialized for acetyl-lysine recognition. ATAD2 directly associates with multiple transcription factors such as ERα, AR, E2F, and Myc; hence, ATAD2 has been proposed to act as a co-factor for oncogenic transcription factors. Furthermore, we have recently reported a novel role for ATAD2 during DNA replication, uncovering interactions between ATAD2 and histone acetylation marks on newly synthesized histone H4. High expression of ATAD2 strongly correlates with poor patient prognosis in multiple tumor types, including gastric, endometrial, hepatocellular, ovarian, breast and lung cancers. However, the exact function of ATAD2 in these tumor types remains unclear. A more thorough validation of ATAD2 as a therapeutic target is hampered by the lack of isoform-selective, potent and cellularly active ATAD2 inhibitors. A systematic assessment of crystal structures of BD-containing protein family predicted that development of selective inhibitors of ATAD2 would be challenging. In line with this prediction, only limited progress in developing lead compounds targeting ATAD2 has been reported so far. A few notable exceptions relied on fragments as starting points, however, their weak potency, insufficient selectivity against other BDs, permeability limitations or modest cellular activity have curbed their further development towards drug candidates. Here we embarked on a novel strategy to identify ATAD2 inhibitors: 11 different DNA-encoded libraries adding up to 67 billion unique encoded compounds were combined and incubated with ATAD2 BD followed by two rounds of affinity-mediated selection. This approach provided with several series of binders, for which specific target engagement of their SMOL moiety upon off-DNA synthesis was confirmed in biochemical and biophysical assays. Several rounds of potency optimization led to the identification of BAY-850, a highly potent and ATAD2 (isoform A) mono-selective inhibitor, which holds an amine substituted 3-(2-furyl)benzamide core. This compound shows - as revealed by size exclusion chromatography and native mass spectrometry - a novel mode of action for a BD inhibitor based on specific target dimerization. In a cellular fluorescence recovery after photobleaching (FRAP) assay BAY-850 displaced wild-type ATAD2 from the chromatin to the same extent as the genetic mutagenesis of ATAD2 BD. In contrast, chemically very similar inactive control compounds showed no major effects on ATAD2 association with the chromatin. These results qualify BAY-850 as the first biologically active ATAD2 isoform A-specific chemical probe, which will enable further elucidation of the cancer biology of this intriguing protein. Citation Format: Amaury E. Fernández-Montalván, Markus Berger, Benno Kuropka, Seong Joo Koo, Volker Badock, Joerg Weiske, Simon J. Holton, Apirat Chaikuad, Laura Díaz-Sáez, James Bennett, Oleg Federov, Kilian Huber, Paolo Centrella, Matthew A. Clark, Christoph E. Dumelin, Eric A. Sigel, Holly S. Soutter, Dawn M. Troast, Ying Zhang, John W. Cuozzo, Anthony D. Keefe, Didier Roche, Vincent Rodeschini, Jan Hübner, Hilmar Weinmann, Ingo V. Hartung, Matyas Gorjanacz. Potent and isoform-selective ATAD2 bromodomain inhibitor with unprecedented chemical structure and mode of action [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 5084. doi:10.1158/1538-7445.AM2017-5084

Published
2017
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278. Modulation of the chromatin phosphoproteome by the Haspin protein kinase

Author

Maiolica, Alessio, de Medina-Redondo, Maria, Schoof, Erwin M, Chaikuad, Apirat, Villa, Fabrizio, Gatti, Marco, et al, Penengo, Lorenza, and University of Zurich

Subjects
1602 Analytical Chemistry, 1303 Biochemistry, 10061 Institute of Molecular Cancer Research, 1312 Molecular Biology, 570 Life sciences, biology, 610 Medicine & health
Published
2014

279. Development of Potent, Selective SRPK1 Inhibitors as Potential Topical Therapeutics for Neovascular Eye Disease

Author

Batson, Jennifer, primary, Toop, Hamish D., additional, Redondo, Clara, additional, Babaei-Jadidi, Roya, additional, Chaikuad, Apirat, additional, Wearmouth, Stephen F., additional, Gibbons, Brian, additional, Allen, Claire, additional, Tallant, Cynthia, additional, Zhang, Jingxue, additional, Du, Chunyun, additional, Hancox, Jules C., additional, Hawtrey, Tom, additional, Da Rocha, Joana, additional, Griffith, Renate, additional, Knapp, Stefan, additional, Bates, David O., additional, and Morris, Jonathan C., additional

Published
2017
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280. This title is unavailable for guests, please login to see more information.

Author

Petersen, L. K., Blakskjær, P., Chaikuad, A., Christensen, A. B., Dietvorst, J., Holmkvist, J., Knapp, S., Kořínek, M., Larsen, L. K., Pedersen, A. E., Röhm, S., Sløk, F. A., Hansen, N. J V, Petersen, L. K., Blakskjær, P., Chaikuad, A., Christensen, A. B., Dietvorst, J., Holmkvist, J., Knapp, S., Kořínek, M., Larsen, L. K., Pedersen, A. E., Röhm, S., Sløk, F. A., and Hansen, N. J V

Published
2016

281. Discovery of a PCAF bromodomain chemical probe

Author

Moustakim, Moses, Clark, Peter G. K., Trulli, Laura, Fuentes de Arriba, Angel L., Ehebauer, Matthias T., Chaikuad, Apirat, Murphy, Emma J., Mendez-Johnson, Jacqui, Daniels, Danette, Hou, Chun-Feng D., Lin, Yu-Hui, Walker, John R., Hui, Raymond, Yang, Hongbing, Dorrell, Lucy, Rogers, Catherine M., Monteiro, Octovia, Fedorov, Oleg, Huber, Kilian, Knapp, Stefan, Heer, Jag, Dixon, Darren, Brennan, Paul E., Moustakim, Moses, Clark, Peter G. K., Trulli, Laura, Fuentes de Arriba, Angel L., Ehebauer, Matthias T., Chaikuad, Apirat, Murphy, Emma J., Mendez-Johnson, Jacqui, Daniels, Danette, Hou, Chun-Feng D., Lin, Yu-Hui, Walker, John R., Hui, Raymond, Yang, Hongbing, Dorrell, Lucy, Rogers, Catherine M., Monteiro, Octovia, Fedorov, Oleg, Huber, Kilian, Knapp, Stefan, Heer, Jag, Dixon, Darren, and Brennan, Paul E.

Abstract

The p300/CBP‐associated factor (PCAF) and related GCN5 bromodomain‐containing lysine acetyl transferases are members of subfamily I of the bromodomain phylogenetic tree. Iterative cycles of rational inhibitor design and biophysical characterization led to the discovery of the triazolopthalazine‐based L‐45 (dubbed L‐Moses) as the first potent, selective, and cell‐active PCAF bromodomain (Brd) inhibitor. Synthesis from readily available (1R,2S)‐(−)‐norephedrine furnished L‐45 in enantiopure form. L‐45 was shown to disrupt PCAF‐Brd histone H3.3 interaction in cells using a nanoBRET assay, and a co‐crystal structure of L‐45 with the homologous Brd PfGCN5 from Plasmodium falciparum rationalizes the high selectivity for PCAF and GCN5 bromodomains. Compound L‐45 shows no observable cytotoxicity in peripheral blood mononuclear cells (PBMC), good cell‐permeability, and metabolic stability in human and mouse liver microsomes, supporting its potential for in vivo use.

Published
2016

282. Back Cover: Discovery of a PCAF Bromodomain Chemical Probe (Angew. Chem. Int. Ed. 3/2017)

Author

Moustakim, Moses, primary, Clark, Peter G. K., additional, Trulli, Laura, additional, Fuentes de Arriba, Angel L., additional, Ehebauer, Matthias T., additional, Chaikuad, Apirat, additional, Murphy, Emma J., additional, Mendez‐Johnson, Jacqui, additional, Daniels, Danette, additional, Hou, Chun‐Feng D., additional, Lin, Yu‐Hui, additional, Walker, John R., additional, Hui, Raymond, additional, Yang, Hongbing, additional, Dorrell, Lucy, additional, Rogers, Catherine M., additional, Monteiro, Octovia P., additional, Fedorov, Oleg, additional, Huber, Kilian V. M., additional, Knapp, Stefan, additional, Heer, Jag, additional, Dixon, Darren J., additional, and Brennan, Paul E., additional

Published
2016
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283. Rücktitelbild: Discovery of a PCAF Bromodomain Chemical Probe (Angew. Chem. 3/2017)

Author

Moustakim, Moses, primary, Clark, Peter G. K., additional, Trulli, Laura, additional, Fuentes de Arriba, Angel L., additional, Ehebauer, Matthias T., additional, Chaikuad, Apirat, additional, Murphy, Emma J., additional, Mendez‐Johnson, Jacqui, additional, Daniels, Danette, additional, Hou, Chun‐Feng D., additional, Lin, Yu‐Hui, additional, Walker, John R., additional, Hui, Raymond, additional, Yang, Hongbing, additional, Dorrell, Lucy, additional, Rogers, Catherine M., additional, Monteiro, Octovia P., additional, Fedorov, Oleg, additional, Huber, Kilian V. M., additional, Knapp, Stefan, additional, Heer, Jag, additional, Dixon, Darren J., additional, and Brennan, Paul E., additional

Published
2016
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285. Discovery of a PCAF Bromodomain Chemical Probe

Author

Moustakim, Moses, primary, Clark, Peter G. K., additional, Trulli, Laura, additional, Fuentes de Arriba, Angel L., additional, Ehebauer, Matthias T., additional, Chaikuad, Apirat, additional, Murphy, Emma J., additional, Mendez‐Johnson, Jacqui, additional, Daniels, Danette, additional, Hou, Chun‐Feng D., additional, Lin, Yu‐Hui, additional, Walker, John R., additional, Hui, Raymond, additional, Yang, Hongbing, additional, Dorrell, Lucy, additional, Rogers, Catherine M., additional, Monteiro, Octovia P., additional, Fedorov, Oleg, additional, Huber, Kilian V. M., additional, Knapp, Stefan, additional, Heer, Jag, additional, Dixon, Darren J., additional, and Brennan, Paul E., additional

Published
2016
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286. An Unusual Binding Model of the Methyl 9-Anilinothiazolo[5,4-f] quinazoline-2-carbimidates (EHT 1610 and EHT 5372) Confers High Selectivity for Dual-Specificity Tyrosine Phosphorylation-Regulated Kinases

Author

Chaikuad, Apirat, primary, Diharce, Julien, additional, Schröder, Martin, additional, Foucourt, Alicia, additional, Leblond, Bertrand, additional, Casagrande, Anne-Sophie, additional, Désiré, Laurent, additional, Bonnet, Pascal, additional, Knapp, Stefan, additional, and Besson, Thierry, additional

Published
2016
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287. Selective JAK3 Inhibitors with a Covalent Reversible Binding Mode Targeting a New Induced Fit Binding Pocket

Author

Forster, Michael, primary, Chaikuad, Apirat, additional, Bauer, Silke M., additional, Holstein, Julia, additional, Robers, Matthew B., additional, Corona, Cesear R., additional, Gehringer, Matthias, additional, Pfaffenrot, Ellen, additional, Ghoreschi, Kamran, additional, Knapp, Stefan, additional, and Laufer, Stefan A., additional

Published
2016
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291. A unique inhibitor binding site in ERK1/2 is associated with slow binding kinetics

Author

Stefan Knapp, Yanke Liang, Nathanael S. Gray, Apirat Chaikuad, Eliana M.C. Tacconi, Jutta Zimmer, and Madalena Tarsounas

Subjects
MAPK/ERK pathway, Indazoles, Mitogen-Activated Protein Kinase 3, Stereochemistry, MAP Kinase Signaling System, Gene Expression, Antineoplastic Agents, Plasma protein binding, Biology, Protein Serine-Threonine Kinases, Piperazines, Protein Structure, Secondary, Protein structure, Cell Line, Tumor, Humans, Mitogen-Activated Protein Kinase 8, Binding site, Enzyme Inhibitors, Molecular Biology, Mitogen-Activated Protein Kinase 1, Binding Sites, Kinase, Intracellular Signaling Peptides and Proteins, Cell Biology, In vitro, Recombinant Proteins, 3. Good health, Protein Structure, Tertiary, Gene Expression Regulation, Neoplastic, Kinetics, Helix, Biophysics, Protein Binding
Abstract

Activation of the ERK pathway is a hallmark of cancer, and targeting of upstream signaling partners led to the development of approved drugs. Recently, SCH772984 has been shown to be a selective and potent ERK1/2 inhibitor. Here we report the structural mechanism for its remarkable selectivity. In ERK1/2, SCH772984 induces a so-far-unknown binding pocket that accommodates the piperazine-phenyl-pyrimidine decoration. This new binding pocket was created by an inactive conformation of the phosphate-binding loop and an outward tilt of helix αC. In contrast, structure determination of SCH772984 with the off-target haspin and JNK1 revealed two canonical but distinct type I binding modes. Notably, the new binding mode with ERK1/2 was associated with slow binding kinetics in vitro as well as in cell-based assay systems. The described binding mode of SCH772984 with ERK1/2 enables the design of a new type of specific kinase inhibitors with prolonged on-target activity.

Published
2014

292. Structure-based approaches towards identification of fragments for the low-druggability ATAD2 bromodomain

Author

Apirat Chaikuad, Jing Xu, Andrew M. Petros, Stefan Knapp, and Oleg Fedorov

Subjects
Pharmacology, Chemical shift, Organic Chemistry, Binding properties, Druggability, Pharmaceutical Science, Patient survival, Computational biology, Biology, Biochemistry, 3. Good health, Bromodomain, Crystallography, Signaling proteins, Drug Discovery, Molecular Medicine, Structure based
Abstract

The transcriptional co-regulator ATAD2 is a prognostic marker for patient survival in many cancers. ATAD2 harbours a bromodomain which may offer an opportunity for pharmacological intervention, but its shallow, polar binding surface makes the development of inhibitors challenging. Here we optimized crystal transfer/soaking conditions enabling crystallographic fragment screening. We describe nine crystal structures of fragments including thymidine, a novel acetyl-lysine mimetic ligand and the evaluation of the binding properties of the identified fragments using NMR chemical shift perturbation experiments. The presented binding modes offer chemical starting points for the development of more potent ATAD2 inhibitors. This journal is

Published
2014

293. Conservation of structure, function and inhibitor binding in UNC-51-like kinase 1 and 2 (ULK1/2).

Author

Chaikuad, Apirat, Koschade, Sebastian E., Stolz, Alexandra, Zivkovic, Katarina, Pohl, Christian, Shaid, Shabnam, Ren, Huiyu, Lambert, Lester J., Cosford, Nicholas D. P., Brandts, Christian H., and Knapp, Stefan

Subjects
*CRYSTAL structure, *STRUCTURAL models, *CHEMICAL models, *KINASES, *CANCER treatment
Abstract

Autophagy is essential for cellular homeostasis and when deregulated this survival mechanism has been associated with disease development. Inhibition of autophagy initiation by inhibiting the kinase ULK1 (Unc-51-like autophagy activating kinase 1) has been proposed as a potential cancer therapy. While inhibitors and crystal structures of ULK1 have been reported, little is known about the other closely related kinase ULK2 (Unc-51-like autophagy activating kinase 2). Here, we present the crystal structure of ULK2 in complex with ATP competitive inhibitors. Surprisingly, the ULK2 structure revealed a dimeric assembly reminiscent of dimeric arrangements of auto-activating kinases suggesting a role for this association in ULK activation. Screening of a kinase focused library of pre-clinical and clinical compounds revealed several potent ULK1/2 inhibitors and good correlation of inhibitor- binding behavior with both ULK kinases. Aurora A was identified as a major off-target of currently used ULK1 inhibitors. Autophagic flux assays demonstrated that this off-target activity by strongly inducing autophagy in different cellular systems conferred an additional layer of complexity in the interpretation of cellular data. The data presented here provide structural models and chemical starting points for the development of ULK1/2 dual inhibitors with improved selectivity for future exploitation of autophagy inhibition. [ABSTRACT FROM AUTHOR]

Published
2019
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294. Targeting low-druggability bromodomains: fragment based screening and inhibitor design against the BAZ2B bromodomain

Author

Chris Abell, Martin Philpott, Frank von Delft, Fleur M. Ferguson, I. Felletar, Stefan Knapp, Alessio Ciulli, Oleg Fedorov, Tom D. Heightman, João R. C. Muniz, and Apirat Chaikuad

Subjects
Models, Molecular, 0303 health sciences, Brief Article, Molecular Structure, PLANEJAMENTO DE FÁRMACOS, 010405 organic chemistry, Druggability, Proteins, Zinc Fingers, Computational biology, Biology, Ligands, Bioinformatics, 01 natural sciences, 0104 chemical sciences, Bromodomain, Structure-Activity Relationship, 03 medical and health sciences, Drug Design, Drug Discovery, Humans, Molecular Medicine, Transcription Factors, General, 030304 developmental biology
Abstract

Bromodomains are epigenetic reader domains that have recently become popular targets. In contrast to BET bromodomains, which have proven druggable, bromodomains from other regions of the phylogenetic tree have shallower pockets. We describe successful targeting of the challenging BAZ2B bromodomain using biophysical fragment screening and structure-based optimization of high ligand-efficiency fragments into a novel series of low-micromolar inhibitors. Our results provide attractive leads for development of BAZ2B chemical probes and indicate the whole family may be tractable.

Published
2013

295. A new class of small molecule inhibitor of BMP signaling

Author

Sanvitale, CE, Kerr, G, Chaikuad, A, Ramel, MC, Mohedas, AH, Reichert, S, Wang, Y, Triffitt, JT, Cuny, GD, Yu, PB, Hill, CS, and Bullock, AN

Subjects
Models, Molecular, General Science & Technology, lcsh:R, Molecular Conformation, lcsh:Medicine, Aminopyridines, Neovascularization, Physiologic, Smad Proteins, Pyrimidines, Phenols, Bone Morphogenetic Proteins, MD Multidisciplinary, Animals, Humans, Pyrazoles, lcsh:Q, lcsh:Science, Activin Receptors, Type I, Protein Kinase Inhibitors, Zebrafish, Body Patterning, Protein Binding, Signal Transduction
Abstract

Growth factor signaling pathways are tightly regulated by phosphorylation and include many important kinase targets of interest for drug discovery. Small molecule inhibitors of the bone morphogenetic protein (BMP) receptor kinase ALK2 (ACVR1) are needed urgently to treat the progressively debilitating musculoskeletal disease fibrodysplasia ossificans progressiva (FOP). Dorsomorphin analogues, first identified in zebrafish, remain the only BMP inhibitor chemotype reported to date. By screening an assay panel of 250 recombinant human kinases we identified a highly selective 2-aminopyridine-based inhibitor K02288 with in vitro activity against ALK2 at low nanomolar concentrations similar to the current lead compound LDN-193189. K02288 specifically inhibited the BMP-induced Smad pathway without affecting TGF-β signaling and induced dorsalization of zebrafish embryos. Comparison of the crystal structures of ALK2 with K02288 and LDN-193189 revealed additional contacts in the K02288 complex affording improved shape complementarity and identified the exposed phenol group for further optimization of pharmacokinetics. The discovery of a new chemical series provides an independent pharmacological tool to investigate BMP signaling and offers multiple opportunities for pre-clinical development.

Published
2013

296. Rücktitelbild: Discovery of a PCAF Bromodomain Chemical Probe (Angew. Chem. 3/2017)

Author

Paul Brennan, Danette L. Daniels, Kilian Huber, Peter G. K. Clark, Ángel L. Fuentes de Arriba, Laura Trulli, Jacqui Mendez‐Johnson, Raymond Hui, Octovia P. Monteiro, Jag Paul Heer, Emma J. Murphy, John R. Walker, Darren J. Dixon, Stefan Knapp, Lucy Dorrell, Moses Moustakim, Y.H. Lin, Matthias T. Ehebauer, Chun-Feng David Hou, Apirat Chaikuad, Catherine M. Rogers, Oleg Fedorov, and Hongbing Yang

Subjects
PCAF, Chemistry, Chemical probe, General Medicine, Combinatorial chemistry, Bromodomain
Published
2016
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297. Back Cover: Discovery of a PCAF Bromodomain Chemical Probe (Angew. Chem. Int. Ed. 3/2017)

Author

Moses Moustakim, Hongbing Yang, Raymond Hui, Darren J. Dixon, Jacqui Mendez‐Johnson, Apirat Chaikuad, Paul Brennan, Stefan Knapp, Ángel L. Fuentes de Arriba, Danette L. Daniels, Kilian Huber, Laura Trulli, Y.H. Lin, Octovia P. Monteiro, Oleg Fedorov, Jag Paul Heer, Peter G. K. Clark, Emma J. Murphy, Chun-Feng David Hou, Catherine M. Rogers, John R. Walker, Matthias T. Ehebauer, and Lucy Dorrell

Subjects
PCAF, Chemistry, Stereochemistry, Cover (algebra), Chemical probe, General Chemistry, Catalysis, Bromodomain
Published
2016
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298. Identification of CLK1 Inhibitors by a Fragment-linking Based Virtual Screening

Author

Laurent Meijer, Oliver Koch, Lutz Preu, Nadège Loaëc, Stefan Knapp, Apirat Chaikuad, Anne Walter, and Conrad Kunick

Subjects
0301 basic medicine, Computational biology, Protein Serine-Threonine Kinases, Biology, CLK1, 03 medical and health sciences, Adenosine Triphosphate, Protein structure, Structural Biology, Drug Discovery, Humans, Amino Acid Sequence, Protein Kinase Inhibitors, Genetics, Virtual screening, Binding Sites, Kinase, Organic Chemistry, Alternative splicing, Protein-Tyrosine Kinases, Computer Science Applications, Molecular Docking Simulation, 030104 developmental biology, Docking (molecular), RNA splicing, Molecular Medicine, Phosphorylation, Sequence Alignment, Databases, Chemical
Abstract

Alternative splicing plays an important role in the regulation of protein biosynthesis. CDC2-like kinases (CLKs) phosphorylate splicing factors rendering them a potential target for treating diseases caused by splicing dysregulation.[1] As selective and potent inhibitors of CLK1 are still lacking, a fragment-linking based virtual screening campaign was successfully applied to identify new inhibitors showing activity on CLK1. These inhibitors exhibit a novel 2,4-substituted 1,3-thiazole scaffold that is suitable for further modification. A subsequently performed docking and protein structure based analysis revealed first hints for inhibitors showing preferred binding activity for CLK1 and DYRK2 over other splicing kinases.

Published
2016
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299. A new class of small molecule inhibitor of BMP signaling

Author

Caroline E, Sanvitale, Georgina, Kerr, Apirat, Chaikuad, Marie-Christine, Ramel, Agustin H, Mohedas, Sabine, Reichert, You, Wang, James T, Triffitt, Gregory D, Cuny, Paul B, Yu, Caroline S, Hill, and Alex N, Bullock

Subjects
Models, Molecular, Molecular Conformation, Biophysics, Aminopyridines, Neovascularization, Physiologic, Smad Proteins, Signal transduction, Biochemistry, Protein Chemistry, Signaling Pathways, Molecular cell biology, Phenols, Chemical Biology, Drug Discovery, Morphogenesis, Animals, Humans, Membrane Receptor Signaling, Biomacromolecule-Ligand Interactions, Protein Kinase Inhibitors, Biology, Zebrafish, Protein kinase signaling cascade, Body Patterning, Proteins, Signaling cascades, Chemistry, Pyrimidines, TGF-beta signaling cascade, Small Molecules, Bone Morphogenetic Proteins, Pyrazoles, Medicinal Chemistry, Activin Receptors, Type I, Protein Binding, Research Article, Developmental Biology
Abstract

Growth factor signaling pathways are tightly regulated by phosphorylation and include many important kinase targets of interest for drug discovery. Small molecule inhibitors of the bone morphogenetic protein (BMP) receptor kinase ALK2 (ACVR1) are needed urgently to treat the progressively debilitating musculoskeletal disease fibrodysplasia ossificans progressiva (FOP). Dorsomorphin analogues, first identified in zebrafish, remain the only BMP inhibitor chemotype reported to date. By screening an assay panel of 250 recombinant human kinases we identified a highly selective 2-aminopyridine-based inhibitor K02288 with in vitro activity against ALK2 at low nanomolar concentrations similar to the current lead compound LDN-193189. K02288 specifically inhibited the BMP-induced Smad pathway without affecting TGF-β signaling and induced dorsalization of zebrafish embryos. Comparison of the crystal structures of ALK2 with K02288 and LDN-193189 revealed additional contacts in the K02288 complex affording improved shape complementarity and identified the exposed phenol group for further optimization of pharmacokinetics. The discovery of a new chemical series provides an independent pharmacological tool to investigate BMP signaling and offers multiple opportunities for pre-clinical development.

Published
2012

300. Structure of human aspartyl aminopeptidase complexed with substrate analogue: insight into catalytic mechanism, substrate specificity and M18 peptidase family

Author

Kathryn L. Kavanagh, Antonio De Riso, Apirat Chaikuad, Wyatt W. Yue, Ewa S. Pilka, Frank von Delft, Catherine Vénien-Bryan, and Udo Oppermann

Subjects
Models, Molecular, Molecular Sequence Data, Static Electricity, Dodecameric tetrahedron, Biology, Crystallography, X-Ray, Glutamyl Aminopeptidase, M18 peptidase, Substrate Specificity, 03 medical and health sciences, Metalloprotease, 0302 clinical medicine, Structural Biology, Catalytic Domain, Hydrolase, Humans, Amino Acid Sequence, Peptide sequence, lcsh:QH301-705.5, 030304 developmental biology, chemistry.chemical_classification, Peptide Metabolism, 0303 health sciences, Bacteria, Substrate (chemistry), Ligand (biochemistry), Amino acid, Protein Structure, Tertiary, Domain swapping, chemistry, Biochemistry, lcsh:Biology (General), Metals, Multigene Family, Glutamyl aminopeptidase, Biocatalysis, Protein Multimerization, Aspartyl aminopeptidase, 030217 neurology & neurosurgery, Research Article
Abstract

Backround Aspartyl aminopeptidase (DNPEP), with specificity towards an acidic amino acid at the N-terminus, is the only mammalian member among the poorly understood M18 peptidases. DNPEP has implicated roles in protein and peptide metabolism, as well as the renin-angiotensin system in blood pressure regulation. Despite previous enzyme and substrate characterization, structural details of DNPEP regarding ligand recognition and catalytic mechanism remain to be delineated. Results The crystal structure of human DNPEP complexed with zinc and a substrate analogue aspartate-β-hydroxamate reveals a dodecameric machinery built by domain-swapped dimers, in agreement with electron microscopy data. A structural comparison with bacterial homologues identifies unifying catalytic features among the poorly understood M18 enzymes. The bound ligands in the active site also reveal the coordination mode of the binuclear zinc centre and a substrate specificity pocket for acidic amino acids. Conclusions The DNPEP structure provides a molecular framework to understand its catalysis that is mediated by active site loop swapping, a mechanism likely adopted in other M18 and M42 metallopeptidases that form dodecameric complexes as a self-compartmentalization strategy. Small differences in the substrate binding pocket such as shape and positive charges, the latter conferred by a basic lysine residue, further provide the key to distinguishing substrate preference. Together, the structural knowledge will aid in the development of enzyme-/family-specific aminopeptidase inhibitors.

Published
2012

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