Your search keyword '"Bzymek KP"' showing total 24 results

1. Enhancing the Prefusion Conformational Stability of SARS-CoV-2 Spike Protein Through Structure-Guided Design.

Author

Riley TP, Chou HT, Hu R, Bzymek KP, Correia AR, Partin AC, Li D, Gong D, Wang Z, Yu X, Manzanillo P, and Garces F

Subjects

Angiotensin-Converting Enzyme 2 metabolism, Antibodies, Neutralizing immunology, Antibodies, Viral immunology, Binding Sites genetics, Binding Sites immunology, COVID-19 immunology, COVID-19 pathology, Cell Line, HEK293 Cells, Humans, Protein Domains genetics, Protein Domains immunology, Protein Stability, SARS-CoV-2 genetics, Protein Interaction Domains and Motifs genetics, Protein Interaction Domains and Motifs immunology, SARS-CoV-2 immunology, Spike Glycoprotein, Coronavirus genetics, Spike Glycoprotein, Coronavirus immunology

Abstract

The worldwide pandemic caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is unprecedented and the impact on public health and the global economy continues to be devastating. Although early therapies such as prophylactic antibodies and vaccines show great promise, there are concerns about the long-term efficacy and universal applicability of these therapies as the virus continues to mutate. Thus, protein-based immunogens that can quickly respond to viral changes remain of continued interest. The Spike protein, the main immunogen of this virus, displays a highly dynamic trimeric structure that presents a challenge for therapeutic development. Here, guided by the structure of the Spike trimer, we rationally design new Spike constructs that show a uniquely high stability profile while simultaneously remaining locked into the immunogen-desirable prefusion state. Furthermore, our approach emphasizes the relationship between the highly conserved S2 region and structurally dynamic Receptor Binding Domains (RBD) to enable vaccine development as well as the generation of antibodies able to resist viral mutation., Competing Interests: Authors TPR, H-TC, RH, KPB, ARC, ACP, DL, DG, ZW, XY, PM, and FG were employed by Amgen Inc., (Copyright © 2021 Riley, Chou, Hu, Bzymek, Correia, Partin, Li, Gong, Wang, Yu, Manzanillo and Garces.)

Published

2021

2. Rational selection of building blocks for the assembly of bispecific antibodies.

Author

Gong D, Riley TP, Bzymek KP, Correia AR, Li D, Spahr C, Robinson JH, Case RB, Wang Z, and Garces F

Subjects

Antibody Affinity immunology, Chromatography, Gel methods, Chromatography, Ion Exchange methods, Chromatography, Liquid methods, Electrophoresis, Capillary methods, Electrophoresis, Polyacrylamide Gel methods, HEK293 Cells, Humans, Mass Spectrometry methods, Protein Engineering methods, Antibodies, Bispecific immunology, Antibodies, Monoclonal immunology, Immunoglobulin G immunology, Immunoglobulin Heavy Chains immunology, Immunoglobulin Light Chains immunology

Abstract

Bispecific antibodies, engineered to recognize two targets simultaneously, demonstrate exceptional clinical potential for the therapeutic intervention of complex diseases. However, these molecules are often composed of multiple polypeptide chains of differing sequences. To meet industrial scale productivity, enforcing the correct quaternary assembly of these chains is critical. Here, we describe Chain Selectivity Assessment (CSA), a high-throughput method to rationally select parental monoclonal antibodies (mAbs) to make bispecific antibodies requiring correct heavy/light chain pairing. By deploying CSA, we have successfully identified mAbs that exhibit a native preference toward cognate chain pairing that enables the production of hetero-IgGs without additional engineering. Furthermore, CSA also identified rare light chains (LCs) that permit positive binding of the non-cognate arm in the common LC hetero-IgGs, also without engineering. This rational selection of parental mAbs with favorable developability characteristics is critical to the successful development of bispecific molecules with optimal manufacturability properties.

Published

2021

3. Template-Catalyzed, Disulfide Conjugation of Monoclonal Antibodies Using a Natural Amino Acid Tag.

Author

King JD, Ma Y, Kuo YC, Bzymek KP, Goodstein LH, Meyer K, Moore RE, Crow D, Colcher DM, Singh G, Horne DA, and Williams JC

Subjects

Animals, Breast Neoplasms diagnostic imaging, Catalysis, Click Chemistry, Female, Fluorescent Dyes chemistry, Humans, Immunoglobulin Fab Fragments chemistry, MCF-7 Cells, Mice, Models, Molecular, Optical Imaging, Trastuzumab chemistry, Amino Acids chemistry, Antibodies, Monoclonal chemistry, Disulfides chemistry, Immunoconjugates chemistry

Abstract

The high specificity and favorable pharmacological properties of monoclonal antibodies (mAbs) have prompted significant interest in re-engineering this class of molecules to add novel functionalities for enhanced therapeutic and diagnostic potential. Here, we used the high affinity, meditope-Fab interaction to template and drive the rapid, efficient, and stable site-specific formation of a disulfide bond. We demonstrate that this template-catalyzed strategy provides a consistent and reproducible means to conjugate fluorescent dyes, cytotoxins, or "click" chemistry handles to meditope-enabled mAbs (memAbs) and memFabs. More importantly, we demonstrate this covalent functionalization is achievable using natural amino acids only, opening up the opportunity to genetically encode cysteine meditope "tags" to biologics. As proof of principle, genetically encoded, cysteine meditope tags were added to the N- and/or C-termini of fluorescent proteins, nanobodies, and affibodies, each expressed in bacteria, purified to homogeneity, and efficiently conjugated to different memAbs and meFabs. We further show that multiple T-cell and Her2-targeting bispecific molecules using this strategy potently activate T-cell signaling pathways in vitro. Finally, the resulting products are highly stable as evidenced by serum stability assays (>14 d at 37 °C) and in vivo imaging of tumor xenographs. Collectively, the platform offers the opportunity to build and exchange an array of functional moieties, including protein biologics, among any cysteine memAb or Fab to rapidly create, test, and optimize stable, multifunctional biologics.

Published

2018

4. Mechanically interlocked functionalization of monoclonal antibodies.

Author

Bzymek KP, Puckett JW, Zer C, Xie J, Ma Y, King JD, Goodstein LH, Avery KN, Colcher D, Singh G, Horne DA, and Williams JC

Subjects

Animals, Antibodies, Monoclonal immunology, Azides chemistry, Binding Sites, Click Chemistry methods, Female, Mice, Mice, Inbred NOD, Mice, SCID, Protein Binding, Receptor, ErbB-2 immunology, Surface Plasmon Resonance, Antibodies, Monoclonal chemistry, Cetuximab chemistry, Drug Carriers chemistry, Immunoglobulin Fab Fragments chemistry, Trastuzumab chemistry

Abstract

Because monoclonal antibodies (mAbs) have exceptional specificity and favorable pharmacology, substantial efforts have been made to functionalize them, either with potent cytotoxins, biologics, radionuclides, or fluorescent groups for therapeutic benefit and/or use as theranostic agents. To exploit our recently discovered meditope-Fab interaction as an alternative means to efficiently functionalize mAbs, we used insights from the structure to enhance the affinity and lifetime of the interaction by four orders of magnitude. To further extend the lifetime of the complex, we created a mechanical bond by incorporating an azide on the meditope, threading the azide through the Fab, and using click chemistry to add a steric group. The mechanically interlocked, meditope-Fab complex retains antigen specificity and is capable of imaging tumors in mice. These studies indicate it is possible to "snap" functionality onto mAbs, opening the possibility of rapidly creating unique combinations of mAbs with an array of cytotoxins, biologics, and imaging agents.

Published

2018

5. Meditope-Fab interaction: threading the hole.

Author

Bzymek KP, Ma Y, Avery KN, Horne DA, and Williams JC

Subjects

Arginine chemistry, Binding Sites, Cetuximab chemistry, Crystallography, X-Ray, Half-Life, Hydrogen Bonding, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments metabolism, Models, Molecular, Protein Conformation, Static Electricity, Structure-Activity Relationship, Surface Plasmon Resonance, Cetuximab metabolism, Peptides, Cyclic chemistry, Peptides, Cyclic metabolism

Abstract

Meditope, a cyclic 12-residue peptide, binds to a unique binding side between the light and heavy chains of the cetuximab Fab. In an effort to improve the affinity of the interaction, it was sought to extend the side chain of Arg8 in the meditope, a residue that is accessible from the other side of the meditope binding site, in order to increase the number of interactions. These modifications included an n-butyl and n-octyl extension as well as hydroxyl, amine and carboxyl substitutions. The atomic structures of the complexes and the binding kinetics for each modified meditope indicated that each extension threaded through the Fab `hole' and that the carboxyethylarginine substitution makes a favorable interaction with the Fab, increasing the half-life of the complex by threefold compared with the unmodified meditope. Taken together, these studies provide a basis for the design of additional modifications to enhance the overall affinity of this unique interaction.

Published

2017

6. Engineering a high-affinity peptide binding site into the anti-CEA mAb M5A.

Author

Zer C, Avery KN, Meyer K, Goodstein L, Bzymek KP, Singh G, and Williams JC

Subjects

Antibodies, Monoclonal chemistry, Antibodies, Monoclonal immunology, Binding Sites genetics, Carcinoembryonic Antigen chemistry, Carcinoembryonic Antigen metabolism, Cell Line, Humans, Models, Molecular, Peptides chemistry, Protein Binding genetics, Antibodies, Monoclonal genetics, Antibodies, Monoclonal metabolism, Carcinoembryonic Antigen immunology, Peptides genetics, Peptides metabolism, Protein Engineering methods

Abstract

We have previously identified a cyclic peptide called meditope which binds to the central cavity of the Fab portion of cetuximab and shown that this peptide binding site can be grafted, or 'meditope-enabled', onto trastuzumab. This peptide has been shown to act as a hitch for the non-covalent attachment of imaging agents to meditope-enabled antibodies. Herein, we explore the process of grafting this peptide binding site onto M5A, an anti-CEA antibody in clinical trials for cancer diagnostics. In order to explore the contributions of the amino acids, we sequentially introduced pairs of amino acid substitutions into the Fab and then we reverse-substituted key residues in the presence of the other substitutions. We demonstrate that Pro40Thr, Gly41Asn, Phe83Ile and Thr85Asp in the light chain are sufficient to recreate the meditope binding site in M5A with single-digit micromolar affinity. We show that Pro40 abrogates peptide binding in the presence of the other 12 residue substitutions, and that the presence of all 13 substitutions does not interfere with antibody:antigen recognition. Collectively, these studies provide detailed insight for defining and fine-tuning the binding affinity of the meditope binding site within an antibody., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

7. Natural and non-natural amino-acid side-chain substitutions: affinity and diffraction studies of meditope-Fab complexes.

Author

Bzymek KP, Avery KA, Ma Y, Horne DA, and Williams JC

Subjects

Amino Acid Sequence, Amino Acid Substitution, Binding Sites, Cetuximab genetics, Crystallography, X-Ray, Epitopes metabolism, Gene Expression, Immunoglobulin Fab Fragments genetics, Kinetics, Models, Molecular, Peptides immunology, Protein Binding, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins immunology, Antigen-Antibody Complex chemistry, Antineoplastic Agents, Immunological chemistry, Cetuximab chemistry, Epitopes chemistry, Immunoglobulin Fab Fragments chemistry, Peptides chemistry

Abstract

Herein, multiple crystal structures of meditope peptide derivatives incorporating natural and unnatural amino acids bound to the cetuximab Fab domain are presented. The affinity of each derivative was determined by surface plasmon resonance and correlated to the atomic structure. Overall, it was observed that the hydrophobic residues in the meditope peptide, Phe3, Leu5 and Leu10, could accommodate a number of moderate substitutions, but these invariably reduced the overall affinity and half-life of the interaction. In one case, the substitution of Phe3 by histidine led to a change in the rotamer conformation, in which the imidazole ring flipped to a solvent-exposed position. Based on this observation, Phe3 was substituted by diphenylalanine and it was found that the phenyl rings in this variant mimic the superposition of the Phe3 and His3 structures, producing a moderate increase, of 1.4-fold, in the half-life of the complex. In addition, it was observed that substitution of Leu5 by tyrosine and glutamate strongly reduced the affinity, whereas the substitution of Leu5 by diphenylalanine moderately reduced the half-life (by approximately fivefold). Finally, it was observed that substitution of Arg8 and Arg9 by citrulline dramatically reduced the overall affinity, presumably owing to lost electrostatic interactions. Taken together, these studies provide insight into the meditope-cetuximab interaction at the atomic level.

Published

2016

8. The Crystal Structure of Peroxiredoxin Asp f3 Provides Mechanistic Insight into Oxidative Stress Resistance and Virulence of Aspergillus fumigatus.

Author

Hillmann F, Bagramyan K, Straßburger M, Heinekamp T, Hong TB, Bzymek KP, Williams JC, Brakhage AA, and Kalkum M

Subjects

Animals, Aspergillosis microbiology, Crystallography, X-Ray, Female, Gene Deletion, Kinetics, Mice, Models, Molecular, Mutant Proteins chemistry, Mutant Proteins metabolism, Oxidation-Reduction, Peroxidase metabolism, Protein Multimerization, Protein Structure, Secondary, Superoxides toxicity, Virulence, Aspergillus fumigatus metabolism, Aspergillus fumigatus pathogenicity, Fungal Proteins chemistry, Oxidative Stress, Peroxiredoxins chemistry

Abstract

Invasive aspergillosis and other fungal infections occur in immunocompromised individuals, including patients who received blood-building stem cell transplants, patients with chronic granulomatous disease (CGD), and others. Production of reactive oxygen species (ROS) by immune cells, which incidentally is defective in CGD patients, is considered to be a fundamental process in inflammation and antifungal immune response. Here we show that the peroxiredoxin Asp f3 of Aspergillus fumigatus inactivates ROS. We report the crystal structure and the catalytic mechanism of Asp f3, a two-cysteine type peroxiredoxin. The latter exhibits a thioredoxin fold and a homodimeric structure with two intermolecular disulfide bonds in its oxidized state. Replacement of the Asp f3 cysteines with serine residues retained its dimeric structure, but diminished Asp f3's peroxidase activity, and extended the alpha-helix with the former peroxidatic cysteine residue C61 by six residues. The asp f3 deletion mutant was sensitive to ROS, and this phenotype was rescued by ectopic expression of Asp f3. Furthermore, we showed that deletion of asp f3 rendered A. fumigatus avirulent in a mouse model of pulmonary aspergillosis. The conserved expression of Asp f3 homologs in medically relevant molds and yeasts prompts future evaluation of Asp f3 as a potential therapeutic target.

Published

2016

9. Cyclization strategies of meditopes: affinity and diffraction studies of meditope-Fab complexes.

Author

Bzymek KP, Ma Y, Avery KA, Horne DA, and Williams JC

Subjects

Crystallography, X-Ray, Cyclization, Protein Conformation, Surface Plasmon Resonance, Immunoglobulin Fab Fragments chemistry

Abstract

Recently, a unique binding site for a cyclic 12-residue peptide was discovered within a cavity formed by the light and heavy chains of the cetuximab Fab domain. In order to better understand the interactions that drive this unique complex, a number of variants including the residues within the meditope peptide and the antibody, as well as the cyclization region of the meditope peptide, were created. Here, multiple crystal structures of meditope peptides incorporating different cyclization strategies bound to the central cavity of the cetuximab Fab domain are presented. The affinity of each cyclic derivative for the Fab was determined by surface plasmon resonance and correlated to structural differences. Overall, it was observed that the disulfide bond used to cyclize the peptide favorably packs against a hydrophobic `pocket' and that amidation and acetylation of the original disulfide meditope increased the overall affinity ∼2.3-fold. Conversely, replacing the terminal cysteines with serines and thus creating a linear peptide reduced the affinity over 50-fold, with much of this difference being reflected in a decrease in the on-rate. Other cyclization methods, including the formation of a lactam, reduced the affinity but not to the extent of the linear peptide. Collectively, the structural and kinetic data presented here indicate that small perturbations introduced by different cyclization strategies can significantly affect the affinity of the meditope-Fab complex.

Published

2016

10. Observation of an E2 (Ubc9)-homodimer by crystallography.

Author

Alontaga AY, Ambaye ND, Li YJ, Vega R, Chen CH, Bzymek KP, Williams JC, Hu W, and Chen Y

Abstract

Post-translational modifications by the small ubiquitin-like modifiers (SUMO), in particular the formation of poly-SUMO-2 and -3 chains, regulates essential cellular functions and its aberration leads to life-threatening diseases (Geoffroy and Hay, 2009) [1]. It was shown previously that the non-covalent interaction between SUMO and the conjugating enzyme (E2) for SUMO, known as Ubc9, is required for poly-SUMO-2/3 chain formation (Knipscheer et al., 2007) [2]. However, the structure of SUMO-Ubc9 non-covalent complex, by itself, could not explain how the poly-SUMO-2/3 chain forms and consequently a Ubc9 homodimer, although never been observed, was proposed for poly-SUMO-2/3 chain formation (Knipscheer et al., 2007) [2]. Here, we solved the crystal structure of a heterotrimer containing a homodimer of Ubc9 and the RWD domain from RWDD3. The asymmetric Ubc9 homodimer is mediated by the N-terminal region of one Ubc9 molecule and a surface near the catalytic Cys of the second Ubc9 molecule (Fig. 1A). This N-terminal surface of Ubc9 that is involved in the homodimer formation also interacts with the RWD domain, the ubiquitin-fold domain of the SUMO activating enzyme (E1), SUMO, and the E3 ligase, RanBP2 (Knipscheer et al., 2007; Tong et al.. 1997; Tatham et al., 2005; Reverter and Lima, 2005; Capili and Lima, 2007; Wang et al., 2009, 2010; Wang and Chen, 2010; Alontaga et al., 2015) [2], [3], [4], [5], [6], [7], [8], [9], [10]. The existence of the Ubc9 homodimer in solution is supported by previously published solution NMR studies of rotational correlation time and chemical shift perturbation (Alontaga et al., 2015; Yuan et al., 1999) [10], [11]. Site-directed mutagenesis and biochemical analysis suggests that this dimeric arrangement of Ubc9 is likely important for poly-SUMO chain formation (Fig. 1B and C). The asymmetric Ubc9 homodimer described for the first time in this work could provide the critical missing link in the poly-SUMO chain formation mechanism. The data presented here are related to the research article entitled, "RWD domain as an E2 (Ubc9) interaction module" (Alontaga et al., 2015) [10]. The data of the crystal structure has been deposited to RCSB protein data bank with identifier: 4Y1L.

Published

2016

11. RWD Domain as an E2 (Ubc9)-Interaction Module.

Author

Alontaga AY, Ambaye ND, Li YJ, Vega R, Chen CH, Bzymek KP, Williams JC, Hu W, and Chen Y

Subjects

Crystallography, X-Ray, Humans, Kinetics, Models, Molecular, Protein Binding, Protein Structure, Tertiary, SUMO-1 Protein chemistry, SUMO-1 Protein genetics, SUMO-1 Protein metabolism, Sumoylation, Ubiquitin-Conjugating Enzymes genetics, Ubiquitin-Protein Ligases chemistry, Ubiquitin-Protein Ligases genetics, Ubiquitin-Protein Ligases metabolism, Ubiquitin-Conjugating Enzymes chemistry, Ubiquitin-Conjugating Enzymes metabolism

Abstract

An RWD domain is a well conserved domain found through bioinformatic analysis of the human proteome sequence; however, its function has been unknown. Ubiquitin-like modifications require the catalysis of three enzymes generally known as E1, E2, and E3. We solved the crystal structure of the E2 for the small ubiquitin-like modifiers (SUMO) in complex with an RWD domain and confirmed the structure using solution NMR analysis. The binding surface of RWD on Ubc9 is located near the N terminus of Ubc9 that is known to be involved in noncovalent binding of the proteins in the conjugation machinery, including a domain of E1, SUMO, and an E3 ligase. NMR data indicate that the RWD domain does not bind to SUMO and E1. The interaction between RWD and Ubc9 has a Kd of 32 ± 4 μM. Consistent with the structure and binding affinity and in contrast to a previous report, the RWD domain and RWDD3 have minimal effects on global SUMOylation. The structural and biochemical information presented here forms the basis for further investigation of the functions of RWD-containing proteins., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

12. Development of a high affinity, non-covalent biologic to add functionality to Fabs.

Author

Avery KN, Zer C, Bzymek KP, and Williams JC

Subjects

Antibodies, Monoclonal genetics, Antibodies, Monoclonal immunology, Binding Sites, Cell Line, Humans, Immunoglobulin Fab Fragments genetics, Immunoglobulin Fab Fragments immunology, Microscopy, Fluorescence, Peptides immunology, Surface Plasmon Resonance, Trastuzumab genetics, Trastuzumab immunology, Antibodies, Monoclonal metabolism, Antibody Affinity physiology, Immunoglobulin Fab Fragments metabolism, Trastuzumab metabolism

Abstract

Functionalization of monoclonal antibodies (mAbs) requires chemical derivatization and/or genetic manipulation. Inherent in these methods are challenges with protein heterogeneity, stability and solubility. Such perturbations could potentially be avoided by using a high affinity, non-covalent intermediate to bridge the desired functionality to a stable mAb. Recently, we engineered a binding site for a peptide named "meditope" within the Fab of trastuzumab. Proximity of the meditope site to that of protein L suggested an opportunity to enhance the meditope's moderate affinity. Joined by a peptide linker, the meditope-protein L construct has a KD ~ 180 pM - a 7000-fold increase in affinity. The construct is highly specific to the engineered trastuzumab, as demonstrated by flow cytometry. Moreover, the fusion of a bulky GFP to this construct did not affect the association with cell surface antigens. Collectively, these data indicate this specific, high affinity construct can be developed to rapidly add new functionality to mAbs.

Published

2015

13. Identification and grafting of a unique peptide-binding site in the Fab framework of monoclonal antibodies.

Author

Donaldson JM, Zer C, Avery KN, Bzymek KP, Horne DA, and Williams JC

Subjects

Amino Acid Sequence, Antibodies, Monoclonal chemistry, Antibodies, Monoclonal genetics, Antibodies, Monoclonal, Humanized chemistry, Antibodies, Monoclonal, Humanized genetics, Antibodies, Monoclonal, Humanized immunology, Binding Sites genetics, Binding Sites immunology, Cell Line, Tumor, Cetuximab, Crystallography, X-Ray, ErbB Receptors immunology, Humans, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments genetics, Microscopy, Fluorescence, Models, Molecular, Molecular Sequence Data, Mutation, Peptides chemistry, Peptides genetics, Protein Binding immunology, Protein Engineering methods, Protein Structure, Tertiary, Receptor, ErbB-2 immunology, Sequence Homology, Amino Acid, Surface Plasmon Resonance, Trastuzumab, Antibodies, Monoclonal immunology, Immunoglobulin Fab Fragments immunology, Peptides immunology

Abstract

Capitalizing on their extraordinary specificity, monoclonal antibodies (mAbs) have become one of the most reengineered classes of biological molecules. A major goal in many of these engineering efforts is to add new functionality to the parental mAb, including the addition of cytotoxins and imaging agents for medical applications. Herein, we present a unique peptide-binding site within the central cavity of the fragment antigen binding framework region of the chimeric, anti-epidermal growth factor receptor mAb cetuximab. We demonstrate through diffraction methods, biophysical studies, and sequence analysis that this peptide, a meditope, has moderate affinity for the Fab, is specific to cetuximab (i.e., does not bind to human IgGs), and has no significant effect on antigen binding. We further demonstrate by diffraction studies and biophysical methods that the meditope binding site can be grafted onto the anti-human epidermal growth factor receptor 2 mAb trastuzumab, and that the antigen binding affinity of the grafted trastuzumab is indistinguishable from the parental mAb. Finally, we demonstrate a bivalent meditope variant binds specifically and stably to antigen-bearing cells only in the presence of the meditope-enabled mAbs. Collectively, this finding and the subsequent characterization and engineering efforts indicate that this unique interface could serve as a noncovalent "linker" for any meditope-enabled mAb with applications in multiple mAb-based technologies including diagnostics, imaging, and therapeutic delivery.

Published

2013

14. Two translation products of Yersinia yscQ assemble to form a complex essential to type III secretion.

Author

Bzymek KP, Hamaoka BY, and Ghosh P

Subjects

Bacterial Proteins metabolism, Escherichia coli genetics, Escherichia coli metabolism, Membrane Proteins metabolism, Models, Molecular, Protein Conformation, Bacterial Proteins chemistry, Membrane Proteins chemistry, Yersinia metabolism

Abstract

The bacterial flagellar C-ring is composed of two essential proteins, FliM and FliN. The smaller protein, FliN, is similar to the C-terminus of the larger protein, FliM, both being composed of SpoA domains. While bacterial type III secretion (T3S) systems encode many proteins in common with the flagellum, they mostly have a single protein in place of FliM and FliN. This protein resembles FliM at its N-terminus and is as large as FliM but is more like FliN at its C-terminal SpoA domain. We have discovered that a FliN-sized cognate indeed exists in the Yersinia T3S system to accompany the FliM-sized cognate. The FliN-sized cognate, YscQ-C, is the product of an internal translation initiation site within the locus encoding the FliM-sized cognate YscQ. Both intact YscQ and YscQ-C were found to be required for T3S, indicating that the internal translation initiation site, which is conserved in some but not all YscQ orthologs, is crucial for function. The crystal structure of YscQ-C revealed a SpoA domain that forms a highly intertwined, domain-swapped homodimer, similar to those observed in FliN and the YscQ ortholog HrcQ(B). A single YscQ-C homodimer associated reversibly with a single molecule of intact YscQ, indicating conformational differences between the SpoA domains of intact YscQ and YscQ-C. A "snap-back" mechanism suggested by the structure can account for this. The 1:2 YscQ-YscQ-C complex is a close mimic of the 1:4 FliM-FliN complex and the likely building block of the putative Yersinia T3S system C-ring.

Published

2012

15. Mycothiol import by Mycobacterium smegmatis and function as a resource for metabolic precursors and energy production.

Author

Bzymek KP, Newton GL, Ta P, and Fahey RC

Subjects

Acetylcysteine chemistry, Acetylcysteine metabolism, Carbon Radioisotopes metabolism, Cysteine chemistry, Glycopeptides chemistry, Inositol chemistry, Inositol Phosphates chemistry, Inositol Phosphates metabolism, Models, Biological, Molecular Structure, Mutation genetics, Mycobacterium smegmatis genetics, Pyruvic Acid chemistry, Pyruvic Acid metabolism, Cysteine metabolism, Glycopeptides metabolism, Inositol metabolism, Mycobacterium smegmatis metabolism

Abstract

Mycothiol ([MSH] AcCys-GlcN-Ins, where Ac is acetyl) is the major thiol produced by Mycobacterium smegmatis and other actinomycetes. Mutants deficient in MshA (strain 49) or MshC (transposon mutant Tn1) of MSH biosynthesis produce no MSH. However, when stationary phase cultures of these mutants were incubated in medium containing MSH, they actively transported it to generate cellular levels of MSH comparable to or greater than the normal content of the wild-type strain. When these MSH-loaded mutants were transferred to MSH-free preconditioned medium, the cellular MSH was catabolized to generate GlcN-Ins and AcCys. The latter was rapidly converted to Cys by a high deacetylase activity assayed in extracts. The Cys could be converted to pyruvate by a cysteine desulfhydrase or used to regenerate MSH in cells with active MshC. Using MSH labeled with [U-(14)C]cysteine or with [6-(3)H]GlcN, it was shown that these residues are catabolized to generate radiolabeled products that are ultimately lost from the cell, indicating extensive catabolism via the glycolytic and Krebs cycle pathways. These findings, coupled with the fact the myo-inositol can serve as a sole carbon source for growth of M. smegmatis, indicate that MSH functions not only as a protective cofactor but also as a reservoir of readily available biosynthetic precursors and energy-generating metabolites potentially important under stress conditions. The half-life of MSH was determined in stationary phase cells to be approximately 50 h in strains with active MshC and 16 +/- 3 h in the MshC-deficient mutant, suggesting that MSH biosynthesis may be a suitable target for drugs to treat dormant tuberculosis.

Published

2007

16. Role of alpha-Asp181, beta-Asp192, and gamma-Asp190 in the distinctive subunits of human NAD-specific isocitrate dehydrogenase.

Author

Bzymek KP and Colman RF

Subjects

Adenosine Diphosphate chemistry, Adenosine Diphosphate metabolism, Asparagine genetics, Aspartic Acid genetics, Catalytic Domain genetics, Humans, Isocitrate Dehydrogenase genetics, Isocitrate Dehydrogenase physiology, Mutagenesis, Site-Directed, NAD genetics, Protein Subunits genetics, Protein Subunits metabolism, Structure-Activity Relationship, Substrate Specificity genetics, Aspartic Acid chemistry, Isocitrate Dehydrogenase chemistry, NAD chemistry, Protein Subunits chemistry

Abstract

Human NAD-dependent isocitrate dehydrogenase (IDH) is allosterically activated by ADP by lowering the Km for isocitrate. The enzyme has three subunit types with distinguishable sequences present in the approximate ratio 2alpha:1beta:1gamma and, per tetramer, binds 2 mol of each ligand. To evaluate whether the subunits also have distinct functions, we replaced equivalent aspartates, one subunit at a time, by asparagines; each expressed, purified enzyme was composed of one mutant and two wild-type subunits. The aspartates were chosen because beta-Asp192 and gamma-Asp190 had previously been affinity labeled by a reactive ADP analogue and alpha-Asp181 is equivalent based on sequence alignments. The alpha-D181N IDH mutant exhibits a 2000-fold decrease in Vmax, with increases of 15-fold in the Kms for Mn(II) and NAD and a much smaller change in the Km for isocitrate. In contrast, the Vmax values of the beta-D192N and gamma-D190N IDHs are only reduced 4-5-fold as compared to wild-type enzyme. The Km for NAD of the beta-D192N enzyme is 9 times that of the normal enzyme with little or no effect on the affinity for Mn(II) or isocitrate, while the Kms for coenzyme and for Mn(II) of the gamma-D190N enzyme are 19 and 72 times, respectively, that of the normal enzyme with a much smaller effect on the Km for isocitrate. Finally, all three mutant enzymes fail to respond to ADP by lowering the Km for isocitrate, although they do bind ADP. Thus, these aspartates are close to but not in the ADP site and are required for communication between the ADP and isocitrate sites. These results demonstrate that alpha-Asp181 is the only one of these aspartates essential for catalysis. Beta-Asp192 is a determinant of the enzyme's affinity for NAD, as is gamma-Asp190, while gamma-Asp190 also influences the enzyme's affinity for metal ion. We conclude that the NAD and ADP sites are shared between alpha- and beta- and alpha- and gamma-subunits, and the Mn(II) site is shared between alpha- and gamma-subunits, while the alpha-subunit is essential for catalysis. Although alpha-Asp181, beta-Asp192, and gamma-Asp190 may have derived from a common progenitor, these aspartates of the three subunits have evolved distinct functions.

Published

2007

17. Biochemistry of the initial steps of mycothiol biosynthesis.

Author

Newton GL, Ta P, Bzymek KP, and Fahey RC

Subjects

Acetylation, Acetylglucosamine metabolism, Biochemical Phenomena, Biochemistry, Chromatography, High Pressure Liquid, Cysteine metabolism, Disaccharides metabolism, Glycosyltransferases metabolism, Inositol Phosphates metabolism, Mass Spectrometry, Mycobacterium smegmatis enzymology, Mycobacterium smegmatis genetics, Uridine Diphosphate metabolism, Cysteine biosynthesis, Glycopeptides biosynthesis, Inositol biosynthesis

Abstract

Mycothiol is the major thiol produced by mycobacteria and is required for growth of Mycobacterium tuberculosis. The final three steps in the biosynthesis of mycothiol have been fully elucidated but the initial steps have been unclear. A glycosyltransferase, MshA, is required for production of the mycothiol precursor, 1-O-(2-acetamido-2-deoxy-alpha-D-glucopyranosyl)-D-myo-inositol, but its substrates and immediate products were unknown. In this study, we show that the N-acetylglucosamine donor is UDP-N-acetylglucosamine and that the N-acetylglucosamine acceptor is 1L-myo-inositol 1-phosphate. The reaction generates UDP and 1-O-(2-acetamido-2-deoxy-alpha-D-glucopyranosyl)-D-myo-inositol 3-phosphate. Using cell-free extracts of M. smegmatis mc(2)155, little activity was obtained with myo-inositol, 1D-myo-inositol 1-phosphate, or myo-inositol 2-phosphate as the N-acetylglucosamine acceptor. A phosphatase, designated MshA2, is required to dephosphorylate 1-O-(2-acetamido-2-deoxy-alpha-glucopyranosyl)-D-myo-inositol 3-phosphate to produce 1-O-(2-acetamido-2-deoxy-alpha-D-glucopyranosyl)-D-myo-inositol. The latter is deacetylated, ligated with cysteine, and the cysteinyl amino group acetylated by acetyl-CoA to complete the mycothiol biosynthesis pathway. Uptake and concentration of myo-[14C]inositol is rapid in Mycobacterium smegmatis and leads to production of radiolabeled inositol 1-phosphate and mycothiol. This demonstrates the presence of a myo-inositol transporter and a kinase that generates 1L-myo-inositol 1-phosphate. The biochemical pathway of mycothiol biosynthesis is now fully elucidated.

Published

2006

18. The high-resolution structures of the neutral and the low pH crystals of aminopeptidase from Aeromonas proteolytica.

Author

Desmarais W, Bienvenue DL, Bzymek KP, Petsko GA, Ringe D, and Holz RC

Subjects

Aeromonas metabolism, Aminopeptidases metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Binding Sites, Crystallization, Crystallography, X-Ray, Hydrogen-Ion Concentration, Models, Chemical, Models, Molecular, Protein Binding, Substrate Specificity, Zinc chemistry, Zinc metabolism, Aeromonas enzymology, Aminopeptidases chemistry, Protein Structure, Tertiary

Abstract

The aminopeptidase from Aeromonas proteolytica (AAP) contains two zinc ions in the active site and catalyzes the degradation of peptides. Herein we report the crystal structures of AAP at 0.95-A resolution at neutral pH and at 1.24-A resolution at low pH. The combination of these structures allowed the precise modeling of atomic positions, the identification of the metal bridging oxygen species, and insight into the physical properties of the metal ions. On the basis of these structures, a new putative catalytic mechanism is proposed for AAP that is likely relevant to all binuclear metalloproteases.

Published

2006

19. Spectroscopic and thermodynamic characterization of the E151D and E151A altered leucine aminopeptidases from Aeromonas proteolytica.

Author

Bzymek KP, Swierczek SI, Bennett B, and Holz RC

Subjects

Aeromonas enzymology, Binding Sites, Calorimetry, Cobalt chemistry, Cobalt metabolism, Electron Spin Resonance Spectroscopy, Glutamic Acid chemistry, Glutamic Acid metabolism, Hydrogen Bonding, Kinetics, Point Mutation, Spectrophotometry, Ultraviolet, Zinc chemistry, Zinc metabolism, Aminopeptidases chemistry, Aminopeptidases metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism

Abstract

Previous kinetic characterization of the glutamate 151 (E151)-substituted forms of the leucine aminopeptidase from Aeromonas proteolytica (Vibrio proteolyticus; AAP) has provided critical evidence that this residue functions as the general acid/base. The close proximity of similar glutamate residues to the bridging water/hydroxide of the dinuclear active sites of metalloenzymes (2.80 and 3.94 angstroms in carboxypeptidase G2 and 3.30 and 3.63 angstroms in AAP), suggests it may also be involved in stabilizing the active-site metal ions. Therefore, the structural perturbations of the dinuclear active site of AAP were examined for two E151-substituted forms, namely E151D-AAP and E151A-AAP, by UV-vis and electron paramagnetic resonance (EPR) spectroscopy. UV-vis spectroscopy of Co(II)-substituted E151A-AAP did not reveal any significant changes in the electronic absorption spectra. However UV-vis spectra of mono- and dicobalt(II) E151D-AAP exhibited a lower molecular absorptivity compared to AAP (23 and 43 M(-1) cm(-1) vs. 56 and 109 M(-1) cm(-1) for E151D-AAP and AAP, respectively) suggesting both Co(II) ions reside in distorted octahedral coordination geometry in E151D-AAP. EPR spectra of [Co_(E151D-AAP)], [ZnCo(E151D-AAP)], and [(CoCo(E151D-AAP)] were identical, with g(perpendicular) = 2.35, g(parallel) = 2.19, and E/D = 0.19, similar to [CoCo(AAP)]. On the other hand, the EPR spectrum of [Co_(E151A-AAP)] was best simulated assuming the presence of two species with (i) g(x,y) = 2.509, g(z) = 2.19, E/D = 0.19, A = 0.0069 cm(-1) and (ii) g(x,y) = 2.565, g(z) = 2.19, E/D = 0.20, A = 0.0082 cm(-1) indicative of a five- or six-coordinate species. Isothermal titration calorimetry experiments revealed a large decrease in Zn(II) affinities, with K(d) values elevated by factors of approximately 850 and approximately 24,000 for the first metal binding events of E151D- and E151A-AAP, respectively. The combination of these data indicates that E151 serves to stabilize the dinuclear active site of AAP.

Published

2005

20. Kinetic, spectroscopic, and X-ray crystallographic characterization of the functional E151H aminopeptidase from Aeromonas proteolytica.

Author

Bzymek KP, Moulin A, Swierczek SI, Ringe D, Petsko GA, Bennett B, and Holz RC

Subjects

Aeromonas hydrophila genetics, Aminopeptidases genetics, Aminopeptidases isolation & purification, Binding Sites, Crystallography, X-Ray, Glutamic Acid genetics, Hydrogen-Ion Concentration, Kinetics, Mutation genetics, Protein Structure, Tertiary, Spectrum Analysis, Temperature, Titrimetry, Aeromonas hydrophila enzymology, Aminopeptidases chemistry, Aminopeptidases metabolism, Glutamic Acid metabolism

Abstract

Glutamate151 (E151) has been shown to be catalytically essential for the aminopeptidase from Vibrio proteolyticus (AAP). E151 acts as the general acid/base during the catalytic mechanism of peptide hydrolysis. However, a glutamate residue is not the only residue capable of functioning as a general acid/base during catalysis for dinuclear metallohydrolases. Recent crystallographic characterization of the D-aminopeptidase from Bacillus subtilis (DppA) revealed a histidine residue that resides in an identical position to E151 in AAP. Because the active-site ligands for DppA and AAP are identical, AAP has been used as a model enzyme to understand the mechanistic role of H115 in DppA. Substitution of E151 with histidine resulted in an active AAP enzyme exhibiting a kcat value of 2.0 min(-1), which is over 2000 times slower than r AAP (4380 min(-1)). ITC experiments revealed that ZnII binds 330 and 3 times more weakly to E151H-AAP compared to r-AAP. UV-vis and EPR spectra of CoII-loaded E151H-AAP indicated that the first metal ion resides in a hexacoordinate/pentacoordinate equilibrium environment, whereas the second metal ion is six-coordinate. pH dependence of the kinetic parameters kcat and K(m) for the hydrolysis of L-leucine p-nitroanilide (L-pNA) revealed a change in an ionization constant in the enzyme-substrate complex from 5.3 in r-AAP to 6.4 in E151H-AAP, consistent with E151 in AAP being the active-site general acid/base. Proton inventory studies at pH 8.50 indicate the transfer of one proton in the rate-limiting step of the reaction. Moreover, the X-ray crystal structure of [ZnZn(E151H-AAP)] has been solved to 1.9 A resolution, and alteration of E151 to histidine does not introduce any major conformational changes to the overall protein structure or the dinuclear ZnII active site. Therefore, a histidine residue can function as the general acid/base in hydrolysis reactions of peptides and, through analogy of the role of E151 in AAP, H115 in DppA likely shuttles a proton to the leaving group of the substrate.

Published

2005

21. Function of the signal peptide and N- and C-terminal propeptides in the leucine aminopeptidase from Aeromonas proteolytica.

Author

Bzymek KP, D'Souza VM, Chen G, Campbell H, Mitchell A, and Holz RC

Subjects

Cloning, Molecular, Electrophoresis, Polyacrylamide Gel, Endopeptidase K chemistry, Escherichia coli metabolism, Kinetics, Models, Biological, Mutagenesis, Site-Directed, Open Reading Frames, Peptides chemistry, Periplasm metabolism, Protein Structure, Secondary, Protein Structure, Tertiary, Recombinant Proteins chemistry, Spectrophotometry, Time Factors, Aeromonas metabolism, Leucyl Aminopeptidase chemistry, Protein Sorting Signals

Abstract

The leucine aminopeptidase from Aeromonas proteolytica (also known as Vibrio proteolyticus) (AAP) is a metalloenzyme with broad substrate specificity. The open reading frame (ORF) for AAP encodes a 54 kDa enzyme, however, the extracellular enzyme has a molecular weight of 43 kDa. This form of AAP is further processed to a mature, thermostable 32 kDa form but the exact nature of this process is unknown. Over-expression of different forms of AAP in Escherichia coli (with AAP's native leader sequence, with and without the N- and/or C-terminal propeptides, and as fusion protein) has allowed a model for the processing of wild-type AAP to be proposed. The role of the A. proteolytica signal peptide in protein secretion as well as comparison to other known signal peptides reveals a close resemblance of the A. proteolytica signal peptide to the outer membrane protein (OmpA) signal peptide. Over-expression of the full 54 kDa AAP enzyme provides an enzyme that is significantly less active, due to a cooperative inhibitory interaction between both propeptides. Over-expression of AAP lacking its C-terminal propeptide provided an enzyme with an identical kcat value to wild-type AAP but exhibited a larger Km value, suggesting competitive inhibition of AAP by the N-terminal propeptide (Ki approximately 0.13 nM). The recombinant 32 kDa form of AAP was characterized by kinetic and spectroscopic methods and was shown to be identical to mature, wild-type AAP. Therefore, the ease of purification and processing of rAAP along with the fact that large quantities can be obtained now allow new detailed mechanistic studies to be performed on AAP through site-directed mutagenesis.

Published

2004

22. The catalytic role of glutamate 151 in the leucine aminopeptidase from Aeromonas proteolytica.

Author

Bzymek KP and Holz RC

Subjects

Aeromonas genetics, Amino Acid Substitution, Aminopeptidases genetics, Aminopeptidases metabolism, Bacterial Proteins genetics, Bacterial Proteins metabolism, Base Sequence, Catalytic Domain genetics, DNA, Bacterial genetics, Deuterium, Glutamic Acid chemistry, Hydrogen-Ion Concentration, Kinetics, Leucyl Aminopeptidase genetics, Leucyl Aminopeptidase metabolism, Metals metabolism, Mutagenesis, Site-Directed, Protons, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Substrate Specificity, Thermodynamics, Aeromonas enzymology, Aminopeptidases chemistry, Bacterial Proteins chemistry, Leucyl Aminopeptidase chemistry

Abstract

Glutamate 151 has been proposed to act as the general acid/base during the peptide hydrolysis reaction catalyzed by the co-catalytic metallohydrolase from Aeromonas proteolytica (AAP). However, to date, no direct evidence has been reported for the role of Glu-151 during catalytic turnover by AAP. In order to elucidate the catalytic role of Glu-151, altered AAP enzymes have been prepared in which Glu-151 has been substituted with a glutamine, an alanine, and an aspartate. The Michaelis constant (K(m)) does not change upon substitution to aspartate or glutamine, but the rate of the reaction changes drastically in the following order: glutamate (100% activity), aspartate (0.05%), glutamine (0.004%), and alanine (0%). Examination of the pH dependence of the kinetic constants k(cat) and K(m) revealed a change in the pK(a) of a group that ionizes at pH 4.8 in recombinant leucine aminopeptidase (rAAP) to 4.2 for E151D-AAP. The remaining pK(a) values at 5.2, 7.5, and 9.9 do not change. Proton inventory studies indicate that one proton is transferred in the rate-limiting step of the reaction at pH 10.50 for both rAAP and E151D-AAP, but at pH 6.50 two protons and general solvation effects are responsible for the observed effects in the reaction catalyzed by rAAP and E151D-AAP, respectively. Based on these data, Glu-151 is intrinsically involved in the peptide hydrolysis reaction catalyzed by AAP and can be assigned the role of a general acid and base.

Published

2004

23. Co-catalytic metallopeptidases as pharmaceutical targets.

Author

Holz RC, Bzymek KP, and Swierczek SI

Subjects

Amidohydrolases antagonists & inhibitors, Amidohydrolases metabolism, Aminopeptidases antagonists & inhibitors, Aminopeptidases metabolism, Animals, Carboxypeptidases antagonists & inhibitors, Carboxypeptidases metabolism, Catalysis, Humans, Metalloendopeptidases antagonists & inhibitors, Metalloendopeptidases drug effects, Protease Inhibitors chemical synthesis, Protease Inhibitors pharmacology, Metalloendopeptidases metabolism

Abstract

Understanding the reaction mechanism of co-catalytic metallopeptidases provides a starting point for the design and synthesis of new molecules that can be screened as potential pharmaceuticals. Many of the enzymes that contain co-catalytic metallo-active sites play important roles in cellular processes such as tissue repair, protein maturation, hormone level regulation, cell-cycle control and protein degradation. Therefore, these enzymes play central roles in several disease states including cancer, HIV, stroke, diabetes, bacterial infections, neurological processes, schizophrenia, seizure disorders, and amyotrophic lateral sclerosis. The mechanism of AAP, an aminopeptidase from Aeromonas proteolytica, is one of the best-characterized examples of a metallopeptidase containing a co-catalytic metallo-active site, although this enzyme is not a specific pharmaceutical target at this time. As a large majority of co-catalytic metallopeptidases contain active sites that are nearly identical to the one observed in AAP, the major steps of their catalytic mechanisms are likely to be very similar. With this in mind, it is possible to propose a general catalytic mechanism for the hydrolysis of amino acid substrates.

Published

2003

24. The 1.20 A resolution crystal structure of the aminopeptidase from Aeromonas proteolytica complexed with tris: a tale of buffer inhibition.

Author

Desmarais WT, Bienvenue DL, Bzymek KP, Holz RC, Petsko GA, and Ringe D

Subjects

Amino Acids chemistry, Amino Acids metabolism, Aminopeptidases metabolism, Binding Sites, Chelating Agents chemistry, Chelating Agents metabolism, Crystallography, X-Ray, Models, Molecular, Molecular Structure, Protein Binding, Tromethamine metabolism, Zinc metabolism, Aeromonas enzymology, Aminopeptidases chemistry, Bacterial Proteins, Tromethamine chemistry

Abstract

The aminopeptidase from Aeromonas proteolytica (AAP) is a bridged bimetallic enzyme that removes the N-terminal amino acid from a peptide chain. To fully understand the metal roles in the reaction pathway of AAP we have solved the 1.20 A resolution crystal structure of native AAP (PDB ID = 1LOK). The high-quality electron density maps showed a single Tris molecule chelated to the active site Zn(2+), alternate side chain conformations for some side chains, a sodium ion that mediates a crystal contact, a surface thiocyanate ion, and several potential hydrogen atoms. In addition, the high precision of the atomic positions has led to insight into the protonation states of some of the active site amino acid side chains.

Published

2002