Your search keyword '"Petros AM"' showing total 71 results

1. Task Allocation Methods and Optimization Techniques in Edge Computing: A Systematic Review of the Literature

Author

Vasilios Patsias, Petros Amanatidis, Dimitris Karampatzakis, Thomas Lagkas, Kalliopi Michalakopoulou, and Alexandros Nikitas

Subjects

task offloading, edge computing, task allocation, optimization algorithms, Information technology, T58.5-58.64

Abstract

Task allocation in edge computing refers to the process of distributing tasks among the various nodes in an edge computing network. The main challenges in task allocation include determining the optimal location for each task based on the requirements such as processing power, storage, and network bandwidth, and adapting to the dynamic nature of the network. Different approaches for task allocation include centralized, decentralized, hybrid, and machine learning algorithms. Each approach has its strengths and weaknesses and the choice of approach will depend on the specific requirements of the application. In more detail, the selection of the most optimal task allocation methods depends on the edge computing architecture and configuration type, like mobile edge computing (MEC), cloud-edge, fog computing, peer-to-peer edge computing, etc. Thus, task allocation in edge computing is a complex, diverse, and challenging problem that requires a balance of trade-offs between multiple conflicting objectives such as energy efficiency, data privacy, security, latency, and quality of service (QoS). Recently, an increased number of research studies have emerged regarding the performance evaluation and optimization of task allocation on edge devices. While several survey articles have described the current state-of-the-art task allocation methods, this work focuses on comparing and contrasting different task allocation methods, optimization algorithms, as well as the network types that are most frequently used in edge computing systems.

Published

2023

2. Cooperative Task Execution for Object Detection in Edge Computing: An Internet of Things Application

Author

Petros Amanatidis, Dimitris Karampatzakis, George Iosifidis, Thomas Lagkas, and Alexandros Nikitas

Subjects

edge AI, task offloading, YOLOv5, edge computing, object detection system, Internet of Things, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999

Abstract

The development of computer hardware and communications has brought with it many exciting applications in the Internet of Things. More and more Single Board Computers (SBC) with high performance and low power consumption are used to infer deep learning models at the edge of the network. In this article, we investigate a cooperative task execution system in an edge computing architecture. In our topology, the edge server offloads different workloads to end devices, which collaboratively execute object detection on the transmitted sets of images. Our proposed system attempts to provide optimization in terms of execution accuracy and execution time for inferencing deep learning models. Furthermore, we focus on implementing new policies to optimize the E2E execution time and the execution accuracy of the system by highlighting the key role of effective image compression and the batch sizes (splitting decisions) received by the end devices from a server at the network edge. In our testbed, we used the You Only Look Once (YOLO) version 5, which is one of the most popular object detectors. In our heterogeneous testbed, an edge server and three different end devices were used with different characteristics like CPU/TPU, different sizes of RAM, and different neural network input sizes to identify sharp trade-offs. Firstly, we implemented the YOLOv5 on our end devices to evaluate the performance of the model using metrics like Precision, Recall, and mAP on the COCO dataset. Finally, we explore optimal trade-offs for different task-splitting strategies and compression decisions to optimize total performance. We demonstrate that offloading workloads on multiple end devices based on different splitting decisions and compression values improves the system’s performance to respond in real-time conditions without needing a server or cloud resources.

Published

2023

3. Low-Cost Automatic Weather Stations in the Internet of Things

Author

Konstantinos Ioannou, Dimitris Karampatzakis, Petros Amanatidis, Vasileios Aggelopoulos, and Ilias Karmiris

Subjects

AWS, Internet of Things, Artificial Intelligence, Edge computing, LPWAN, LoRa, Information technology, T58.5-58.64

Abstract

Automatic Weather Stations (AWS) are extensively used for gathering meteorological and climatic data. The World Meteorological Organization (WMO) provides publications with guidelines for the implementation, installation, and usages of these stations. Nowadays, in the new era of the Internet of Things, there is an ever-increasing necessity for the implementation of automatic observing systems that will provide scientists with the real-time data needed to design and apply proper environmental policy. In this paper, an extended review is performed regarding the technologies currently used for the implementation of Automatic Weather Stations. Furthermore, we also present the usage of new emerging technologies such as the Internet of Things, Edge Computing, Deep Learning, LPWAN, etc. in the implementation of future AWS-based observation systems. Finally, we present a case study and results from a testbed AWS (project AgroComp) developed by our research team. The results include test measurements from low-cost sensors installed on the unit and predictions provided by Deep Learning algorithms running locally.

Published

2021

4. LIGAND-BINDING EFFECTS ON THE KRINGLE-4 DOMAIN FROM HUMAN-PLASMINOGEN - A STUDY BY LASER PHOTO-CIDNP H-1-NMR SPECTROSCOPY

Author

DEMARCO, A, PETROS, AM, LLINAS, M, KAPTEIN, R, and BOELENS, R

Published

1989

5. KRINGLE-4 FROM HUMAN-PLASMINOGEN - A PROTON MAGNETIC-RESONANCE STUDY VIA TWO-DIMENSIONAL PHOTOCHEMICALLY INDUCED DYNAMIC NUCLEAR-POLARIZATION SPECTROSCOPY

Author

Demarco, A., Zetta, L., Petros, Am, Llinas, M., Rolf Boelens, and Kaptein, R.

6. Efficiently driving protein-based fragment screening and lead discovery using two-dimensional NMR.

Author

Peng C, Namanja AT, Munoz E, Wu H, Frederick TE, Maestre-Martinez M, Iglesias Fernandez I, Sun Q, Cobas C, Sun C, and Petros AM

Subjects

Ligands, Nuclear Magnetic Resonance, Biomolecular, Drug Discovery, Magnetic Resonance Imaging, Algorithms

Abstract

Fragment-based drug discovery (FBDD) and validation of small molecule binders using NMR spectroscopy is an established and widely used method in the early stages of drug discovery. Starting from a library of small compounds, ligand- or protein-observed NMR methods are employed to detect binders, typically weak, that become the starting points for structure-activity relationships (SAR) by NMR. Unlike the more frequently used ligand-observed 1D NMR techniques, protein-observed 2D 1 H- 15 N or 1 H- 13 C heteronuclear correlation (HSQC or HMQC) methods offer insights that include the mechanism of ligand engagement on the target and direct binding affinity measurements in addition to routine screening. We hereby present the development of a set of software tools within the MestReNova (Mnova) package for analyzing 2D NMR for FBDD and hit validation purposes. The package covers three main tasks: (1) unsupervised profiling of raw data to identify outlier data points to exclude in subsequent analyses; (2) batch processing of single-point spectra to identify and rank binders based on chemical shift perturbations or spectral peak intensity changes; and (3) batch processing of multiple titration series to derive binding affinities (K D ) by tracing the changes in peak locations or measuring global spectral changes. Toward this end, we implemented and evaluated a set of algorithms for automated peak tracing, spectral binning, and variance analysis by PCA, and a new tool for spectral data intensity comparison using ECHOS. The accuracy and speed of the tools are demonstrated on 2D NMR binding data collected on ligands used in the development of potential inhibitors of the anti-apoptotic MCL-1 protein., (© 2022. The Author(s), under exclusive licence to Springer Nature B.V.)

Published

2023

7. Identification and structure-based drug design of cell-active inhibitors of interleukin 17A at a novel C-terminal site.

Author

Goedken ER, Argiriadi MA, Dietrich JD, Petros AM, Krishnan N, Panchal SC, Qiu W, Wu H, Zhu H, Adams AM, Bodelle PM, Goguen L, Richardson PL, Slivka PF, Srikumaran M, Upadhyay AK, Wu B, Judge RA, Vasudevan A, Gopalakrishnan SM, Cox PB, Stoll VS, and Sun C

Subjects

Cytokines, Drug Design, Humans, Arthritis, Psoriatic, Axial Spondyloarthritis, Interleukin-17 antagonists & inhibitors, Psoriasis

Abstract

Anti-IL17A therapies have proven effective for numerous inflammatory diseases including psoriasis, axial spondylitis and psoriatic arthritis. Modulating and/or antagonizing protein-protein interactions of IL17A cytokine binding to its cell surface receptors with oral therapies offers the promise to bring forward biologics-like efficacy in a pill to patients. We used an NMR-based fragment screen of recombinant IL17A to uncover starting points for small molecule IL17A antagonist discovery. By examining chemical shift perturbations in 2D [ 1 H, 13 C-HSQC] spectra of isotopically labeled IL17A, we discovered fragments binding the cytokine at a previously undescribed site near the IL17A C-terminal region, albeit with weak affinity (> 250 µM). Importantly this binding location was distinct from previously known chemical matter modulating cytokine responses. Subsequently through analog screening, we identified related compounds that bound symmetrically in this novel site with two copies. From this observation we employed a linking strategy via structure-based drug design and obtained compounds with increased binding affinity (< 50 nM) and showed functional inhibition of IL17A-induced cellular signaling (IC 50 ~1 µM). We also describe a fluorescence-based probe molecule suitable to discern/screen for additional molecules binding in this C-terminal site., (© 2022. The Author(s).)

Published

2022

8. Insights into the Conformation and Self-Association of a Concentrated Monoclonal Antibody using Isothermal Chemical Denaturation and Nuclear Magnetic Resonance.

Author

Xu J, Namanja A, Chan SL, Son C, Petros AM, Sun C, Radziejewski C, and Ihnat PM

Subjects

Hydrogen-Ion Concentration, Magnetic Resonance Spectroscopy, Protein Conformation, Protein Denaturation, Viscosity, Antibodies, Monoclonal chemistry, Immunoglobulin G chemistry

Abstract

The purpose of this investigation was to highlight the utility of nuclear magnetic resonance (NMR) as a multi-attribute method for the characterization of therapeutic antibodies. In this case study, we compared results from isothermal chemical denaturation (ICD) and NMR with standard methods to relate conformational states of a model monoclonal antibody (mAb1) with protein-protein interactions (PPI) that lead to self - association in concentrated solutions. The increase in aggregation rate and relative viscosity for mAb1 was found to be both concentration and pH dependent. The free energy of unfolding (∆G⁰) from ICD and thermal analysis in dilute solutions indicated that although the native state predominated between pH 4 - pH 7, it was disrupted at the CH 2 and unfolded noncooperatively under acidic conditions. One-dimensional (1D) 1 H NMR and two-dimensional (2D) 13 C- 1 H NMR performed, in concentrated solutions, confirmed that PPI between pH 4-7 occurred while mAb1 was in the native state. NMR corroborated that mAb1 maintained a dominant native state at formulation-relevant conditions at the tested pH range, had increased global molecular tumbling dynamics at lower pH and confirmed increased PPI at higher pH conditions. This report aligns and compares typical characterization of an IgG1 with assessment of structure by NMR and provided a more precise assessment and deeper insight into the conformation of an IgG1 in concentrated solutions., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper The authors declare the following financial interests/personal relationships which may be considered as potential competing interests, (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

9. Development of Orally Efficacious Allosteric Inhibitors of TNFα via Fragment-Based Drug Design.

Author

Dietrich JD, Longenecker KL, Wilson NS, Goess C, Panchal SC, Swann SL, Petros AM, Hobson AD, Ihle D, Song D, Richardson P, Comess KM, Cox PB, Dombrowski A, Sarris K, Donnelly-Roberts DL, Duignan DB, Gomtsyan A, Jung P, Krueger AC, Mathieu S, McClure A, Stoll VS, Wetter J, Mankovich JA, Hajduk PJ, Vasudevan A, Stoffel RH, and Sun C

Subjects

Administration, Oral, Allosteric Regulation, Animals, Arthritis, Rheumatoid drug therapy, Autoimmune Diseases drug therapy, Biological Products pharmacology, Biological Products therapeutic use, Ligands, Mice, Tumor Necrosis Factor-alpha metabolism, Biological Products chemical synthesis, Drug Design, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

Tumor necrosis factor α (TNFα) is a soluble cytokine that is directly involved in systemic inflammation through the regulation of the intracellular NF-κB and MAPK signaling pathways. The development of biologic drugs that inhibit TNFα has led to improved clinical outcomes for patients with rheumatoid arthritis and other chronic autoimmune diseases; however, TNFα has proven to be difficult to drug with small molecules. Herein, we present a two-phase, fragment-based drug discovery (FBDD) effort in which we first identified isoquinoline fragments that disrupt TNFα ligand-receptor binding through an allosteric desymmetrization mechanism as observed in high-resolution crystal structures. The second phase of discovery focused on the de novo design and optimization of fragments with improved binding efficiency and drug-like properties. The 3-indolinone-based lead presented here displays oral, in vivo efficacy in a mouse glucose-6-phosphate isomerase (GPI)-induced paw swelling model comparable to that seen with a TNFα antibody.

Published

2021

10. NMR-based fragment screening and lead discovery accelerated by principal component analysis.

Author

Namanja AT, Xu J, Wu H, Sun Q, Upadhyay AK, Sun C, Van Doren SR, and Petros AM

Subjects

Ligands, Peptide Fragments chemistry, Peptide Fragments metabolism, Protein Binding, Drug Discovery methods, Nuclear Magnetic Resonance, Biomolecular methods, Principal Component Analysis methods

Abstract

Protein-based NMR spectroscopy has proven to be a very robust method for finding fragment leads to protein targets. However, one limitation of protein-based NMR is that the data acquisition and analysis can be time consuming. In order to streamline the scoring of protein-based NMR fragment screening data and the determination of ligand affinities using 2D NMR experiments we have developed a data analysis workflow based on principal component analysis (PCA) within the TREND NMR Pro software package. We illustrate this using four different proteins and sets of ligands which interact with these proteins over a range of affinities. Also, these PCA-based methods can be successfully applied even to systems where ligand binding to target proteins is in intermediate or even slow exchange on the NMR time scale. Finally, these methods will work for scoring of fragment binding data using protein spectra that are either highly overlapped or lower in resolution.

Published

2019

11. Fragment-Based Discovery of an Apolipoprotein E4 (apoE4) Stabilizer.

Author

Petros AM, Korepanova A, Jakob CG, Qiu W, Panchal SC, Wang J, Dietrich JD, Brewer JT, Pohlki F, Kling A, Wilcox K, Lakics V, Bahnassawy L, Reinhardt P, Partha SK, Bodelle PM, Lake M, Charych EI, Stoll VS, Sun C, and Mohler EG

Subjects

Alzheimer Disease drug therapy, Alzheimer Disease metabolism, Alzheimer Disease pathology, Amidines chemistry, Amidines metabolism, Apolipoprotein E4 chemistry, Apolipoprotein E4 genetics, Binding Sites, Crystallography, X-Ray, Drug Discovery, Humans, Liposomes chemistry, Liposomes metabolism, Magnetic Resonance Spectroscopy, Molecular Dynamics Simulation, Mutagenesis, Site-Directed, Protein Domains, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Small Molecule Libraries metabolism, Small Molecule Libraries therapeutic use, Structure-Activity Relationship, Transition Temperature, Apolipoprotein E4 metabolism, Small Molecule Libraries chemistry

Abstract

Apolipoprotein E is a 299-residue lipid carrier protein produced in both the liver and the brain. The protein has three major isoforms denoted apoE2, apoE3, and apoE4 which differ at positions 112 and 158 and which occur at different frequencies in the human population. Genome-wide association studies indicate that the possession of two apoE4 alleles is a strong genetic risk factor for late-onset Alzheimer's disease (LOAD). In an attempt to identify a small molecule stabilizer of apoE4 function that may have utility as a therapy for Alzheimer's disease, we carried out an NMR-based fragment screen on the N-terminal domain of apoE4 and identified a benzyl amidine based fragment binder. In addition to NMR, binding was characterized using various other biophysical techniques, and a crystal structure of the bound core was obtained. Core elaboration ultimately yielded a compound that showed activity in an IL-6 and IL-8 cytokine release assay.

Published

2019

12. Targeting lysine specific demethylase 4A (KDM4A) tandem TUDOR domain - A fragment based approach.

Author

Upadhyay AK, Judge RA, Li L, Pithawalla R, Simanis J, Bodelle PM, Marin VL, Henry RF, Petros AM, and Sun C

Subjects

Dose-Response Relationship, Drug, Humans, Hydrogen Bonding, Hydrophobic and Hydrophilic Interactions, Jumonji Domain-Containing Histone Demethylases metabolism, Molecular Structure, Nuclear Magnetic Resonance, Biomolecular, Structure-Activity Relationship, Tudor Domain, Jumonji Domain-Containing Histone Demethylases chemistry

Abstract

The tandem TUDOR domains present in the non-catalytic C-terminal half of the KDM4A, 4B and 4C enzymes play important roles in regulating their chromatin localizations and substrate specificities. They achieve this regulatory role by binding to different tri-methylated lysine residues on histone H3 (H3-K4me3, H3-K23me3) and histone H4 (H4-K20me3) depending upon the specific chromatin environment. In this work, we have used a 2D-NMR based fragment screening approach to identify a novel fragment (1a), which binds to the KDM4A-TUDOR domain and shows modest competition with H3-K4me3 binding in biochemical as well as in vitro cell based assays. A co-crystal structure of KDM4A TUDOR domain in complex with 1a shows that the fragment binds stereo-specifically to the methyl lysine binding pocket forming a network of strong hydrogen bonds and hydrophobic interactions. We anticipate that the fragment 1a can be further developed into a novel allosteric inhibitor of the KDM4 family of enzymes through targeting their C-terminal tandem TUDOR domain., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

13. Fragment-based discovery of a potent NAMPT inhibitor.

Author

Korepanova A, Longenecker KL, Pratt SD, Panchal SC, Clark RF, Lake M, Gopalakrishnan SM, Raich D, Sun C, and Petros AM

Subjects

Acrylamides chemical synthesis, Acrylamides chemistry, Cytokines genetics, Cytokines metabolism, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Fluorescence Resonance Energy Transfer, Humans, Molecular Docking Simulation, Molecular Structure, Nicotinamide Phosphoribosyltransferase genetics, Nicotinamide Phosphoribosyltransferase metabolism, Piperidines chemical synthesis, Piperidines chemistry, Structure-Activity Relationship, Acrylamides pharmacology, Cytokines antagonists & inhibitors, Drug Discovery, Enzyme Inhibitors pharmacology, Nicotinamide Phosphoribosyltransferase antagonists & inhibitors, Piperidines pharmacology

Abstract

NAMPT expression is elevated in many cancers, making this protein a potential target for anticancer therapy. We have carried out both NMR based and TR-FRET based fragment screens against human NAMPT and identified six novel binders with a range of potencies. Co-crystal structures were obtained for two of the fragments bound to NAMPT while for the other four fragments force-field driven docking was employed to generate a bound pose. Based on structural insights arising from comparison of the bound fragment poses to that of bound FK866 we were able to synthetically elaborate one of the fragments into a potent NAMPT inhibitor., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2018

14. Erratum: The EED protein-protein interaction inhibitor A-395 inactivates the PRC2 complex.

Author

He Y, Selvaraju S, Curtin ML, Jakob CG, Zhu H, Comess KM, Shaw B, The J, Lima-Fernandes E, Szewczyk MM, Cheng D, Klinge KL, Li HQ, Pliushchev M, Algire MA, Maag D, Guo J, Dietrich J, Panchal SC, Petros AM, Sweis RF, Torrent M, Bigelow LJ, Senisterra G, Li F, Kennedy S, Wu Q, Osterling DJ, Lindley DJ, Gao W, Galasinski S, Barsyte-Lovejoy D, Vedadi M, Buchanan FG, Arrowsmith CH, Chiang GG, Sun C, and Pappano WN

Published

2017

15. Methylpyrrole inhibitors of BET bromodomains.

Author

Hasvold LA, Sheppard GS, Wang L, Fidanze SD, Liu D, Pratt JK, Mantei RA, Wada CK, Hubbard R, Shen Y, Lin X, Huang X, Warder SE, Wilcox D, Li L, Buchanan FG, Smithee L, Albert DH, Magoc TJ, Park CH, Petros AM, Panchal SC, Sun C, Kovar P, Soni NB, Elmore SW, Kati WM, and McDaniel KF

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents therapeutic use, Binding Sites, Cell Line, Tumor, Cell Proliferation drug effects, Crystallography, X-Ray, Drug Design, Half-Life, Humans, Mice, Molecular Dynamics Simulation, Multiple Myeloma drug therapy, Nuclear Proteins metabolism, Pyrroles chemical synthesis, Pyrroles pharmacokinetics, Pyrroles therapeutic use, Structure-Activity Relationship, Transcription Factors metabolism, Transplantation, Heterologous, Antineoplastic Agents chemistry, Nuclear Proteins antagonists & inhibitors, Pyrroles chemistry, Transcription Factors antagonists & inhibitors

Abstract

An NMR fragment screen for binders to the bromodomains of BRD4 identified 2-methyl-3-ketopyrroles 1 and 2. Elaboration of these fragments guided by structure-based design provided lead molecules with significant activity in a mouse tumor model. Further modifications to the methylpyrrole core provided compounds with improved properties and enhanced activity in a mouse model of multiple myeloma., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

16. Fragment-Based, Structure-Enabled Discovery of Novel Pyridones and Pyridone Macrocycles as Potent Bromodomain and Extra-Terminal Domain (BET) Family Bromodomain Inhibitors.

Author

Wang L, Pratt JK, Soltwedel T, Sheppard GS, Fidanze SD, Liu D, Hasvold LA, Mantei RA, Holms JH, McClellan WJ, Wendt MD, Wada C, Frey R, Hansen TM, Hubbard R, Park CH, Li L, Magoc TJ, Albert DH, Lin X, Warder SE, Kovar P, Huang X, Wilcox D, Wang R, Rajaraman G, Petros AM, Hutchins CW, Panchal SC, Sun C, Elmore SW, Shen Y, Kati WM, and McDaniel KF

Subjects

Animals, Crystallography, X-Ray, Drug Discovery, Macrocyclic Compounds pharmacokinetics, Molecular Structure, Pyridones pharmacokinetics, Rats, Structure-Activity Relationship, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacology, Pyridones chemistry, Pyridones pharmacology

Abstract

Members of the BET family of bromodomain containing proteins have been identified as potential targets for blocking proliferation in a variety of cancer cell lines. A two-dimensional NMR fragment screen for binders to the bromodomains of BRD4 identified a phenylpyridazinone fragment with a weak binding affinity (1, K i = 160 μM). SAR investigation of fragment 1, aided by X-ray structure-based design, enabled the synthesis of potent pyridone and macrocyclic pyridone inhibitors exhibiting single digit nanomolar potency in both biochemical and cell based assays. Advanced analogs in these series exhibited high oral exposures in rodent PK studies and demonstrated significant tumor growth inhibition efficacy in mouse flank xenograft models.

Published

2017

17. The EED protein-protein interaction inhibitor A-395 inactivates the PRC2 complex.

Author

He Y, Selvaraju S, Curtin ML, Jakob CG, Zhu H, Comess KM, Shaw B, The J, Lima-Fernandes E, Szewczyk MM, Cheng D, Klinge KL, Li HQ, Pliushchev M, Algire MA, Maag D, Guo J, Dietrich J, Panchal SC, Petros AM, Sweis RF, Torrent M, Bigelow LJ, Senisterra G, Li F, Kennedy S, Wu Q, Osterling DJ, Lindley DJ, Gao W, Galasinski S, Barsyte-Lovejoy D, Vedadi M, Buchanan FG, Arrowsmith CH, Chiang GG, Sun C, and Pappano WN

Subjects

Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Indans chemistry, Models, Molecular, Molecular Structure, Polycomb Repressive Complex 2 chemistry, Polycomb Repressive Complex 2 metabolism, Protein Binding drug effects, Structure-Activity Relationship, Sulfonamides chemistry, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Indans pharmacology, Polycomb Repressive Complex 2 antagonists & inhibitors, Sulfonamides pharmacology

Abstract

Polycomb repressive complex 2 (PRC2) is a regulator of epigenetic states required for development and homeostasis. PRC2 trimethylates histone H3 at lysine 27 (H3K27me3), which leads to gene silencing, and is dysregulated in many cancers. The embryonic ectoderm development (EED) protein is an essential subunit of PRC2 that has both a scaffolding function and an H3K27me3-binding function. Here we report the identification of A-395, a potent antagonist of the H3K27me3 binding functions of EED. Structural studies demonstrate that A-395 binds to EED in the H3K27me3-binding pocket, thereby preventing allosteric activation of the catalytic activity of PRC2. Phenotypic effects observed in vitro and in vivo are similar to those of known PRC2 enzymatic inhibitors; however, A-395 retains potent activity against cell lines resistant to the catalytic inhibitors. A-395 represents a first-in-class antagonist of PRC2 protein-protein interactions (PPI) for use as a chemical probe to investigate the roles of EED-containing protein complexes.

Published

2017

18. Turning a Substrate Peptide into a Potent Inhibitor for the Histone Methyltransferase SETD8.

Author

Judge RA, Zhu H, Upadhyay AK, Bodelle PM, Hutchins CW, Torrent M, Marin VL, Yu W, Vedadi M, Li F, Brown PJ, Pappano WN, Sun C, and Petros AM

Abstract

SETD8 is a histone H4-K20 methyltransferase that plays an essential role in the maintenance of genomic integrity during mitosis and in DNA damage repair, making it an intriguing target for cancer research. While some small molecule inhibitors for SETD8 have been reported, the structural binding modes for these inhibitors have not been revealed. Using the complex structure of the substrate peptide bound to SETD8 as a starting point, different natural and unnatural amino acid substitutions were tested, and a potent ( K i 50 nM, IC 50 0.33 μM) and selective norleucine containing peptide inhibitor has been obtained.

Published

2016

19. Correction to Structure-Guided Design of a Series of MCL-1 Inhibitors with High Affinity and Selectivity.

Author

Bruncko M, Wang L, Sheppard GS, Phillips DC, Tahir SK, Xue J, Erickson S, Fidanze S, Fry E, Hasvold L, Jenkins GJ, Jin S, Judge RA, Kovar PJ, Madar D, Nimmer P, Park C, Petros AM, Rosenberg SH, Smith ML, Song X, Sun C, Tao ZF, Wang X, Xiao Y, Zhang H, Tse C, Leverson JD, Elmore SW, and Souers AJ

Published

2015

20. Structure-guided design of a series of MCL-1 inhibitors with high affinity and selectivity.

Author

Bruncko M, Wang L, Sheppard GS, Phillips DC, Tahir SK, Xue J, Erickson S, Fidanze S, Fry E, Hasvold L, Jenkins GJ, Jin S, Judge RA, Kovar PJ, Madar D, Nimmer P, Park C, Petros AM, Rosenberg SH, Smith ML, Song X, Sun C, Tao ZF, Wang X, Xiao Y, Zhang H, Tse C, Leverson JD, Elmore SW, and Souers AJ

Subjects

Apoptosis drug effects, Cell Survival drug effects, Crystallography, X-Ray, Databases, Factual, High-Throughput Screening Assays, Humans, Molecular Docking Simulation, Molecular Structure, Multiple Myeloma metabolism, Multiple Myeloma pathology, Myeloid Cell Leukemia Sequence 1 Protein metabolism, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms pathology, Protein Binding, Structure-Activity Relationship, Tumor Cells, Cultured, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Drug Design, Multiple Myeloma drug therapy, Myeloid Cell Leukemia Sequence 1 Protein chemistry, Pancreatic Neoplasms drug therapy

Abstract

Myeloid cell leukemia 1 (MCL-1) is a BCL-2 family protein that has been implicated in the progression and survival of multiple tumor types. Herein we report a series of MCL-1 inhibitors that emanated from a high throughput screening (HTS) hit and progressed via iterative cycles of structure-guided design. Advanced compounds from this series exhibited subnanomolar affinity for MCL-1 and excellent selectivity over other BCL-2 family proteins as well as multiple kinases and GPCRs. In a MCL-1 dependent human tumor cell line, administration of compound 30b rapidly induced caspase activation with associated loss in cell viability. The small molecules described herein thus comprise effective tools for studying MCL-1 biology.

Published

2015

21. Discovery of a Potent and Selective BCL-XL Inhibitor with in Vivo Activity.

Author

Tao ZF, Hasvold L, Wang L, Wang X, Petros AM, Park CH, Boghaert ER, Catron ND, Chen J, Colman PM, Czabotar PE, Deshayes K, Fairbrother WJ, Flygare JA, Hymowitz SG, Jin S, Judge RA, Koehler MF, Kovar PJ, Lessene G, Mitten MJ, Ndubaku CO, Nimmer P, Purkey HE, Oleksijew A, Phillips DC, Sleebs BE, Smith BJ, Smith ML, Tahir SK, Watson KG, Xiao Y, Xue J, Zhang H, Zobel K, Rosenberg SH, Tse C, Leverson JD, Elmore SW, and Souers AJ

Abstract

A-1155463, a highly potent and selective BCL-XL inhibitor, was discovered through nuclear magnetic resonance (NMR) fragment screening and structure-based design. This compound is substantially more potent against BCL-XL-dependent cell lines relative to our recently reported inhibitor, WEHI-539, while possessing none of its inherent pharmaceutical liabilities. A-1155463 caused a mechanism-based and reversible thrombocytopenia in mice and inhibited H146 small cell lung cancer xenograft tumor growth in vivo following multiple doses. A-1155463 thus represents an excellent tool molecule for studying BCL-XL biology as well as a productive lead structure for further optimization.

Published

2014

22. Fragment-based discovery of potent inhibitors of the anti-apoptotic MCL-1 protein.

Author

Petros AM, Swann SL, Song D, Swinger K, Park C, Zhang H, Wendt MD, Kunzer AR, Souers AJ, and Sun C

Subjects

Binding Sites, Biphenyl Compounds chemistry, Crystallography, X-Ray, Magnetic Resonance Spectroscopy, Molecular Dynamics Simulation, Myeloid Cell Leukemia Sequence 1 Protein metabolism, Protein Binding, Protein Structure, Tertiary, Salicylic Acid chemistry, Salicylic Acid metabolism, Sulfonamides chemistry, Sulfonamides metabolism, Drug Design, Myeloid Cell Leukemia Sequence 1 Protein antagonists & inhibitors

Abstract

Apoptosis is regulated by the BCL-2 family of proteins, which is comprised of both pro-death and pro-survival members. Evasion of apoptosis is a hallmark of malignant cells. One way in which cancer cells achieve this evasion is thru overexpression of the pro-survival members of the BCL-2 family. Overexpression of MCL-1, a pro-survival protein, has been shown to be a resistance factor for Navitoclax, a potent inhibitor of BCL-2 and BCL-XL. Here we describe the use of fragment screening methods and structural biology to drive the discovery of novel MCL-1 inhibitors from two distinct structural classes. Specifically, cores derived from a biphenyl sulfonamide and salicylic acid were uncovered in an NMR-based fragment screen and elaborated using high throughput analog synthesis. This culminated in the discovery of selective and potent inhibitors of MCL-1 that may serve as promising leads for medicinal chemistry optimization efforts., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

23. Discovery and development of potent and selective inhibitors of histone methyltransferase g9a.

Author

Sweis RF, Pliushchev M, Brown PJ, Guo J, Li F, Maag D, Petros AM, Soni NB, Tse C, Vedadi M, Michaelides MR, Chiang GG, and Pappano WN

Abstract

G9a is a histone lysine methyltransferase responsible for the methylation of histone H3 lysine 9. The discovery of A-366 arose from a unique diversity screening hit, which was optimized by incorporation of a propyl-pyrrolidine subunit to occupy the enzyme lysine channel. A-366 is a potent inhibitor of G9a (IC50: 3.3 nM) with greater than 1000-fold selectivity over 21 other methyltransferases.

Published

2014

24. Cracking the molecular weight barrier: fragment screening of an aminotransferase using an NMR-based functional assay.

Author

Mendoza R, Petros AM, Liu Y, Thimmapaya R, Surowy CS, Leise WF, Pereda-Lopez A, Panchal SC, and Sun C

Subjects

Biocatalysis, Carbon Isotopes, Dose-Response Relationship, Drug, Enzyme Inhibitors chemistry, Ligands, Molecular Structure, Molecular Weight, Organic Chemicals chemistry, Structure-Activity Relationship, Transaminases chemistry, Transaminases metabolism, Enzyme Inhibitors pharmacology, Nuclear Magnetic Resonance, Biomolecular methods, Organic Chemicals pharmacology, Transaminases antagonists & inhibitors

Abstract

NMR-based screening of protein targets has become a well established part of the drug discovery process especially with respect to fragments. However, as target size increases the two-dimensional spectra typically used for such screening become more crowded due to the increased number of signals, and the individual signals broaden due to the decreased rotational correlation time of the protein. Here we present an NMR-based functional assay for the branched-chain aminotransferase BCATc, a dimer with a total molecular weight of 88 kDa, which overcomes the limitations of the typical protein-based NMR screening method. BCATc is involved in glutamate production in the brain and is a therapeutic target for neuronal disorders involving a glutamatergic mechanism. Several fragments which inhibit BCATc were discovered using this assay and these may serve as novel cores for the development of potent BCATc inhibitors., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

25. Fragment-based lead discovery: challenges and opportunities.

Author

Sun C, Petros AM, and Hajduk PJ

Subjects

Binding Sites, Combinatorial Chemistry Techniques, Crystallography, X-Ray, Humans, Ligands, Magnetic Resonance Spectroscopy, Drug Discovery trends, Drug Industry trends, Peptide Fragments chemistry, Proteins chemistry

Abstract

Fragment-based lead discovery has undergone remarkable changes over the last 15 years. During this time, the pharmaceutical industry has changed dramatically as well, and continued evolution of the industry is assured. These changes present many challenges but also several opportunities for executing fragment-based drug design. This article will explore some of the more significant changes in the industry and how they may affect future discovery efforts related to fragment-based initiatives.

Published

2011

26. N-aryl-benzimidazolones as novel small molecule HSP90 inhibitors.

Author

Bruncko M, Tahir SK, Song X, Chen J, Ding H, Huth JR, Jin S, Judge RA, Madar DJ, Park CH, Park CM, Petros AM, Tse C, Rosenberg SH, and Elmore SW

Subjects

Benzimidazoles chemical synthesis, Benzimidazoles pharmacology, Binding Sites, Cell Line, Tumor, Crystallography, X-Ray, HSP90 Heat-Shock Proteins metabolism, Humans, Protein Structure, Tertiary, Structure-Activity Relationship, Benzimidazoles chemistry, HSP90 Heat-Shock Proteins antagonists & inhibitors

Abstract

We describe the development of a novel series of N-aryl-benzimidazolone HSP90 inhibitors (9) targeting the N-terminal ATP-ase site. SAR development was influenced by structure-based design based around X-ray structures of ligand bound HSP90 complexes. Lead compounds exhibited high binding affinities, ATP-ase inhibition and cellular client protein degradation., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

27. Discovery of a potent and selective Bcl-2 inhibitor using SAR by NMR.

Author

Petros AM, Huth JR, Oost T, Park CM, Ding H, Wang X, Zhang H, Nimmer P, Mendoza R, Sun C, Mack J, Walter K, Dorwin S, Gramling E, Ladror U, Rosenberg SH, Elmore SW, Fesik SW, and Hajduk PJ

Subjects

Models, Molecular, Structure-Activity Relationship, Magnetic Resonance Spectroscopy methods, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors

Abstract

The Bcl-2 family of proteins plays a major role in the regulation of apoptosis, or programmed cell death. Overexpression of the anti-apoptotic members of this family (Bcl-2, Bcl-x(L), and Mcl-1) can render cancer cells resistant to chemotherapeutic agents and therefore these proteins are important targets for the development of new anti-cancer agents. Here we describe the discovery of a potent, highly selective, Bcl-2 inhibitor using SAR by NMR and structure-based drug design which could serve as a starting point for the development of a Bcl-2 selective anti-cancer agent. Such an agent would potentially overcome the Bcl-x(L) mediated thrombocytopenia observed with ABT-263., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

28. Labeled Ligand Displacement: Extending NMR-Based Screening of Protein Targets.

Author

Swann SL, Song D, Sun C, Hajduk PJ, and Petros AM

Abstract

NMR spectroscopy has enjoyed widespread success as a method for screening protein targets, especially in the area of fragment-based drug discovery. However, current methods for NMR-based screening all suffer certain limitations. Two-dimensional methods like "SAR by NMR" require isotopically labeled protein and are limited to proteins less than about 50 kDa. For one-dimensional, ligand-based methods, results can be confounded by nonspecific compound binding, resonance overlap, or the need for a special NMR probe. We present here a ligand-based method that relies on the exchange broadening observed for a (13)C-labeled molecule upon binding to a protein target (labeled ligand displacement). This method can be used to screen both individual compounds and mixtures and is free of the artifacts inherent in other ligand-based methods.

Published

2010

29. Discovery and design of novel HSP90 inhibitors using multiple fragment-based design strategies.

Author

Huth JR, Park C, Petros AM, Kunzer AR, Wendt MD, Wang X, Lynch CL, Mack JC, Swift KM, Judge RA, Chen J, Richardson PL, Jin S, Tahir SK, Matayoshi ED, Dorwin SA, Ladror US, Severin JM, Walter KA, Bartley DM, Fesik SW, Elmore SW, and Hajduk PJ

Subjects

Aminopyridines chemistry, Aminopyridines metabolism, Crystallography, X-Ray, Humans, Ligands, Models, Molecular, Molecular Sequence Data, Molecular Structure, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, Drug Design, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, HSP90 Heat-Shock Proteins antagonists & inhibitors, Peptide Fragments chemistry, Peptide Fragments metabolism

Abstract

The molecular chaperone HSP90 has been shown to facilitate cancer cell survival by stabilizing key proteins responsible for a malignant phenotype. We report here the results of parallel fragment-based drug design approaches in the design of novel HSP90 inhibitors. Initial aminopyrimidine leads were elaborated using high-throughput organic synthesis to yield nanomolar inhibitors of the enzyme. Second site leads were also identified which bound to HSP90 in two distinct conformations, an 'open' and 'closed' form. Intriguingly, linked fragment approaches targeting both of these conformations were successful in producing novel, micromolar inhibitors. Overall, this study shows that, with only a few fragment hits, multiple lead series can be generated for HSP90 due to the inherent flexibility of the active site. Thus, ample opportunities exist to use these lead series in the development of clinically useful HSP90 inhibitors for the treatment of cancers.

Published

2007

30. Studies leading to potent, dual inhibitors of Bcl-2 and Bcl-xL.

Author

Bruncko M, Oost TK, Belli BA, Ding H, Joseph MK, Kunzer A, Martineau D, McClellan WJ, Mitten M, Ng SC, Nimmer PM, Oltersdorf T, Park CM, Petros AM, Shoemaker AR, Song X, Wang X, Wendt MD, Zhang H, Fesik SW, Rosenberg SH, and Elmore SW

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Biphenyl Compounds chemistry, Biphenyl Compounds pharmacology, Cell Line, Tumor, Drug Screening Assays, Antitumor, Humans, Lymphoma, Mice, Mice, SCID, Models, Molecular, Nitrophenols chemistry, Nitrophenols pharmacology, Piperazines chemical synthesis, Piperazines chemistry, Piperazines pharmacology, Proto-Oncogene Proteins c-bcl-2 chemistry, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Transplantation, Heterologous, bcl-X Protein antagonists & inhibitors, bcl-X Protein chemistry, Antineoplastic Agents chemical synthesis, Biphenyl Compounds chemical synthesis, Nitrophenols chemical synthesis, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors, Sulfonamides chemical synthesis

Abstract

Overexpression of the antiapototic proteins Bcl-2 and Bcl-xL provides a common mechanism through which cancer cells gain a survival advantage and become resistant to conventional chemotherapy. Inhibition of these prosurvival proteins is an attractive strategy for cancer therapy. We recently described the discovery of a selective Bcl-xL antagonist that potentiates the antitumor activity of chemotherapy and radiation. Here we describe the use of structure-guided design to exploit a deep hydrophobic binding pocket on the surface of these proteins to develop the first dual, subnanomolar inhibitors of Bcl-xL and Bcl-2. This study culminated in the identification of 2, which exhibited EC50 values of 8 nM and 30 nM in Bcl-2 and Bcl-xL dependent cells, respectively. Compound 2 demonstrated single agent efficacy against human follicular lymphoma cell lines that overexpress Bcl-2, and efficacy in a murine xenograft model of lymphoma when given both as a single agent and in combination with etoposide.

Published

2007

31. Design, synthesis, and computational studies of inhibitors of Bcl-XL.

Author

Park CM, Oie T, Petros AM, Zhang H, Nimmer PM, Henry RF, and Elmore SW

Subjects

Binding Sites, Computer Simulation, Crystallography, X-Ray, Ligands, Magnetic Resonance Spectroscopy, Models, Molecular, Protein Structure, Tertiary, bcl-X Protein chemistry, bcl-X Protein metabolism, Drug Design, bcl-X Protein antagonists & inhibitors

Abstract

One of the primary objectives in the design of protein inhibitors is to shape the three-dimensional structures of small molecules to be complementary to the binding site of a target protein. In the course of our efforts to discover potent inhibitors of Bcl-2 family proteins, we found a unique folded conformation adopted by tethered aromatic groups in the ligand that significantly enhanced binding affinity to Bcl-XL. This finding led us to design compounds that were biased by nonbonding interactions present in a urea tether to adopt this bioactive, folded motif. To characterize the key interactions that induce the desired conformational bias, a series of substituted N,N'-diarylureas were prepared and analyzed using X-ray crystallography and quantum mechanical calculations. Stabilizing pi-stacking interactions and destabilizing steric interactions were predicted to work in concert in two of the substitution patterns to promote the bioactive conformation as a global energy minimum and result in a high target binding affinity. Conversely, intramolecular hydrogen bonding present in the third substitution motif promotes a less active, extended conformer as the energetically favored geometry. These findings were corroborated when the inhibition constant of binding to Bcl-XL was determined for fully elaborated analogues bearing these structural motifs. Finally, we obtained the NMR solution structure of the disubstituted N,N'-diarylurea bound to Bcl-XL demonstrating the folded conformation of the urea motif engaged in extensive pi-interactions with the protein.

Published

2006

32. Discovery and structure-activity relationship of antagonists of B-cell lymphoma 2 family proteins with chemopotentiation activity in vitro and in vivo.

Author

Wendt MD, Shen W, Kunzer A, McClellan WJ, Bruncko M, Oost TK, Ding H, Joseph MK, Zhang H, Nimmer PM, Ng SC, Shoemaker AR, Petros AM, Oleksijew A, Marsh K, Bauch J, Oltersdorf T, Belli BA, Martineau D, Fesik SW, Rosenberg SH, and Elmore SW

Subjects

Aniline Compounds chemistry, Aniline Compounds pharmacology, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Biological Availability, Cell Line, Tumor, Drug Screening Assays, Antitumor, Drug Synergism, Fluorescence Polarization, Humans, Magnetic Resonance Spectroscopy, Mice, Mice, SCID, Paclitaxel pharmacology, Piperidines chemistry, Piperidines pharmacology, Protein Binding, Protein Structure, Tertiary, Serum, Serum Albumin chemistry, Stereoisomerism, Sulfonamides chemistry, Sulfonamides pharmacology, Transplantation, Heterologous, Ultraviolet Rays, Aniline Compounds chemical synthesis, Antineoplastic Agents chemical synthesis, Piperidines chemical synthesis, Sulfonamides chemical synthesis, bcl-X Protein antagonists & inhibitors

Abstract

Development of a rationally designed potentiator of cancer chemotherapy, via inhibition of Bcl-X(L) function, is described. Lead compounds generated by NMR screening and directed parallel synthesis displayed sub-microM binding but were strongly deactivated in the presence of serum. The dominant component of serum deactivation was identified as domain III of human serum albumin (HSA); NMR solution structures of inhibitors bound to both Bcl-X(L) and HSA domain III indicated two potential optimization sites for separation of affinities. Modifications at both sites resulted in compounds with improved Bcl-X(L) binding and greatly increased activity in the presence of human serum, culminating in 73R, which bound to Bcl-X(L) with a K(i) of 0.8 nM. In a cellular assay 73R reversed the protection afforded by Bcl-X(L) overexpression against cytokine deprivation in FL5.12 cells with an EC(50) of 0.47 microM. 73R showed little effect on the viability of the human non small cell lung cancer cell line A549. However, consistent with the proposed mechanism, 73R potentiated the activity of paclitaxel and UV irradiation in vitro and potentiated the antitumor efficacy of paclitaxel in a mouse xenograft model.

Published

2006

33. Discovery of a potent inhibitor of the antiapoptotic protein Bcl-xL from NMR and parallel synthesis.

Author

Petros AM, Dinges J, Augeri DJ, Baumeister SA, Betebenner DA, Bures MG, Elmore SW, Hajduk PJ, Joseph MK, Landis SK, Nettesheim DG, Rosenberg SH, Shen W, Thomas S, Wang X, Zanze I, Zhang H, and Fesik SW

Subjects

Aniline Compounds chemistry, Binding Sites, Hydrophobic and Hydrophilic Interactions, Ligands, Magnetic Resonance Spectroscopy, Protein Binding, Solubility, Structure-Activity Relationship, Sulfonamides chemistry, bcl-X Protein chemistry, Aniline Compounds chemical synthesis, Models, Molecular, Sulfonamides chemical synthesis, bcl-X Protein antagonists & inhibitors

Abstract

The antiapoptotic proteins Bcl-x(L) and Bcl-2 play key roles in the maintenance of normal cellular homeostasis. However, their overexpression can lead to oncogenic transformation and is responsible for drug resistance in certain types of cancer. This makes Bcl-x(L) and Bcl-2 attractive targets for the development of potential anticancer agents. Here we describe the structure-based discovery of a potent Bcl-x(L) inhibitor directed at a hydrophobic groove on the surface of the protein. This groove represents the binding site for BH3 peptides from proapoptotic Bcl-2 family members such as Bak and Bad. Application of NMR-based screening yielded an initial biaryl acid with an affinity (K(d)) of approximately 300 microM for the protein. Following the classical "SAR by NMR" approach, a second-site ligand was identified that bound proximal to the first-site ligand in the hydrophobic groove. From NMR-based structural studies and parallel synthesis, a potent ligand was obtained, which binds to Bcl-x(L) with an inhibition constant (K(i)) of 36 +/- 2 nM.

Published

2006

34. A surface groove essential for viral Bcl-2 function during chronic infection in vivo.

Author

Loh J, Huang Q, Petros AM, Nettesheim D, van Dyk LF, Labrada L, Speck SH, Levine B, Olejniczak ET, and Virgin HW 4th

Abstract

Antiapoptotic Bcl-2 family proteins inhibit apoptosis in cultured cells by binding BH3 domains of proapoptotic Bcl-2 family members via a hydrophobic BH3 binding groove on the protein surface. We investigated the physiological importance of the BH3 binding groove of an antiapoptotic Bcl-2 protein in mammals in vivo by analyzing a viral Bcl-2 family protein. We show that the gamma-herpesvirus 68 (gammaHV68) Bcl-2 family protein (gammaHV68 v-Bcl-2), which is known to inhibit apoptosis in cultured cells, inhibits both apoptosis in primary lymphocytes and Bax toxicity in yeast. Nuclear magnetic resonance determination of the gammaHV68 v-Bcl-2 structure revealed a BH3 binding groove that binds BH3 domain peptides from proapoptotic Bcl-2 family members Bax and Bak via a molecular mechanism shared with host Bcl-2 family proteins, involving a conserved arginine in the BH3 peptide binding groove. Mutations of this conserved arginine and two adjacent amino acids to alanine (SGR to AAA) within the BH3 binding groove resulted in a properly folded protein that lacked the capacity of the wild-type gammaHV68 v-Bcl-2 to bind Bax BH3 peptide and to block Bax toxicity in yeast. We tested the physiological importance of this v-Bcl-2 domain during viral infection by engineering viral mutants encoding a v-Bcl-2 containing the SGR to AAA mutation. This mutation resulted in a virus defective for both efficient reactivation of gammaHV68 from latency and efficient persistent gammaHV68 replication. These studies demonstrate an essential functional role for amino acids in the BH3 peptide binding groove of a viral Bcl-2 family member during chronic infection.

Published

2005

35. 1H, 13C and 15N resonance assignments of a Bcl-xL/Bad peptide complex.

Author

Petros AM, Fesik SW, and Olejniczak ET

Subjects

Apoptosis, Carbon Isotopes, Hydrogen, Magnetic Resonance Spectroscopy methods, Nitrogen Isotopes, Peptide Fragments chemistry, Protein Conformation

Published

2005

36. An inhibitor of Bcl-2 family proteins induces regression of solid tumours.

Author

Oltersdorf T, Elmore SW, Shoemaker AR, Armstrong RC, Augeri DJ, Belli BA, Bruncko M, Deckwerth TL, Dinges J, Hajduk PJ, Joseph MK, Kitada S, Korsmeyer SJ, Kunzer AR, Letai A, Li C, Mitten MJ, Nettesheim DG, Ng S, Nimmer PM, O'Connor JM, Oleksijew A, Petros AM, Reed JC, Shen W, Tahir SK, Thompson CB, Tomaselli KJ, Wang B, Wendt MD, Zhang H, Fesik SW, and Rosenberg SH

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis drug effects, Biphenyl Compounds chemical synthesis, Biphenyl Compounds chemistry, Carcinoma, Small Cell drug therapy, Carcinoma, Small Cell pathology, Cell Line, Tumor, Cytochromes c metabolism, Disease Models, Animal, Drug Synergism, Humans, Lymphoma drug therapy, Lymphoma pathology, Magnetic Resonance Spectroscopy, Mice, Mitochondria drug effects, Mitochondria metabolism, Models, Molecular, Nitrophenols, Paclitaxel pharmacology, Piperazines, Proto-Oncogene Proteins c-bcl-2 metabolism, Structure-Activity Relationship, Sulfonamides, Survival Rate, Antineoplastic Agents therapeutic use, Biphenyl Compounds pharmacology, Biphenyl Compounds therapeutic use, Neoplasms drug therapy, Neoplasms pathology, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors, Proto-Oncogene Proteins c-bcl-2 classification

Abstract

Proteins in the Bcl-2 family are central regulators of programmed cell death, and members that inhibit apoptosis, such as Bcl-X(L) and Bcl-2, are overexpressed in many cancers and contribute to tumour initiation, progression and resistance to therapy. Bcl-X(L) expression correlates with chemo-resistance of tumour cell lines, and reductions in Bcl-2 increase sensitivity to anticancer drugs and enhance in vivo survival. The development of inhibitors of these proteins as potential anti-cancer therapeutics has been previously explored, but obtaining potent small-molecule inhibitors has proved difficult owing to the necessity of targeting a protein-protein interaction. Here, using nuclear magnetic resonance (NMR)-based screening, parallel synthesis and structure-based design, we have discovered ABT-737, a small-molecule inhibitor of the anti-apoptotic proteins Bcl-2, Bcl-X(L) and Bcl-w, with an affinity two to three orders of magnitude more potent than previously reported compounds. Mechanistic studies reveal that ABT-737 does not directly initiate the apoptotic process, but enhances the effects of death signals, displaying synergistic cytotoxicity with chemotherapeutics and radiation. ABT-737 exhibits single-agent-mechanism-based killing of cells from lymphoma and small-cell lung carcinoma lines, as well as primary patient-derived cells, and in animal models, ABT-737 improves survival, causes regression of established tumours, and produces cures in a high percentage of the mice.

Published

2005

37. Structure of the N-terminal RNA-binding domain of the SARS CoV nucleocapsid protein.

Author

Huang Q, Yu L, Petros AM, Gunasekera A, Liu Z, Xu N, Hajduk P, Mack J, Fesik SW, and Olejniczak ET

Subjects

Animals, Binding Sites, Humans, Ligands, Models, Molecular, Molecular Sequence Data, Molecular Structure, Nuclear Magnetic Resonance, Biomolecular, Protein Folding, RNA metabolism, Nucleocapsid Proteins chemistry, Protein Structure, Tertiary, Severe acute respiratory syndrome-related coronavirus chemistry

Abstract

The severe acute respiratory syndrome (SARS) virus belongs to the Coronaviridea family of viruses. Its virion encodes several proteins including a replicase and four structural proteins. Here we describe the three-dimensional structure of the N-terminal domain of the SARS coronavirus (CoV) nucleocapsid protein. The protein consists of a five-stranded beta sheet with a folding topology distinct from other RNA-binding proteins. Single-stranded RNAs bind to the protein surface at the junction between a flexible, positively charged beta hairpin and the core structure. NMR-based screening was used to identify low molecular weight compounds that bind to this site.

Published

2004

38. Discovery of novel inhibitors of Bcl-xL using multiple high-throughput screening platforms.

Author

Qian J, Voorbach MJ, Huth JR, Coen ML, Zhang H, Ng SC, Comess KM, Petros AM, Rosenberg SH, Warrior U, and Burns DJ

Subjects

Apoptosis genetics, Apoptosis physiology, Binding, Competitive, Carrier Proteins analysis, Carrier Proteins metabolism, Dimethyl Sulfoxide chemistry, Fluorescence Polarization, Inhibitory Concentration 50, Magnetic Resonance Spectroscopy, Mass Spectrometry, Titrimetry, bcl-X Protein, Combinatorial Chemistry Techniques methods, Pharmaceutical Preparations analysis, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors

Abstract

Bcl-xL is a member of the Bcl-2 family of proteins that are implicated to play a vital role in several diseases including cancer. Bcl-xL suppresses apoptosis; thus the inhibition of Bcl-xL function could restore the apoptotic process. To identify antagonists of Bcl-xL function, two ultra-high-throughput screens were implemented. An activity assay utilized fluorescence polarization, based on the binding of fluorescein-labeled peptide [the BH3 domain of BAD protein (F-Bad 6)] to Bcl-xL. A 384-well plate assay with mixtures of 10 drug compounds per well, combined with a fast plate reader, resulted in a throughput of 46,080 data points/day. Utilizing this screening format, 370,400 compounds were screened in duplicate and 425 inhibitors with an IC(50) below 100 microM were identified. The second assay format, affinity selection/mass spectrometry (ASMS), used ultrafiltration to separate Bcl-xL binders from nonbinders in mixtures of 2400 compounds. The bound species were subsequently separated from the protein and analyzed by flow injection electrospray mass spectrometry. Utilizing the ASMS format, 263,382 compounds were screened in duplicate and 29 binders with affinities below 100 microM were identified. Two novel classes of Bcl-xL inhibitors were identified by both methods and confirmed to bind (13)C-labeled Bcl-xL using heteronuclear magnetic resonance spectroscopy.

Published

2004

39. Structural biology of the Bcl-2 family of proteins.

Author

Petros AM, Olejniczak ET, and Fesik SW

Subjects

Amino Acid Sequence, Apoptosis Regulatory Proteins, BH3 Interacting Domain Death Agonist Protein, Carrier Proteins chemistry, Membrane Proteins chemistry, Models, Molecular, Molecular Sequence Data, Oncogene Proteins, Proteins chemistry, Proto-Oncogene Proteins chemistry, Sequence Alignment, Viral Proteins chemistry, bcl-2 Homologous Antagonist-Killer Protein, bcl-2-Associated X Protein, bcl-Associated Death Protein, bcl-X Protein, Proto-Oncogene Proteins c-bcl-2 chemistry

Abstract

The proteins of the Bcl-2 family are important regulators of programmed cell death. Structural studies of Bcl-2 family members have provided many important insights into their molecular mechanism of action and how members of this family interact with one another. To date, structural studies have been performed on six Bcl-2 family members encompassing both anti- (Bcl-x(L), Bcl-2, KSHV-Bcl-2, Bcl-w) and pro-apoptotic (Bax, Bid) members. They all show a remarkably similar fold despite an overall divergence in amino acid sequence and function (pro-apoptotic versus anti-apoptotic). The three-dimensional structures of Bcl-2 family members consist of two central, predominantly hydrophobic alpha-helices surrounded by six or seven amphipathic alpha-helices of varying lengths. A long, unstructured loop is present between the first two alpha-helices. The structures of the Bcl-2 proteins show a striking similarity to the overall fold of the pore-forming domains of bacterial toxins. This finding led to experiments which demonstrated that Bcl-x(L), Bcl-2, and Bax all form pores in artificial membranes. A prominent hydrophobic groove is present on the surface of the anti-apoptotic proteins. This groove is the binding site for peptides that mimic the BH3 region of various pro-apoptotic proteins such as Bak and Bad. Structures of Bcl-x(L) in complex with these BH3 peptides showed that they bind as an amphipathic alpha-helix and make extensive hydrophobic contacts with the protein. These data have not only helped to elucidate the interactions important for hetero-dimerization of Bcl-2 family members but have also been used to guide the discovery of small molecules that block Bcl-x(L) and Bcl-2 function. In the recently determined structure of the anti-apoptotic Bcl-w protein, the protein was also found to have a hydrophobic groove on its surface capable of binding BH3-containing proteins and peptides. However, in the native protein an additional carboxy-terminal alpha-helix interacts with the hydrophobic groove. This is reminiscent of how the carboxy-terminal alpha-helix of the pro-apoptotic protein Bax binds into its hydrophobic groove. This interaction may play a regulatory role and for Bax may explain why it is found predominately in the cytoplasm prior to activation. The hydrophobic groove of the pro-apoptotic protein, Bid protein, is neither as long nor as deep as that found in Bcl-x(L), Bcl-2, or Bax. In addition, Bid contains an extra alpha-helix, which is located between alpha1 and alpha2 with respect to Bcl-x(L), Bcl-2, and Bax. Although there are still many unanswered questions regarding the exact mechanism by which the Bcl-2 family of proteins modulates apoptosis, structural studies of these proteins have deepened our understanding of apoptosis on the molecular level.

Published

2004

40. Defining the p53 DNA-binding domain/Bcl-x(L)-binding interface using NMR.

Author

Petros AM, Gunasekera A, Xu N, Olejniczak ET, and Fesik SW

Subjects

Binding Sites, Carrier Proteins chemistry, DNA, Complementary chemistry, DNA, Complementary metabolism, Gene Library, Humans, Models, Molecular, Peptide Fragments pharmacology, Tumor Suppressor Protein p53 metabolism, bcl-Associated Death Protein, Nuclear Magnetic Resonance, Biomolecular methods, Tumor Suppressor Protein p53 chemistry

Abstract

p53 exerts its tumor suppressor activity through both transcription-dependent and transcription-independent processes. Although the transcription-dependent activity of p53 has been extensively studied, the mechanism for transcription-independent p53-mediated tumor suppression is less well known. Recently, it was reported that p53 can directly induce mitochondrial permeabilization and promote apoptosis. This occurs through complexation of the DNA-binding region of p53 with the anti-apoptotic proteins Bcl-x(L) and Bcl-2 (Mihara, M. et al. (2003) Mol. Cell 11, 577-590). Using nuclear magnetic resonance (NMR) spectroscopy we show that the interaction surface on p53 involves the same region that is used by the protein to contact DNA. The p53-binding site on Bcl-x(L) consists of the carboxy-terminus of the first alpha-helix, the loop between alpha3 and alpha4, and the loop between alpha5 and alpha6 of Bcl-x(L). Furthermore, the interaction of p53 with Bcl-x(L) is blocked by the binding of a 25-residue peptide derived from the BH3 region of the pro-apoptotic protein referred to as Bad.

Published

2004

41. Divergence of Genbank and human tumor Bcl-2 sequences and implications for binding affinity to key apoptotic proteins.

Author

Joseph MK, Solomon LR, Petros AM, Cai J, Simmer RL, Zhang H, Rosenberg S, and Ng SC

Subjects

Amino Acid Sequence, Base Sequence, DNA Primers, Humans, Models, Molecular, Molecular Sequence Data, Protein Binding, Proto-Oncogene Proteins c-bcl-2 chemistry, Proto-Oncogene Proteins c-bcl-2 metabolism, Sequence Homology, Amino Acid, Apoptosis, Databases, Nucleic Acid, Proto-Oncogene Proteins c-bcl-2 genetics

Abstract

Heterodimerization of antiapoptotic and pro-apoptotic Bcl-2 family of proteins provides an important mechanism for apoptosis regulation. Knowledge about key amino acids in the binding groove of native Bcl-2 contributing to this interaction will greatly facilitate the design of Bcl-2-specific inhibitors. There are two different Bcl-2 sequences, M13994 and M14745, in Genbank. Chimeric proteins Bcl-2(1) and Bcl-2(2) derived from the above sequences, although similar in structure, showed different binding affinities to Bak and Bad BH3 peptides (Petros et al., 2001). In this study, we show that the Bcl-2(1) sequence in normal and tumor human tissue samples differs from M13994 and M14745, and contains P59, T96, R110, S117 and G237. The actual sequence in the binding pocket matches the Bcl-2-Ig fusion sequence X06487, originally identified in a t(14:18) translocation of the Bcl-2 gene, associated with follicular lymphoma. The possible effects of the observed amino acid differences compared to M13994 and M14745 were investigated by combining structural data with fluorescence anisotropy. G110R substitution confers on Bcl-2(1) substantially increased binding affinity to Bak, Bad and Bax BH3 peptides, demonstrating that R110 is a key contributor to the BH3 binding affinity of Bcl-2. Although NMR structure did not predict R110 involvement in binding to these BH3 peptides, fluorescence anisotropy data clearly points to a critical role for this residue in binding to pro-apoptotic Bcl-2 family members.

Published

2004

42. Solution structure of the BHRF1 protein from Epstein-Barr virus, a homolog of human Bcl-2.

Author

Huang Q, Petros AM, Virgin HW, Fesik SW, and Olejniczak ET

Subjects

Amino Acid Sequence, Apoptosis, Binding Sites, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Peptides chemistry, Protein Binding, Protein Conformation, Protein Structure, Secondary, Herpesvirus 4, Human metabolism, Proto-Oncogene Proteins c-bcl-2 chemistry, Viral Proteins chemistry

Abstract

The three-dimensional structure of BHRF1, the Bcl-2 homolog from Epstein-Barr virus (EBV), has been determined by NMR spectroscopy. Although the overall structure is similar to other Bcl-2 family members, there are important structural differences. Unlike some of the other Bcl-2 family members, BHRF1 does not contain the prominent hydrophobic groove that mediates binding to pro-apoptotic family members. In addition, in contrast to the anti-apoptotic Bcl-2 proteins, BHRF1 does not bind tightly to peptides derived from the pro-apoptotic proteins Bak, Bax, Bik, and Bad. The lack of an exposed, pre-formed binding groove in BHRF1 and the lack of significant binding to peptides derived from pro-apoptotic family members that bind to other anti-apoptotic family members, suggest that the mechanism of the BHRF1 anti-apoptotic activity does not parallel that of cellular Bcl-x(L) or Bcl-2.

Published

2003

43. Ligand binding to domain-3 of human serum albumin: a chemometric analysis.

Author

Hajduk PJ, Mendoza R, Petros AM, Huth JR, Bures M, Fesik SW, and Martin YC

Subjects

Binding Sites, Drug Design, Humans, Ligands, Models, Chemical, Nuclear Magnetic Resonance, Biomolecular, Peptide Fragments metabolism, Protein Binding, Protein Structure, Tertiary, Quantitative Structure-Activity Relationship, Serum Albumin chemistry, Spectrometry, Fluorescence, Serum Albumin metabolism

Abstract

A detailed chemometric analysis of ligand binding to domain-3A of human serum albumin is described. NMR and fluorescence data on a set of 889 chemically diverse compounds were used to develop a group contribution model based on 74 chemical fragments that is in good agreement with the experimental data (R2 = 0.94, Q2 = 0.90). The structural descriptors used in this analysis comprise a convenient look-up table for quantitatively estimating the effect that a particular group will have on albumin binding. This information can be valuable for optimizing a particular series of compounds for drug development.

Published

2003

44. Solution structure of a Bcl-2 homolog from Kaposi sarcoma virus.

Author

Huang Q, Petros AM, Virgin HW, Fesik SW, and Olejniczak ET

Subjects

Amino Acid Sequence, Apoptosis, Hydrophobic and Hydrophilic Interactions, Membrane Proteins chemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Models, Molecular, Molecular Sequence Data, Mutation, Nuclear Magnetic Resonance, Biomolecular, Oncogene Proteins, Peptide Fragments chemistry, Peptide Fragments metabolism, Protein Binding, Protein Structure, Quaternary, Protein Structure, Secondary, Proto-Oncogene Proteins c-bcl-2 metabolism, Sequence Alignment, Solutions, Substrate Specificity, Viral Proteins metabolism, bcl-2 Homologous Antagonist-Killer Protein, bcl-X Protein, Herpesvirus 8, Human chemistry, Proto-Oncogene Proteins c-bcl-2 chemistry, Sequence Homology, Amino Acid, Viral Proteins chemistry

Abstract

Kaposi sarcoma-associated herpes virus (KSHV) contains a gene that has functional and sequence homology to the apoptotic Bcl-2 family of proteins [Sarid, R., Sato, T., Bohenzky, R. A., Russo, J. J. & Chang, Y. (1997) Nat. Med. 3, 293-298]. The viral Bcl-2 protein promotes survival of infected cells and may contribute to the development of Kaposi sarcoma tumors [Boshoff, C. & Chang, Y. (2001) Annu. Rev. Med. 52, 453-470]. Here we describe the solution structure of the viral Bcl-2 homolog from KSHV. Comparison of the KSHV Bcl-2 structure to that of Bcl-2 and Bcl-x(L) shows that although the overall fold is the same, there are key differences in the lengths of the helices and loops. Binding studies on peptides derived from the Bcl-2 homology region 3 of proapoptotic family members indicate that the specificity of the viral protein is very different from what was previously observed for Bcl-x(L) and Bcl-2, suggesting that the viral protein has evolved to have a different mechanism of action than the host proteins.

Published

2002

45. Solution structure of the antiapoptotic protein bcl-2.

Author

Petros AM, Medek A, Nettesheim DG, Kim DH, Yoon HS, Swift K, Matayoshi ED, Oltersdorf T, and Fesik SW

Subjects

Amino Acid Sequence, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular methods, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Structure, Tertiary, Proto-Oncogene Proteins c-bcl-2 genetics, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Solutions, bcl-X Protein, Proto-Oncogene Proteins c-bcl-2 chemistry

Abstract

The structures of two isoforms of Bcl-2 that differ by two amino acids have been determined by NMR spectroscopy. Because wild-type Bcl-2 behaved poorly in solution, the structures were determined by using Bcl-2/Bcl-x(L) chimeras in which part of the putative unstructured loop of Bcl-2 was replaced with a shortened loop from Bcl-x(L). These chimeric proteins have a low pI compared with the wild-type protein and are soluble. The structures of the two Bcl-2 isoforms consist of 6 alpha-helices with a hydrophobic groove on the surface similar to that observed for the homologous protein, Bcl-x(L). Comparison of the Bcl-2 structures to that of Bcl-x(L) shows that although the overall fold is the same, there are differences in the structural topology and electrostatic potential of the binding groove. Although the structures of the two isoforms of Bcl-2 are virtually identical, differences were observed in the ability of the proteins to bind to a 25-residue peptide from the proapoptotic Bad protein and a 16-residue peptide from the proapoptotic Bak protein. These results suggest that there are subtle differences in the hydrophobic binding groove in Bcl-2 that may translate into differences in antiapoptotic activity for the two isoforms.

Published

2001

46. Rationale for Bcl-xL/Bad peptide complex formation from structure, mutagenesis, and biophysical studies.

Author

Petros AM, Nettesheim DG, Wang Y, Olejniczak ET, Meadows RP, Mack J, Swift K, Matayoshi ED, Zhang H, Thompson CB, and Fesik SW

Subjects

Amino Acid Sequence, Apoptosis, Binding Sites, Carrier Proteins metabolism, Humans, Models, Molecular, Mutagenesis, Site-Directed, Nuclear Magnetic Resonance, Biomolecular, Peptides chemical synthesis, Peptides metabolism, Protein Binding, Protein Engineering, Protein Structure, Secondary, Protein Structure, Tertiary, Proto-Oncogene Proteins c-bcl-2 metabolism, Structure-Activity Relationship, bcl-Associated Death Protein, bcl-X Protein, Carrier Proteins chemistry, Proto-Oncogene Proteins c-bcl-2 chemistry

Abstract

The three-dimensional structure of the anti-apoptotic protein Bcl-xL complexed to a 25-residue peptide from the death promoting region of Bad was determined using NMR spectroscopy. Although the overall structure is similar to Bcl-xL bound to a 16-residue peptide from the Bak protein (Sattler et al., 1997), the Bad peptide forms additional interactions with Bcl-xL. However, based upon site-directed mutagenesis experiments, these additional contacts do not account for the increased affinity of the Bad 25-mer for Bcl-xL compared to the Bad 16-mer. Rather, the increased helix propensity of the Bad 25-mer is primarily responsible for its greater affinity for Bcl-xL. Based on this observation, a pair of 16-residue peptides were designed and synthesized that were predicted to have a high helix propensity while maintaining the interactions important for complexation with Bcl-xL. Both peptides showed an increase in helix propensity compared to the wild-type and exhibited an enhanced affinity for Bcl-xL.

Published

2000

47. Retention of immunosuppressant activity in an ascomycin analogue lacking a hydrogen-bonding interaction with FKBP12.

Author

Wiedeman PE, Fesik SW, Petros AM, Nettesheim DG, Mollison KW, Lane BC, Or YS, and Luly JR

Subjects

Amino Acid Sequence, Animals, Humans, Hyperplasia, Immunophilins chemistry, Immunophilins genetics, Immunosuppressive Agents chemistry, Immunosuppressive Agents metabolism, Immunosuppressive Agents pharmacology, Lymph Nodes drug effects, Lymph Nodes immunology, Lymph Nodes pathology, Lymphocyte Culture Test, Mixed, Magnetic Resonance Spectroscopy, Male, Models, Molecular, Molecular Sequence Data, Nucleotidyltransferases genetics, Peptidylprolyl Isomerase chemistry, Peptidylprolyl Isomerase genetics, Protein Binding, Rats, Rats, Inbred Lew, Rats, Sprague-Dawley, Recombinant Fusion Proteins metabolism, Tacrolimus chemical synthesis, Tacrolimus chemistry, Tacrolimus metabolism, Tacrolimus pharmacology, Tacrolimus Binding Proteins, Immunophilins metabolism, Immunosuppressive Agents chemical synthesis, Peptidylprolyl Isomerase metabolism, Tacrolimus analogs & derivatives

Abstract

C24-Deoxyascomycin was prepared in a two-step process from ascomycin and evaluated for its immunosuppressant activity relative to ascomycin and FK506. An intermediate in the synthetic pathway, Delta(23,24)-dehydroascomycin, was likewise evaluated. Despite lacking the hydrogen-bonding interactions associated with the C24-hydroxyl moiety of ascomycin, C24-deoxyascomycin was found to be equipotent to the parent compound both in its immunosuppressive potency and in its interaction with the immunophilin, FKBP12. Conversely, Delta(23,24)-dehydroascomycin which also lacks the same hydrogen-bonding interactions did not exhibit this potency. NMR studies were conducted on the FKBP12/C24-deoxyascomycin complex in an attempt to understand this phenomenon at the molecular level. The NMR structures of the complexes formed between FKBP12 and ascomcyin or C24-deoxyascomcyin were very similar, suggesting that hydrogen-bonding interactions with the C24 hydroxyl moiety are not important for complex formation.

Published

1999

48. Solution structure of an rRNA methyltransferase (ErmAM) that confers macrolide-lincosamide-streptogramin antibiotic resistance.

Author

Yu L, Petros AM, Schnuchel A, Zhong P, Severin JM, Walter K, Holzman TF, and Fesik SW

Subjects

Amino Acid Sequence, Binding Sites, Drug Design, Enzyme Inhibitors chemistry, Lincosamides, Macrolides pharmacology, Magnetic Resonance Spectroscopy methods, Models, Molecular, Molecular Sequence Data, Protein Conformation, Protein Folding, Sequence Homology, Amino Acid, Virginiamycin pharmacology, Anti-Bacterial Agents pharmacology, Drug Resistance, Microbial physiology, Methyltransferases chemistry, Methyltransferases metabolism

Abstract

The Erm family of methyltransferases is responsible for the development of resistance to the macrolide-lincosamide-streptogramin type B (MLS) antibiotics. These enzymes methylate an adenine of 23S ribosomal RNA that prevents the MLS antibiotics from binding to the ribosome and exhibiting their antibacterial activity. Here we describe the three-dimensional structure of an Erm family member, ErmAM, as determined by NMR spectroscopy. The catalytic domain of ErmAM is structurally similar to that found in other methyltransferases and consists of a seven-stranded beta-sheet flanked by alpha-helices and a small two-stranded beta-sheet. In contrast to the catalytic domain, the substrate binding domain is different from other methyltransferases and adopts a novel fold that consists of four alpha-helices.

Published

1997

49. Solution structure of the DNA-binding domain of a human papillomavirus E2 protein: evidence for flexible DNA-binding regions.

Author

Liang H, Petros AM, Meadows RP, Yoon HS, Egan DA, Walter K, Holzman TF, Robins T, and Fesik SW

Subjects

Amino Acid Sequence, Bovine papillomavirus 1 chemistry, Crystallography, X-Ray, DNA-Binding Proteins metabolism, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Protein Conformation, Protein Folding, Sequence Homology, Amino Acid, Solvents chemistry, Viral Proteins metabolism, DNA-Binding Proteins chemistry, Fibroblast Growth Factor 1 chemistry, Papillomaviridae chemistry, Viral Proteins chemistry

Abstract

The three-dimensional structure of the DNA-binding domain of the E2 protein from human papillomavirus-31 was determined by using multidimensional heteronuclear nuclear magnetic resonance (NMR) spectroscopy. A total of 1429 NMR-derived distance and dihedral angle restraints were obtained for each of the 83-residue subunits of this symmetric dimer. The average root mean square deviations of 20 structures calculated using a distance geometry-simulated annealing protocol are 0.59 and 0.90 angstroms for the backbone and all heavy atoms, respectively, for residues 2-83. The structure of the human virus protein free in solution consists of an eight-stranded beta-barrel and two pairs of alpha-helices. Although the overall fold of the protein is similar to the crystal structure of the bovine papillomavirus-1 E2 protein when complexed to DNA, several small but interesting differences were observed between these two structures at the subunit interface. In addition, a beta-hairpin that contacts DNA in the crystal structure of the protein-DNA complex is disordered in the NMR structures, and steady-state 1H-15N heteronuclear NOE measurements indicate that this region is highly mobile in the absence of DNA. The recognition helix also appears to be flexible, as evidenced by fast amide exchange rates. This phenomenon has also been observed for a number of other DNA-binding proteins and may constitute a common theme in protein/DNA recognition.

Published

1996

50. Structure and ligand recognition of the phosphotyrosine binding domain of Shc.

Author

Zhou MM, Ravichandran KS, Olejniczak EF, Petros AM, Meadows RP, Sattler M, Harlan JE, Wade WS, Burakoff SJ, and Fesik SW

Subjects

Amino Acid Sequence, Binding Sites, Blood Proteins chemistry, Ligands, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Peptide Fragments metabolism, Phospholipids metabolism, Phosphopeptides chemistry, Phosphopeptides metabolism, Protein Conformation, Protein Structure, Secondary, Proteins metabolism, Proto-Oncogene Proteins chemistry, Proto-Oncogene Proteins metabolism, Receptor Protein-Tyrosine Kinases chemistry, Receptor Protein-Tyrosine Kinases metabolism, Receptor, trkA, Receptors, Nerve Growth Factor chemistry, Receptors, Nerve Growth Factor metabolism, Shc Signaling Adaptor Proteins, Signal Transduction, src Homology Domains, Adaptor Proteins, Signal Transducing, Adaptor Proteins, Vesicular Transport, Phosphoproteins, Phosphotyrosine metabolism, Proteins chemistry

Abstract

The nuclear magnetic resonance structure of the phosphotyrosine binding (PTB) domain of Shc complexed to a phosphopeptide reveals an alternative means of recognizing tyrosine-phosphorylated proteins. Unlike in SH2 domains, the phosphopeptide forms an antiparallel beta-strand with a beta-sheet of the protein, interacts with a hydrophobic pocket through the (pY-5) residue, and adopts a beta-turn. The PTB domain is structurally similar to pleckstrin homology domains (a beta-sandwich capped by an alpha-helix) and binds to acidic phospholipids, suggesting a possible role in membrane localization.

Published

1995