Your search keyword '"Sarah Barelier"' showing total 24 results

1. Lineage-Specific Viral Hijacking of Non-canonical E3 Ubiquitin Ligase Cofactors in the Evolution of Vif Anti-APOBEC3 Activity

Author

Joshua R. Kane, David J. Stanley, Judd F. Hultquist, Jeffrey R. Johnson, Nicole Mietrach, Jennifer M. Binning, Stefán R. Jónsson, Sarah Barelier, Billy W. Newton, Tasha L. Johnson, Kathleen E. Franks-Skiba, Ming Li, William L. Brown, Hörður I. Gunnarsson, Adalbjorg Adalbjornsdóttir, James S. Fraser, Reuben S. Harris, Valgerður Andrésdóttir, John D. Gross, and Nevan J. Krogan

Subjects

Biology (General), QH301-705.5

Abstract

HIV-1 encodes the accessory protein Vif, which hijacks a host Cullin-RING ubiquitin ligase (CRL) complex as well as the non-canonical cofactor CBFβ, to antagonize APOBEC3 antiviral proteins. Non-canonical cofactor recruitment to CRL complexes by viral factors, to date, has only been attributed to HIV-1 Vif. To further study this phenomenon, we employed a comparative approach combining proteomic, biochemical, structural, and virological techniques to investigate Vif complexes across the lentivirus genus, including primate (HIV-1 and simian immunodeficiency virus macaque [SIVmac]) and non-primate (FIV, BIV, and MVV) viruses. We find that CBFβ is completely dispensable for the activity of non-primate lentiviral Vif proteins. Furthermore, we find that BIV Vif requires no cofactor and that MVV Vif requires a novel cofactor, cyclophilin A (CYPA), for stable CRL complex formation and anti-APOBEC3 activity. We propose modular conservation of Vif complexes allows for potential exaptation of functions through the acquisition of non-CRL-associated host cofactors while preserving anti-APOBEC3 activity.

Published

2015

2. Roles for ordered and bulk solvent in ligand recognition and docking in two related cavities.

Author

Sarah Barelier, Sarah E Boyce, Inbar Fish, Marcus Fischer, David B Goodin, and Brian K Shoichet

Subjects

Medicine, Science

Abstract

A key challenge in structure-based discovery is accounting for modulation of protein-ligand interactions by ordered and bulk solvent. To investigate this, we compared ligand binding to a buried cavity in Cytochrome c Peroxidase (CcP), where affinity is dominated by a single ionic interaction, versus a cavity variant partly opened to solvent by loop deletion. This opening had unexpected effects on ligand orientation, affinity, and ordered water structure. Some ligands lost over ten-fold in affinity and reoriented in the cavity, while others retained their geometries, formed new interactions with water networks, and improved affinity. To test our ability to discover new ligands against this opened site prospectively, a 534,000 fragment library was docked against the open cavity using two models of ligand solvation. Using an older solvation model that prioritized many neutral molecules, three such uncharged docking hits were tested, none of which was observed to bind; these molecules were not highly ranked by the new, context-dependent solvation score. Using this new method, another 15 highly-ranked molecules were tested for binding. In contrast to the previous result, 14 of these bound detectably, with affinities ranging from 8 µM to 2 mM. In crystal structures, four of these new ligands superposed well with the docking predictions but two did not, reflecting unanticipated interactions with newly ordered waters molecules. Comparing recognition between this open cavity and its buried analog begins to isolate the roles of ordered solvent in a system that lends itself readily to prospective testing and that may be broadly useful to the community.

Published

2013

3. Discovery of fragment molecules that bind the human peroxiredoxin 5 active site.

Author

Sarah Barelier, Dominique Linard, Julien Pons, André Clippe, Bernard Knoops, Jean-Marc Lancelin, and Isabelle Krimm

Subjects

Medicine, Science

Abstract

The search for protein ligands is a crucial step in the inhibitor design process. Fragment screening represents an interesting method to rapidly find lead molecules, as it enables the exploration of a larger portion of the chemical space with a smaller number of compounds as compared to screening based on drug-sized molecules. Moreover, fragment screening usually leads to hit molecules that form few but optimal interactions with the target, thus displaying high ligand efficiencies. Here we report the screening of a homemade library composed of 200 highly diverse fragments against the human Peroxiredoxin 5 protein. Peroxiredoxins compose a family of peroxidases that share the ability to reduce peroxides through a conserved cysteine. The three-dimensional structures of these enzymes ubiquitously found throughout evolution have been extensively studied, however, their biological functions are still not well understood and to date few inhibitors have been discovered against these enzymes. Six fragments from the library were shown to bind to the Peroxiredoxin 5 active site and ligand-induced chemical shift changes were used to drive the docking of these small molecules into the protein structure. The orientation of the fragments in the binding pocket was confirmed by the study of fragment homologues, highlighting the role of hydroxyl functions that hang the ligands to the Peroxiredoxin 5 protein. Among the hit fragments, the small catechol molecule was shown to significantly inhibit Peroxiredoxin 5 activity in a thioredoxin peroxidase assay. This study reports novel data about the ligand-Peroxiredoxin interactions that will help considerably the development of potential Peroxiredoxin inhibitors.

Published

2010

4. Supplementary Methods from Tumor Protein 53–Induced Nuclear Protein 1 Is a Major Mediator of p53 Antioxidant Function

Author

Alice Carrier, Juan L. Iovanna, Nelson J. Dusetti, Marie-Josèphe Pébusque, Rose P. Spoto, Sophie Vasseur, Sarah Barelier, Mylène Seux, Stéphane Garcia, Marcel Culcasi, Sylvia Pietri, Julien Gommeaux, and Carla E. Cano

Abstract

Supplementary Methods from Tumor Protein 53–Induced Nuclear Protein 1 Is a Major Mediator of p53 Antioxidant Function

Published

2023

5. Supplementary Figures 1-6 from Tumor Protein 53–Induced Nuclear Protein 1 Is a Major Mediator of p53 Antioxidant Function

Author

Alice Carrier, Juan L. Iovanna, Nelson J. Dusetti, Marie-Josèphe Pébusque, Rose P. Spoto, Sophie Vasseur, Sarah Barelier, Mylène Seux, Stéphane Garcia, Marcel Culcasi, Sylvia Pietri, Julien Gommeaux, and Carla E. Cano

Abstract

Supplementary Figures 1-6 from Tumor Protein 53–Induced Nuclear Protein 1 Is a Major Mediator of p53 Antioxidant Function

Published

2023

6. The long-awaited structure of human fucosidase FucA1 opens novel avenues for the treatment of fucosidosis

Author

Sarah Barelier, Gerlind Sulzenbacher, Architecture et fonction des macromolécules biologiques (AFMB), and Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)

Subjects

Fucosidosis, alpha-L-Fucosidase, Structural Biology, [SDV]Life Sciences [q-bio], Humans, Molecular Biology

Abstract

International audience; In this issue of Structure, Armstrong and colleagues probe the structure of human fucosidase FucA1. Their work resolves an ongoing debate around the enzyme’s catalytic mechanism and provides a valid structural template to guide the design of drugs alleviating the rare, yet severe, lysosomal storage disease fucosidosis.

Published

2022

7. Direct capture, inhibition and crystal structure of HsaD (Rv3569c) from M. tuberculosis

Author

Sarah Barelier, Romain Avellan, Giri Raj Gnawali, Patrick Fourquet, Véronique Roig‐Zamboni, Isabelle Poncin, Vanessa Point, Yves Bourne, Stéphane Audebert, Luc Camoin, Christopher D. Spilling, Stéphane Canaan, Jean‐François Cavalier, Gerlind Sulzenbacher, Architecture et fonction des macromolécules biologiques (AFMB), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Laboratoire d'ingénierie des systèmes macromoléculaires (LISM), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), University of Missouri [St. Louis], University of Missouri System, Centre de Recherche en Cancérologie de Marseille (CRCM), Aix Marseille Université (AMU)-Institut Paoli-Calmettes, Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), ANR-19-CE44-0011,LipInTB,Utilisation de nouveaux inhibiteurs sélectifs pour décrypter le métabolisme lipidique et de la virulence chez M. tb(2019), Cavalier, Jean-François, and Utilisation de nouveaux inhibiteurs sélectifs pour décrypter le métabolisme lipidique et de la virulence chez M. tb - - LipInTB2019 - ANR-19-CE44-0011 - AAPG2019 - VALID

Subjects

[SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], [CHIM.ORGA]Chemical Sciences/Organic chemistry, [SDV.BBM.BS] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], [CHIM.THER] Chemical Sciences/Medicinal Chemistry, click chemistry activity-based protein profiling, Cell Biology, [CHIM.THER]Chemical Sciences/Medicinal Chemistry, [CHIM.ORGA] Chemical Sciences/Organic chemistry, Biochemistry, Antituberculous molecules, Cholesterol metabolism, Inhibition mechanism, Cyclipostins and Cyclophostin, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, [SDV.BBM.BC] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM]

Abstract

International audience; A hallmark of Mycobacterium tuberculosis (M. tb), the etiologic agent of tuberculosis, is its ability to metabolize host-derived lipids. However, the enzymes and mechanisms underlying such metabolism are still largely unknown. We previously reported that the Cyclophostin & Cyclipostins (CyC) analogs, a new family of potent antimycobacterial molecules, react specifically and covalently with (Ser/Cys)-based enzymes mostly involved in bacterial lipid metabolism. Here, we report the synthesis of new CyC alkyne-containing inhibitors (CyCyne) and their use for the direct fishing of target proteins in M. tb culture via bio-orthogonal click-chemistry activity-based protein profiling (CC-ABPP). This approach led to the capture and identification of a variety of enzymes, many of them involved in lipid or steroid metabolisms. One of the captured enzymes, HsaD (Rv3569c), is required for the survival of M. tb within macrophages and is thus a potential therapeutic target. This prompted us to further explore and validate, through a combination of biochemical and structural approaches, the specificity of HsaD inhibition by the CyC analogs. We confirmed that the CyC bind covalently to the catalytic Ser114 residue, leading to a total loss of enzyme activity. These data were supported by the X-ray structures of four HsaD-CyC complexes, obtained at resolutions between 1.6-2.6 Å. The identification of mycobacterial enzymes directly captured by the CyCyne probes through CC-ABPP paves the way to better understand and potentially target key players at crucial stages of the bacilli life-cycle.

Published

2022

8. Structure-guided optimization of adenosine mimetics as selective and potent inhibitors of coronavirus nsp14 N7-methyltransferases

Author

Marcel Hausdorff, Adrien Delpal, Sarah Barelier, Laura Nicollet, Bruno Canard, Franck Touret, Agathe Colmant, Bruno Coutard, Jean-Jacques Vasseur, Etienne Decroly, Françoise Debart, Institut des Biomolécules Max Mousseron [Pôle Chimie Balard] (IBMM), Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université de Montpellier (UM)-Ecole Nationale Supérieure de Chimie de Montpellier (ENSCM), Université de Montpellier (UM), Architecture et fonction des macromolécules biologiques (AFMB), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), and Institut Hospitalier Universitaire Méditerranée Infection (IHU Marseille)

Subjects

bisubstrate, Pharmacology, SARS-CoV-2, Organic Chemistry, Drug Discovery, RNA cap methyltransferase, structure-guided design, [CHIM.THER]Chemical Sciences/Medicinal Chemistry, General Medicine, arylsulfonamide, 7-deaza-adenine

Abstract

International audience; The COVID-19 pandemic reveals the urgent need to develop new therapeutics targeting the SARS-CoV-2 replication machinery. The first antiviral drugs were nucleoside analogues targeting RdRp and protease inhibitors active on nsp5 Mpro. In addition to these common antiviral targets, SARS-CoV-2 codes for the highly conserved protein nsp14 harbouring N7methyltransferase (MTase) activity. Nsp14 is involved in cap N7-methylation of viral RNA and its inhibition impairs viral RNA translation and immune evasion, making it an attractive new antiviral target. In this work, we followed a structure-guided drug design approach to design bisubstrates mimicking the S-adenosylmethionine methyl donor and RNA cap. We developed adenosine mimetics with an N-arylsulfonamide moiety in the 5'-position, recently described as a guanine mimicking the cap structure in a potent adenosine-derived nsp14 inhibitor. Here, the adenine moiety was replaced by hypoxanthine, N 6-methyladenine, or C7-substituted 7-deazaadenine. 26 novel adenosine mimetics were synthesized, one of which selectively inhibits nsp14 N7-MTase activity with a subnanomolar IC50 (and seven with a single-digit nanomolar IC50). In the most potent inhibitors, adenine was replaced by two different 7-deaza-adenines bearing either a phenyl or a 3-quinoline group at the C7-position via an ethynyl linker. These more complex compounds are barely active on the cognate human N7-MTase and docking experiments reveal that their selectivity of inhibition might result from the positioning of their C7 substitution in a SAM entry tunnel present in the nsp14 structure and absent in the hN7-MTase. These compounds show moderate antiviral activity against SARS-CoV-2 replication in cell culture, suggesting delivery or stability issue.

Published

2023

9. Author response for 'Direct capture, inhibition and crystal structure of <scp>HsaD</scp> (Rv3569c) from M. tuberculosis'

Author

null Sarah Barelier, null Romain Avellan, null Giri Raj Gnawali, null Patrick Fourquet, null Véronique Roig‐Zamboni, null Isabelle Poncin, null Vanessa Point, null Yves Bourne, null Stéphane Audebert, null Luc Camoin, null Christopher D. Spilling, null Stéphane Canaan, null Jean‐François Cavalier, and null Gerlind Sulzenbacher

Published

2022

10. Molecular basis for substrate recognition and septum cleavage by AtlA, the major N-acetylglucosaminidase of Enterococcus faecalis

Author

Véronique Roig-Zamboni, Sarah Barelier, Robert Dixon, Nicola F. Galley, Amani Ghanem, Quoc Phong Nguyen, Héloize Cahuzac, Bartłomiej Salamaga, Peter J. Davis, Yves Bourne, Stéphane Mesnage, Florence Vincent, Centre National de la Recherche Scientifique (CNRS), Architecture et fonction des macromolécules biologiques (AFMB), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), University of Sheffield [Sheffield], Royal Society (to S. M. and F. V.) (grant no.: IEC∖R2∖170260)., and University of Sheffield

Subjects

structure–function, crystal structure, [SDV.BBM.BS]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Structural Biology [q-bio.BM], [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, Cell Biology, Peptidoglycan, Biochemistry, [SDV.BBM.BP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biophysics, Bacterial Proteins, Acetylglucosaminidase, Enterococcus faecalis, cell wall, Animals, glycoside hydrolase, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Molecular Biology, ComputingMilieux_MISCELLANEOUS, Enterococcus, Zebrafish

Abstract

International audience; The cleavage of septal peptidoglycan at the end of cell division facilitates the separation of the two daughter cells. The hydrolases involved in this process (called autolysins) are potentially lethal enzymes that can cause cell death; their activity, therefore, must be tightly controlled during cell growth. In Enterococcus faecalis, the N-acetylglucosaminidase AtlA plays a predominant role in cell separation. atlA mutants form long cell chains and are significantly less virulent in the zebrafish model of infection. The attenuated virulence of atlA mutants is underpinned by a limited dissemination of bacterial chains in the host organism and a more efficient uptake by phagocytes that clear the infection. AtlA has structural homologs in other important pathogens, such as Listeria monocytogenes and Salmonella typhimurium, and therefore represents an attractive model to design new inhibitors of bacterial pathogenesis. Here, we provide a 1.45 Å crystal structure of the E. faecalis AtlA catalytic domain that reveals a closed conformation of a conserved β-hairpin and a complex network of hydrogen bonds that bring two catalytic residues to the ideal distance for an inverting mechanism. Based on the model of the AtlA–substrate complex, we identify key residues critical for substrate recognition and septum cleavage during bacterial growth. We propose that this work will provide useful information for the rational design of specific inhibitors targeting this enterococcal virulence factor and its orthologs in other pathogens.

Published

2022

11. Substrate Deconstruction and the Nonadditivity of Enzyme Recognition

Author

Jennifer A. Cummings, Steven C. Almo, Brian K. Shoichet, Alissa M. Rauwerdink, Jeremiah D. Farelli, Frank M. Raushel, Sarah Barelier, Karen N. Allen, and Daniel S. Hitchcock

Subjects

Models, Molecular, chemistry.chemical_classification, Molecular Structure, Chemistry, Stereochemistry, Small Molecule Libraries, Substrate (chemistry), General Chemistry, Crystallography, X-Ray, Biochemistry, Article, Catalysis, Enzymes, Structure-Activity Relationship, Colloid and Surface Chemistry, Enzyme, Atomic resolution, Hydrolase, Structure–activity relationship, Molecule, Enzyme Inhibitors, Function (biology)

Abstract

Predicting substrates for enzymes of unknown function is a major postgenomic challenge. Substrate discovery, like inhibitor discovery, is constrained by our ability to explore chemotypes; it would be expanded by orders of magnitude if reactive sites could be probed with fragments rather than fully elaborated substrates, as is done for inhibitor discovery. To explore the feasibility of this approach, substrates of six enzymes from three different superfamilies were deconstructed into 41 overlapping fragments that were tested for activity or binding. Surprisingly, even those fragments containing the key reactive group had little activity, and most fragments did not bind measurably, until they captured most of the substrate features. Removing a single atom from a recognized substrate could often reduce catalytic recognition by 6 log-orders. To explore recognition at atomic resolution, the structures of three fragment complexes of the β-lactamase substrate cephalothin were determined by X-ray crystallography. Substrate discovery may be difficult to reduce to the fragment level, with implications for function discovery and for the tolerance of enzymes to metabolite promiscuity. Pragmatically, this study supports the development of libraries of fully elaborated metabolites as probes for enzyme function, which currently do not exist.

Published

2014

12. Fragment-guided design of subnanomolar β-lactamase inhibitors active in vivo

Author

Oliv Eidam, Sarah Barelier, Emilia Caselli, Brian K. Shoichet, Chiara Romagnoli, Fabio Prati, Guillaume Dalmasso, R. Bonnet, University of California [San Francisco] (UCSF), University of California, Università degli Studi di Modena e Reggio Emilia (UNIMORE), Microbes, Intestin, Inflammation et Susceptibilité de l'Hôte (M2iSH), Institut National de la Recherche Agronomique (INRA)-Université d'Auvergne - Clermont-Ferrand I (UdA), CHU Clermont-Ferrand, National Institutes of Health [GM63815], Institut National de la Sante et de la Recherche Medicale, Institut National de la Recherche Agronomique, University of California [San Francisco] (UC San Francisco), University of California (UC), and Università degli Studi di Modena e Reggio Emilia = University of Modena and Reggio Emilia (UNIMORE)

Subjects

Models, Molecular, antibiotic resistance, Cefotaxime, [SDV]Life Sciences [q-bio], medicine.disease_cause, 01 natural sciences, chemistry.chemical_compound, X-Ray Diffraction, Models, ENZYME-INHIBITORS, Enzyme Inhibitors, TRANSITION-STATE ANALOG, 0303 health sciences, Multidisciplinary, Drug discovery, BORONIC ACIDS, Biological Sciences, Anti-Bacterial Agents, structure-based, Infectious Diseases, 5.1 Pharmaceuticals, HOT-SPOTS, STRUCTURE-BASED OPTIMIZATION, Development of treatments and therapeutic interventions, Infection, beta-Lactamase Inhibitors, medicine.drug, Clearance, Stereochemistry, BACTERIAL-RESISTANCE, Microbial Sensitivity Tests, Biology, BINDING-SITES, drug discovery, antimicrobial, CHEMICAL UNIVERSE, 03 medical and health sciences, β lactamase inhibitor, In vivo, medicine, Derivatization, Escherichia coli, 030304 developmental biology, Bacteria, 010405 organic chemistry, Fragment (computer graphics), Molecular, 0104 chemical sciences, VIRTUAL EXPLORATION, chemistry, Drug Design, structure-based boronic acid

Abstract

Fragment-based design was used to guide derivatization of a lead series of β-lactamase inhibitors that had heretofore resisted optimization for in vivo activity. X-ray structures of fragments overlaid with the lead suggested new, unanticipated functionality and points of attachment. Synthesis of three derivatives improved affinity over 20-fold and improved efficacy in cell culture. Crystal structures were consistent with the fragment-based design, enabling further optimization to a K i of 50 pM, a 500-fold improvement that required the synthesis of only six derivatives. One of these, compound 5 , was tested in mice. Whereas cefotaxime alone failed to cure mice infected with β-lactamase-expressing Escherichia coli , 65% were cleared of infection when treated with a cefotaxime: 5 combination. Fragment complexes offer a path around design hurdles, even for advanced molecules; the series described here may provide leads to overcome β-lactamase-based resistance, a key clinical challenge.

Published

2012

13. Aspartate 458 of human glutathione synthetase is important for cooperativity and active site structure

Author

Amanda Crutchfield, Mary E. Anderson, Michael L. Drummond, Sarah Barelier, Teresa Brown, Thomas R. Cundari, Kerri D. Slavens, Adriana Dinescu, Stress Cellulaire, Université de la Méditerranée - Aix-Marseille 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire Chimie Provence (LCP), and Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

genetic structures, Molecular Sequence Data, Allosteric regulation, Biophysics, MESH: Catalytic Domain, MESH: Protein Structure, Secondary, Cooperativity, MESH: Amino Acid Sequence, MESH: Allosteric Regulation, MESH: Aspartic Acid, Biochemistry, Catalysis, Glutathione Synthase, Protein Structure, Secondary, Article, chemistry.chemical_compound, Allosteric Regulation, Catalytic Domain, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Amino Acid Sequence, Molecular Biology, MESH: Glutathione Synthase, Alanine, Aspartic Acid, MESH: Humans, MESH: Molecular Sequence Data, biology, Chemistry, Active site, Cooperative binding, Cell Biology, Glutathione, MESH: Catalysis, Glutathione synthase, Glutathione synthetase, biology.protein

Abstract

International audience; Human glutathione synthetase (hGS) catalyzes the second ATP-dependent step in the biosynthesis of glutathione (GSH) and is negatively cooperative to the γ-glutamyl substrate. The hGS active site is composed of three highly conserved catalytic loops, notably the alanine rich A-loop. Experimental and computational investigations of the impact of mutation of Asp458 are reported, and thus the role of this A-loop residue on hGS structure, activity, negativity cooperativity and stability is defined. Several Asp458 hGS mutants (D458A, D458N and D458R) were constructed using site-directed mutagenesis and their activities determined (10%, 15% and 7% of wild-type hGS, respectively). The Michaelis-Menten constant (K(m)) was determined for all three substrates (glycine, GAB and ATP): glycine K(m) increased by 30-115-fold, GAB K(m) decreased by 8-17-fold, and the ATP K(m) was unchanged. All Asp458 mutants display a change in cooperativity from negative cooperativity to non-cooperative. All mutants show similar stability as compared to wild-type hGS, as determined by differential scanning calorimetry. The findings indicate that Asp458 is essential for hGS catalysis and that it impacts the allostery of hGS.

Published

2011

14. Tumor Protein 53–Induced Nuclear Protein 1 Is a Major Mediator of p53 Antioxidant Function

Author

Marcel Culcasi, Carla E. Cano, Juan L. Iovanna, Sylvia Pietri, Sarah Barelier, Nelson Dusetti, Julien Gommeaux, Marie-Josèphe Pébusque, Sophie Vasseur, Rose P. Spoto, Mylène Seux, Stéphane Garcia, Alice Carrier, Stress Cellulaire, Université de la Méditerranée - Aix-Marseille 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire Chimie Provence (LCP), Centre National de la Recherche Scientifique (CNRS)-Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC), Institut National de la Sante´ et de la Recherche Me´dicale, CentreNational de la Recherche Scientifique, Institut National du Cancer, and La LigueNationale Contre le Cancer. C.E. Cano and J. Gommeaux were supported by La LigueNationale Contre le Cancer and the Association pour la Recherche sur le Cancer., CARRIER, Alice, and Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Cancer Research, Cell cycle checkpoint, Lymphoma, Transcription, Genetic, Tumor suppressor gene, [SDV]Life Sciences [q-bio], Cell Growth Processes, Oxidative phosphorylation, Biology, medicine.disease_cause, Cell Line, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Nuclear protein, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Cell growth, Nuclear Proteins, Hydrogen Peroxide, Fibroblasts, Cell biology, [SDV] Life Sciences [q-bio], Oxidative Stress, Oncology, 030220 oncology & carcinogenesis, Cancer research, Phosphorylation, Tumor Suppressor Protein p53, Reactive Oxygen Species, Intracellular, Oxidative stress

Abstract

p53 exerts its tumor suppressor function mainly through transcriptional induction of target genes involved in several processes, including cell cycle checkpoints, apoptosis, and regulation of cell redox status. p53 antioxidant function is dependent on its transcriptional activity and proceeds by sequential induction of antioxidant and proapoptotic targets. However, none of the thus far renowned p53 targets have proved able to abolish on their own the intracellular reactive oxygen species (ROS) accumulation caused by p53 deficiency, therefore pointing to the existence of other prominent and yet unknown p53 antioxidant targets. Here, we show that TP53INP1 represents such a target. Indeed, TP53INP1 transcript induction on oxidative stress is strictly dependent on p53. Mouse embryonic fibroblasts (MEF) and splenocytes derived from TP53INP1-deficient (inp1−/−) mice accumulate intracellular ROS, whereas overexpression of TP53INP1 in p53-deficient MEFs rescues ROS levels to those of p53-proficient cells, indicating that TP53INP1 antioxidant function is p53 independent. Furthermore, accumulation of ROS in inp1−/− cells on oxidant challenge is associated with decreased expression of p53 targets p21/Cdkn1a, Sesn2, TAp73, Puma, and Bax. Mutation of p53 Ser58 (equivalent to human p53 Ser46) abrogates transcription of these genes, indicating that TP53INP1-mediated p53 Ser58 phosphorylation is implicated in this process. In addition, TP53INP1 deficiency results in an antioxidant (N-acetylcysteine)-sensitive acceleration of cell proliferation. Finally, TP53INP1 deficiency increases oxidative stress–related lymphoma incidence and decreases survival of p53+/− mice. In conclusion, our data show that TP53INP1 is a major actor of p53-driven oxidative stress response that possesses both a p53-independent intracellular ROS regulatory function and a p53-dependent transcription regulatory function. [Cancer Res 2009;69(1):219–26]

Published

2008

15. Roles for ordered and bulk solvent in ligand recognition and docking in two related cavities

Author

Inbar Fish, Sarah Barelier, David B. Goodin, S.E. Boyce, Marcus Fischer, and Brian K. Shoichet

Subjects

Models, Molecular, Protein Conformation, Biophysics, lcsh:Medicine, Crystal structure, Ligands, Biochemistry, Biophysics Simulations, Computational Chemistry, Protein structure, Drug Discovery, Biochemical Simulations, Molecule, Biomacromolecule-Ligand Interactions, Biochemistry Simulations, lcsh:Science, Biology, Crystallography, Multidisciplinary, Cytochrome c peroxidase, Chemistry, lcsh:R, Solvation, Computational Biology, Water, Empirical Methods, Cytochrome-c Peroxidase, Ligand (biochemistry), Affinities, Small Molecules, Docking (molecular), Solvents, Biophysic Al Simulations, lcsh:Q, Medicinal Chemistry, Research Article, Protein Binding

Abstract

A key challenge in structure-based discovery is accounting for modulation of protein-ligand interactions by ordered and bulk solvent. To investigate this, we compared ligand binding to a buried cavity in Cytochrome c Peroxidase (CcP), where affinity is dominated by a single ionic interaction, versus a cavity variant partly opened to solvent by loop deletion. This opening had unexpected effects on ligand orientation, affinity, and ordered water structure. Some ligands lost over ten-fold in affinity and reoriented in the cavity, while others retained their geometries, formed new interactions with water networks, and improved affinity. To test our ability to discover new ligands against this opened site prospectively, a 534,000 fragment library was docked against the open cavity using two models of ligand solvation. Using an older solvation model that prioritized many neutral molecules, three such uncharged docking hits were tested, none of which was observed to bind; these molecules were not highly ranked by the new, context-dependent solvation score. Using this new method, another 15 highly-ranked molecules were tested for binding. In contrast to the previous result, 14 of these bound detectably, with affinities ranging from 8 µM to 2 mM. In crystal structures, four of these new ligands superposed well with the docking predictions but two did not, reflecting unanticipated interactions with newly ordered waters molecules. Comparing recognition between this open cavity and its buried analog begins to isolate the roles of ordered solvent in a system that lends itself readily to prospective testing and that may be broadly useful to the community.

Published

2013

16. Probing hot spots on protein-protein interfaces using fragment-based drug design

Author

Sarah Barelier, Isabelle Krimm, Bussy, Agnès, Institut des Sciences Analytiques (ISA), Institut de Chimie du CNRS (INC)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), Criblage de fragment, and Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC)-Université Claude Bernard Lyon 1 (UCBL)

Subjects

[CHIM.ANAL] Chemical Sciences/Analytical chemistry, [CHIM.ANAL]Chemical Sciences/Analytical chemistry, education, health care economics and organizations

Abstract

communication par affiche; International audience; Probing hot spots on protein-protein interfaces using Fragment-Based Drug Design

Published

2012

17. Ligand specificity, privileged substructures and protein druggability from fragment-based screening

Author

Isabelle Krimm, Sarah Barelier, Criblage de fragment, Institut des Sciences Analytiques (ISA), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL), and Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

MAXIMAL AFFINITY, BCL-2 FAMILY, Stereochemistry, INHIBITOR DISCOVERY, Fragment-based lead discovery, Druggability, Computational biology, Ligands, Sensitivity and Specificity, 01 natural sciences, Biochemistry, BINDING-SITES, Analytical Chemistry, Small Molecule Libraries, Structure-Activity Relationship, 03 medical and health sciences, MOLECULES, Fragment (logic), DESIGN, ANTAGONISTS, [CHIM.ANAL]Chemical Sciences/Analytical chemistry, Humans, Structure–activity relationship, Organic Chemicals, Binding site, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], PHARMACOLOGY, 030304 developmental biology, 0303 health sciences, Binding Sites, 010405 organic chemistry, Drug discovery, Chemistry, Ligand, Proteins, NMR, 0104 chemical sciences, DRUG DISCOVERY, Protein Binding

Abstract

International audience; Fragment-based screening has now become an established method for the generation of lead molecules against therapeutic targets. Fragment molecules are simple, low molecular-weight compounds with few chemical functionalities. These characteristics lead to high hit rates for fragment screening as compared to the more classical High-Throughput Screening of drug-like molecules and raise the question of the specificity of fragment molecules. This review analyzes recent outcomes of fragment screenings published in the literature, showing that the specificity of the fragments can be related to their structures and physico-chemical properties. We also discuss both the concept of privileged fragment scaffolds and the role of fragment-based screening in predicting protein druggability, highlighted by recent publications in the field.

Published

2011

18. The Role of the Glycine Triad In Human Glutathione Synthetase

Author

Thomas R. Cundari, Mary E. Anderson, Teresa Brown, Sarah Barelier, Adriana Dinescu, Stress Cellulaire, Université de la Méditerranée - Aix-Marseille 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire Chimie Provence (LCP), and Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Protein Conformation, Mutant, Biophysics, Glycine, Biochemistry, Article, Glutathione Synthase, chemistry.chemical_compound, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Amino Acid Sequence, Molecular Biology, chemistry.chemical_classification, biology, Chemistry, Cooperative binding, Active site, Cell Biology, Glutathione, Glutathione synthase, Molecular biology, Glutathione synthetase, Enzyme, Mutation, biology.protein

Abstract

Experimental kinetics and computational modeling of human glutathione synthetase (hGS) support the significant role of the G-loop glycine triad (G369, G370, G371) for activity of this ATP-grasp enzyme. Enzyme kinetic experiments indicate that G369V and G370V mutant hGS have little activity (

Published

2010

19. Ligand specificity in fragment-based drug design

Author

Isabelle Krimm, Kalle Gehring, Sarah Barelier, Julien Pons, and Jean-Marc Lancelin

Subjects

Magnetic Resonance Spectroscopy, Druggability, Ligands, Structure-Activity Relationship, Drug Discovery, medicine, Molecule, Humans, Serum Albumin, Chemistry, Ligand, Nuclear magnetic resonance spectroscopy, Peroxiredoxins, Protein superfamily, Human serum albumin, Biochemistry, Pharmaceutical Preparations, Proto-Oncogene Proteins c-bcl-2, Solubility, Drug Design, Molecular Medicine, Peroxiredoxin, Hydrophobic and Hydrophilic Interactions, Macromolecule, medicine.drug, Protein Binding

Abstract

Fragment-based drug design consists of identifying low-molecular weight compounds that weakly bind to a target macromolecule and will then be modified or linked to yield potent inhibitors. The specificity of these low-complexity and low-affinity molecules has rarely been discussed in the literature. To address this question, NMR spectroscopy was used to investigate the interactions of 150 fragments with five proteins: three proteins from the Bcl-2 family (Bcl-x(L), Bcl-w, and Mcl-1), human peroxiredoxin 5, for which very few ligands have been reported, and human serum albumin, which is known to bind a large number of ligands. Our results show that the fragments are rather versatile binders and able to identify binding hot spots in very different targets. Despite the different hit rates observed related to the druggability of the proteins, two scaffolds appear as preferred binders for all proteins. Low specificity was observed between homologous proteins or unrelated poorly druggable proteins, while higher specificity could be achieved with highly druggable targets.

Published

2010

20. Fragment-Based Deconstruction of Bcl-xL Inhibitors

Author

Isabelle Krimm, Olivier Marcillat, Jean-Marc Lancelin, Sarah Barelier, Julien Pons, Stress Cellulaire, Université de la Méditerranée - Aix-Marseille 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire Chimie Provence (LCP), Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Institut de Chimie et Biochimie Moléculaires et Supramoléculaires (ICBMS), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-École Supérieure de Chimie Physique Électronique de Lyon (CPE)-Institut National des Sciences Appliquées de Lyon (INSA Lyon), Université de Lyon-Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Sciences Analytiques (SA), Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Criblage de fragment, Institut des Sciences Analytiques (ISA), and Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL)

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Stereochemistry, Bioactive molecules, bcl-X Protein, Bcl-xL, [CHIM.THER]Chemical Sciences/Medicinal Chemistry, Ligands, Binding, Competitive, Structure-Activity Relationship, Fragment (logic), Drug Discovery, Humans, Molecule, Organic Chemicals, Binding site, Binding Sites, Molecular Structure, biology, Chemistry, Recombinant Proteins, Protein Structure, Tertiary, Molecular Weight, Antiapoptotic protein, Drug Design, biology.protein, Molecular Medicine, Protein Binding

Abstract

Fragment-based drug design consists of screening low-molecular-weight compounds in order to identify low-affinity ligands that are then modified or linked to yield potent inhibitors. The method thus attempts to build bioactive molecules in a modular way and relies on the hypothesis that the fragment binding mode will be conserved upon elaboration of the active molecule. If the inverse process is considered, do the fragments resulting from the deconstruction of high-affinity inhibitors recapitulate their binding mode in the large molecule? Few studies deal with this issue. Here, we report the analysis of 22 fragments resulting from the dissection of 9 inhibitors of the antiapoptotic protein Bcl-x(L). To determine if the fragments retained affinity toward the protein and identify their binding site, ligand-observed and protein-observed NMR experiments were used. The analysis of the fragments behavior illustrates the complexity of low-affinity protein-ligand interactions involved in the fragment-based construction of bioactive molecules.

Published

2010

21. Discovery of Fragment Molecules That Bind the Human Peroxiredoxin 5 Active Site

Author

Isabelle Krimm, Sarah Barelier, Dominique Linard, Bernard Knoops, André Clippe, Jean-Marc Lancelin, Julien Pons, Stress Cellulaire, Université de la Méditerranée - Aix-Marseille 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire Chimie Provence (LCP), Université de Provence - Aix-Marseille 1-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Laboratoire de Biologie Cellulaire, Université Catholique de Louvain = Catholic University of Louvain (UCL)-Institut des Sciences de la Vie, Criblage de fragment, Institut des Sciences Analytiques (ISA), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL), and Université de Lyon-Université de Lyon-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Protein Conformation, lcsh:Medicine, [CHIM.THER]Chemical Sciences/Medicinal Chemistry, Crystallography, X-Ray, Ligands, Protein structure, Catalytic Domain, Humans, Cysteine, Binding site, lcsh:Science, Biochemistry/Biomacromolecule-Ligand Interactions, Multidisciplinary, Binding Sites, biology, Chemistry, lcsh:R, Active site, Peroxiredoxins, respiratory system, Small molecule, Enzyme structure, Kinetics, Biochemistry, Models, Chemical, Peroxidases, Biochemistry/Bioinformatics, Docking (molecular), biology.protein, lcsh:Q, Biochemistry/Drug Discovery, Peroxiredoxin, Protein ligand, Protein Binding, Research Article

Abstract

The search for protein ligands is a crucial step in the inhibitor design process. Fragment screening represents an interesting method to rapidly find lead molecules, as it enables the exploration of a larger portion of the chemical space with a smaller number of compounds as compared to screening based on drug-sized molecules. Moreover, fragment screening usually leads to hit molecules that form few but optimal interactions with the target, thus displaying high ligand efficiencies. Here we report the screening of a homemade library composed of 200 highly diverse fragments against the human Peroxiredoxin 5 protein. Peroxiredoxins compose a family of peroxidases that share the ability to reduce peroxides through a conserved cysteine. The three-dimensional structures of these enzymes ubiquitously found throughout evolution have been extensively studied, however, their biological functions are still not well understood and to date few inhibitors have been discovered against these enzymes. Six fragments from the library were shown to bind to the Peroxiredoxin 5 active site and ligand-induced chemical shift changes were used to drive the docking of these small molecules into the protein structure. The orientation of the fragments in the binding pocket was confirmed by the study of fragment homologues, highlighting the role of hydroxyl functions that hang the ligands to the Peroxiredoxin 5 protein. Among the hit fragments, the small catechol molecule was shown to significantly inhibit Peroxiredoxin 5 activity in a thioredoxin peroxidase assay. This study reports novel data about the ligand-Peroxiredoxin interactions that will help considerably the development of potential Peroxiredoxin inhibitors.

Published

2010

22. C‐Terminal Residues of Glutathione Synthetase

Author

Mary E. Anderson, Thomas R. Cundari, Adriana Dinescu, Teresa Brown, and Sarah Barelier

Subjects

GPX1, GPX3, Biochemistry, Terminal (electronics), Chemistry, Genetics, Molecular Biology, GPX6, Glutathione synthetase, Biotechnology

Published

2008

23. Ligand Specificity in Fragment-Based Drug Design.

Author

Sarah Barelier, Julien Pons, Kalle Gehring, Jean-Marc Lancelin, and Isabelle Krimm

Subjects

*LIGANDS (Biochemistry), *DRUG design, *FRAGMENTATION reactions, *DRUG synergism, *NUCLEAR magnetic resonance spectroscopy, *PROTEIN-protein interactions

Abstract

Fragment-based drug design consists of identifying low-molecular weight compounds that weakly bind to a target macromolecule and will then be modified or linked to yield potent inhibitors. The specificity of these low-complexity and low-affinity molecules has rarely been discussed in the literature. To address this question, NMR spectroscopy was used to investigate the interactions of 150 fragments with five proteins: three proteins from the Bcl-2 family (Bcl-xL, Bcl-w, and Mcl-1), human peroxiredoxin 5, for which very few ligands have been reported, and human serum albumin, which is known to bind a large number of ligands. Our results show that the fragments are rather versatile binders and able to identify binding hot spots in very different targets. Despite the different hit rates observed related to the druggability of the proteins, two scaffolds appear as preferred binders for all proteins. Low specificity was observed between homologous proteins or unrelated poorly druggable proteins, while higher specificity could be achieved with highly druggable targets. [ABSTRACT FROM AUTHOR]

Published

2010

24. Lineage-Specific Viral Hijacking of Non-canonical E3 Ubiquitin Ligase Cofactors in the Evolution of Vif Anti-APOBEC3 Activity

Author

Ming Li, Valgerður Andrésdóttir, Reuben S. Harris, John D. Gross, Billy W. Newton, Kathleen Franks-Skiba, Joshua Kane, Jeffrey R. Johnson, Sarah Barelier, Stefán R. Jónsson, James S. Fraser, Nevan J. Krogan, William L. Brown, Jennifer M. Binning, Judd F. Hultquist, Adalbjorg Adalbjornsdóttir, Hörður Ingi Gunnarsson, Tasha L. Johnson, David J. Stanley, and Nicole Mietrach

Subjects

Gene Products, vif, Ubiquitin-Protein Ligases, viruses, Cypa, Plasma protein binding, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Article, Cytosine Deaminase, Cyclophilin A, Cytidine Deaminase, medicine, Animals, Humans, APOBEC Deaminases, lcsh:QH301-705.5, Sheep, biology, virus diseases, Cytidine deaminase, Simian immunodeficiency virus, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Virology, 3. Good health, Ubiquitin ligase, lcsh:Biology (General), Lentivirus, biology.protein, HIV-1, Protein Binding

Abstract

SummaryHIV-1 encodes the accessory protein Vif, which hijacks a host Cullin-RING ubiquitin ligase (CRL) complex as well as the non-canonical cofactor CBFβ, to antagonize APOBEC3 antiviral proteins. Non-canonical cofactor recruitment to CRL complexes by viral factors, to date, has only been attributed to HIV-1 Vif. To further study this phenomenon, we employed a comparative approach combining proteomic, biochemical, structural, and virological techniques to investigate Vif complexes across the lentivirus genus, including primate (HIV-1 and simian immunodeficiency virus macaque [SIVmac]) and non-primate (FIV, BIV, and MVV) viruses. We find that CBFβ is completely dispensable for the activity of non-primate lentiviral Vif proteins. Furthermore, we find that BIV Vif requires no cofactor and that MVV Vif requires a novel cofactor, cyclophilin A (CYPA), for stable CRL complex formation and anti-APOBEC3 activity. We propose modular conservation of Vif complexes allows for potential exaptation of functions through the acquisition of non-CRL-associated host cofactors while preserving anti-APOBEC3 activity.