Your search keyword '"Fairbrother WJ"' showing total 122 results

51. X chromosome-linked inhibitor of apoptosis regulates cell death induction by proapoptotic receptor agonists.

Author

Varfolomeev E, Alicke B, Elliott JM, Zobel K, West K, Wong H, Scheer JM, Ashkenazi A, Gould SE, Fairbrother WJ, and Vucic D

Subjects

Animals, BH3 Interacting Domain Death Agonist Protein genetics, BH3 Interacting Domain Death Agonist Protein metabolism, Caspases metabolism, Cell Line, Tumor, Etanercept, Humans, Immunoglobulin G genetics, Immunoglobulin G metabolism, Mice, RNA, Small Interfering genetics, RNA, Small Interfering metabolism, Receptors, TNF-Related Apoptosis-Inducing Ligand metabolism, Receptors, Tumor Necrosis Factor genetics, Receptors, Tumor Necrosis Factor metabolism, Signal Transduction physiology, Transplantation, Heterologous, Tumor Necrosis Factor-alpha metabolism, X-Linked Inhibitor of Apoptosis Protein genetics, Apoptosis physiology, Cell Death physiology, Fas Ligand Protein metabolism, Receptors, TNF-Related Apoptosis-Inducing Ligand agonists, X-Linked Inhibitor of Apoptosis Protein antagonists & inhibitors, X-Linked Inhibitor of Apoptosis Protein metabolism

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

52. NMR assignments of the human cytokine interleukin-33.

Author

Lingel A and Fairbrother WJ

Subjects

Humans, Interleukin-33, Nuclear Magnetic Resonance, Biomolecular, Interleukins chemistry

Abstract

We report near complete NMR backbone and side chain assignments of the human cytokine interleukin-33 (IL-33) in solution. IL-33 is the latest addition to the family of interleukin-1 homologous cytokines and was shown to be involved in inflammation and autoimmune diseases.

Published

2009

53. Structure of IL-33 and its interaction with the ST2 and IL-1RAcP receptors--insight into heterotrimeric IL-1 signaling complexes.

Author

Lingel A, Weiss TM, Niebuhr M, Pan B, Appleton BA, Wiesmann C, Bazan JF, and Fairbrother WJ

Subjects

Binding Sites, Crystallography, X-Ray, Humans, Interleukin-1 chemistry, Interleukin-1 Receptor-Like 1 Protein, Interleukin-33, Models, Molecular, Protein Conformation, Receptors, Cell Surface metabolism, Interleukin-1 metabolism, Interleukin-1 Receptor Accessory Protein chemistry, Interleukins chemistry, Interleukins metabolism, Receptors, Cell Surface chemistry, Signal Transduction

Abstract

Members of the interleukin-1 (IL-1) family of cytokines play major roles in host defense and immune system regulation in infectious and inflammatory diseases. IL-1 cytokines trigger a biological response in effector cells by assembling a heterotrimeric signaling complex with two IL-1 receptor chains, a high-affinity primary receptor and a low-affinity coreceptor. To gain insights into the signaling mechanism of the novel IL-1-like cytokine IL-33, we first solved its solution structure and then performed a detailed biochemical and structural characterization of the interaction between IL-33, its primary receptor ST2, and the coreceptor IL-1RAcP. Using nuclear magnetic resonance data, we obtained a model of the IL-33/ST2 complex in solution that is validated by small-angle X-ray scattering (SAXS) data and is similar to the IL-1beta/IL-1R1 complex. We extended our SAXS analysis to the IL-33/ST2/IL-1RAcP and IL-1beta/IL-1R1/IL-1RAcP complexes and propose a general model of the molecular architecture of IL-1 ternary signaling complexes.

Published

2009

54. Phosphorylation of a borealin dimerization domain is required for proper chromosome segregation.

Author

Bourhis E, Lingel A, Phung Q, Fairbrother WJ, and Cochran AG

Subjects

Amino Acid Sequence, Cell Cycle Proteins chemistry, Cell Cycle Proteins genetics, Dimerization, Humans, Microscopy, Fluorescence, Molecular Sequence Data, Mutagenesis, Site-Directed, Nuclear Magnetic Resonance, Biomolecular, Phosphorylation, Protein Conformation, Sequence Homology, Amino Acid, Tandem Mass Spectrometry, Cell Cycle Proteins metabolism, Chromosomes, Human

Abstract

The chromosomal passenger complex (CPC) has been identified as a master regulator of mitosis. In particular, proper chromosome segregation and cytokinesis depend on the correct localization and function of the CPC. Within the complex, the kinase Aurora B associates with Incenp, Survivin, and Borealin. The stoichiometry of the complex as well as a complete understanding of how these four components interact with each other remains to be elucidated. Here, we identify a new domain of Borealin. We determined its structure using NMR spectroscopy and discovered a novel dimerization motif. Interestingly, we found that substitutions at Borealin T230, recently identified as an Mps1 phosphorylation site, can modulate the dimerization state of Borealin. Mutation of this single residue to alanine or valine impairs Aurora B activity during mitosis and causes chromosome segregation defects. This study reveals that Mps1 regulates the CPC through a novel Borealin domain.

Published

2009

55. Antagonism of c-IAP and XIAP proteins is required for efficient induction of cell death by small-molecule IAP antagonists.

Author

Ndubaku C, Varfolomeev E, Wang L, Zobel K, Lau K, Elliott LO, Maurer B, Fedorova AV, Dynek JN, Koehler M, Hymowitz SG, Tsui V, Deshayes K, Fairbrother WJ, Flygare JA, and Vucic D

Subjects

Binding Sites, Cell Death drug effects, Cell Line, Humans, Inhibitor of Apoptosis Proteins chemistry, Inhibitor of Apoptosis Proteins metabolism, Melanoma pathology, Models, Molecular, Molecular Structure, NF-kappa B metabolism, Protein Binding, Structure-Activity Relationship, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Neoplasms drug therapy, X-Linked Inhibitor of Apoptosis Protein antagonists & inhibitors

Abstract

The inhibitor of apoptosis (IAP) proteins are critical regulators of cancer cell survival, which makes them attractive targets for therapeutic intervention in cancers. Herein, we describe the structure-based design of IAP antagonists with high affinities and selectivity (>2000-fold) for c-IAP1 over XIAP and their functional characterization as activators of apoptosis in tumor cells. Although capable of inducing cell death and preventing clonogenic survival, c-IAP-selective antagonists are significantly less potent in promoting apoptosis when compared to pan-selective compounds. However, both pan-IAP- and c-IAP-selective antagonists stimulate c-IAP1 and c-IAP2 degradation and activation of NF-kappaB pathways with comparable potencies. Therefore, although compounds that specifically target c-IAP1 and c-IAP2 are capable of inducing apoptosis, antagonism of the c-IAP proteins and XIAP is required for efficient induction of cancer cell death by IAP antagonists.

Published

2009

56. Orally bioavailable antagonists of inhibitor of apoptosis proteins based on an azabicyclooctane scaffold.

Author

Cohen F, Alicke B, Elliott LO, Flygare JA, Goncharov T, Keteltas SF, Franklin MC, Frankovitz S, Stephan JP, Tsui V, Vucic D, Wong H, and Fairbrother WJ

Subjects

Administration, Oral, Azabicyclo Compounds administration & dosage, Azabicyclo Compounds pharmacokinetics, Biological Availability, Cell Line, Tumor, Humans, Models, Molecular, Structure-Activity Relationship, Azabicyclo Compounds chemistry, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Octanes chemistry

Abstract

A series of IAP antagonists based on an azabicyclooctane scaffold was designed and synthesized. The most potent of these compounds, 14b, binds to the XIAP BIR3 domain, the BIR domain of ML-IAP, and the BIR3 domain of c-IAP1 with K(i) values of 140, 38, and 33 nM, respectively. These compounds promote degradation of c-IAP1, activate caspases, and lead to decreased viability of breast cancer cells without affecting normal mammary epithelial cells. Finally, compound 14b inhibits tumor growth when dosed orally in a breast cancer xenograft model.

Published

2009

57. Ubiquitin binding modulates IAP antagonist-stimulated proteasomal degradation of c-IAP1 and c-IAP2(1).

Author

Blankenship JW, Varfolomeev E, Goncharov T, Fedorova AV, Kirkpatrick DS, Izrael-Tomasevic A, Phu L, Arnott D, Aghajan M, Zobel K, Bazan JF, Fairbrother WJ, Deshayes K, and Vucic D

Subjects

Amino Acid Sequence, Binding Sites genetics, Calorimetry, Cell Line, Cell Line, Tumor, Circular Dichroism, Humans, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Inhibitor of Apoptosis Proteins chemistry, Kinetics, Magnetic Resonance Spectroscopy, Mass Spectrometry, Molecular Sequence Data, NF-kappa B metabolism, Polyubiquitin metabolism, Protein Binding, Protein Serine-Threonine Kinases metabolism, Protein Structure, Secondary, Protein Structure, Tertiary, Receptors, Tumor Necrosis Factor, Type I metabolism, Sequence Homology, Amino Acid, Surface Plasmon Resonance, Ubiquitination, NF-kappaB-Inducing Kinase, Inhibitor of Apoptosis Proteins metabolism, Proteasome Endopeptidase Complex metabolism, Ubiquitin metabolism

Abstract

A family of anti-apoptotic regulators known as IAP (inhibitor of apoptosis) proteins interact with multiple cellular partners and inhibit apoptosis induced by a variety of stimuli. c-IAP (cellular IAP) 1 and 2 are recruited to TNFR1 (tumour necrosis factor receptor 1)-associated signalling complexes, where they mediate receptor-induced NF-kappaB (nuclear factor kappaB) activation. Additionally, through their E3 ubiquitin ligase activities, c-IAP1 and c-IAP2 promote proteasomal degradation of NIK (NF-kappaB-inducing kinase) and regulate the non-canonical NF-kappaB pathway. In the present paper, we describe a novel ubiquitin-binding domain of IAPs. The UBA (ubiquitin-associated) domain of IAPs is located between the BIR (baculovirus IAP repeat) domains and the CARD (caspase activation and recruitment domain) or the RING (really interesting new gene) domain of c-IAP1 and c-IAP2 or XIAP (X-linked IAP) respectively. The c-IAP1 UBA domain binds mono-ubiquitin and Lys(48)- and Lys(63)-linked polyubiquitin chains with low-micromolar affinities as determined by surface plasmon resonance or isothermal titration calorimetry. NMR analysis of the c-IAP1 UBA domain-ubiquitin interaction reveals that this UBA domain binds the classical hydrophobic patch surrounding Ile(44) of ubiquitin. Mutations of critical amino acid residues in the highly conserved MGF (Met-Gly-Phe) binding loop of the UBA domain completely abrogate ubiquitin binding. These mutations in the UBA domain do not overtly affect the ubiquitin ligase activity of c-IAP1 or the participation of c-IAP1 and c-IAP2 in the TNFR1 signalling complex. Treatment of cells with IAP antagonists leads to proteasomal degradation of c-IAP1 and c-IAP2. Deletion or mutation of the UBA domain decreases this degradation, probably by diminishing the interaction of the c-IAPs with the proteasome. These results suggest that ubiquitin binding may be an important mechanism for rapid turnover of auto-ubiquitinated c-IAP1 and c-IAP2.

Published

2009

58. c-IAP1 and c-IAP2 are critical mediators of tumor necrosis factor alpha (TNFalpha)-induced NF-kappaB activation.

Author

Varfolomeev E, Goncharov T, Fedorova AV, Dynek JN, Zobel K, Deshayes K, Fairbrother WJ, and Vucic D

Subjects

Animals, Cell Death physiology, Cell Line, Tumor, GTPase-Activating Proteins genetics, GTPase-Activating Proteins metabolism, Humans, Inhibitor of Apoptosis Proteins genetics, Mice, Mice, Knockout, NF-kappa B genetics, Nuclear Pore Complex Proteins genetics, Nuclear Pore Complex Proteins metabolism, RNA-Binding Proteins genetics, RNA-Binding Proteins metabolism, Receptors, Tumor Necrosis Factor, Type I genetics, Tumor Necrosis Factor-alpha genetics, Ubiquitination physiology, Inhibitor of Apoptosis Proteins metabolism, NF-kappa B metabolism, Receptors, Tumor Necrosis Factor, Type I metabolism, Signal Transduction physiology, Tumor Necrosis Factor-alpha metabolism

Abstract

The inhibitor of apoptosis (IAP) proteins are a family of anti-apoptotic regulators found in viruses and metazoans. c-IAP1 and c-IAP2 are recruited to tumor necrosis factor receptor 1 (TNFR1)-associated complexes where they can regulate receptor-mediated signaling. Both c-IAP1 and c-IAP2 have been implicated in TNFalpha-stimulated NF-kappaB activation. However, individual c-IAP1 and c-IAP2 gene knock-outs in mice did not reveal changes in TNF signaling pathways, and the phenotype of a combined deficiency of c-IAPs has yet to be reported. Here we investigate the role of c-IAP1 and c-IAP2 in TNFalpha-stimulated activation of NF-kappaB. We demonstrate that TNFalpha-induced NF-kappaB activation is severely diminished in the absence of both c-IAP proteins. In addition, combined absence of c-IAP1 and c-IAP2 rendered cells sensitive to TNFalpha-induced cell death. Using cells with genetic ablation of c-IAP1 or cells where the c-IAP proteins were eliminated using IAP antagonists, we show that TNFalpha-induced RIP1 ubiquitination is abrogated in the absence of c-IAPs. Furthermore, we reconstitute the ubiquitination process with purified components in vitro and demonstrate that c-IAP1, in collaboration with the ubiquitin conjugating enzyme (E2) enzyme UbcH5a, mediates polymerization of Lys-63-linked chains on RIP1. Therefore, c-IAP1 and c-IAP2 are required for TNFalpha-stimulated RIP1 ubiquitination and NF-kappaB activation.

Published

2008

59. Microphthalmia-associated transcription factor is a critical transcriptional regulator of melanoma inhibitor of apoptosis in melanomas.

Author

Dynek JN, Chan SM, Liu J, Zha J, Fairbrother WJ, and Vucic D

Subjects

Cell Survival genetics, Cells, Cultured, Cyclic AMP metabolism, DNA Damage physiology, Humans, Melanocytes metabolism, Microphthalmia-Associated Transcription Factor metabolism, Promoter Regions, Genetic, Protein Binding, Signal Transduction genetics, Transcription, Genetic, Transfection, Tumor Necrosis Factor-alpha physiology, Wnt Proteins physiology, Adaptor Proteins, Signal Transducing genetics, Gene Expression Regulation, Inhibitor of Apoptosis Proteins genetics, Melanoma genetics, Microphthalmia-Associated Transcription Factor physiology, Neoplasm Proteins genetics

Abstract

Melanoma inhibitor of apoptosis (ML-IAP) is a potent inhibitor of apoptosis, which is highly expressed in melanomas and likely contributes to their resistance to chemotherapeutic treatments. Herein, we show that the lineage survival oncogene microphthalmia-associated transcription factor (MITF) is a critical regulator of ML-IAP transcription in melanoma cells. The ML-IAP promoter contains two MITF consensus sites, and analysis of MITF and ML-IAP mRNA levels revealed a high correlation in melanoma tumor samples and cell lines. In reporter assays, MITF promoted a strong stimulation of transcriptional activity from the ML-IAP promoter, and MITF bound the endogenous ML-IAP promoter in melanoma cells by chromatin immunoprecipitation and electrophoretic mobility shift assay. Strikingly, small interfering RNA (siRNA)-mediated knockdown of MITF in melanoma cells led to a dramatic decrease in ML-IAP mRNA and protein levels, establishing that ML-IAP expression in melanoma cells is MITF dependent. Additionally, cyclic AMP-mediated induction of MITF expression in melanocytes resulted in increased ML-IAP expression, suggesting that melanocytes can express ML-IAP when MITF levels are heightened. Disruption of MITF by siRNA led to a decrease in melanoma cell viability, which could be rescued by ectopic expression of ML-IAP. Collectively, these findings implicate MITF as a major transcriptional regulator of ML-IAP expression in melanomas, and suggest that ML-IAP contributes to the prosurvival activity of MITF in melanoma progression.

Published

2008

60. IAP antagonists induce autoubiquitination of c-IAPs, NF-kappaB activation, and TNFalpha-dependent apoptosis.

Author

Varfolomeev E, Blankenship JW, Wayson SM, Fedorova AV, Kayagaki N, Garg P, Zobel K, Dynek JN, Elliott LO, Wallweber HJ, Flygare JA, Fairbrother WJ, Deshayes K, Dixit VM, and Vucic D

Subjects

Animals, Cell Line, Humans, Inhibitor of Apoptosis Proteins genetics, Mice, Molecular Structure, Neoplasms metabolism, Neoplasms pathology, Proteasome Endopeptidase Complex metabolism, Protein Structure, Tertiary, Signal Transduction physiology, Ubiquitination, Apoptosis physiology, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Inhibitor of Apoptosis Proteins metabolism, NF-kappa B metabolism, Polyubiquitin metabolism, Tumor Necrosis Factor-alpha metabolism

Abstract

Inhibitor of apoptosis (IAP) proteins are antiapoptotic regulators that block cell death in response to diverse stimuli. They are expressed at elevated levels in human malignancies and are attractive targets for the development of novel cancer therapeutics. Herein, we demonstrate that small-molecule IAP antagonists bind to select baculovirus IAP repeat (BIR) domains resulting in dramatic induction of auto-ubiquitination activity and rapid proteasomal degradation of c-IAPs. The IAP antagonists also induce cell death that is dependent on TNF signaling and de novo protein biosynthesis. Additionally, the c-IAP proteins were found to function as regulators of NF-kappaB signaling. Through their ubiquitin E3 ligase activities c-IAP1 and c-IAP2 promote proteasomal degradation of NIK, the central ser/thr kinase in the noncanonical NF-kappaB pathway.

Published

2007

61. The inhibitor of apoptosis proteins as therapeutic targets in cancer.

Author

Vucic D and Fairbrother WJ

Subjects

Animals, Apoptosis, Caspases metabolism, Humans, Models, Biological, Models, Chemical, Neoplasm Metastasis, Neoplasm Proteins metabolism, Neoplasms metabolism, Gene Expression Regulation, Neoplastic, Inhibitor of Apoptosis Proteins physiology, Neoplasms drug therapy, Neoplasms pathology

Abstract

Apoptosis is a cell suicide process with a major role in development and homeostasis in vertebrates and invertebrates. Inhibition of apoptosis enhances the survival of cancer cells and facilitates their escape from immune surveillance and cytotoxic therapies. Among the principal molecules contributing to this phenomenon are the inhibitor of apoptosis (IAP) proteins, a family of antiapoptotic regulators that block cell death in response to diverse stimuli through interactions with inducers and effectors of apoptosis. IAP proteins are expressed in the majority of human malignancies at elevated levels and play an active role in promoting tumor maintenance through the inhibition of cellular death and participation in signaling pathways associated with malignancies. Here, we discuss the role of IAP proteins in cancer and options for targeting IAP proteins for therapeutic intervention.

Published

2007

62. Evaluation of assay technologies for the identification of protein-Peptide interaction antagonists.

Author

Kadkhodayan S, Elliott LO, Mausisa G, Wallweber HA, Deshayes K, Feng B, and Fairbrother WJ

Subjects

Biotin chemistry, Data Interpretation, Statistical, Escherichia coli genetics, Escherichia coli metabolism, Fluoresceins chemistry, Fluorescence Polarization, Peptides chemical synthesis, Biological Assay methods, Drug Evaluation, Preclinical methods, Peptides antagonists & inhibitors, Peptides chemistry, Proteins antagonists & inhibitors, Proteins chemistry

Abstract

An increasing number of assay detection technologies are routinely used in small molecule drug discovery and lead optimization. These assays range from solid-phase heterogeneous assays such as enzyme-linked immunosorbent assay and dissociation-enhanced lanthanide fluorescent immunoassay (DELFIA, PerkinElmer Life and Analytical Sciences, Boston, MA) to solution phase, bead-based assays such as electrochemiluminescence assay (BioVeris [Gaithersburg, MD] technology) and amplified luminescent proximity homogeneous assay (AlphaScreen, PerkinElmer Life and Analytical Sciences) to completely solution-based homogeneous assays such as time-resolved fluorescence resonance energy transfer and fluorescence polarization. The aim of this study is to compare these assay technologies and assess the advantages and disadvantages of each in the context of our efforts to develop small molecule antagonists to the melanoma inhibitor of apoptosis protein. In this study, seven peptides have been evaluated for their potencies in each assay format. Our results indicate that these assay technologies produce similar relative potencies; however, some methods may be more susceptible to interference than others. Consequently, the choice of the method used frequently depends on a number of factors in addition to assay reproducibility and performance, such as throughput of the assay, cost, compound interference, and ease of use.

Published

2007

63. Structure of C3b in complex with CRIg gives insights into regulation of complement activation.

Author

Wiesmann C, Katschke KJ, Yin J, Helmy KY, Steffek M, Fairbrother WJ, McCallum SA, Embuscado L, DeForge L, Hass PE, and van Lookeren Campagne M

Subjects

Complement C3-C5 Convertases antagonists & inhibitors, Complement C3-C5 Convertases metabolism, Complement C3c chemistry, Complement C3c metabolism, Complement C5 antagonists & inhibitors, Complement C5 metabolism, Crystallography, X-Ray, Humans, Models, Molecular, Mutation genetics, Protein Binding, Protein Conformation, Receptors, Complement genetics, Receptors, Complement 3b, Structure-Activity Relationship, Complement Activation, Complement C3b chemistry, Complement C3b metabolism, Receptors, Complement chemistry, Receptors, Complement metabolism

Abstract

The complement system is a key part of the innate immune system, and is required for clearance of pathogens from the bloodstream. After exposure to pathogens, the third component of the complement system, C3, is cleaved to C3b which, after recruitment of factor B, initiates formation of the alternative pathway convertases. CRIg, a complement receptor expressed on macrophages, binds to C3b and iC3b mediating phagocytosis of the particles, but it is unknown how CRIg selectively recognizes proteolytic C3-fragments and whether binding of CRIg to C3b inhibits convertase activation. Here we present the crystal structure of C3b in complex with CRIg and, using CRIg mutants, provide evidence that CRIg acts as an inhibitor of the alternative pathway of complement. The structure shows that activation of C3 induces major structural rearrangements, including a dramatic movement (>80 A) of the thioester-bond-containing domain through which C3b attaches to pathogen surfaces. We show that CRIg is not only a phagocytic receptor, but also a potent inhibitor of the alternative pathway convertases. The structure provides insights into the complex macromolecular structural rearrangements that occur during complement activation and inhibition. Moreover, our structure-function studies relating the structural basis of complement activation and the means by which CRIg inhibits the convertases provide important clues to the development of therapeutics that target complement.

Published

2006

64. Structure of SAP18: a ubiquitin fold in histone deacetylase complex assembly.

Author

McCallum SA, Bazan JF, Merchant M, Yin J, Pan B, de Sauvage FJ, and Fairbrother WJ

Subjects

Carrier Proteins metabolism, Co-Repressor Proteins, Histone Deacetylases chemistry, Histone Deacetylases metabolism, Humans, Multiprotein Complexes chemistry, Multiprotein Complexes metabolism, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Tertiary, RNA-Binding Proteins, Transcription Factors chemistry, Transcription Factors metabolism, Transcription, Genetic physiology, Ubiquitin metabolism, Carrier Proteins chemistry, Protein Folding, Ubiquitin chemistry

Abstract

Signal transduction pathways are frequently found to repress transcription of target genes in the absence of stimulation and, conversely, to upregulate transcription in the presence of a signal. Transcription factors are central in this dual regulatory mechanism and widely use a generalized mechanism to repress transcription through recruitment of a Sin3-histone deacetylase (HDAC) complex to their binding sites on DNA. The protein SAP18 (Sin3-associated polypeptide of 18 kDa) has been shown to play a key role in gene-specific recruitment of the HDAC complex by a number of transcription factors including Gli, GAGA, and Bicoid. The solution structure of SAP18 reveals a ubiquitin-like fold with several large loop insertions relative to other family members. This fold supports the functional role of SAP18 as a protein-protein adapter module and provides insight for how SAP18 may bridge the Sin3-HDAC complex to transcription factors.

Published

2006

65. The inhibitor of apoptosis protein fusion c-IAP2.MALT1 stimulates NF-kappaB activation independently of TRAF1 AND TRAF2.

Author

Varfolomeev E, Wayson SM, Dixit VM, Fairbrother WJ, and Vucic D

Subjects

Amino Acid Sequence, Down-Regulation, Humans, Molecular Conformation, Molecular Sequence Data, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Mutation, Protein Structure, Tertiary, Recombinant Fusion Proteins chemistry, Sequence Homology, Amino Acid, Apoptosis, Caspases metabolism, Inhibitor of Apoptosis Proteins metabolism, NF-kappa B metabolism, Neoplasm Proteins metabolism, TNF Receptor-Associated Factor 1 physiology, TNF Receptor-Associated Factor 2 physiology

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

66. Design, synthesis, and biological activity of a potent Smac mimetic that sensitizes cancer cells to apoptosis by antagonizing IAPs.

Author

Zobel K, Wang L, Varfolomeev E, Franklin MC, Elliott LO, Wallweber HJ, Okawa DC, Flygare JA, Vucic D, Fairbrother WJ, and Deshayes K

Subjects

Binding Sites, Biomimetic Materials chemical synthesis, Biomimetic Materials chemistry, Caspases metabolism, Cell Line, Crystallography, X-Ray, Enzyme Activation drug effects, Humans, Inhibitor of Apoptosis Proteins metabolism, Intracellular Signaling Peptides and Proteins metabolism, Models, Molecular, Neoplasms genetics, Protein Binding, Protein Structure, Tertiary, Apoptosis drug effects, Biomimetic Materials pharmacology, Drug Design, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Intracellular Signaling Peptides and Proteins chemistry, Neoplasms metabolism, Neoplasms pathology

Abstract

Designed second mitochondrial activator of caspases (Smac) mimetics based on an accessible [7,5]-bicyclic scaffold bind to and antagonize protein interactions involving the inhibitor of apoptosis (IAP) proteins, X-chromosome-linked IAP (XIAP), melanoma IAP (ML-IAP), and c-IAPs 1 and 2 (cIAP1 and cIAP2). The design rationale is based on a combination of phage-panning data, peptide binding studies, and a survey of potential isosteres. The synthesis of two scaffolds is described. These compounds bind the XIAP-baculoviral IAP repeat 3 (BIR3), cIAP1-BIR3, cIAP2-BIR3, and ML-IAP-BIR domains with submicromolar affinities. The most potent Smac mimetic binds the cIAP1-BIR3 and ML-IAP-BIR domains with a K i of 50 nM. The X-ray crystal structure of this compound bound to an ML-IAP/XIAP chimeric BIR domain protein is compared with that of a complex with a phage-derived tetrapeptide, AVPW. The structures show that these compounds bind to the Smac-binding site on ML-IAP with identical hydrogen-bonding patterns and similar hydrophobic interactions. Consistent with the structural data, coimmunoprecipitation experiments demonstrate that the compounds can effectively block Smac interactions with ML-IAP. The compounds are further demonstrated to activate caspase-3 and -7, to reduce cell viability in assays using MDA-MB-231 breast cancer cells and A2058 melanoma cells, and to enhance doxorubicin-induced apoptosis in MDA-MB-231 cells.

Published

2006

67. 1H, 13C, and 15N resonance assignments of SAP18.

Author

McCallum SA, Yin J, and Fairbrother WJ

Subjects

Acetylation, Amino Acid Sequence, Amino Acids, Aromatic chemistry, Carbon Isotopes, Carrier Proteins genetics, Carrier Proteins metabolism, Co-Repressor Proteins, Histone Deacetylases metabolism, Histones metabolism, Humans, Nitrogen Isotopes, Peptides chemistry, Proline chemistry, Protein Structure, Secondary, Protons, RNA-Binding Proteins, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Transcription Factors genetics, Transcription Factors metabolism, Transcription, Genetic, Carrier Proteins chemistry, Nuclear Magnetic Resonance, Biomolecular, Transcription Factors chemistry

Published

2005

68. Engineering ML-IAP to produce an extraordinarily potent caspase 9 inhibitor: implications for Smac-dependent anti-apoptotic activity of ML-IAP.

Author

Vucic D, Franklin MC, Wallweber HJ, Das K, Eckelman BP, Shin H, Elliott LO, Kadkhodayan S, Deshayes K, Salvesen GS, and Fairbrother WJ

Subjects

Adaptor Proteins, Signal Transducing chemistry, Adaptor Proteins, Signal Transducing genetics, Amino Acid Sequence, Apoptosis Regulatory Proteins, Binding Sites, Carrier Proteins chemistry, Carrier Proteins genetics, Caspase 9, Caspases metabolism, Cell Line, Cell Line, Tumor, Crystallography, X-Ray, Cysteine Proteinase Inhibitors genetics, Electron Spin Resonance Spectroscopy, Humans, Inhibitor of Apoptosis Proteins, Intracellular Signaling Peptides and Proteins, Kinetics, Mitochondrial Proteins chemistry, Mitochondrial Proteins genetics, Models, Molecular, Molecular Sequence Data, Neoplasm Proteins chemistry, Neoplasm Proteins genetics, Protein Binding, Protein Structure, Tertiary, Proteins chemistry, Proteins genetics, Proteins metabolism, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, X-Linked Inhibitor of Apoptosis Protein, Adaptor Proteins, Signal Transducing metabolism, Apoptosis, Carrier Proteins metabolism, Caspase Inhibitors, Cysteine Proteinase Inhibitors chemistry, Cysteine Proteinase Inhibitors metabolism, Mitochondrial Proteins metabolism, Neoplasm Proteins metabolism, Protein Engineering

Abstract

ML-IAP (melanoma inhibitor of apoptosis) is a potent anti-apoptotic protein that is strongly up-regulated in melanoma and confers protection against a variety of pro-apoptotic stimuli. The mechanism by which ML-IAP regulates apoptosis is unclear, although weak inhibition of caspases 3 and 9 has been reported. Here, the binding to and inhibition of caspase 9 by the single BIR (baculovirus IAP repeat) domain of ML-IAP has been investigated and found to be significantly less potent than the ubiquitously expressed XIAP (X-linked IAP). Engineering of the ML-IAP-BIR domain, based on comparisons with the third BIR domain of XIAP, resulted in a chimeric BIR domain that binds to and inhibits caspase 9 significantly better than either ML-IAP-BIR or XIAP-BIR3. Mutational analysis of the ML-IAP-BIR domain demonstrated that similar enhancements in caspase 9 affinity can be achieved with only three amino acid substitutions. However, none of these modifications affected binding of the ML-IAP-BIR domain to the IAP antagonist Smac (second mitochondrial activator of caspases). ML-IAP-BIR was found to bind mature Smac with low nanomolar affinity, similar to that of XIAP-BIR2-BIR3. Correspondingly, increased expression of ML-IAP results in formation of a ML-IAP-Smac complex and disruption of the endogenous interaction between XIAP and mature Smac. These results suggest that ML-IAP might regulate apoptosis by sequestering Smac and preventing it from antagonizing XIAP-mediated inhibition of caspases, rather than by direct inhibition of caspases.

Published

2005

69. Convergent recognition of the IgE binding site on the high-affinity IgE receptor.

Author

Stamos J, Eigenbrot C, Nakamura GR, Reynolds ME, Yin J, Lowman HB, Fairbrother WJ, and Starovasnik MA

Subjects

Amino Acid Sequence, Cells, Cultured, Crystallography, X-Ray, Humans, Immunoglobulin E chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Peptides metabolism, Protein Binding, Protein Conformation, Receptors, IgE chemistry, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Binding, Competitive, Immunoglobulin E metabolism, Peptides chemistry, Receptors, IgE metabolism

Abstract

Two structurally distinct classes of peptides were recently identified by phage display that bind the high-affinity IgE receptor, FcepsilonRI, and block IgE binding and subsequent receptor activation. Both classes adopt highly stable structures in solution, one forming a beta hairpin, with the other forming a helical "zeta" structure. Despite these differences, the two classes bind competitively to the same site on the receptor. Structural analyses of both peptide-receptor complexes by NMR spectroscopy and/or X-ray crystallography reveal that the unrelated peptide scaffolds have nevertheless converged to present a similar three-dimensional surface to interact with FcepsilonRI and that their modes of interaction share a key feature of the IgE-FcepsilonRI complex, the proline/tryptophan sandwich.

Published

2004

70. Structure and function analysis of peptide antagonists of melanoma inhibitor of apoptosis (ML-IAP).

Author

Franklin MC, Kadkhodayan S, Ackerly H, Alexandru D, Distefano MD, Elliott LO, Flygare JA, Mausisa G, Okawa DC, Ong D, Vucic D, Deshayes K, and Fairbrother WJ

Subjects

Amino Acid Sequence, Carrier Proteins genetics, Crystallography, X-Ray, Genetic Linkage, Inhibitor of Apoptosis Proteins, Models, Molecular, Molecular Sequence Data, Neoplasm Proteins genetics, Sequence Homology, Amino Acid, Structure-Activity Relationship, X Chromosome, Adaptor Proteins, Signal Transducing, Carrier Proteins chemistry, Carrier Proteins physiology, Neoplasm Proteins chemistry, Neoplasm Proteins physiology

Abstract

Melanoma inhibitor of apoptosis (ML-IAP) is a potent anti-apoptotic protein that is upregulated in a number of melanoma cell lines but not expressed in most normal adult tissues. Overexpression of IAP proteins, such as ML-IAP or the ubiquitously expressed X-chromosome-linked IAP (XIAP), in human cancers has been shown to suppress apoptosis induced by a variety of stimuli. Peptides based on the processed N-terminus of Smac/DIABLO can negate the ability of overexpressed ML-IAP or XIAP to suppress drug-induced apoptosis. Such peptides have been demonstrated to bind to the single baculovirus IAP repeat (BIR) of ML-IAP and the third BIR of XIAP with similar high affinities (approximately 0.5 microM). Herein, we use phage-display of naïve peptide libraries and synthetic peptides to investigate the peptide-binding properties of ML-IAP-BIR and XIAP-BIR3. X-ray crystal structures of ML-IAP-BIR in complex with Smac- and phage-derived peptides, together with peptide structure-activity-relationship data, indicate that the peptides can be modified to provide increased binding affinity and selectivity for ML-IAP-BIR relative to XIAP-BIR3. For instance, substitution of Pro3' in the Smac-based peptide (AVPIAQKSE) with (2S,3S)-3-methylpyrrolidine-2-carboxylic acid [(3S)-methyl-proline] results in a peptide with 7-fold greater affinity for ML-IAP-BIR and about 100-fold specificity for ML-IAP-BIR relative to XIAP-BIR3.

Published

2003

71. BAFF/BLyS receptor 3 comprises a minimal TNF receptor-like module that encodes a highly focused ligand-binding site.

Author

Gordon NC, Pan B, Hymowitz SG, Yin J, Kelley RF, Cochran AG, Yan M, Dixit VM, Fairbrother WJ, and Starovasnik MA

Subjects

Amino Acid Sequence, B-Cell Activating Factor, B-Cell Activation Factor Receptor, Binding Sites, Cysteine chemistry, Humans, In Vitro Techniques, Ligands, Membrane Proteins genetics, Membrane Proteins metabolism, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Secondary, Protein Structure, Tertiary, Receptors, Tumor Necrosis Factor genetics, Receptors, Tumor Necrosis Factor metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Solutions, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha metabolism, Membrane Proteins chemistry, Receptors, Tumor Necrosis Factor chemistry, Tumor Necrosis Factor-alpha chemistry

Abstract

BAFF/BLyS, a member of the tumor necrosis family (TNF) superfamily of ligands, is a crucial survival factor for B cells. BAFF binds three receptors, TACI, BCMA, and BR3, with signaling through BR3 being essential for promoting B cell function. Typical TNF receptor (TNFR) family members bind their cognate ligands through interactions with two cysteine-rich domains (CRDs). However, the extracellular domain (ECD) of BR3 consists of only a partial CRD, with cysteine spacing distinct from other modules described previously. Herein, we report the solution structure of the BR3 ECD. A core region of only 19 residues adopts a stable structure in solution. The BR3 fold is analogous to the first half of a canonical TNFR CRD but is stabilized by an additional noncanonical disulfide bond. BAFF-binding determinants were identified by shotgun alanine-scanning mutagenesis of the BR3 ECD expressed on phage. Several of the key BAFF-binding residues are presented from a beta-turn that we have shown previously to be sufficient for ligand binding when transferred to a structured beta-hairpin scaffold [Kayagaki, N., Yan, M., Seshasayee, D., Wang, H., Lee, W., French, D. M., Grewal, I. S., Cochran, A. G., Gordon, N. C., Yin, J., Starovasnik, M. A, and Dixit, V. M. (2002) Immunity 10, 515-524]. Outside of the turn, mutagenesis identifies additional hydrophobic contacts that enhance the BAFF-BR3 interaction. The crystal structure of the minimal hairpin peptide, bhpBR3, in complex with BAFF reveals intimate packing of the six-residue BR3 turn into a cavity on the ligand surface. Thus, BR3 binds BAFF through a highly focused interaction site, unprecedented in the TNFR family.

Published

2003

72. Exploring protein-protein interactions with phage display.

Author

Sidhu SS, Fairbrother WJ, and Deshayes K

Subjects

Animals, Epitope Mapping, Extracellular Space metabolism, Humans, Models, Molecular, Molecular Mimicry, Proteins physiology, Peptide Library, Proteins chemistry

Abstract

Protein-protein interactions mediate essentially all biological processes. A detailed understanding of these interactions is thus a major goal of modern biological chemistry. In recent years, genome sequencing efforts have revealed tens of thousands of novel genes, but the benefits of genome sequences will only be realized if these data can be translated to the level of protein function. While genome databases offer tremendous opportunities to expand our knowledge of protein-protein interactions, they also present formidable challenges to traditional protein chemistry methods. Indeed, it has become apparent that efficient analysis of proteins on a proteome-wide scale will require the use of rapid combinatorial approaches. In this regard, phage display is an established combinatorial technology that is likely to play an even greater role in the future of biology. This article reviews recent applications of phage display to the analysis of protein-protein interactions. With combinatorial mutagenesis strategies, it is now possible to rapidly map the binding energetics at protein-protein interfaces through statistical analysis of phage-displayed protein libraries. In addition, naïve phage-displayed peptide libraries can be used to obtain small peptide ligands to essentially any protein of interest, and in many cases, these binding peptides act as antagonists or even agonists of natural protein functions. These methods are accelerating the pace of research by enabling the study of complex protein-protein interactions with simple molecular biology methods. With further optimization and automation, it may soon be possible to study hundreds of different proteins in parallel with efforts comparable to those currently expended on the analysis of individual proteins.

Published

2003

73. SMAC negatively regulates the anti-apoptotic activity of melanoma inhibitor of apoptosis (ML-IAP).

Author

Vucic D, Deshayes K, Ackerly H, Pisabarro MT, Kadkhodayan S, Fairbrother WJ, and Dixit VM

Subjects

Amino Acid Sequence, Caspase 9, Caspases metabolism, Cell Line, Complement Membrane Attack Complex, Complement System Proteins, Dose-Response Relationship, Drug, Escherichia coli metabolism, Humans, Immunoblotting, Inhibitor of Apoptosis Proteins, Models, Molecular, Molecular Sequence Data, Mutation, Peptides chemistry, Plasmids metabolism, Precipitin Tests, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Time Factors, Transfection, Tumor Cells, Cultured, Adaptor Proteins, Signal Transducing, Apoptosis, Carrier Proteins metabolism, Glycoproteins metabolism, Neoplasm Proteins metabolism, Nucleosomes metabolism

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

74. Identification of a novel homotypic interaction motif required for the phosphorylation of receptor-interacting protein (RIP) by RIP3.

Author

Sun X, Yin J, Starovasnik MA, Fairbrother WJ, and Dixit VM

Subjects

Amino Acid Motifs, Antigens, CD metabolism, Humans, Jurkat Cells, NF-kappa B metabolism, Phosphorylation, Proteins metabolism, Receptor-Interacting Protein Serine-Threonine Kinases, Receptors, Tumor Necrosis Factor metabolism, Receptors, Tumor Necrosis Factor, Type I, Tumor Necrosis Factor-alpha antagonists & inhibitors, U937 Cells, Protein Kinases metabolism, Proteins chemistry

Abstract

Receptor-interacting protein (RIP), a Ser/Thr kinase component of the tumor necrosis factor (TNF) receptor-1 signaling complex, mediates activation of the nuclear factor kappaB (NF-kappaB) pathway. RIP2 and RIP3 are related kinases that share extensive sequence homology with the kinase domain of RIP. Unlike RIP, which has a C-terminal death domain, and RIP2, which has a C-terminal caspase activation and recruitment domain, RIP3 possesses a unique C terminus. RIP3 binds RIP through this unique C-terminal segment to inhibit RIP- and TNF receptor-1-mediated NF-kappaB activation. We have identified a unique homotypic interaction motif at the C terminus of both RIP and RIP3 that is required for their association. Sixty-four amino acids within RIP3 and 88 residues within RIP are sufficient for interaction of the two proteins. This interaction is a prerequisite for RIP3-mediated phosphorylation of RIP and subsequent attenuation of TNF-induced NF-kappaB activation.

Published

2002

75. Identification of a novel death domain-containing adaptor molecule for ectodysplasin-A receptor that is mutated in crinkled mice.

Author

Yan M, Zhang Z, Brady JR, Schilbach S, Fairbrother WJ, and Dixit VM

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, DNA, Complementary genetics, Edar Receptor, Edar-Associated Death Domain Protein, Exons, Humans, Ligands, Mice, Mice, Mutant Strains, Molecular Sequence Data, Mutation, NF-kappa B metabolism, Phenotype, Protein Structure, Tertiary, Proteins metabolism, Sequence Homology, Amino Acid, TNF Receptor-Associated Factor 2, Tissue Distribution, Adaptor Proteins, Signal Transducing, Carrier Proteins genetics, Carrier Proteins metabolism, Ectodermal Dysplasia genetics, Ectodermal Dysplasia metabolism, Fish Proteins genetics, Fish Proteins metabolism

Abstract

Hypohydrotic Ectodermal Dysplasia (HED) is a genetic disease seen in humans and mice. It is characterized by loss of hair, sweat glands, and teeth. The predominant X-linked form results from mutations in ectodysplasin-A (EDA), a TNF-like ligand. A phenotypically indistinguishable autosomal form of the disease results from mutations in the receptor for EDA (EDAR). EDAR is a NF-kappaB-activating, death domain-containing member of the TNF receptor family. crinkled, a distinct autosomal form of HED, was discovered in a mouse strain in which both the ligand (EDA) and receptor (EDAR) were wild-type, suggestive of a disruption further downstream in the signaling pathway. Employing a forward genetic approach, we have cloned crinkled (CR) and find it to encode a novel death domain-containing adaptor. crinkled binds EDAR through a homotypic death domain interaction and mediates engagement of the NF-kappaB pathway, possibly by recruiting TRAF2 to the receptor-signaling complex. This is an unprecedented example of naturally occurring mutations in ligand, receptor, or adaptor giving rise to the same phenotypic disease characterized by a defect in the proper development of epidermal appendages.

Published

2002

76. Solution structure of a phage-derived peptide antagonist in complex with vascular endothelial growth factor.

Author

Pan B, Li B, Russell SJ, Tom JY, Cochran AG, and Fairbrother WJ

Subjects

Alanine genetics, Alanine metabolism, Amino Acid Sequence, Binding Sites, Crystallography, X-Ray, Dimerization, Disulfides metabolism, Endothelial Growth Factors genetics, Endothelial Growth Factors metabolism, Humans, Hydrophobic and Hydrophilic Interactions, Lymphokines genetics, Lymphokines metabolism, Models, Molecular, Molecular Sequence Data, Mutation genetics, Nuclear Magnetic Resonance, Biomolecular, Peptides chemical synthesis, Peptides metabolism, Protein Structure, Quaternary, Protein Structure, Secondary, Protein Structure, Tertiary, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogene Proteins chemistry, Proto-Oncogene Proteins metabolism, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Receptor Protein-Tyrosine Kinases chemistry, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Growth Factor antagonists & inhibitors, Receptors, Growth Factor chemistry, Receptors, Growth Factor metabolism, Receptors, Vascular Endothelial Growth Factor, Solutions, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factor Receptor-1, Vascular Endothelial Growth Factors, Bacteriophages chemistry, Endothelial Growth Factors antagonists & inhibitors, Endothelial Growth Factors chemistry, Lymphokines antagonists & inhibitors, Lymphokines chemistry, Peptides chemistry, Peptides pharmacology

Abstract

Vascular endothelial growth factor (VEGF) is a potent endothelial cell-specific mediator of angiogenesis and vasculogenesis. VEGF is involved pathologically in cancer, proliferative retinopathy and rheumatoid arthritis, and as such represents an important therapeutic target. Three classes of disulfide-constrained peptides that antagonize binding of the VEGF dimer to its receptors, KDR and Flt-1, were identified previously using phage display methods. NMR studies of a representative peptide from the most potent class of these peptide antagonists, v107 (GGNECDAIRMWEWECFERL), were undertaken to characterize its interactions with VEGF. v107 has no defined structure free in solution, but binding to VEGF induces folding of the peptide. The solution structure of the VEGF receptor-binding domain-v107 complex was determined using 3940 (1970 per VEGF monomer) internuclear distance and 476 (238 per VEGF monomer) dihedral angle restraints derived from NMR data obtained using samples containing either (13)C/(15)N-labeled protein plus excess unlabeled peptide or (13)C/(15)N-labeled peptide plus excess unlabeled protein. Residual dipolar coupling restraints supplemented the structure determination of the complex and were found to increase significantly both the global precision of VEGF in the complex and the agreement with available crystal structures of VEGF. The calculated ensemble of structures is of high precision and is in excellent agreement with the experimental restraints. v107 has a turn-helix conformation with hydrophobic residues partitioned to one face of the peptide and polar or charged residues at the other face. Contacts between two v107 peptides and the VEGF dimer are mediated by primarily hydrophobic side-chain interactions. The v107-binding site on VEGF overlaps partially with the binding site of KDR and is similar to that for domain 2 of Flt-1. The structure of the VEGF-v107 complex provides new insight into how binding to VEGF can be achieved that may be useful for the design of small molecule antagonists., (Copyright 2002 Elsevier Science Ltd.)

Published

2002

77. 1H, 13C, and 15N resonance assignment of the vascular endothelial growth factor receptor-binding domain in complex with a receptor-blocking peptide.

Author

Pan B and Fairbrother WJ

Subjects

Binding Sites, Carbon Isotopes, Humans, Nitrogen Isotopes, Protein Binding, Protein Structure, Tertiary, Protons, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Endothelial Growth Factors chemistry, Intercellular Signaling Peptides and Proteins chemistry, Lymphokines chemistry, Nuclear Magnetic Resonance, Biomolecular, Peptides chemistry, Receptors, Vascular Endothelial Growth Factor antagonists & inhibitors

Published

2002

78. The PYRIN domain: a member of the death domain-fold superfamily.

Author

Fairbrother WJ, Gordon NC, Humke EW, O'Rourke KM, Starovasnik MA, Yin JP, and Dixit VM

Subjects

Amino Acid Sequence, Circular Dichroism, Cytoskeletal Proteins, Models, Molecular, Molecular Sequence Data, Protein Folding, Protein Structure, Tertiary, Proteins metabolism, Pyrin, Sequence Alignment, Sequence Homology, Amino Acid, Apoptosis, Proteins chemistry

Abstract

PYRIN domains were identified recently as putative protein-protein interaction domains at the N-termini of several proteins thought to function in apoptotic and inflammatory signaling pathways. The approximately 95 residue PYRIN domains have no statistically significant sequence homology to proteins with known three-dimensional structure. Using secondary structure prediction and potential-based fold recognition methods, however, the PYRIN domain is predicted to be a member of the six-helix bundle death domain-fold superfamily that includes death domains (DDs), death effector domains (DEDs), and caspase recruitment domains (CARDs). Members of the death domain-fold superfamily are well established mediators of protein-protein interactions found in many proteins involved in apoptosis and inflammation, indicating further that the PYRIN domains serve a similar function. An homology model of the PYRIN domain of CARD7/DEFCAP/NAC/NALP1, a member of the Apaf-1/Ced-4 family of proteins, was constructed using the three-dimensional structures of the FADD and p75 neurotrophin receptor DDs, and of the Apaf-1 and caspase-9 CARDs, as templates. Validation of the model using a variety of computational techniques indicates that the fold prediction is consistent with the sequence. Comparison of a circular dichroism spectrum of the PYRIN domain of CARD7/DEFCAP/NAC/NALP1 with spectra of several proteins known to adopt the death domain-fold provides experimental support for the structure prediction.

Published

2001

79. ICEBERG: a novel inhibitor of interleukin-1beta generation.

Author

Humke EW, Shriver SK, Starovasnik MA, Fairbrother WJ, and Dixit VM

Subjects

Caspase 1 chemistry, Cells, Cultured, Molecular Sequence Data, Monomeric GTP-Binding Proteins metabolism, Monomeric GTP-Binding Proteins pharmacology, Protein Serine-Threonine Kinases chemistry, Receptor-Interacting Protein Serine-Threonine Kinase 2, Receptor-Interacting Protein Serine-Threonine Kinases, Sequence Analysis, Protein, Tumor Necrosis Factor-alpha metabolism, Tumor Necrosis Factor-alpha pharmacology, ran GTP-Binding Protein, Amino Acid Sequence physiology, Carrier Proteins genetics, Caspase 1 metabolism, Inflammation Mediators metabolism, Interleukin-1 antagonists & inhibitors, Interleukin-1 biosynthesis, Intracellular Signaling Peptides and Proteins, Protein Serine-Threonine Kinases metabolism

Abstract

ProIL-1beta is a proinflammatory cytokine that is proteolytically processed to its active form by caspase-1. Upon receipt of a proinflammatory stimulus, an upstream adaptor, RIP2, binds and oligomerizes caspase-1 zymogen, promoting its autoactivation. ICEBERG is a novel protein that inhibits generation of IL-1beta by interacting with caspase-1 and preventing its association with RIP2. ICEBERG is induced by proinflammatory stimuli, suggesting that it may be part of a negative feedback loop. Consistent with this, enforced retroviral expression of ICEBERG inhibits lipopolysaccharide-induced IL-1beta generation. The structure of ICEBERG reveals it to be a member of the death-domain-fold superfamily. The distribution of surface charge is complementary to the homologous prodomain of caspase-1, suggesting that charge-charge interactions mediate binding of ICEBERG to the prodomain of caspase-1.

Published

2000

80. Characterization of the binding interface between the E-domain of staphylococcal protein A and an antibody Fv-fragment

Author

Meininger DP, Rance M, Starovasnik MA, Fairbrother WJ, and Skelton NJ

Published

2000

81. Characterization of the binding interface between the E-domain of Staphylococcal protein A and an antibody Fv-fragment.

Author

Meininger DP, Rance M, Starovasnik MA, Fairbrother WJ, and Skelton NJ

Subjects

Amino Acid Sequence, Binding Sites, Antibody genetics, Genetic Vectors chemical synthesis, Humans, Immunoglobulin Fragments genetics, Immunoglobulin Fragments metabolism, Immunoglobulin Heavy Chains chemistry, Immunoglobulin Heavy Chains genetics, Immunoglobulin Heavy Chains metabolism, Immunoglobulin Variable Region chemistry, Immunoglobulin Variable Region genetics, Immunoglobulin Variable Region metabolism, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Peptide Mapping, Protein Conformation, Protein Structure, Tertiary, Receptor, ErbB-2 chemistry, Receptor, ErbB-2 genetics, Receptor, ErbB-2 metabolism, Staphylococcal Protein A genetics, Staphylococcal Protein A metabolism, Thermodynamics, Immunoglobulin Fragments chemistry, Staphylococcal Protein A chemistry, Staphylococcal Protein A immunology

Abstract

Staphylococcal protein A (SpA) is a cell-surface component of Staphylococcus aureus. In addition to the well-characterized interaction between SpA and the Fc-region of human IgG, an alternative binding interaction between SpA and the Fab-region of immunoglobulin domains encoded by the V(H)3 gene family has been described. To characterize structurally the interface formed by SpA repeats and type-3 V(H)-domains, we have studied the 32-kDa complex formed between an E-domain mutant (EZ4) and the Fv-fragment of the humanized anti-HER2 antibody (Hu4D5-8) using heteronuclear NMR spectroscopy. Protocols were established for efficient incorporation of (15)N, (13)C, and (2)H into EZ4 and the V(H)- and V(L)-domains of the Fv, allowing backbone resonances to be assigned sequentially for EZ4 and the V(H)-domain in both free and complexed states. Broadening of certain V(H)-resonances in the free and bound Fv-fragment suggests microsecond to millisecond time-scale motion in CDR3. Residues experiencing significant chemical shift changes of backbone (1)H(N), (15)N, and (13)CO resonances upon complex formation delineate contiguous surfaces on EZ4 and the V(H)-domain that define the binding interfaces of the two proteins. The interaction surfaces identified by chemical shift mapping are comprised of predominantly hydrophilic residues. This is in contrast to the SpA-Fc interface which is predominantly hydrophobic in nature. Further analysis of the surface properties suggests a probable binding orientation for SpA- and V(H)3-domains.

Published

2000

82. Antibody variable region binding by Staphylococcal protein A: thermodynamic analysis and location of the Fv binding site on E-domain.

Author

Starovasnik MA, O'Connell MP, Fairbrother WJ, and Kelley RF

Subjects

Binding Sites, Calorimetry, Differential Scanning, Humans, Immunoglobulin Variable Region metabolism, Magnetic Resonance Spectroscopy, Models, Molecular, Protein Denaturation, Staphylococcal Protein A chemistry, Staphylococcal Protein A metabolism, Thermodynamics, Immunoglobulin Variable Region immunology, Staphylococcal Protein A immunology

Abstract

Immunoglobulins of human heavy chain subgroup III have a binding site for Staphylococcal protein A on the heavy chain variable domain (V(H)), in addition to the well-known binding site on the Fc portion of the antibody. Thermodynamic characterization of this binding event and localization of the Fv-binding site on a domain of protein A is described. Isothermal titration calorimetry (ITC) was used to characterize the interaction between protein A or fragments of protein A and variants of the hu4D5 antibody Fab fragment. Analysis of binding isotherms obtained for titration of hu4D5 Fab with intact protein A suggests that 3-4 of the five immunoglobulin binding domains of full length protein A can bind simultaneously to Fab with a Ka of 5.5+/-0.5 x 10(5) M(-1). A synthetic single immunoglobulin binding domain, Z-domain, does not bind appreciably to hu4D5 Fab, but both the E and D domains are functional for hu4D5 Fab binding. Thermodynamic parameters for titration of the E-domain with hu4D5 Fab are n = 1.0+/-0.1, Ka = 2.0+/-0.3 x 10(5) M(-1), and deltaH = -7.1+/-0.4 kcal mol(-1). Similar binding thermodynamics are obtained for titration of the isolated V(H) domain with E-domain indicating that the E-domain binding site on Fab resides within V(H). E-domain binding to an IgG1 Fc yields a higher affinity interaction with thermodynamic parameters n = 2.2+/-0.1, Ka > 1.0 x 10(7) M(-1), and deltaH = -24.6+/-0.6 kcal mol(-1). Fc does not compete with Fab for binding to E-domain indicating that the two antibody fragments bind to different sites. Amide 1H and 15N resonances that undergo large changes in NMR chemical shift upon Fv binding map to a surface defined by helix-2 and helix-3 of E-domain, distinct from the Fc-binding site observed in the crystal structure of the B-domain/Fc complex. The Fv-binding region contains negatively charged residues and a small hydrophobic patch which complements the basic surface of the region of the V(H) domain implicated previously in protein A binding.

Published

1999

83. Novel peptides selected to bind vascular endothelial growth factor target the receptor-binding site.

Author

Fairbrother WJ, Christinger HW, Cochran AG, Fuh G, Keenan CJ, Quan C, Shriver SK, Tom JY, Wells JA, and Cunningham BC

Subjects

Amino Acid Sequence, Base Sequence, Binding Sites drug effects, Cell Division drug effects, Cells, Cultured, Endothelial Growth Factors chemistry, Endothelium, Vascular cytology, Growth Inhibitors pharmacology, Humans, Lymphokines chemistry, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Peptide Library, Peptides chemistry, Peptides pharmacology, Random Allocation, Receptor Protein-Tyrosine Kinases chemistry, Receptors, Growth Factor chemistry, Receptors, Vascular Endothelial Growth Factor, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Endothelial Growth Factors metabolism, Lymphokines metabolism, Peptides metabolism, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Growth Factor metabolism

Abstract

Peptides that inhibit binding of vascular endothelial growth factor (VEGF) to its receptors, KDR and Flt-1, have been produced using phage display. Libraries of short disulfide-constrained peptides yielded three distinct classes of peptides that bind to the receptor-binding domain of VEGF with micromolar affinities. The highest affinity peptide was also shown to antagonize VEGF-induced proliferation of primary human umbilical vascular endothelial cells. The peptides bind to a region of VEGF known to contain the contact surface for Flt-1 and the functional determinants for KDR binding. This suggests that the receptor-binding region of VEGF is a binding "hot spot" that is readily targeted by selected peptides and supports earlier assertions that phage-derived peptides frequently target protein-protein interaction sites. Such peptides may lead to the development of pharmacologically useful VEGF antagonists.

Published

1998

84. Crystal structure of the complex between VEGF and a receptor-blocking peptide.

Author

Wiesmann C, Christinger HW, Cochran AG, Cunningham BC, Fairbrother WJ, Keenan CJ, Meng G, and de Vos AM

Subjects

Amino Acid Sequence, Computer Simulation, Crystallization, Crystallography, X-Ray, Endothelial Growth Factors metabolism, Humans, Lymphokines metabolism, Macromolecular Substances, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Peptides metabolism, Peptides pharmacology, Protein Binding, Receptor Protein-Tyrosine Kinases chemistry, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Growth Factor chemistry, Receptors, Growth Factor metabolism, Receptors, Vascular Endothelial Growth Factor, Solutions, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Endothelial Growth Factors chemistry, Lymphokines chemistry, Peptides chemistry, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Receptors, Growth Factor antagonists & inhibitors

Abstract

Vascular endothelial growth factor (VEGF) is a specific and potent angiogenic factor and, therefore, a prime therapeutic target for the development of antagonists for the treatment of cancer. As a first step toward this goal, phage display was used to generate peptides that bind to the receptor-binding domain (residues 8-109) of VEGF and compete with receptor [Fairbrother, W. J., Christinger, H. W., Cochran, A. G., Fuh, G., Keenan, C. J., Quan, C., Shriver, S. K., Tom, J. Y. K., Wells, J. A., and Cunningham, B. C. (1999) Biochemistry 38, 17754-17764]. The crystal structure of VEGF in complex with one of these peptides was solved and refined to a resolution of 1.9 A. The 20-mer peptide is unstructured in solution and adopts a largely extended conformation when bound to VEGF. Residues 3-8 form a beta-strand which pairs with strand beta6 of VEGF via six hydrogen bonds. The C-terminal four residues of the peptide point away from the growth factor, consistent with NMR data indicating that these residues are flexible in the complex in solution. In contrast, shortening the N-terminus of the peptide leads to decreased binding affinities. Truncation studies show that the peptide can be reduced to 14 residues with only moderate effect on binding affinity. However, because of the extended conformation and the scarcity of specific side-chain interactions with VEGF, the peptide is not a promising lead for small-molecule development. The interface between the peptide and VEGF contains a subset of the residues recognized by a neutralizing Fab fragment and overlaps partially with the binding site for the Flt-1 receptor. The location of the peptide-binding site and the hydrophilic character of the interactions with VEGF resemble more the binding mode of the Fab fragment than that of the receptor.

Published

1998

85. A His19 to Ala mutant of melanoma growth-stimulating activity is a partial antagonist of the CXCR2 receptor.

Author

Baly DL, Horuk R, Yansura DG, Simmons LC, Fairbrother WJ, Kotts C, Wirth CM, Gillece-Castro BL, Toy K, Hesselgesser J, and Allison DE

Subjects

Antigens, CD genetics, Antigens, CD metabolism, Calcium Signaling drug effects, Cell Line, Chemokine CXCL1, Chemotactic Factors genetics, Chemotaxis, Leukocyte drug effects, Cytochalasin B pharmacology, Growth Substances genetics, Humans, Interleukin-8 pharmacology, Leukocyte Elastase metabolism, Neutrophils drug effects, Neutrophils physiology, Receptors, Chemokine genetics, Receptors, Chemokine metabolism, Receptors, Interleukin genetics, Receptors, Interleukin metabolism, Receptors, Interleukin-8A, Receptors, Interleukin-8B, Recombinant Fusion Proteins antagonists & inhibitors, Recombinant Fusion Proteins metabolism, Signal Transduction physiology, Transfection, Amino Acid Substitution, Chemokines, CXC, Chemotactic Factors pharmacology, Growth Substances pharmacology, Intercellular Signaling Peptides and Proteins, Receptors, Chemokine antagonists & inhibitors, Receptors, Interleukin antagonists & inhibitors

Abstract

Melanoma growth stimulating activity (MGSA) and IL-8 are related chemokines that are potent chemoattractants and activators of neutrophils both in vitro and in vivo. Increasing evidence suggests that these molecules play an important role in inflammation; thus, antagonists of their action could be useful therapeutically as antiinflammatory agents. We have generated an MGSA mutant, H19A, that shows a dissociation between receptor binding and biologic activity. The biologic activity of the H19A mutant is between 133-fold and 282-fold less potent than that of wild-type MGSA measured by three independent assays of neutrophil function, i.e., elastase release chemotaxis and the up-regulation of CD18. In addition, pretreatment of cells with the H19A mutant inhibited the ability of MGSA to induce elastase release and chemotaxis and to increase intracellular calcium. However, competition binding studies in cells transfected with the CXCR2 receptor and in neutrophils demonstrate that the receptor affinity of the H19A mutant is only 13-fold less than that of wild-type MGSA. These studies suggest that the mutant MGSA is defective in activating signaling through the receptor and indicate that binding to the receptor is not sufficient to activate a biologic response. The dissociation between receptor binding and activation for this mutant suggests that it should be possible to design antagonists of MGSA that may be of clinical utility.

Published

1998

86. Backbone dynamics of the EGF-like domain of heregulin-alpha.

Author

Fairbrother WJ, Liu J, Pisacane PI, Sliwkowski MX, and Palmer AG 3rd

Subjects

Magnetic Resonance Spectroscopy, Mathematics, Models, Molecular, Neuregulins, Protein Conformation, Ultracentrifugation, Epidermal Growth Factor chemistry, Glycoproteins chemistry

Abstract

The backbone dynamics of the 63 residue epidermal growth factor (EGF)-like domain of heregulin-alpha (HRG-alpha) have been characterized by measurement of longitudinal relaxation rate constants (R1), transverse relaxation rate constants (R2), and steady-state ¿1H¿-15N nuclear Overhauser effects for the 15N nuclear spins using proton-detected heteronuclear NMR spectroscopy. Analysis of the R2/R1 ratios in conjunction with the known structure of the HRG-alpha EGF-like domain yields a rotational correlation time of approximately 8.4 ns, suggesting that the protein aggregates under the solution conditions used (3.8 mM protein, 50 mM sodium acetate, pH 4.5, 20 degreesC), and that it tumbles with an axially symmetric diffusion tensor (D parallel/D perpendicular=1.4). Sedimentation equilibrium experiments confirm that the EGF-like domain of HRG-alpha undergoes weak self-association under these conditions and are consistent with a simple monomer-dimer equilibrium with a dimer-dissociation constant Kd=1.6(+/-0.4) mM. The relaxation data were analyzed using a reduced spectral density mapping approach to avoid systematic effects of aggregation on the usual model-free formalism. The reduced spectral densities show that residues near the N terminus (residues 3 to 5 and 7 to 12), in the Omega-loop between beta-strands 2 and 3 (residues 24 to 31), and in particular the C-terminal 13 residues (residues 51 to 63), have significant mobility on a picosecond/nanosecond time-scale. In addition, conformational exchange on a microsecond time-scale was identified for residues 44 to 46 on the basis of observed differences in R2 at 11.7 and 14.1 T. The mobility identified near the N terminus and in the vicinity of residues 44 to 46 may be important in allowing the interactions of heregulin with multiple receptors., (Copyright 1998 Academic Press.)

Published

1998

87. Solution structure of the heparin-binding domain of vascular endothelial growth factor.

Author

Fairbrother WJ, Champe MA, Christinger HW, Keyt BA, and Starovasnik MA

Subjects

Amino Acid Sequence, Binding Sites, Endothelial Growth Factors genetics, Endothelial Growth Factors metabolism, Lymphokines genetics, Lymphokines metabolism, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Peptide Fragments genetics, Peptide Fragments metabolism, Protein Conformation, Protein Folding, Recombinant Proteins chemistry, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Endothelial Growth Factors chemistry, Heparin metabolism, Lymphokines chemistry, Peptide Fragments chemistry

Abstract

Background: Vascular endothelial growth factor (VEGF) is an endothelial cell-specific mitogen and is a potent angiogenic and vascular permeabilizing factor. VEGF is also an important mediator of pathological angiogenesis associated with cancer, rheumatoid arthritis and proliferative retinopathy. The binding of VEGF to its two known receptors, KDR and Flt-1, is modulated by cell-surface-associated heparin-like glycosaminoglycans and exogenous heparin or heparan sulfate. Heparin binding to VEGF165, the most abundantly expressed isoform of VEGF, has been localized to the carboxy-terminal 55 residues; plasmin cleavage of VEGF165 yields a homodimeric 110-residue amino-terminal receptor-binding domain (VEGF110) and two 55-residue carboxy-terminal heparin-binding fragments. The endothelial cell mitogenic potency of VEGF110 is decreased significantly relative to VEGF165, indicating that the heparin-binding domains are critical for stimulating endothelial cell proliferation., Results: The solution structure of the 55-residue heparin-binding domain of VEGF165 has been solved using data from two-dimensional homonuclear and three-dimensional heteronuclear NMR spectroscopy. The structure has two subdomains, each containing two disulfide bridges and a short two-stranded antiparallel beta sheet; the carboxy-terminal subdomain also contains a short alpha helix. Hydrophobic interactions are limited to sidechains packing against the disulfide bridges., Conclusions: The heparin-binding domain of VEGF has no significant sequence or structural similarity to any known proteins and thus represents a novel heparin-binding domain. Most of the positively charged amino acid sidechains are localized on one side of the carboxy-terminal subdomain or on an adjacent disordered loop in the amino-terminal subdomain. The observed distribution of surface charges suggests that these residues constitute a heparin interaction site.

Published

1998

88. Binding interaction of the heregulinbeta egf domain with ErbB3 and ErbB4 receptors assessed by alanine scanning mutagenesis.

Author

Jones JT, Ballinger MD, Pisacane PI, Lofgren JA, Fitzpatrick VD, Fairbrother WJ, Wells JA, and Sliwkowski MX

Subjects

Alanine, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Carrier Proteins chemistry, Carrier Proteins ultrastructure, Enzyme Activation, Glycoproteins chemistry, Glycoproteins ultrastructure, Humans, Ligands, Models, Molecular, Mutagenesis, Site-Directed, Nuclear Magnetic Resonance, Biomolecular, Phosphorylation, Protein Binding, Protein Structure, Secondary, Receptor, ErbB-3, Receptor, ErbB-4, Signal Transduction, Structure-Activity Relationship, Tumor Cells, Cultured, Carrier Proteins metabolism, ErbB Receptors metabolism, Glycoproteins metabolism, Neuregulin-1, Proto-Oncogene Proteins metabolism

Abstract

Individual residues of the heregulinbeta (HRG) egf domain were mutated to alanine and displayed monovalently on phagemid particles as gene III fusion proteins. Wild type HRGbeta egf domain displayed on phage was properly folded as evidenced by its ability to bind ErbB3 and ErbB4 receptor-IgG fusion proteins with affinities close to those measured for bacterially produced HRGbeta egf domain. Binding to ErbB3 and ErbB4 receptors was affected by mutation of residues throughout the egf domain; including the NH2 terminus (His2 and Leu3), the two beta-turns (Val15-Gly18 and Gly42-Gln46), and some discontinuous residues (including Leu3, Val4, Phe13, Val23, and Leu33) that form a patch on the major beta-sheet and the COOH-terminal region (Tyr48 and Met50-Phe53). Binding affinity was least changed by mutations throughout the Omega-loop and the second strand of the major beta-sheet. More mutants had greater affinity loss for ErbB3 compared with ErbB4 implying that it has more stringent binding requirements. Many residues important for HRG binding to its receptors correspond to critical residues for epidermal growth factor (EGF) and transforming growth factor alpha binding to the EGF receptor. Specificity may be determined in part by bulky groups that prevent binding to the unwanted receptor. All of the mutants tested were able to induce phosphorylation and mitogen-activated protein kinase activation through ErbB4 receptors and were able to modulate a transphosphorylation signal from ErbB3 to ErbB2 in MCF7 cells. An understanding of binding similarities and differences among the EGF family of ligands may facilitate the development of egf-like analogs with broad or narrow specificity.

Published

1998

89. Selection of heregulin variants having higher affinity for the ErbB3 receptor by monovalent phage display.

Author

Ballinger MD, Jones JT, Lofgren JA, Fairbrother WJ, Akita RW, Sliwkowski MX, and Wells JA

Subjects

Amino Acid Sequence, Bacteriophage M13, Binding Sites, Ligands, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Peptide Library, Protein Binding, Receptor, ErbB-3, Recombinant Proteins, Structure-Activity Relationship, Carrier Proteins chemistry, ErbB Receptors metabolism, Glycoproteins chemistry, Neuregulin-1, Proto-Oncogene Proteins metabolism

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

90. Solution structure of the fourth metal-binding domain from the Menkes copper-transporting ATPase.

Author

Gitschier J, Moffat B, Reilly D, Wood WI, and Fairbrother WJ

Subjects

Adenosine Triphosphatases chemistry, Amino Acid Sequence, Apoproteins chemistry, Apoproteins ultrastructure, Binding Sites, Carrier Proteins chemistry, Copper-Transporting ATPases, Cysteine chemistry, Humans, Membrane Proteins ultrastructure, Metals, Heavy, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Secondary, Protein Structure, Tertiary, Recombinant Proteins, Sequence Alignment, Sequence Homology, Amino Acid, Solutions, Structure-Activity Relationship, Adenosine Triphosphatases ultrastructure, Carrier Proteins ultrastructure, Cation Transport Proteins, Copper, Recombinant Fusion Proteins

Abstract

Menkes disease is an X-linked disorder in copper transport that results in death during early childhood. The solution structures of both apo and Ag(I)-bound forms of the fourth metal-binding domain (mbd4) from the Menkes copper-transporting ATPase have been solved. The 72-residue mbd4 has a ferredoxin-like beta alpha beta beta alpha beta fold. Structural differences between the two forms are limited to the metal-binding loop, which is disordered in the apo structure but well ordered in the Ag(I)-bound structure. Ag(I) binds in a linear bicoordinate manner to the two Cys residues of the conserved GMTCxxC motif; Cu(I) likely coordinates in a similar manner. Menkes mbd4 is thus the first bicoordinate copper-binding protein to be characterized structurally. Sequence comparisons with other heavy-metal-binding domains reveal a conserved hydrophobic core and metal-binding motif.

Published

1998

91. Potent alpha 4 beta 1 peptide antagonists as potential anti-inflammatory agents.

Author

Jackson DY, Quan C, Artis DR, Rawson T, Blackburn B, Struble M, Fitzgerald G, Chan K, Mullins S, Burnier JP, Fairbrother WJ, Clark K, Berisini M, Chui H, Renz M, Jones S, and Fong S

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal metabolism, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Antibodies, Monoclonal immunology, Binding, Competitive, Cell Adhesion drug effects, Cell Movement drug effects, Integrin alpha4beta1, Integrins immunology, Integrins metabolism, Lymphocytes drug effects, Magnetic Resonance Spectroscopy, Mass Spectrometry, Mice, Models, Molecular, Molecular Structure, Peptides, Cyclic chemistry, Peptides, Cyclic metabolism, Peptides, Cyclic pharmacology, Receptors, Lymphocyte Homing immunology, Receptors, Lymphocyte Homing metabolism, Structure-Activity Relationship, Vascular Cell Adhesion Molecule-1 chemistry, Vascular Cell Adhesion Molecule-1 immunology, Vascular Cell Adhesion Molecule-1 metabolism, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Integrins antagonists & inhibitors, Lymphocytes physiology, Peptides, Cyclic chemical synthesis, Receptors, Lymphocyte Homing antagonists & inhibitors

Abstract

The migration, adhesion, and subsequent extravasation of leukocytes into inflamed tissues contribute to the pathogenesis of a variety of inflammatory diseases including asthma, rheumatoid arthritis, inflammatory bowel disease, and multiple sclerosis. The integrin adhesion receptor alpha 4 beta 1 expressed on leukocytes binds to the extracellular matrix protein fibronectin and to the cytokine inducible vascular cell adhesion molecule-1 (VCAM-1) at inflamed sites. Binding of alpha 4 beta 1 to VCAM-1 initiates firm adhesion of the leukocyte to the vascular endothelium followed by extravasation into the tissue. Monoclonal antibodies generated against either alpha 4 beta 1 or VCAM-1 can moderate this inflammatory response in a variety of animal models. Recently peptides containing a consensus LDV sequence based on the connecting segment-1 (CS-1) of fibronectin and cyclic peptides containing an RCD motif have shown promise in modulating leukocyte migration and inflammation presumably by blocking the interaction of alpha 4 beta 1 with VCAM-1. Here we describe novel, highly potent, cyclic peptides that competitively inhibit alpha 4 beta 1 binding to VCAM-1 and fibronectin at sub nanomolar concentrations. The structure of a representative analog was determined via NMR spectroscopy and used to facilitate optimization of peptide leads. The peptides discussed here utilize similar functional groups as the binding epitope of VCAM-1, inhibit lymphocyte migration in vivo, and are highly selective for alpha 4 beta 1. Furthermore the structure--activity relationships described here have provided a template for the structure-based design of small molecule antagonists of alpha 4 beta 1-mediated cell adhesion processes.

Published

1997

92. 1H, 13C, and 15N backbone assignment and secondary structure of the receptor-binding domain of vascular endothelial growth factor.

Author

Fairbrother WJ, Champe MA, Christinger HW, Keyt BA, and Starovasnik MA

Subjects

Binding Sites, Crystallization, Dimerization, Endothelial Growth Factors metabolism, Humans, Hydrogen-Ion Concentration, Lymphokines metabolism, Receptors, Vascular Endothelial Growth Factor, Recombinant Proteins, Vascular Endothelial Growth Factor A, Vascular Endothelial Growth Factors, Endothelial Growth Factors chemistry, Lymphokines chemistry, Magnetic Resonance Spectroscopy, Protein Structure, Secondary, Receptor Protein-Tyrosine Kinases metabolism, Receptors, Growth Factor metabolism

Abstract

Nearly complete sequence-specific 1H, 13C, and 15N resonance assignments are reported for the backbone atoms of the receptor-binding domain of vascular endothelial growth factor (VEGF), a 23-kDa homodimeric protein that is a major regulator of both normal and pathological angiogenesis. The assignment strategy relied on the use of seven 3D triple-resonance experiments [HN(CO)CA, HNCA, HNCO, (HCA)CONH, HN(COCA)HA, HN(CA)HA, and CBCA-(CO)NH] and a 3D 15N-TOCSY-HSQC experiment recorded on a 0.5 mM (12 mg/mL) sample at 500 MHz, pH 7.0, 45 degrees C. Under these conditions, 15N relaxation data show that the protein has a rotational correlation time of 15.0 ns. Despite this unusually long correlation time, assignments were obtained for 94 of the 99 residues; 8 residues lack amide 1H and 15N assignments, presumably due to rapid exchange of the amide 1H with solvent under the experimental conditions used. The secondary structure of the protein was deduced from the chemical shift indices of the 1H alpha, 13C alpha, 13C beta, and 13CO nuclei, and from analysis of backbone NOEs observed in a 3D 15N-NOESY-HSQC spectrum. Two helices and a significant amount of beta-sheet structure were identified, in general agreement with the secondary structure found in a recently determined crystal structure of a similar VEGF construct [Muller YA et al., 1997, Proc Natl Acad Sci USA 94:7192-7197].

Published

1997

93. Monomeric variants of IL-8: effects of side chain substitutions and solution conditions upon dimer formation.

Author

Lowman HB, Fairbrother WJ, Slagle PH, Kabakoff R, Liu J, Shire S, and Hébert CA

Subjects

Amino Acid Sequence, Antigens, CD chemistry, Biopolymers, Humans, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Protein Conformation, Protein Folding, Receptors, Interleukin chemistry, Receptors, Interleukin-8A, Receptors, Interleukin-8B, Solutions, X-Ray Diffraction, Antigens, CD metabolism, Interleukin-8 chemistry, Receptors, Interleukin metabolism

Abstract

IL-8 dimers have been observed in NMR and X-ray structures of the protein. We have engineered IL-8 monomers by mutations of residues throughout the dimer interface, which introduce hindrance determinants to dimerization. These IL-8 variants are shown by NMR to have wild-type monomer folding, but by ultracentrifugation to have a range of dimerization constants from microM to mM, as compared with a dimerization constant of about 10 microM for wild-type IL-8, under physiological salt and temperature conditions. The monomeric variants of IL-8 bind the erythrocyte chemokine receptor DARC, as well as the neutrophil IL-8 receptors CXCR1 and CXCR2 with affinities similar to that of wild-type IL-8. In addition, the monomeric variants were shown to have agonist activity, with similar potency to wild-type, in both Ca(2+)-flux assays on CXCR1 and CXCR2 transfected cells, and in chemotaxis assays on neutrophils. Thus, these variants confirm that monomeric IL-8 is functionally equivalent to wild-type in vitro assays. We have also investigated the effects of various solution conditions upon IL-8 dimer formation using analytical ultracentrifugation. At salt concentrations, temperatures, and pH conditions lower than physiological, the dimerization affinity of IL-8 is greatly enhanced. This suggests that, under some conditions, IL-8 dimer formation may occur at concentrations of IL-8 considerably lower than 10 microM, with consequences in vivo that are yet to be determined.

Published

1997

94. Molecular approaches to structure-function analysis of interleukin-8.

Author

Fairbrother WJ and Lowman HB

Subjects

Amino Acid Sequence, Animals, Antigens, CD metabolism, Binding, Competitive, Cell Line, Chemotactic Factors chemistry, Chemotactic Factors metabolism, Escherichia coli genetics, Gene Expression, Growth Substances chemistry, Growth Substances metabolism, Interleukin-8 genetics, Interleukin-8 isolation & purification, Models, Molecular, Molecular Sequence Data, Mutation genetics, Peptides chemistry, Peptides metabolism, Plasmids, Receptors, Interleukin metabolism, Receptors, Interleukin-8A, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Sequence Alignment, Structure-Activity Relationship, beta-Thromboglobulin, Interleukin-8 chemistry, Interleukin-8 metabolism

Published

1997

95. Solution structure of the E-domain of staphylococcal protein A.

Author

Starovasnik MA, Skelton NJ, O'Connell MP, Kelley RF, Reilly D, and Fairbrother WJ

Subjects

Amino Acid Sequence, Immunoglobulin Fc Fragments metabolism, Kinetics, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Sequence Alignment, Software, Staphylococcal Protein A metabolism, Staphylococcal Protein A chemistry

Abstract

The E-domain of staphylococcal protein A is one of five homologous IgG-binding domains designated E, D, A, B, and C that comprise the extracellular portion of protein A. The E-domain binds tightly to Fc fragments of IgG and binds certain Fv fragments with micromolar affinity. To explore further the structural features of Fc binding by protein A, and as a first step in developing a structural understanding of E-domain/Fv complex formation, we have determined the solution structure of the uncomplexed E-domain using 2D homonuclear and heteronuclear NMR spectroscopy. Complete 1H and 15N resonance assignments were obtained, and the structure was determined from 383 NOE-derived distance restrains, 34 phi and 19 chi 1 dihedral angle restraints, and 54 restraints for 27 H-bonds. 3JH alpha-H beta coupling constants and long-range NOEs involving Phe11 indicate the side chain exists in more than one conformation with differing chi 1 values. NOE restraints that were incompatible with chi 1 = -60 degrees were removed from one set of structure calculations, and those incompatible with chi 1 = 180 degrees were removed from a second set to allow Phe11 to explore both rotamer wells. Thus, two sets of 20 final structures, having no distance or dihedral angle restraint violations greater than 0.12 A or 1.6 degrees, respectively, represent the solution structure of the E-domain. Backbone atomic rms differences with respect to the mean coordinates for each set of 20 structures for residues 8-53 averaged 0.41 +/- 0.06 and 0.35 +/- 0.06 A. No significant differences in the overall structure result from the different orientations of Phe11. The solution structure of the E-domain consists of three alpha-helices that pack together to form a compact helical bundle. A detailed comparison between the E-domain ensembles and the previously determined structure for the B-domain in complex with Fc indicates that only the 180 degrees chi 1 rotamer of Phe11 is competent for binding; the -60 degrees chi 1 rotamer must reorient to 180 degrees to create a cavity that is filled by Ile253 from the CH2 domain of Fc in the Fc-bound complex.

Published

1996

96. Exchanging interleukin-8 and melanoma growth-stimulating activity receptor binding specificities.

Author

Lowman HB, Slagle PH, DeForge LE, Wirth CM, Gillece-Castro BL, Bourell JH, and Fairbrother WJ

Subjects

Amino Acid Sequence, Animals, Antigens, CD biosynthesis, Binding Sites, Cell Line, Chemokine CXCL1, Chemokines metabolism, Chemotactic Factors biosynthesis, Chemotactic Factors chemistry, Cloning, Molecular, Computer Simulation, Escherichia coli, Growth Substances biosynthesis, Growth Substances chemistry, Humans, Interleukin-8 biosynthesis, Interleukin-8 chemistry, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Point Mutation, Protein Conformation, Rabbits, Receptors, Cytokine biosynthesis, Receptors, Interleukin biosynthesis, Receptors, Interleukin-8A, Receptors, Interleukin-8B, Recombinant Proteins biosynthesis, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Sequence Homology, Amino Acid, Software, Substrate Specificity, Transfection, Antigens, CD metabolism, Chemokines, CXC, Chemotactic Factors metabolism, Growth Substances metabolism, Intercellular Signaling Peptides and Proteins, Interleukin-8 metabolism, Receptors, Cytokine metabolism, Receptors, Interleukin metabolism

Abstract

Interleukin-8 (IL-8), a CXC chemokine, is known to bring about chemotaxis and activation of neutrophils through high affinity binding to at least two distinct receptors, receptor-A and receptor-B. The IL-8 homolog melanoma growth stimulating activity (MGSA) is also active toward neutrophils. In contrast to IL-8, MGSA binds receptor-B with high affinity and binds receptor-A with approximately 400-fold lower affinity. Using the structure of IL-8 (Clore et al.(1990) Biochemistry, 29, 1689-1696; Baldwin et al. (1991) Proc. Natl. Acad. Sci. U.S.A. 88, 502-506) and the NMR-determined structure of MGSA (Fairbrother et al. (1994) J. Mol. Biol. 242, 252-270), we designed variants of both IL-8 and MGSA to investigate the basis of specificity for binding of these chemokines to the IL-8 receptors. The most outstanding structural difference between IL-8 and MGSA lies in the loop preceding the first beta-strand. When the corresponding (shorter) loop from MGSA was swapped into IL-8, both receptor-A and receptor-B binding affinities were significantly (>300-fold) reduced. However, with additional mutations that affect packing interactions, an IL-8 variant specific for receptor-B binding was produced. Conversely, when the same loop from IL-8 was swapped into MGSA, receptor-B binding was maintained with only a approximately 30-fold reduction in receptor-A affinity. Again, mutations affecting packing of the loop yielded a MGSA variant with high affinity for both receptors, like IL-8. Finally, we show, through point mutations in a monomeric IL-8 framework, that individual side chain substitutions can affect receptor specificity.

Published

1996

97. High-resolution solution structure of the EGF-like domain of heregulin-alpha.

Author

Jacobsen NE, Abadi N, Sliwkowski MX, Reilly D, Skelton NJ, and Fairbrother WJ

Subjects

Amino Acid Sequence, Disulfides chemistry, Humans, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Neuregulins, Peptides chemistry, Protein Structure, Secondary, Protein Structure, Tertiary, Recombinant Proteins, Sequence Alignment, Solutions, Glycoproteins chemistry

Abstract

The solution structure of the 63-residue heregulin-alpha (HRG-alpha) epidermal growth factor (EGF)-like domain, corresponding to residues 177-239 of HRG-alpha, has been determined to high resolution using data from two-dimensional and three-dimensional homo- and heteronuclear NMR spectroscopy. The structure is based on a total of 887 internuclear distance and dihedral restraints derived from data obtained using unlabeled and uniformly 15N-labeled protein samples, at pH 4.5, 20 degrees C. A total of 20 structures were calculated using a hybrid distance geometry-simulated annealing approach with the program DGII, followed by restrained molecular dynamics using the program DISCOVER. The average maximum violations are 0.12 +/- 0.01 angstroms and 1.4 +/- 0.3 degrees for distance and dihedral restraints, respectively. The backbone (N,C(alpha),C) atomic rms distribution about the mean coordinates for residues 3-23 and 31-49 is 0.29 +/- 0/07 angstroms. The N-and C-terminal residues (1-2 and 50-63) and 24-30 are disordered. Comparison of the HRG-alpha EGF-like domain structure with the previously determined structure of human EGF [Hommel et al. (1992) J. Mol. Biol. 227, 271-282] reveals a high degree of structural similarity; excluding the N-terminal region (residues 1-13), the disordered phi-loop region (residues 24-30) that contains a three-residue insertion in HRG-alpha relative to hEGF, and the disordered C-terminal region (residues 50-63), the C(alpha) alignment between the HRG-alpha and hEGF minimized mean structures has a rms difference of approximately 1 angstrom. In HRG-alpha the N-terminal residues 2-6 form a well-defined beta strand rather than being disordered as found for hEGF. This structural difference correlates with functional data which suggest that the N-terminal region of the HRG-alpha EGF-like domain is responsible for the observed receptor specificity differences between HRG-alpha and EGF.

Published

1996

98. Structure of the saponin adjuvant QS-21 and its base-catalyzed isomerization product by 1H and natural abundance 13C NMR spectroscopy.

Author

Jacobsen NE, Fairbrother WJ, Kensil CR, Lim A, Wheeler DA, and Powell MF

Subjects

Carbohydrate Conformation, Carbohydrate Sequence, Chromatography, High Pressure Liquid, Fatty Acids chemistry, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Oligosaccharides chemistry, Stereoisomerism, Terpenes chemistry, Adjuvants, Immunologic chemistry, Saponins chemistry

Abstract

The saponin QS-21, derived from the bark of the Quillaja saponaria Molina tree, has shown great potential as an adjuvant with a number of vaccines. Kinetic studies carried out to establish the stability of vaccine formulations show that commercially supplied QS-21 (primarily QS-21A) is converted slowly at pH 5.5, and rapidly at higher pH, to an equilibrium mixture of two regioisomers, QS-21A and QS-21B, in a ratio of 20:1. NMR studies show that QS-21A and QS-21B differ only in the point of attachment of the fatty acyl moiety to the fucose sugar ring. The major isomer, QS-21A, has the fatty acyl portion attached at the 4-hydroxyl group whereas the minor isomer, QS-21B, has the fatty acyl portion attached at the 3-hydroxyl group. The isomerization most likely involves ionization of the 3-hydroxy group and intramolecular acyl transfer from the 4-hydroxy group. The relative stereochemistry of the triterpene and the sugar anomeric centers is also established by NMR methods.

Published

1996

99. Minimization of a polypeptide hormone.

Author

Li B, Tom JY, Oare D, Yen R, Fairbrother WJ, Wells JA, and Cunningham BC

Subjects

Amino Acid Sequence, Atrial Natriuretic Factor genetics, Atrial Natriuretic Factor immunology, Atrial Natriuretic Factor metabolism, Base Sequence, Cell Line, Cyclic GMP metabolism, Epitopes, Guanylate Cyclase metabolism, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Protein Conformation, Receptors, Atrial Natriuretic Factor metabolism, Atrial Natriuretic Factor chemistry, Protein Engineering

Abstract

A stepwise approach for reducing the size of a polypeptide hormone, atrial natriuretic peptide (ANP), from 28 residues to 15 while retaining high biopotency is described. Systematic structural and functional analysis identified a discontinuous functional epitope for receptor binding and activation, most of which was placed onto a smaller ring (Cys6 to Cys17) that was created by repositioning the ANP native disulfide bond (Cys7 to Cys23). High affinity was subsequently restored by optimizing the remaining noncritical residues by means of phage display. Residues that flanked the mini-ring structure were then deleted in stages, and affinity losses were rectified by additional phage-sorting experiments. Thus, structural and functional data on hormones, coupled with phage display methods, can be used to shrink the hormones to moieties more amendable to small-molecule design.

Published

1995

100. Growth hormone secretagogues: characterization, efficacy, and minimal bioactive conformation.

Author

McDowell RS, Elias KA, Stanley MS, Burdick DJ, Burnier JP, Chan KS, Fairbrother WJ, Hammonds RG, Ingle GS, Jacobsen NE, Mortensen DL, Rawson TE, Won WB, Clark RG, and Somers TC

Subjects

Amino Acid Sequence, Animals, Consensus Sequence, Female, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Pituitary Gland, Anterior metabolism, Protein Structure, Secondary, Rats, Rats, Sprague-Dawley, Secretory Rate, Structure-Activity Relationship, Growth Hormone metabolism, Hormones chemistry, Oligopeptides chemistry, Peptides, Cyclic chemistry

Abstract

Another class of growth hormone (GH) secretagogues has been discovered by altering the backbone structure of a flexible linear GH-releasing peptide (GHRP). In vitro and in vivo characterization confirms these GH secretagogues as the most potent and smallest (M(r) < 500) reported. Anabolic efficacy is demonstrated in rodents with intermittent delivery. A convergent model of the bioactive conformation of GHRPs is developed and is supported by the NMR structure of a highly potent cyclic analog of GHRP-2. The model and functional data provide a logical framework for the further design of low-molecular weight secretagogues and illustrate the utility of an interdisciplinary approach to elucidating potential bound-state conformations of flexible peptide ligands.

Published

1995