Your search keyword '"Wayne J. Fairbrother"' showing total 5 results

1. X Chromosome-linked Inhibitor of Apoptosis Regulates Cell Death Induction by Proapoptotic Receptor Agonists

Author

Kerry Zobel, J. Michael Elliott, Harvey Wong, Domagoj Vucic, Justin Scheer, Eugene Varfolomeev, Kristina West, Avi Ashkenazi, Stephen E. Gould, Wayne J. Fairbrother, and Bruno Alicke

Subjects

Agonist, Programmed cell death, Fas Ligand Protein, medicine.drug_class, Transplantation, Heterologous, Apoptosis, X-Linked Inhibitor of Apoptosis Protein, Inhibitor of apoptosis, Biochemistry, Receptors, Tumor Necrosis Factor, Fas ligand, Etanercept, Mice, Cell Line, Tumor, medicine, Animals, Humans, RNA, Small Interfering, Receptor, Molecular Biology, Cell Death, Tumor Necrosis Factor-alpha, Chemistry, Mechanisms of Signal Transduction, Cell Biology, Cell biology, XIAP, Receptors, TNF-Related Apoptosis-Inducing Ligand, Caspases, Immunoglobulin G, Cancer research, Tumor necrosis factor alpha, biological phenomena, cell phenomena, and immunity, BH3 Interacting Domain Death Agonist Protein, Signal Transduction

Abstract

Proapoptotic receptor agonists cause cellular demise through the activation of the extrinsic and intrinsic apoptotic pathways. Inhibitor of apoptosis (IAP) proteins block apoptosis induced by diverse stimuli. Here, we demonstrate that IAP antagonists in combination with Fas ligand (FasL) or the death receptor 5 (DR5) agonist antibody synergistically stimulate death in cancer cells and inhibit tumor growth. Single-agent activity of IAP antagonists relies on tumor necrosis factor-alpha signaling. By contrast, blockade of tumor necrosis factor-alpha does not affect the synergistic activity of IAP antagonists with FasL or DR5 agonist antibody. In most cancer cells, proapoptotic receptor agonist-induced cell death depends on amplifying the apoptotic signal via caspase-8-mediated activation of Bid and subsequent activation of the caspase-9-dependent mitochondrial apoptotic pathway. In the investigated cancer cell lines, induction of apoptosis by FasL or DR5 agonist antibody can be inhibited by knockdown of Bid. However, knockdown of X chromosome-linked IAP (XIAP) or antagonism of XIAP allows FasL or DR5 agonist antibody to induce activation of effector caspases efficiently without the need for mitochondrial amplification of the apoptotic signal and thus rescues the effect of Bid knockdown in these cells.

Published

2009

2. The Inhibitor of Apoptosis Protein Fusion c-IAP2·MALT1 Stimulates NF-κB Activation Independently of TRAF1 AND TRAF2

Author

Wayne J. Fairbrother, Sarah M. Wayson, Vishva M. Dixit, Domagoj Vucic, and Eugene Varfolomeev

Subjects

TRAF2, Recombinant Fusion Proteins, T cell, Molecular Sequence Data, TRAF1, Molecular Conformation, Down-Regulation, Apoptosis, Biology, Inhibitor of apoptosis, Biochemistry, Inhibitor of Apoptosis Proteins, medicine, Humans, Amino Acid Sequence, Molecular Biology, Inhibitor of apoptosis domain, Sequence Homology, Amino Acid, NF-kappa B, Cell Biology, Paracaspase, TNF Receptor-Associated Factor 2, TNF Receptor-Associated Factor 1, Fusion protein, Neoplasm Proteins, Protein Structure, Tertiary, Cell biology, MALT1, medicine.anatomical_structure, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Caspases, Mutation, Cancer research

Abstract

The inhibitors of apoptosis (IAPs) are a family of cell death inhibitors found in viruses and metazoans. All members of the IAP family have at least one baculovirus IAP repeat (BIR) motif that is essential for their anti-apoptotic activity. The t(11, 18)(q21;q21) translocation fuses the BIR domains of c-IAP2 with the paracaspase/MALT1 (mucosa-associated lymphoid tissue) protein, a critical mediator of T cell receptor-stimulated activation of NF-kappaB. The c-IAP2.MALT1 fusion protein constitutively activates the NF-kappaB pathway, and this is considered critical to malignant B cell transformation and lymphoma progression. The BIR domains of c-IAP1 and c-IAP2 interact with tumor necrosis factor receptor-associated factors 1 and 2 (TRAF1 and TRAF2). Here we investigated the importance of TRAF1 and TRAF2 for c-IAP2.MALT1-stimulated NF-kappaB activation. We identified a novel epitope within the BIR1 domains of c-IAP1 and c-IAP2 that is crucial for their physical interaction with TRAF1 and TRAF2. The c-IAP2.MALT1 fusion protein associates with TRAF1 and TRAF2 using the same binding site. We explored the functional relevance of this interaction and established that binding to TRAF1 and TRAF2 is not required for c-IAP2.MALT1-stimulated NF-kappaB activation. Furthermore, gene ablation of TRAF2 or combined down-regulation of TRAF1 and TRAF2 did not affect c-IAP2.MALT1-stimulated signaling. However, TRAF1/2-binding mutants of c-IAP2.MALT1 still oligomerize and activate NF-kappaB, suggesting that oligomerization might be important for signaling of the fusion protein. Therefore, the t(11, 18)(q21;q21) translocation creating the c-IAP2.MALT1 fusion protein activates NF-kappaB and contributes to human malignancy in the absence of signaling adaptors that might otherwise regulate its activity.

Published

2006

3. Selective Inhibition of Fibroblast Activation Protein Protease Based on Dipeptide Substrate Specificity

Author

Christian Wiesmann, Thuy Tran, Wayne J. Fairbrother, J. Michael Elliott, Helga Raab, Conrad Yap Edosada, Mark Reynolds, Beni Wolf, Dan Sutherlin, and Clifford Quan

Subjects

Models, Molecular, Time Factors, Light, Adenosine Deaminase, medicine.medical_treatment, Amino Acid Motifs, Oligopeptidase, Peptide, Plasma protein binding, Biochemistry, Substrate Specificity, chemistry.chemical_compound, Fibroblast activation protein, alpha, Scattering, Radiation, Cloning, Molecular, chemistry.chemical_classification, Hydrolysis, Serine Endopeptidases, Transmembrane protein, Gelatinases, Chromatography, Gel, Dimerization, Protein Binding, congenital, hereditary, and neonatal diseases and abnormalities, DNA, Complementary, animal structures, Dipeptidyl Peptidase 4, Biotin, Cell Line, Antigens, Neoplasm, Endopeptidases, Biomarkers, Tumor, medicine, Humans, Molecular Biology, Dipeptidyl peptidase-4, Glycoproteins, Protease, Dipeptide, Dose-Response Relationship, Drug, Membrane Proteins, Cell Biology, Fibroblasts, Molecular biology, digestive system diseases, Acetylcysteine, Kinetics, Models, Chemical, chemistry, Peptides, Peptide Hydrolases

Abstract

Fibroblast activation protein (FAP) is a transmembrane serine peptidase that belongs to the prolyl peptidase family. FAP has been implicated in cancer; however, its specific role remains elusive because inhibitors that distinguish FAP from other prolyl peptidases like dipeptidyl peptidase-4 (DPP-4) have not been developed. To identify peptide motifs for FAP-selective inhibitor design, we used P(2)-Pro(1) and acetyl (Ac)-P(2)-Pro(1) dipeptide substrate libraries, where P(2) was varied and substrate hydrolysis occurs between Pro(1) and a fluorescent leaving group. With the P(2)-Pro(1) library, FAP preferred Ile, Pro, or Arg at the P(2) residue; however, DPP-4 showed broad reactivity against this library, precluding selectivity. By contrast, with the Ac-P(2)-Pro(1) library, FAP cleaved only Ac-Gly-Pro, whereas DPP-4 showed little reactivity with all substrates. FAP also cleaved formyl-, benzyloxycarbonyl-, biotinyl-, and peptidyl-Gly-Pro substrates, which DPP-4 cleaved poorly, suggesting an N-acyl-Gly-Pro motif for inhibitor design. Therefore, we synthesized and tested the compound Ac-Gly-prolineboronic acid, which inhibited FAP with a K(i) of 23 +/- 3 nm. This was approximately 9- to approximately 5400-fold lower than the K(i) values for other prolyl peptidases, including DPP-4, DPP-7, DPP-8, DPP-9, prolyl oligopeptidase, and acylpeptide hydrolase. These results identify Ac-Gly-BoroPro as a FAP-selective inhibitor and suggest that N-acyl-Gly-Pro-based inhibitors will allow testing of FAP as a therapeutic target.

Published

2006

4. SMAC Negatively Regulates the Anti-apoptotic Activity of Melanoma Inhibitor of Apoptosis (ML-IAP)

Author

Vishva M. Dixit, Maria Teresa Pisabarro, Saloumeh Kadkhodayan, Domagoj Vucic, Wayne J. Fairbrother, Heidi Ackerly, and Kurt Deshayes

Subjects

Models, Molecular, Time Factors, Protein Conformation, viruses, Apoptosis, Complement Membrane Attack Complex, Biochemistry, Inhibitor of Apoptosis Proteins, Tumor Cells, Cultured, Caspase, biology, Effector, Melanoma, Caspase 9, Neoplasm Proteins, Nucleosomes, Cell biology, Caspases, biological phenomena, cell phenomena, and immunity, Plasmids, Protein Binding, musculoskeletal diseases, Programmed cell death, Proteases, Immunoblotting, Molecular Sequence Data, Transfection, Inhibitory postsynaptic potential, Inhibitor of apoptosis, Cell Line, Escherichia coli, medicine, Humans, Amino Acid Sequence, Molecular Biology, Adaptor Proteins, Signal Transducing, Glycoproteins, Dose-Response Relationship, Drug, Sequence Homology, Amino Acid, Complement System Proteins, Cell Biology, medicine.disease, Precipitin Tests, Molecular biology, Protein Structure, Tertiary, body regions, Mutation, biology.protein, Carrier Proteins, Peptides

Abstract

Inhibitors of apoptosis (IAPs) physically interact with a variety of pro-apoptotic proteins and inhibit apoptosis induced by diverse stimuli. X-linked IAP (X-IAP) is a prototype IAP family member that inhibits several caspases, the effector proteases of apoptosis. The inhibitory activity of X-IAP is regulated by SMAC, a protein that is processed to its active form upon receipt of a death stimulus. Cleaved SMAC binds X-IAP and antagonizes its anti-apoptotic activity. Here we show that melanoma IAP (ML-IAP), a potent anti-cell death protein and caspase inhibitor, physically interacts with SMAC through its BIR (baculovirus IAP repeat) domain. In addition to binding full-length SMAC, ML-IAP BIR associates with SMAC peptides that are derived from the amino terminus of active, processed SMAC. This high affinity interaction is very specific and can be completely abolished by single amino acid mutations either in the amino terminus of active SMAC or in the BIR domain of ML-IAP. In cells expressing ML-IAP and X-IAP, SMAC coexpression or addition of SMAC peptides abrogates the ability of the IAPs to inhibit cell death. These results demonstrate the feasibility of using SMAC peptides as a way to sensitize IAP-expressing cells to pro-apoptotic stimuli such as chemotherapeutic agents.

Published

2002

5. Selection of Heregulin Variants Having Higher Affinity for the ErbB3 Receptor by Monovalent Phage Display

Author

Wayne J. Fairbrother, Julie A. Lofgren, James A. Wells, Robert W. Akita, Marcus Ballinger, Jennifer T. Jones, and Mark X. Sliwkowski

Subjects

Models, Molecular, Phage display, Receptor, ErbB-3, Neuregulin-1, Molecular Sequence Data, Plasma protein binding, Biology, Ligands, Biochemistry, Structure-Activity Relationship, Peptide Library, Epidermal growth factor, Proto-Oncogene Proteins, Amino Acid Sequence, Binding site, Receptor, Nuclear Magnetic Resonance, Biomolecular, Molecular Biology, Peptide sequence, ERBB4, Glycoproteins, Binding Sites, Cell Biology, Alanine scanning, Molecular biology, Recombinant Proteins, ErbB Receptors, Carrier Proteins, Bacteriophage M13, Protein Binding

Abstract

Heregulins (HRGs) are epidermal growth factor (egf) domain containing polypeptide growth factors that bind and activate several members of the ErbB receptor family. Although HRG can bind to ErbB3 and ErbB4 homodimers, the highest affinity and most intracellularly active receptor complexes are hetero-oligomers containing ErbB2. The HRGbeta egf domain was displayed on the surface of M13 phage to facilitate mutagenic analysis and optimize for binding to a homodimeric ErbB3-immunoglobulin (IgG) fusion. Nine libraries were constructed in which virtually the entire sequence was randomized in stretches of four to six amino acids. These were selected separately for binding to immobilized ErbB3-IgG. Analysis of the resulting sequences revealed some areas that diverged radically from the wild-type, whereas others showed strong conservation. The degree of wild-type conservation correlated strongly with the functional importance of the residues as determined by alanine scanning mutagenesis (Jones, J. T., Ballinger, M. D., Pisacane, P. I., Lofgren, J. A., Fitzpatrick, V. D., Fairbrother, W. J., Wells, J. A., and Sliwkowski, M. X. (1998) J. Biol. Chem. 273, 11667-11674). Some variants from several libraries showed significant improvements in binding affinity to the ErbB3-IgG. These optimized segments were combined in various ways in the same molecule to generate variants (containing up to 16 mutations) that had >50-fold higher affinity than wild-type HRGbeta. The optimized variants stimulated ErbB2 phophorylation on MCF7 cells at levels similar to wild-type. This indicates wild-type affinity is optimized for potency and that factors other than affinity for ErbB3 are limiting. These variants showed enhanced affinity toward the ErbB4 homodimer, suggesting these receptors use very similar binding determinants despite them having 65% sequence identity.

Published

1998