Your search keyword '"Emmanuelle Thinon"' showing total 21 results

1. Synthesis and characterisation of 5-acyl-6,7-dihydrothieno[3,2-c]pyridine inhibitors of Hedgehog acyltransferase

Author

Thomas Lanyon-Hogg, Naoko Masumoto, George Bodakh, Antonio D. Konitsiotis, Emmanuelle Thinon, Ursula R. Rodgers, Raymond J. Owens, Anthony I. Magee, and Edward W. Tate

Subjects

Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390

Abstract

In this data article we describe synthetic and characterisation data for four members of the 5-acyl-6,7-dihydrothieno[3,2-c]pyridine (termed “RU-SKI”) class of inhibitors of Hedgehog acyltransferase, including associated NMR spectra for final compounds. RU-SKI compounds were selected for synthesis based on their published high potencies against the enzyme target. RU-SKI 41 (9a), RU-SKI 43 (9b), RU-SKI 101 (9c), and RU-SKI 201 (9d) were profiled for activity in the related article “Click chemistry armed enzyme linked immunosorbent assay to measure palmitoylation by Hedgehog acyltransferase” (Lanyon-Hogg et al., 2015) [1]. 1H NMR spectral data indicate different amide conformational ratios between the RU-SKI inhibitors, as has been observed in other 5-acyl-6,7-dihydrothieno[3,2-c]pyridines. The synthetic and characterisation data supplied in the current article provide validated access to the class of RU-SKI inhibitors. Keywords: Synthesis, Inhibitors, Hedgehog acyltransferase, Conformation

Published

2016

2. IFITM3 directly engages and shuttles incoming virus particles to lysosomes

Author

Jennifer S. Spence, Hans Heinrich Hoffmann, Ruina He, Kartik Chandran, Emmanuelle Thinon, Tandrila Das, Charles M. Rice, Howard C. Hang, and Tao Peng

Subjects

Endosomes, Biology, Antiviral Agents, Virus, Article, 03 medical and health sciences, Viral entry, Animals, Humans, Transport Vesicles, Molecular Biology, 030304 developmental biology, 0303 health sciences, Innate immune system, Effector, 030302 biochemistry & molecular biology, Optical Imaging, Virion, Membrane Proteins, RNA-Binding Proteins, Cell Biology, Virus Internalization, Antigens, Differentiation, Transmembrane protein, 3. Good health, Transport protein, Cell biology, Protein Transport, Endocytic vesicle, Membrane protein, A549 Cells, Lysosomes, HeLa Cells

Abstract

Interferon-induced transmembrane proteins (IFITMs 1, 2 and 3) have emerged as important innate immune effectors that prevent diverse virus infections in vertebrates. However, the cellular mechanisms and live-cell imaging of these small membrane proteins have been challenging to evaluate during viral entry of mammalian cells. Using CRISPR-Cas9-mediated IFITM-mutant cell lines, we demonstrate that human IFITM1, IFITM2 and IFITM3 act cooperatively and function in a dose-dependent fashion in interferon-stimulated cells. Through site-specific fluorophore tagging and live-cell imaging studies, we show that IFITM3 is on endocytic vesicles that fuse with incoming virus particles and enhances the trafficking of this pathogenic cargo to lysosomes. IFITM3 trafficking is specific to restricted viruses, requires S-palmitoylation and is abrogated with loss-of-function mutants. The site-specific protein labeling and live-cell imaging approaches described here should facilitate the functional analysis of host factors involved in pathogen restriction as well as their mechanisms of regulation.

Published

2019

3. Selective Enrichment and Direct Analysis of Protein S-Palmitoylation Sites

Author

Emmanuelle Thinon, Henrik Molina, Joseph Fernandez, and Howard C. Hang

Subjects

Proteomics, 0301 basic medicine, Acylation, Lipoylation, Palmitic Acid, Hydroxylamine, Thioester, 01 natural sciences, Biochemistry, Mass Spectrometry, Article, Protein S, 03 medical and health sciences, Palmitoylation, Animals, Humans, Cysteine, chemistry.chemical_classification, Binding Sites, Staining and Labeling, biology, 010405 organic chemistry, Fatty Acids, Membrane Proteins, RNA-Binding Proteins, Fatty acid, General Chemistry, 0104 chemical sciences, 030104 developmental biology, chemistry, Covalent bond, biology.protein, lipids (amino acids, peptides, and proteins), Lipid modification, Fatty acylation, Protein Processing, Post-Translational

Abstract

S-Fatty-acylation is the covalent attachment of long chain fatty acids, predominately palmitate (C16:0, S-palmitoylation), to cysteine (Cys) residues via a thioester linkage on proteins. This post-translational and reversible lipid modification regulates protein function and localization in eukaryotes and is important in mammalian physiology and human diseases. While chemical labeling methods have improved the detection and enrichment of S-fatty-acylated proteins, mapping sites of modification and characterizing the endogenously attached fatty acids are still challenging. Here, we describe the integration and optimization of fatty acid chemical reporter labeling with hydroxylamine-mediated enrichment of S-fatty-acylated proteins and direct tagging of modified Cys residues to selectively map lipid modification sites. This afforded improved enrichment and direct identification of many protein S-fatty-acylation sites compared to previously described methods. Notably, we directly identified the S-fatty-acylation sites of IFITM3, an important interferon-stimulated inhibitor of virus entry, and we further demonstrated that the highly conserved Cys residues are primarily modified by palmitic acid. The methods described here should facilitate the direct analysis of protein S-fatty-acylation sites and their endogenously attached fatty acids in diverse cell types and activation states important for mammalian physiology and diseases.

Published

2018

4. Chemical Proteomic Analysis of S-Fatty Acylated Proteins and Their Modification Sites

Author

Emmanuelle, Thinon and Howard C, Hang

Subjects

Proteomics, Acylation, Lipoproteins, Lipoylation, Humans, Protein Processing, Post-Translational, HeLa Cells

Abstract

Protein S-fatty-acylation, the covalent addition of a long-chain fatty acid, predominantly palmitate (S-palmitoylation), to cysteine, is a highly dynamic and regulated process that controls protein function and localization of membrane-associated proteins in eukaryotes. The analysis of S-fatty acylated peptides by mass spectrometry remains challenging due to the hydrophobic and potentially labile thioester linkage of the S-fatty acylated peptides.Here we describe an optimized protocol for the global analysis of S-palmitoylated proteins based on the combination of an alkyne-tagged chemical reporter of palmitoylation, alk-16 with hydroxylamine-selective hydrolysis of thioester bonds. This protocol decreased the number of false positive proteins and was applied to identify S-fatty acylation sites, providing modification sites for 44 proteins out of the 106 S-fatty acylated proteins identified.

Published

2019

5. Chemical Proteomic Analysis of S-Fatty Acylated Proteins and Their Modification Sites

Author

Howard C. Hang and Emmanuelle Thinon

Subjects

chemistry.chemical_classification, 0303 health sciences, 030302 biochemistry & molecular biology, Fatty acid, Thioester, Mass spectrometry, Acylation, 03 medical and health sciences, Hydrolysis, Palmitoylation, Biochemistry, chemistry, Covalent bond, lipids (amino acids, peptides, and proteins), 030304 developmental biology, Cysteine

Abstract

Protein S-fatty-acylation, the covalent addition of a long-chain fatty acid, predominantly palmitate (S-palmitoylation), to cysteine, is a highly dynamic and regulated process that controls protein function and localization of membrane-associated proteins in eukaryotes. The analysis of S-fatty acylated peptides by mass spectrometry remains challenging due to the hydrophobic and potentially labile thioester linkage of the S-fatty acylated peptides.Here we describe an optimized protocol for the global analysis of S-palmitoylated proteins based on the combination of an alkyne-tagged chemical reporter of palmitoylation, alk-16 with hydroxylamine-selective hydrolysis of thioester bonds. This protocol decreased the number of false positive proteins and was applied to identify S-fatty acylation sites, providing modification sites for 44 proteins out of the 106 S-fatty acylated proteins identified.

Published

2019

6. Click chemistry armed enzyme-linked immunosorbent assay to measure palmitoylation by hedgehog acyltransferase

Author

Emmanuelle Thinon, Ursula R. Rodgers, Antonio D. Konitsiotis, Anthony I. Magee, Naoko Masumoto, Edward W. Tate, George Bodakh, Raymond J. Owens, Thomas Lanyon-Hogg, and Cancer Research UK

Subjects

YnC15, heptadec-16-ynoic acid, Peptide, Protein lipidation, 01 natural sciences, Biochemistry, OTG, n-octyl β-d-glucopyranoside, Substrate Specificity, PATHWAY, PCR, polymerase chain reaction, SONIC-HEDGEHOG, Protein palmitoylation, TBTA, tris[(1-benzyl-1H-1,2,3-triazol-4-yl)methyl]amine, Enzyme Inhibitors, Sonic hedgehog, PROTEIN LIPIDATION, chemistry.chemical_classification, 0303 health sciences, Palmitoyl Coenzyme A, biology, Click chemistry, Chemistry, HRP, horseradish peroxidase, HTS, high-throughput screen, Hedgehog signaling pathway, MBOAT, membrane bound O-acyltransferase, Acyltransferase, Hh, hedgehog, Physical Sciences, Fatty Acids, Unsaturated, Shh, sonic hedgehog, RT, room temperature, Oligopeptides, Life Sciences & Biomedicine, 0301 Analytical Chemistry, CoA, coenzyme A, Biochemistry & Molecular Biology, SDS, sodium dodecyl sulfate, TCEP, tris(2-carboxyethyl)phosphine, Lipoylation, Recombinant Fusion Proteins, Detergents, cat–ELCCA, catalytic assay using an enzyme-linked click chemistry assay, PBS, phosphate-buffered saline, Biophysics, Enzyme-Linked Immunosorbent Assay, click–ELISA, click chemistry armed enzyme-linked immunosorbent assay, CHAPS, 3-[(3-cholamidopropyl)dimethylammonio]-1-propanesulfonate, HEK293a, human embryonic kidney 293a, Article, Biochemical Research Methods, PROBES, 03 medical and health sciences, Palmitoylation, HHAT, Hhat, hedgehog acyltransferase, 0399 Other Chemical Sciences, Hedgehog acyltransferase, Humans, Biotinylation, Hedgehog Proteins, Maltose, DDM, n-dodecyl β-d-maltopyranoside, Molecular Biology, PAGE, polyacrylamide gel electrophoresis, 030304 developmental biology, Science & Technology, 010405 organic chemistry, HUMAN-CELLS, GOAT, ghrelin-O-acyltransferase, Chemistry, Analytical, CANCER PROGRESSION, 0601 Biochemistry And Cell Biology, Cell Biology, Peptide Fragments, MBOAT, 0104 chemical sciences, HEK293 Cells, Immobilized Proteins, Solubility, biology.protein, BSA, bovine serum albumin, Streptavidin, PTM, posttranslational modification, INHIBITORS, Protein Processing, Post-Translational, Acyltransferases

Abstract

Hedgehog signaling is critical for correct embryogenesis and tissue development. However, on maturation, signaling is also found to be aberrantly activated in many cancers. Palmitoylation of the secreted signaling protein sonic hedgehog (Shh) by the enzyme hedgehog acyltransferase (Hhat) is required for functional signaling. To quantify this important posttranslational modification, many in vitro Shh palmitoylation assays employ radiolabeled fatty acids, which have limitations in terms of cost and safety. Here we present a click chemistry armed enzyme-linked immunosorbent assay (click–ELISA) for assessment of Hhat activity through acylation of biotinylated Shh peptide with an alkyne-tagged palmitoyl-CoA (coenzyme A) analogue. Click chemistry functionalization of the alkyne tag with azido-FLAG peptide allows analysis through an ELISA protocol and colorimetric readout. This assay format identified the detergent n-dodecyl β-d-maltopyranoside as an improved solubilizing agent for Hhat activity. Quantification of the potency of RU-SKI small molecule Hhat inhibitors by click–ELISA indicated IC50 values in the low- or sub-micromolar range. A stopped assay format was also employed that allows measurement of Hhat kinetic parameters where saturating substrate concentrations exceed the binding capacity of the streptavidin-coated plate. Therefore, click–ELISA represents a nonradioactive method for assessing protein palmitoylation in vitro that is readily expandable to other classes of protein lipidation.

Published

2015

7. Chemical reporters for exploring protein acylation

Author

Emmanuelle Thinon and Howard C. Hang

Subjects

Proteomics, chemistry.chemical_classification, Cell signaling, Acylation, Proteins, Biology, Biochemistry, Article, Amino acid, chemistry.chemical_compound, Protein acylation, chemistry, Acetylation, Humans, lipids (amino acids, peptides, and proteins), Protein Interaction Maps, Azide, Bioorthogonal chemistry, Protein Processing, Post-Translational, Metabolic Networks and Pathways

Abstract

Proteins are acylated by a variety of metabolites that regulates many important cellular pathways in all kingdoms of life. Acyl groups in cells can vary in structure from the smallest unit, acetate, to modified long-chain fatty acids, all of which can be activated and covalently attached to diverse amino acid side chains and consequently modulate protein function. For example, acetylation of Lys residues can alter the charge state of proteins and generate new recognition elements for protein–protein interactions. Alternatively, long-chain fatty-acylation targets proteins to membranes and enables spatial control of cell signalling. To facilitate the analysis of protein acylation in biology, acyl analogues bearing alkyne or azide tags have been developed that enable fluorescent imaging and proteomic profiling of modified proteins using bioorthogonal ligation methods. Herein, we summarize the currently available acylation chemical reporters and highlight their utility to discover and quantify the roles of protein acylation in biology.

Published

2015

8. Automated multiwell fluorescence lifetime imaging for Förster resonance energy transfer assays and high content analysis

Author

Douglas J. Kelly, Natalie J. Welsh, Mark A. A. Neil, Yuriy Alexandrov, Edward J. Murray, Sunil Kumar, Edward W. Tate, Paul M. W. French, Ian Munro, Remigiusz A. Serwa, Vania M.M. Braga, Anca Margineanu, Christopher Dunsby, Emmanuelle Thinon, James McGinty, Mesayamas Kongsema, Frank Stuhmeier, Clifford Talbot, Sean C. Warren, Eric Lam, Jessica McCormack, and Dominic Alibhai

Subjects

Fluorescence-lifetime imaging microscopy, Fluorophore, General Chemical Engineering, Systems biology, General Engineering, Nanotechnology, Fluorescence, Analytical Chemistry, chemistry.chemical_compound, Förster resonance energy transfer, chemistry, High-content screening, Microscopy, Plate reader

Abstract

Fluorescence lifetime measurements can provide quantitative assays of the local fluorophore environment and can be applied to read out biomolecular interactions via Forster resonance energy transfer (FRET). Fluorescence lifetime imaging (FLIM) can be automated for high content analysis (HCA) to map protein–protein interactions with applications in drug discovery, systems biology and basic research. The automated acquisition of FLIM data over 100's of fields of view provides statistical power to overcome noise in instrumentation and biological systems and thus exploit relatively small changes in mean lifetime to provide useful readouts that would not be practically achievable in manual microscopy experiments. We present here an automated HCA system with the ability to perform rapid unsupervised optically sectioned FLIM of fixed and live biological samples and illustrate its potential through exemplar applications of different FRET readouts.

Published

2015

9. Isosteric Substitutions of Urea to Thiourea and Selenourea in Aliphatic Oligourea Foldamers: Site-Specific Perturbation of the Helix Geometry

Author

Brice Kauffmann, Stéphanie Antunes, Yella Reddy Nelli, Céline Douat, Gilles Guichard, Stéphane Massip, Arnaud Salaün, and Emmanuelle Thinon

Subjects

Models, Molecular, Molecular Structure, Stereochemistry, Circular Dichroism, Selenourea, Organic Chemistry, Thiourea, Geometry, General Chemistry, Catalysis, chemistry.chemical_compound, chemistry, Organoselenium Compounds, X-ray crystallography, Urea

Abstract

Nearly isosteric oxo to thioxo substitution was employed to interrogate the structure of foldamers with a urea backbone and explore the relationship between helical folding and hydrogen-bonding interactions. A series of oligomers with urea bonds substituted by thiourea bonds at discrete or all positions in the sequence have been prepared and their folding propensity was studied by using a combination of spectroscopic methods and X-ray diffraction. The outcome of oxo to thioxo replacements on the helical folding was found to depend on whether central or terminal ureas were modified. The canonical helix geometry was not affected upon insertion of thioureas close to the negative end of the helix dipole, whereas thioureas close to the positive pole were found to increase the terminal flexibility and cause helix fraying. Perturbation was amplified when a selenourea was incorporated instead, leading to a structure that is only partly folded.

Published

2014

10. Mass-Tag Labeling Using Acyl-PEG Exchange for the Determination of Endogenous Protein S-Fatty Acylation

Author

Avital, Percher, Emmanuelle, Thinon, and Howard, Hang

Subjects

Maleimides, HEK293 Cells, Acrylates, Acylation, Fatty Acids, Humans, Proteins, lipids (amino acids, peptides, and proteins), Cysteine, Article, Cell Line, Polyethylene Glycols, Protein Binding

Abstract

The covalent coupling of fatty acids to proteins provides an important mechanism of regulation in cells. In eukaryotes, cysteine fatty acylation (S-fatty acylation) has been shown to be critical for protein function in a variety of cellular pathways as well as microbial pathogenesis. While methods developed over the past decade have improved the detection and profiling of S-fatty acylation, these are hampered in their ability to characterize endogenous protein S-fatty acylation levels under physiological conditions. Furthermore, understanding the contribution of specific sites and levels of S-fatty acylation remains a major challenge. To evaluate S-fatty acylation of endogenous proteins as well as to determine the number of S-fatty acylation events, we developed the acyl-PEG exchange (APE) that utilizes cysteine-specific chemistry to exchange S-fatty acylation sites with mass-tags of defined size, which can be readily observed by western blotting. APE provides a readily accessible approach to investigate endogenous S-fatty acylation from any sample source, with high sensitivity and broad applicability that complements the current toolbox of methods for thioester-based post-translational modifications. © 2017 by John WileySons, Inc.

Published

2017

11. Mass-Tag Labeling Using Acyl-PEG Exchange for the Determination of Endogenous Protein S-Fatty Acylation

Author

Emmanuelle Thinon, Howard C. Hang, and Avital Percher

Subjects

0301 basic medicine, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Endogeny, Thioester, Acylation, Blot, 03 medical and health sciences, 030104 developmental biology, Biochemistry, chemistry, Covalent bond, PEGylation, lipids (amino acids, peptides, and proteins), Fatty acylation, Cysteine

Abstract

The covalent coupling of fatty acids to proteins provides an important mechanism of regulation in cells. In eukaryotes, cysteine fatty acylation (S-fatty acylation) has been shown to be critical for protein function in a variety of cellular pathways as well as microbial pathogenesis. While methods developed over the past decade have improved the detection and profiling of S-fatty acylation, these are hampered in their ability to characterize endogenous protein S-fatty acylation levels under physiological conditions. Furthermore, understanding the contribution of specific sites and levels of S-fatty acylation remains a major challenge. To evaluate S-fatty acylation of endogenous proteins as well as to determine the number of S-fatty acylation events, we developed the acyl-PEG exchange (APE) that utilizes cysteine-specific chemistry to exchange S-fatty acylation sites with mass-tags of defined size, which can be readily observed by western blotting. APE provides a readily accessible approach to investigate endogenous S-fatty acylation from any sample source, with high sensitivity and broad applicability that complements the current toolbox of methods for thioester-based post-translational modifications. © 2017 by John Wiley & Sons, Inc.

Published

2017

12. Open Source High Content Analysis Utilizing Automated Fluorescence Lifetime Imaging Microscopy

Author

Yuriy Alexandrov, Edward J. Murray, Clifford Talbot, James McGinty, Sunil Kumar, Dominic Alibhai, Emmanuelle Thinon, Paul M. W. French, Remigiusz A. Serwa, Vincenzo da Paola, Mark A. A. Neil, Edwin Garcia, Ian Munro, Frank Stuhmeier, Lucien West, Douglas J. Kelly, Edward W. Tate, Christopher Dunsby, Sean C. Warren, Frederik Görlitz, Biotechnology and Biological Sciences Research Council (BBSRC), Wellcome Trust, Engineering & Physical Science Research Council (E, and Medical Research Council (MRC)

Subjects

Fluorescence-lifetime imaging microscopy, Computer science, General Chemical Engineering, PROTEIN, 02 engineering and technology, Biosensing Techniques, RESONANCE ENERGY-TRANSFER, gag Gene Products, Human Immunodeficiency Virus, fluorescence microscopy, 0302 clinical medicine, open source, BIOSENSOR, Chlorocebus aethiops, Fluorescence microscope, Fluorescence Resonance Energy Transfer, HCA, 030212 general & internal medicine, LIVING CELLS, General Neuroscience, Optical Imaging, 021001 nanoscience & nanotechnology, TIME, Multidisciplinary Sciences, High-content screening, COS Cells, Science & Technology - Other Topics, 0210 nano-technology, Biological system, STANDARDS, FLIM, Biophysics, automated microscopy, General Biochemistry, Genetics and Molecular Biology, drug discovery, 03 medical and health sciences, Open source data, Animals, Humans, Issue 119, Science & Technology, General Immunology and Microbiology, Open source, Förster resonance energy transfer, Microscopy, Fluorescence, Time course, NADH, FRET, Biosensor, Software

Abstract

We present an open source high content analysis instrument utilizing automated fluorescence lifetime imaging (FLIM) for assaying protein interactions using Förster resonance energy transfer (FRET) based readouts of fixed or live cells in multiwell plates. This provides a means to screen for cell signaling processes read out using intramolecular FRET biosensors or intermolecular FRET of protein interactions such as oligomerization or heterodimerization, which can be used to identify binding partners. We describe here the functionality of this automated multiwell plate FLIM instrumentation and present exemplar data from our studies of HIV Gag protein oligomerization and a time course of a FRET biosensor in live cells. A detailed description of the practical implementation is then provided with reference to a list of hardware components and a description of the open source data acquisition software written in μ Manager. The application of FLIMfit, an open source MATLAB- based client for the OMERO platform, to analyze arrays of multiwell plate FLIM data is also presented. The protocols for imaging fixed and live cells are outlined and a demonstration of an automated multiwell plate FLIM experiment using cells expressing fluorescent protein-based FRET constructs is presented. This is complemented by a walk-through of the data analysis for this specific FLIM FRET data set.

Published

2017

13. Bioorthogonal Chemical Reporters for Monitoring Unsaturated Fatty-Acylated Proteins

Author

Howard C. Hang, Emmanuelle Thinon, and Avital Percher

Subjects

0301 basic medicine, Proteomics, Acylation, Quantitative proteomics, Biochemistry, Article, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Mice, In vivo, Lipid droplet, Animals, Humans, Molecular Biology, Unsaturated fatty acid, 030102 biochemistry & molecular biology, Organic Chemistry, Proteins, Oleic acid, 030104 developmental biology, chemistry, Covalent bond, Fatty Acids, Unsaturated, Molecular Medicine, Bioorthogonal chemistry, Fatty acylation, HeLa Cells

Abstract

Dietary unsaturated fatty acids, such as oleic acid, have been shown to be covalently incorporated into a small subset of proteins but the generality and diversity of this protein modification has not been studied. We synthesized unsaturated fatty acid chemical reporters and determined their protein targets in mammalian cells. The unsaturated fatty acid chemical reporters can induce the formation of lipid droplets and be incorporated site-specifically onto known fatty-acylated proteins and label many proteins in mammalian cells. Quantitative proteomics analysis revealed that unsaturated fatty acids modify similar protein targets to saturated fatty acids, including several immunity-associated proteins, which demonstrates unsaturated fatty acids may directly modify many proteins to exert their unique and often beneficial physiological effects in vivo.

Published

2016

14. Automated fluorescence lifetime imaging plate reader and its application to Förster resonant energy transfer readout of Gag protein aggregation

Author

Edward W. Tate, Yuriy Alexandrov, Edward J. Murray, Frank Stuhmeier, Paul M. W. French, Christopher Dunsby, Emmanuelle Thinon, Mark A. A. Neil, Sunil Kumar, Anca Margineau, Sean C. Warren, Douglas J. Kelly, Dominic Alibhai, and Remigiusz A. Serwa

Subjects

Resonant inductive coupling, Fluorescence-lifetime imaging microscopy, protein-protein interactions, General Physics and Astronomy, 01 natural sciences, gag Gene Products, Human Immunodeficiency Virus, chemistry.chemical_compound, Automation, BIOSENSOR, Fluorescence Resonance Energy Transfer, General Materials Science, HCA, LIVING CELLS, SPATIAL-RESOLUTION, 0303 health sciences, fluorescence lifetime imaging microscopy (FLIM), Chemistry, General Engineering, MICROSCOPY, Fluorescence, NETWORKS, 3. Good health, Molecular Imaging, HIV-1 Gag, Physical Sciences, Life Sciences & Biomedicine, Plate reader, Biochemistry & Molecular Biology, FLIM, Fluorophore, Biophysics, CONTRAST, Nanotechnology, Biochemical Research Methods, General Biochemistry, Genetics and Molecular Biology, 010309 optics, 03 medical and health sciences, Full Article, 0103 physical sciences, Humans, Protein Structure, Quaternary, 030304 developmental biology, Science & Technology, IDENTIFICATION, Optics, General Chemistry, Editor's Choice, Förster resonance energy transfer, FRET, Molecular imaging, Protein Multimerization, Biosensor, HeLa Cells

Abstract

Fluorescence lifetime measurements can provide quantitative readouts of local fluorophore environment and can be applied to biomolecular interactions via Förster resonant energy transfer (FRET). Fluorescence lifetime imaging (FLIM) can therefore provide a high content analysis (HCA) modality to map protein-protein interactions (PPIs) with applications in drug discovery, systems biology and basic research. We present here an automated multiwell plate reader able to perform rapid unsupervised optically sectioned FLIM of fixed and live biological samples and illustrate its potential to assay PPIs through application to Gag protein aggregation during the HIV life cycle. We demonstrate both hetero-FRET and homo-FRET readouts of protein aggregation and report the first quantitative evaluation of a FLIM HCA assay by generating dose response curves through addition of an inhibitor of Gag myristoylation. Z ′ factors exceeding 0.6 are realised for this FLIM FRET assay. Fluorescence lifetime plate map with representative images of high and low FRET cells and corresponding dose response plot.

Published

2012

15. Synthesis and characterisation of 5-acyl-6,7-dihydrothieno[3,2-c]pyridine inhibitors of Hedgehog acyltransferase

Author

Thomas, Lanyon-Hogg, Naoko, Masumoto, George, Bodakh, Antonio D, Konitsiotis, Emmanuelle, Thinon, Ursula R, Rodgers, Raymond J, Owens, Anthony I, Magee, and Edward W, Tate

Subjects

Synthesis, Inhibitors, Hedgehog acyltransferase, Conformation, Data Article

Abstract

In this data article we describe synthetic and characterisation data for four members of the 5-acyl-6,7-dihydrothieno[3,2-c]pyridine (termed "RU-SKI") class of inhibitors of Hedgehog acyltransferase, including associated NMR spectra for final compounds. RU-SKI compounds were selected for synthesis based on their published high potencies against the enzyme target. RU-SKI 41 (9a), RU-SKI 43 (9b), RU-SKI 101 (9c), and RU-SKI 201 (9d) were profiled for activity in the related article "Click chemistry armed enzyme linked immunosorbent assay to measure palmitoylation by Hedgehog acyltransferase" (Lanyon-Hogg et al., 2015) [1]. (1)H NMR spectral data indicate different amide conformational ratios between the RU-SKI inhibitors, as has been observed in other 5-acyl-6,7-dihydrothieno[3,2-c]pyridines. The synthetic and characterisation data supplied in the current article provide validated access to the class of RU-SKI inhibitors.

Published

2015

16. Global profiling of protein lipidation using chemical proteomic technologies

Author

Edward W, Tate, Karunakaran A, Kalesh, Thomas, Lanyon-Hogg, Elisabeth M, Storck, and Emmanuelle, Thinon

Subjects

Proteomics, endocrine system, Proteome, Glycosylphosphatidylinositols, Acylation, Proteins, Lipid Metabolism, Lipids, Article, Cholesterol, Animals, Humans, lipids (amino acids, peptides, and proteins), Protein Processing, Post-Translational

Abstract

Highlights • Protein lipidation is an essential modification (PTM) in all forms of life. • Key modifications include acylation, prenylation, cholesterylation and GPI anchors. • Global profiling of this class of PTM is beyond the scope of standard technologies. • Metabolic chemical tagging can reveal the full scope of protein lipidation in vivo. • Chemical proteomics will have a deep impact on understanding of protein lipidation., Protein lipidation is unique amongst post-translational modifications (PTMs) in enabling direct interaction with cell membranes, and is found in every form of life. Lipidation is important in normal function and in disease, but its intricate interplay with disease context presents a challenging for drug development. Global whole-proteome profiling of protein lipidation lies beyond the range of standard methods, but is well-suited to metabolic tagging with small ‘clickable’ chemical reporters that do not disrupt metabolism and function; chemoselective reactions are then used to add multifunctional labels exclusively to tagged-lipidated proteins. This chemical proteomic technology has opened up the first quantitative whole-proteome studies of the known major classes of protein lipidation, and the first insights into their full scope in vivo.

Published

2014

17. Inside Cover: Bioorthogonal Chemical Reporters for Monitoring Unsaturated Fatty-Acylated Proteins (ChemBioChem 19/2016)

Author

Avital Percher, Emmanuelle Thinon, and Howard C. Hang

Subjects

Chemistry, Organic Chemistry, Quantitative proteomics, Molecular Medicine, Organic chemistry, Cover (algebra), Bioorthogonal chemistry, Fatty acylation, Molecular Biology, Biochemistry, Combinatorial chemistry

Published

2016

18. Multifunctional protein labeling via enzymatic N-terminal tagging and elaboration by click chemistry

Author

Megan H. Wright, Edward W. Tate, Emmanuelle Thinon, and William P. Heal

Subjects

Proteomics, Staining and Labeling, Myristic acid, Proteins, General Biochemistry, Genetics and Molecular Biology, chemistry.chemical_compound, Affinity chromatography, chemistry, Biochemistry, Saturated fatty acid, Click chemistry, Escherichia coli, Transferase, Click Chemistry, Target protein, Azide, Protein Processing, Post-Translational, Acyltransferases, Myristoylation

Abstract

A protocol for selective and site-specific enzymatic labeling of proteins is described. The method exploits the protein co-/post-translational modification known as myristoylation, the transfer of myristic acid (a 14-carbon saturated fatty acid) to an N-terminal glycine catalyzed by the enzyme myristoyl-CoA:protein N-myristoyltransferase (NMT). Escherichia coli, having no endogenous NMT, is used for the coexpression of both the transferase and the target protein to be labeled, which participate in the in vivo N-terminal attachment of synthetically derived tagged analogs of myristic acid bearing a 'clickable' tag. This tag is a functional group that can undergo bio-orthogonal ligation via 'click' chemistry, for example, an azide, and can be used as a handle for further site-specific labeling in vitro. Here we provide protocols for in vivo N-terminal tagging of recombinant protein, and the synthesis and application of multifunctional reagents that enable protein labeling via click chemistry for affinity purification and detection by fluorescence. In addition to general N-terminal protein labeling, the protocol would be of particular use in providing evidence for native myristoylation of proteins of interest, proof of activity/selectivity of NMTs and cross-species reactivity of NMTs without resorting to the use of radioactive isotopes.

Published

2011

19. A fluorescence-based assay for N-myristoyltransferase activity

Author

Goncalves, James A. Brannigan, Emmanuelle Thinon, T.O. Olaleye, Remigiusz A. Serwa, Edward W. Tate, S Lanzarone, Robin J. Leatherbarrow, and Anthony J. Wilkinson

Subjects

Biochemistry & Molecular Biology, N-Myristoyltransferase (NMT), Coenzyme A, Biophysics, Myristic acid, COA, Biochemistry, Article, Biochemical Research Methods, Fluorescence, chemistry.chemical_compound, Coumarins, MYRISTOYL TRANSFERASE, Peptide bond, Humans, Molecular Biology, IN-VIVO, Fluorescent Dyes, chemistry.chemical_classification, GAG, Science & Technology, Chemistry, Analytical, NMT2, Fatty acid, Cell Biology, Molecular biology, Small molecule, Kinetics, Chemistry, Enzyme, TARGET, chemistry, Glycine, Physical Sciences, Screening, lipids (amino acids, peptides, and proteins), MEMBRANE, INHIBITORS, Myristic Acids, Protein Processing, Post-Translational, Life Sciences & Biomedicine, Acyltransferases, 7-Diethylamino-3-(4-maleimido-phenyl)-4-methylcoumarin (CPM)

Abstract

N-myristoylation is the irreversible attachment of a C(14) fatty acid, myristic acid, to the N-terminal glycine of a protein via formation of an amide bond. This modification is catalyzed by myristoyl-coenzyme A (CoA):protein N-myristoyltransferase (NMT), an enzyme ubiquitous in eukaryotes that is up-regulated in several cancers. Here we report a sensitive fluorescence-based assay to study the enzymatic activity of human NMT1 and NMT2 based on detection of CoA by 7-diethylamino-3-(4-maleimido-phenyl)-4-methylcoumarin. We also describe expression and characterization of NMT1 and NMT2 and assay validation with small molecule inhibitors. This assay should be broadly applicable to NMTs from a range of organisms.

Published

2011

20. Current Protocols in Protein Science

Author

Avital Percher, Emmanuelle Thinon, and Howard Hang

Published

2001

21. Proteomic analysis of fatty-acylated proteins

Author

Emmanuelle Thinon, Tao Peng, and Howard C. Hang

Subjects

Proteomics, 0301 basic medicine, Proteomics methods, Acylation, Computational biology, Biology, Bioinformatics, 01 natural sciences, Biochemistry, Article, Analytical Chemistry, 03 medical and health sciences, Animals, Humans, 010405 organic chemistry, Extramural, Fatty Acids, Proteins, Lipid structure, 0104 chemical sciences, 030104 developmental biology, Post translational, Proteins metabolism, Protein processing, lipids (amino acids, peptides, and proteins), Identification (biology), Protein Processing, Post-Translational

Abstract

Protein fatty-acylation in eukaryotes has been associated with many fundamental biological processes. However, the diversity, abundance and regulatory mechanisms of protein fatty-acylation in vivo remain to be explored. Herein, we review the proteomic analysis of fatty-acylated proteins, with a focus on N-myristoylation and S-palmitoylation. We then highlight major challenges and emerging methods for direct site identification, quantitation, and lipid structure characterization to understand the functions and regulatory mechanisms of fatty-acylated proteins in physiology and disease.