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

1. The discovery and structural basis of two distinct state-dependent inhibitors of BamA.

Author

Sun D, Storek KM, Tegunov D, Yang Y, Arthur CP, Johnson M, Quinn JG, Liu W, Han G, Girgis HS, Alexander MK, Murchison AK, Shriver S, Tam C, Ijiri H, Inaba H, Sano T, Yanagida H, Nishikawa J, Heise CE, Fairbrother WJ, Tan MW, Skelton N, Sandoval W, Sellers BD, Ciferri C, Smith PA, Reid PC, Cunningham CN, Rutherford ST, and Payandeh J

Subjects

Binding Sites, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Protein Conformation, Peptides chemistry, Peptides metabolism, Peptides pharmacology, Protein Binding, Models, Molecular, Escherichia coli Proteins metabolism, Escherichia coli Proteins chemistry, Escherichia coli Proteins genetics, Bacterial Outer Membrane Proteins metabolism, Bacterial Outer Membrane Proteins chemistry, Escherichia coli metabolism, Escherichia coli drug effects

Abstract

BamA is the central component of the essential β-barrel assembly machine (BAM), a conserved multi-subunit complex that dynamically inserts and folds β-barrel proteins into the outer membrane of Gram-negative bacteria. Despite recent advances in our mechanistic and structural understanding of BamA, there are few potent and selective tool molecules that can bind to and modulate BamA activity. Here, we explored in vitro selection methods and different BamA/BAM protein formulations to discover peptide macrocycles that kill Escherichia coli by targeting extreme conformational states of BamA. Our studies show that Peptide Targeting BamA-1 (PTB1) targets an extracellular divalent cation-dependent binding site and locks BamA into a closed lateral gate conformation. By contrast, PTB2 targets a luminal binding site and traps BamA into an open lateral gate conformation. Our results will inform future antibiotic discovery efforts targeting BamA and provide a template to prospectively discover modulators of other dynamic integral membrane proteins., (© 2024. The Author(s).)

Published

2024

2. Potency-Enhanced Peptidomimetic VHL Ligands with Improved Oral Bioavailability.

Author

Wu H, Murray J, Ishisoko N, Frommlet A, Deshmukh G, DiPasquale A, Mulvihill MM, Zhang D, Quinn JG, Blake RA, Fairbrother WJ, and Fuhrmann J

Subjects

Humans, Ligands, Structure-Activity Relationship, Administration, Oral, Animals, Von Hippel-Lindau Tumor Suppressor Protein metabolism, Von Hippel-Lindau Tumor Suppressor Protein chemistry, Peptidomimetics chemistry, Peptidomimetics pharmacokinetics, Peptidomimetics pharmacology, Biological Availability

Abstract

The von Hippel-Lindau (VHL) protein plays a pivotal role in regulating the hypoxic stress response and has been extensively studied and utilized in the targeted protein degradation field, particularly in the context of bivalent degraders. In this study, we present a comprehensive peptidomimetic structure-activity relationship (SAR) approach, combined with cellular NanoBRET target engagement assays to enhance the existing VHL ligands. Through systematic modifications of the molecule, we identified the 1,2,3-triazole group as an optimal substitute of the left-hand side amide bond that yields 10-fold higher binding activity. Moreover, incorporating conformationally constrained alterations on the methylthiazole benzylamine moiety led to the development of highly potent VHL ligands with picomolar binding affinity and significantly improved oral bioavailability. We anticipate that our optimized VHL ligand, GNE7599 , will serve as a valuable tool compound for investigating the VHL pathway and advancing the field of targeted protein degradation.

Published

2024

3. Targeted degradation via direct 26S proteasome recruitment.

Author

Bashore C, Prakash S, Johnson MC, Conrad RJ, Kekessie IA, Scales SJ, Ishisoko N, Kleinheinz T, Liu PS, Popovych N, Wecksler AT, Zhou L, Tam C, Zilberleyb I, Srinivasan R, Blake RA, Song A, Staben ST, Zhang Y, Arnott D, Fairbrother WJ, Foster SA, Wertz IE, Ciferri C, and Dueber EC

Subjects

Cryoelectron Microscopy, Proteasome Endopeptidase Complex metabolism, Proteolysis, Ligases metabolism, Ubiquitin-Protein Ligases metabolism, Nuclear Proteins metabolism, Transcription Factors metabolism

Abstract

Engineered destruction of target proteins by recruitment to the cell's degradation machinery has emerged as a promising strategy in drug discovery. The majority of molecules that facilitate targeted degradation do so via a select number of ubiquitin ligases, restricting this therapeutic approach to tissue types that express the requisite ligase. Here, we describe a new strategy of targeted protein degradation through direct substrate recruitment to the 26S proteasome. The proteolytic complex is essential and abundantly expressed in all cells; however, proteasomal ligands remain scarce. We identify potent peptidic macrocycles that bind directly to the 26S proteasome subunit PSMD2, with a 2.5-Å-resolution cryo-electron microscopy complex structure revealing a binding site near the 26S pore. Conjugation of this macrocycle to a potent BRD4 ligand enabled generation of chimeric molecules that effectively degrade BRD4 in cells, thus demonstrating that degradation via direct proteasomal recruitment is a viable strategy for targeted protein degradation., (© 2022. Genentech, Inc. 2022.)

Published

2023

4. IAP antagonist GDC-0917 is more potent than Debio1143 in promoting cell death, c-IAP1 degradation and tumor growth inhibition.

Author

Alicke B, Varfolomeev E, Lee SHK, Frommlet A, Ubhayakar S, Quinn JG, Fairbrother WJ, Jones R, Gould SE, and Vucic D

Subjects

Apoptosis, Cell Death, Humans, Inhibitor of Apoptosis Proteins metabolism, Neoplasms drug therapy

Published

2022

5. Ribosomal Synthesis of Macrocyclic Peptides with Linear γ 4 - and β-Hydroxy-γ 4 -amino Acids.

Author

Adaligil E, Song A, Cunningham CN, and Fairbrother WJ

Subjects

Stereoisomerism, Amino Acids chemistry, Peptides, Cyclic chemical synthesis, Ribosomes chemistry

Abstract

Herein, we report the ribosomal elongation of linear γ 4 - and β-hydroxy-γ 4 -amino acids (statines) to expand the nonproteinogenic amino acid repertoire of natural product-like combinatorial peptide libraries. First, we demonstrated the successful ribosomal incorporation of four linear γ 4 -amino acids (γ 4 Gly, ( S )-γ 4 Ala, ( S )-γ 4 Nva, and ( R )-γ 4 Leu) into a 10-mer macrocyclic peptide scaffold. Given the promising effects reported for statines on the cell permeability of macrocyclic peptides, we also designed and tested the ribosomal incorporation of six statines derived from Ala and d-val. Four Ala-derived statines were successfully incorporated into peptides, and γ 4S Ala 3R-OH ( GP2 ) showed a similar efficiency of incorporation to that of ( S )-β 2 hAla and l-Ala. These new building blocks might confer the important pharmacological properties of protease resistance and membrane permeability to macrocyclic peptides and expand the diversity of future combinatorial peptide libraries that can be translated by the ribosome.

Published

2021

6. Primary Amine Tethered Small Molecules Promote the Degradation of X-Linked Inhibitor of Apoptosis Protein.

Author

den Besten W, Verma K, Yamazoe S, Blaquiere N, Phung W, Izrael-Tomasevic A, Mulvihill MM, Helgason E, Prakash S, Goncharov T, Vucic D, Dueber E, Fairbrother WJ, Wertz I, Yu K, and Staben ST

Subjects

Amines chemistry, Crystallography, X-Ray, Humans, Models, Molecular, Molecular Structure, Small Molecule Libraries chemistry, X-Linked Inhibitor of Apoptosis Protein metabolism, Amines pharmacology, Small Molecule Libraries pharmacology, X-Linked Inhibitor of Apoptosis Protein antagonists & inhibitors

Abstract

We hypothesized that the proximity-driven ubiquitylation of E3-interacting small molecules could affect the degradation of E3 ubiquitin ligases. A series of XIAP BIR2 domain-binding small molecules was modified to append a nucleophilic primary amine. This modification transforms XIAP binders into inducers of XIAP degradation. The degradation of XIAP is E1- and proteasome-dependent, dependent on the ligase function of XIAP, and is rescued by subtle modifications of the small molecule that would obviate ubiquitylation. We demonstrate in vitro ubiquitylation of the small molecule that is dependent on its interaction with XIAP. Taken together, these results demonstrate the designed ubiquitylation of an engineered small molecule and a novel approach for the degradation of E3 ubiquitin ligases.

Published

2021

7. Ribosomal Synthesis of Macrocyclic Peptides with β 2 - and β 2,3 -Homo-Amino Acids for the Development of Natural Product-Like Combinatorial Libraries.

Author

Adaligil E, Song A, Hallenbeck KK, Cunningham CN, and Fairbrother WJ

Subjects

Acylation, Amination, Amino Acids chemistry, Amino Acids metabolism, Biological Products chemistry, Biological Products metabolism, Macrocyclic Compounds chemistry, Peptides chemistry, Stereoisomerism, Macrocyclic Compounds metabolism, Peptide Library, Peptides metabolism, Ribosomes metabolism

Abstract

The development of large, natural-product-like, combinatorial macrocyclic peptide libraries is essential in the quest to develop therapeutics for "undruggable" cellular targets. Herein we report the ribosomal synthesis of macrocyclic peptides containing one or more β 2 -homo-amino acids (β 2 haa) to enable their incorporation into mRNA display-based selection libraries. We confirmed the compatibility of 14 β 2 -homo-amino acids, ( S )- and ( R )-stereochemistry, for single incorporation into a macrocyclic peptide with low to high translation efficiency. Interestingly, N-methylation of the backbone amide of β 2 haa prevented the incorporation of this amino acid subclass by the ribosome. Additionally, we designed and incorporated several α,β-disubstituted β 2,3 -homo-amino acids (β 2,3 haa) with different R-groups on the α- and β-carbons of the same amino acid. Incorporation of these β 2,3 haa enables increased diversity in a single position of a macrocyclic peptide without significantly increasing the overall molecular weight, which is an important consideration for passive cell permeability. We also successfully incorporated multiple ( S )-β 2 hAla into a single macrocycle with other non-proteinogenic amino acids, confirming that this class of β-amino acid is suitable for development of large scale macrocyclic peptide libraries.

Published

2021

8. Discovery of A-1331852, a First-in-Class, Potent, and Orally-Bioavailable BCL-X L Inhibitor.

Author

Wang L, Doherty GA, Judd AS, Tao ZF, Hansen TM, Frey RR, Song X, Bruncko M, Kunzer AR, Wang X, Wendt MD, Flygare JA, Catron ND, Judge RA, Park CH, Shekhar S, Phillips DC, Nimmer P, Smith ML, Tahir SK, Xiao Y, Xue J, Zhang H, Le PN, Mitten MJ, Boghaert ER, Gao W, Kovar P, Choo EF, Diaz D, Fairbrother WJ, Elmore SW, Sampath D, Leverson JD, and Souers AJ

Abstract

Herein we describe the discovery of A-1331852, a first-in-class orally active BCL-X L inhibitor that selectively and potently induces apoptosis in BCL-X L -dependent tumor cells. This molecule was generated by re-engineering our previously reported BCL-X L inhibitor A-1155463 using structure-based drug design. Key design elements included rigidification of the A-1155463 pharmacophore and introduction of sp 3 -rich moieties capable of generating highly productive interactions within the key P4 pocket of BCL-X L . A-1331852 has since been used as a critical tool molecule for further exploring BCL-2 family protein biology, while also representing an attractive entry into a drug discovery program., Competing Interests: The authors declare the following competing financial interest(s): AbbVie and Genentech participated in interpretation of data and review and approval of publication. L.W., G.A.D., A.S.J., Z-F.T., T. M. H., R.R.F., X.S., M.B., A.R.K., X.W., M.D.W., N.D.C., S.S., D.C.P., R.A.J., P.N., M.L.S., S.K.T., Y.X., J.X., H.Z., P.N.L., M.J.M., E.R.B., W.G., P.K., S.W.E., J.D.L., and A.J.S. are employees of AbbVie, Inc. C.H.P. was an employee of AbbVie, Inc at the time of the study. E.C. and W.J.F. are employees of Genentech, Inc. J.A.F., D.D., and D.S. were employees of Genentech, Inc. at the time of the study.

Published

2020

9. Heterobifunctional Molecules Induce Dephosphorylation of Kinases-A Proof of Concept Study.

Author

Yamazoe S, Tom J, Fu Y, Wu W, Zeng L, Sun C, Liu Q, Lin J, Lin K, Fairbrother WJ, and Staben ST

Subjects

Cell Line, ErbB Receptors metabolism, Humans, Ligands, Proof of Concept Study, Protein Processing, Post-Translational drug effects, Proto-Oncogene Proteins c-akt metabolism, Small Molecule Libraries chemistry, Drug Discovery, Phosphorylation drug effects, Phosphotransferases metabolism, Protein Phosphatase 1 metabolism, Small Molecule Libraries pharmacology

Abstract

Heterobifunctional molecules have proven powerful tools to induce ligase-dependent ubiquitination of target proteins. We describe here a chemical strategy for controlling a different post-translational modification (PTM): phosphorylation. Heterobifunctional molecules were designed to promote the proximity of a protein phosphatase (PP1) to protein targets. The synthesized molecules induced the PP1-dependent dephosphorylation of AKT and EGFR. To our knowledge, this work represents the first examples of small molecules recruiting non-native partners to induce removal of a PTM.

Published

2020

10. Structures of autoinhibited and polymerized forms of CARD9 reveal mechanisms of CARD9 and CARD11 activation.

Author

Holliday MJ, Witt A, Rodríguez Gama A, Walters BT, Arthur CP, Halfmann R, Rohou A, Dueber EC, and Fairbrother WJ

Subjects

B-Cell CLL-Lymphoma 10 Protein metabolism, CARD Signaling Adaptor Proteins genetics, CARD Signaling Adaptor Proteins immunology, CARD Signaling Adaptor Proteins metabolism, Cryoelectron Microscopy, Guanylate Cyclase genetics, Guanylate Cyclase immunology, Guanylate Cyclase metabolism, HEK293 Cells, Humans, Mutation, Nuclear Magnetic Resonance, Biomolecular, Protein Conformation, alpha-Helical, Protein Multimerization immunology, Recombinant Proteins genetics, Recombinant Proteins immunology, Recombinant Proteins metabolism, Recombinant Proteins ultrastructure, Signal Transduction immunology, CARD Signaling Adaptor Proteins ultrastructure, Guanylate Cyclase ultrastructure, Protein Domains

Abstract

CARD9 and CARD11 drive immune cell activation by nucleating Bcl10 polymerization, but are held in an autoinhibited state prior to stimulation. Here, we elucidate the structural basis for this autoinhibition by determining the structure of a region of CARD9 that includes an extensive interface between its caspase recruitment domain (CARD) and coiled-coil domain. We demonstrate, for both CARD9 and CARD11, that disruption of this interface leads to hyperactivation in cells and to the formation of Bcl10-templating filaments in vitro, illuminating the mechanism of action of numerous oncogenic mutations of CARD11. These structural insights enable us to characterize two similar, yet distinct, mechanisms by which autoinhibition is relieved in the course of canonical CARD9 or CARD11 activation. We also dissect the molecular determinants of helical template assembly by solving the structure of the CARD9 filament. Taken together, these findings delineate the structural mechanisms of inhibition and activation within this protein family.

Published

2019

11. Cyclodextrin Reduces Intravenous Toxicity of a Model Compound.

Author

Mantik P, Xie M, Wong H, La H, Steigerwalt RW, Devanaboyina U, Ganem G, Shih D, Flygare JA, Fairbrother WJ, Chakravarty P, Russell D, Fernandez GE, and Narang AS

Subjects

2-Hydroxypropyl-beta-cyclodextrin administration & dosage, Animals, Cyclohexanes administration & dosage, Cyclohexanes pharmacokinetics, Dose-Response Relationship, Drug, Drug Interactions, Excipients administration & dosage, Hemolysis drug effects, Injections, Intravenous, Injections, Subcutaneous, Male, Maximum Tolerated Dose, Models, Animal, Pyrroles administration & dosage, Pyrroles pharmacokinetics, Rats, Solubility, 2-Hydroxypropyl-beta-cyclodextrin pharmacokinetics, Cyclohexanes toxicity, Drug Evaluation, Preclinical methods, Excipients pharmacokinetics, Pyrroles toxicity, Toxicity Tests, Acute methods

Abstract

Solubilization of new chemical entities for toxicity assessment must use excipients that do not negatively impact drug pharmacokinetics and toxicology. In this study, we investigated the tolerability of a model freebase compound, GDC-0152, solubilized by pH adjustment with succinic acid and complexation with hydroxypropyl-β-cyclodextrin (HP-β-CD) to enable intravenous use. Solubility, critical micelle concentration, and association constant with HP-β-CD were determined. Blood compatibility and potential for hemolysis were assessed in vitro. Local tolerability was assessed after intravenous and subcutaneous injections in rats. A pharmacokinetic study was conducted in rats after intravenous bolus administration. GDC-0152 exhibited pH-dependent solubility that was influenced by self-association. The presence of succinic acid increased solubility in a concentration-dependent manner. HP-β-CD alone also increased solubility, but the extent of solubility enhancement was significantly lower than succinic acid alone. Inclusion of HP-β-CD in the solution of GDC-0152 improved blood compatibility, reduced hemolytic potential by ∼20-fold in vitro, and increased the maximum tolerated dose to 80 mg/kg., (Copyright © 2019 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2019

12. Picomolar zinc binding modulates formation of Bcl10-nucleating assemblies of the caspase recruitment domain (CARD) of CARD9.

Author

Holliday MJ, Ferrao R, de Leon Boenig G, Estevez A, Helgason E, Rohou A, Dueber EC, and Fairbrother WJ

Subjects

B-Cell CLL-Lymphoma 10 Protein chemistry, B-Cell CLL-Lymphoma 10 Protein genetics, CARD Signaling Adaptor Proteins chemistry, CARD Signaling Adaptor Proteins genetics, Crystallography, X-Ray, Humans, NF-kappa B genetics, NF-kappa B metabolism, Polymerization, Protein Binding, Protein Domains, Signal Transduction, Zinc chemistry, p38 Mitogen-Activated Protein Kinases genetics, p38 Mitogen-Activated Protein Kinases metabolism, B-Cell CLL-Lymphoma 10 Protein metabolism, CARD Signaling Adaptor Proteins metabolism, Zinc metabolism

Abstract

The caspase recruitment domain-containing protein 9 (CARD9)-B-cell lymphoma/leukemia 10 (Bcl10) signaling axis is activated in myeloid cells during the innate immune response to a variety of diverse pathogens. This signaling pathway requires a critical caspase recruitment domain (CARD)-CARD interaction between CARD9 and Bcl10 that promotes downstream activation of factors, including NF-κB and the mitogen-activated protein kinase (MAPK) p38. Despite these insights, CARD9 remains structurally uncharacterized, and little mechanistic understanding of its regulation exists. We unexpectedly found here that the CARD in CARD9 binds to Zn 2+ with picomolar affinity-a concentration comparable with the levels of readily accessible Zn 2+ in the cytosol. NMR solution structures of the CARD9-CARD in the apo and Zn 2+ -bound states revealed that Zn 2+ has little effect on the ground-state structure of the CARD; yet the stability of the domain increased considerably upon Zn 2+ binding, with a concomitant reduction in conformational flexibility. Moreover, Zn 2+ binding inhibited polymerization of the CARD9-CARD into helical assemblies. Here, we also present a 20-Å resolution negative-stain EM (NS-EM) structure of these filamentous assemblies and show that they adopt a similar helical symmetry as reported previously for filaments of the Bcl10 CARD. Using both bulk assays and direct NS-EM visualization, we further show that the CARD9-CARD assemblies can directly template and thereby nucleate Bcl10 polymerization, a capacity considered critical to propagation of the CARD9-Bcl10 signaling cascade. Our findings indicate that CARD9 is a potential target of Zn 2+ -mediated signaling that affects Bcl10 polymerization in innate immune responses., Competing Interests: The authors declare that they have no conflicts of interest with the contents of this article., (© 2018 Holliday et al.)

Published

2018

13. Publisher Correction: A selective peptide inhibitor of Frizzled 7 receptors disrupts intestinal stem cells.

Author

Nile AH, de Sousa E Melo F, Mukund S, Piskol R, Hansen S, Zhou L, Zhang Y, Fu Y, Gogol EB, Kömüves LG, Modrusan Z, Angers S, Franke Y, Koth C, Fairbrother WJ, Wang W, de Sauvage FJ, and Hannoush RN

Abstract

The version of this article originally published contained older versions of the Life Sciences Reporting Summary and the Supplementary Text and Figures. The error has been corrected in the HTML and PDF versions of the article.

Published

2018

14. A selective peptide inhibitor of Frizzled 7 receptors disrupts intestinal stem cells.

Author

Nile AH, de Sousa E Melo F, Mukund S, Piskol R, Hansen S, Zhou L, Zhang Y, Fu Y, Gogol EB, Kömüves LG, Modrusan Z, Angers S, Franke Y, Koth C, Fairbrother WJ, Wang W, de Sauvage FJ, and Hannoush RN

Subjects

Animals, Binding Sites, CHO Cells, Cell Membrane metabolism, Cricetulus, Crystallography, X-Ray, Drug Discovery, Female, Flow Cytometry, HEK293 Cells, Humans, Intestines cytology, Lipids chemistry, Mice, Mice, Inbred C57BL, Peptides chemistry, Protein Binding, Protein Multimerization, Regeneration, Sequence Analysis, RNA, Signal Transduction drug effects, Stem Cells pathology, Surface Plasmon Resonance, Wnt Signaling Pathway, Frizzled Receptors antagonists & inhibitors, Frizzled Receptors metabolism, Intestines drug effects, Stem Cells drug effects

Abstract

Regeneration of the adult intestinal epithelium is mediated by a pool of cycling stem cells, which are located at the base of the crypt, that express leucine-rich-repeat-containing G-protein-coupled receptor 5 (LGR5). The Frizzled (FZD) 7 receptor (FZD7) is enriched in LGR5 + intestinal stem cells and plays a critical role in their self-renewal. Yet, drug discovery approaches and structural bases for targeting specific FZD isoforms remain poorly defined. FZD proteins interact with Wnt signaling proteins via, in part, a lipid-binding groove on the extracellular cysteine-rich domain (CRD) of the FZD receptor. Here we report the identification of a potent peptide that selectively binds to the FZD7 CRD at a previously uncharacterized site and alters the conformation of the CRD and the architecture of its lipid-binding groove. Treatment with the FZD7-binding peptide impaired Wnt signaling in cultured cells and stem cell function in intestinal organoids. Together, our data illustrate that targeting the lipid-binding groove holds promise as an approach for achieving isoform-selective FZD receptor inhibition.

Published

2018

15. Disruption of XIAP-RIP2 Association Blocks NOD2-Mediated Inflammatory Signaling.

Author

Goncharov T, Hedayati S, Mulvihill MM, Izrael-Tomasevic A, Zobel K, Jeet S, Fedorova AV, Eidenschenk C, deVoss J, Yu K, Shaw AS, Kirkpatrick DS, Fairbrother WJ, Deshayes K, and Vucic D

Subjects

Animals, Cells, Cultured, Humans, Inflammation metabolism, Inflammation pathology, Mice, Inbred C57BL, Mitogen-Activated Protein Kinases metabolism, Nod2 Signaling Adaptor Protein metabolism, Phosphorylation, Receptor-Interacting Protein Serine-Threonine Kinase 2 antagonists & inhibitors, Signal Transduction, Ubiquitin metabolism, Ubiquitination, X-Linked Inhibitor of Apoptosis Protein antagonists & inhibitors, Aminoquinolines pharmacology, Inflammation prevention & control, Nod2 Signaling Adaptor Protein antagonists & inhibitors, Protein Interaction Domains and Motifs drug effects, Receptor-Interacting Protein Serine-Threonine Kinase 2 metabolism, Sulfones pharmacology, X-Linked Inhibitor of Apoptosis Protein metabolism

Abstract

Inflammatory responses mediated by NOD2 rely on RIP2 kinase and ubiquitin ligase XIAP for the activation of nuclear factor κB (NF-κB), mitogen-activated protein kinases (MAPKs), and cytokine production. Herein, we demonstrate that selective XIAP antagonism blocks NOD2-mediated inflammatory signaling and cytokine production by interfering with XIAP-RIP2 binding, which removes XIAP from its ubiquitination substrate RIP2. We also establish that the kinase activity of RIP2 is dispensable for NOD2 signaling. Rather, the conformation of the RIP2 kinase domain functions to regulate binding to the XIAP-BIR2 domain. Effective RIP2 kinase inhibitors block NOD2 signaling by disrupting RIP2-XIAP interaction. Finally, we identify NOD2 signaling and XIAP-dependent ubiquitination sites on RIP2 and show that mutating these lysine residues adversely affects NOD2 pathway signaling. Overall, these results reveal a critical role for the XIAP-RIP2 interaction in NOD2 inflammatory signaling and provide a molecular basis for the design of innovative therapeutic strategies based on XIAP antagonists and RIP2 kinase inhibitors., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

16. Found in Translation: How Preclinical Research Is Guiding the Clinical Development of the BCL2-Selective Inhibitor Venetoclax.

Author

Leverson JD, Sampath D, Souers AJ, Rosenberg SH, Fairbrother WJ, Amiot M, Konopleva M, and Letai A

Subjects

Antineoplastic Agents pharmacology, Apoptosis, Bridged Bicyclo Compounds, Heterocyclic pharmacology, Drug Design, Humans, Sulfonamides pharmacology, Antineoplastic Agents therapeutic use, Bridged Bicyclo Compounds, Heterocyclic therapeutic use, Proto-Oncogene Proteins c-bcl-2 metabolism, Sulfonamides therapeutic use

Abstract

Since the discovery of apoptosis as a form of programmed cell death, targeting the apoptosis pathway to induce cancer cell death has been a high-priority goal for cancer therapy. After decades of effort, drug-discovery scientists have succeeded in generating small-molecule inhibitors of antiapoptotic BCL2 family proteins. Innovative medicinal chemistry and structure-based drug design, coupled with a strong fundamental understanding of BCL2 biology, were essential to the development of BH3 mimetics such as the BCL2-selective inhibitor venetoclax. We review a number of preclinical studies that have deepened our understanding of BCL2 biology and facilitated the clinical development of venetoclax. Significance: Basic research into the pathways governing programmed cell death have paved the way for the discovery of apoptosis-inducing agents such as venetoclax, a BCL2-selective inhibitor that was recently approved by the FDA and the European Medicines Agency. Preclinical studies aimed at identifying BCL2-dependent tumor types have translated well into the clinic thus far and will likely continue to inform the clinical development of venetoclax and other BCL2 family inhibitors. Cancer Discov; 7(12); 1376-93. ©2017 AACR., (©2017 American Association for Cancer Research.)

Published

2017

17. BCL2 mutations do not confer adverse prognosis in follicular lymphoma patients treated with rituximab.

Author

Huet S, Szafer-Glusman E, Tesson B, Xerri L, Fairbrother WJ, Mukhyala K, Bolen C, Punnoose E, Tonon L, Chassagne-Clément C, Feugier P, Viari A, Jardin F, Salles G, and Sujobert P

Subjects

Antineoplastic Agents therapeutic use, Female, Humans, Lymphoma, Follicular drug therapy, Male, Prognosis, Rituximab therapeutic use, Translocation, Genetic, Treatment Outcome, Lymphoma, Follicular genetics, Lymphoma, Follicular mortality, Mutation, Proto-Oncogene Proteins c-bcl-2 genetics

Abstract

BCL2 mutations have been suggested to confer an adverse prognosis to follicular lymphoma (FL) patients, but their prognostic value has not been assessed in patients treated with a rituximab-containing regimen. Here we evaluated the prognostic value of BCL2 mutations in a large prospective cohort of 252 patients with FL treated with immunochemotherapy in the PRIMA randomized trial. Using a DNA-targeted sequencing approach, we detected amino acid altering mutations in 135 patients (54%) and showed that these mutations were probably mediated by the over-activation of AICDA (activation-induced cytidine deaminase) in the context of the t(14;18) translocation. The BCL2 variants identified in PRIMA patients affected the BH1, BH2, and BH3 functional motifs at a lower frequency than the N-terminus and flexible loop domain, with mostly conservative aminoacid changes. With a median follow-up of 6.7 years, we did not observe any impact of BCL2 mutations either on overall survival or progression-free survival., (© 2017 Wiley Periodicals, Inc.)

Published

2017

18. From basic apoptosis discoveries to advanced selective BCL-2 family inhibitors.

Author

Ashkenazi A, Fairbrother WJ, Leverson JD, and Souers AJ

Subjects

Antineoplastic Agents chemistry, Humans, Molecular Structure, Neoplasms enzymology, Neoplasms pathology, Protein Interaction Domains and Motifs, Antineoplastic Agents therapeutic use, Apoptosis drug effects, Molecular Targeted Therapy methods, Neoplasms drug therapy, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors

Abstract

Members of the B cell lymphoma 2 (BCL-2) gene family have a central role in regulating programmed cell death by controlling pro-apoptotic and anti-apoptotic intracellular signals. In cancer, apoptosis evasion through dysregulation of specific BCL-2 family genes is a recurring event; accordingly, selective inhibition of specific anti-apoptotic BCL-2 family proteins represents an exciting therapeutic opportunity. A combination of nuclear magnetic resonance (NMR)-based screening and structure-based drug design has yielded the first bona fide BCL-2 homology 3 (BH3) mimetics, including the BCL-2 and BCL-X L dual antagonist navitoclax, which is the first BCL-2 family inhibitor to show efficacy in patients with cancer. Clinical experience with navitoclax prompted the generation of the highly selective BCL-2 inhibitor venetoclax, which is now approved in the United States for the treatment of patients with chronic lymphocytic leukaemia with 17p deletion who have received at least one prior therapy. Recent advances have also been made in the development of potent and selective inhibitors of BCL-X L and myeloid cell leukaemia 1 (MCL1), which are additional BCL-2 family members with established anti-apoptotic roles in cancer. Here we review the latest progress in direct and selective targeting of BCL-2 family proteins for cancer therapy.

Published

2017

19. A Phase I Dose-Escalation Study Evaluating the Safety Tolerability and Pharmacokinetics of CUDC-427, a Potent, Oral, Monovalent IAP Antagonist, in Patients with Refractory Solid Tumors.

Author

Tolcher AW, Bendell JC, Papadopoulos KP, Burris HA, Patnaik A, Fairbrother WJ, Wong H, Budha N, Darbonne WC, Peale F, Mamounas M, Royer-Joo S, Yu R, Portera CC, and Infante JR

Subjects

Administration, Oral, Adult, Aged, Aged, 80 and over, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Biomarkers, Cytokines blood, Cytokines metabolism, Drug Resistance, Neoplasm, Female, Humans, Male, Middle Aged, Neoplasms diagnosis, Neoplasms metabolism, Retreatment, Treatment Outcome, Antineoplastic Agents administration & dosage, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Neoplasms drug therapy

Abstract

Purpose: To determine the dose-limiting toxicities (DLT), adverse events (AE), pharmacokinetics, and preliminary evidence of antitumor activity of CUDC-427 (formerly GDC-0917), a selective antagonist of inhibitor of apoptosis (IAP) proteins., Experimental Design: Patients with advanced solid malignancies were treated with escalating doses of CUDC-427 orally on a daily 14-day on/7-day off schedule in 21-day cycles using a modified continuous reassessment method design. Blood samples were assayed to determine the pharmacokinetic properties, pharmacodynamic alterations of cellular IAP levels in peripheral blood mononuclear cells (PBMC), and monocyte chemoattractant protein-1 (MCP-1) levels., Results: Forty-two patients received 119 cycles of CUDC-427. Overall, the most common treatment-related toxicities were fatigue, nausea, vomiting, and rash. One DLT (grade 3 fatigue) occurred in a patient at 450 mg dose level during cycle 1, and 5 patients experienced AEs related to CUDC-427 that led to discontinuation and included grade 3 pruritus, and fatigue, and grade 2 drug hypersensitivity, pneumonitis, rash, and QT prolongation. The maximum planned dose of 600 mg orally daily for 2 weeks was reached, which allometrically scaled to exceed the IC90 in preclinical xenograft studies. Significant decreases in cIAP-1 levels in PBMCs were observed in all patients 6 hours after initial dosing. Responses included durable complete responses in one patient with ovarian cancer and one patient with MALT lymphoma., Conclusions: CUDC-427 can be administered safely at doses up to 600 mg daily for 14 days every 3 weeks. The absence of severe toxicities, inhibition of cIAP-1 in PBMC, and antitumor activity warrant further studies. Clin Cancer Res; 22(18); 4567-73. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published

2016

20. Expression Profile of BCL-2, BCL-XL, and MCL-1 Predicts Pharmacological Response to the BCL-2 Selective Antagonist Venetoclax in Multiple Myeloma Models.

Author

Punnoose EA, Leverson JD, Peale F, Boghaert ER, Belmont LD, Tan N, Young A, Mitten M, Ingalla E, Darbonne WC, Oleksijew A, Tapang P, Yue P, Oeh J, Lee L, Maiga S, Fairbrother WJ, Amiot M, Souers AJ, and Sampath D

Subjects

Animals, Bcl-2-Like Protein 11 metabolism, Bortezomib pharmacology, Cell Line, Tumor, Disease Models, Animal, Drug Resistance, Neoplasm genetics, Drug Therapy, Combination, Humans, Immunohistochemistry, Mice, Multiple Myeloma drug therapy, Multiple Myeloma metabolism, Protein Binding, Proto-Oncogene Proteins c-bcl-2 metabolism, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Bridged Bicyclo Compounds, Heterocyclic pharmacology, Gene Expression Regulation, Neoplastic, Multiple Myeloma genetics, Myeloid Cell Leukemia Sequence 1 Protein genetics, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors, Proto-Oncogene Proteins c-bcl-2 genetics, Sulfonamides pharmacology, bcl-X Protein genetics

Abstract

BCL-2 family proteins dictate survival of human multiple myeloma cells, making them attractive drug targets. Indeed, multiple myeloma cells are sensitive to antagonists that selectively target prosurvival proteins such as BCL-2/BCL-XL (ABT-737 and ABT-263/navitoclax) or BCL-2 only (ABT-199/GDC-0199/venetoclax). Resistance to these three drugs is mediated by expression of MCL-1. However, given the selectivity profile of venetoclax it is unclear whether coexpression of BCL-XL also affects antitumor responses to venetoclax in multiple myeloma. In multiple myeloma cell lines (n = 21), BCL-2 is expressed but sensitivity to venetoclax correlated with high BCL-2 and low BCL-XL or MCL-1 expression. Multiple myeloma cells that coexpress BCL-2 and BCL-XL were resistant to venetoclax but sensitive to a BCL-XL-selective inhibitor (A-1155463). Multiple myeloma xenograft models that coexpressed BCL-XL or MCL-1 with BCL-2 were also resistant to venetoclax. Resistance to venetoclax was mitigated by cotreatment with bortezomib in xenografts that coexpressed BCL-2 and MCL-1 due to upregulation of NOXA, a proapoptotic factor that neutralizes MCL-1. In contrast, xenografts that expressed BCL-XL, MCL-1, and BCL-2 were more sensitive to the combination of bortezomib with a BCL-XL selective inhibitor (A-1331852) but not with venetoclax cotreatment when compared with monotherapies. IHC of multiple myeloma patient bone marrow biopsies and aspirates (n = 95) revealed high levels of BCL-2 and BCL-XL in 62% and 43% of evaluable samples, respectively, while 34% were characterized as BCL-2(High)/BCL-XL (Low) In addition to MCL-1, our data suggest that BCL-XL may also be a potential resistance factor to venetoclax monotherapy and in combination with bortezomib. Mol Cancer Ther; 15(5); 1132-44. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published

2016

21. Erratum: Phosphorylation and linear ubiquitin direct A20 inhibition of inflammation.

Author

Wertz IE, Newton K, Seshasayee D, Kusam S, Lam C, Zhang J, Popovych N, Helgason E, Schoeffler A, Jeet S, Ramamoorthi N, Kategaya L, Newman RJ, Horikawa K, Dugger D, Sandoval W, Mukund S, Zindal A, Martin F, Quan C, Tom J, Fairbrother WJ, Townsend M, Warming S, DeVoss J, Liu J, Dueber E, Caplazi P, Lee WP, Goodnow CC, Balazs M, Yu K, Kolumam G, and Dixit VM

Published

2016

22. Palmitoylation of TEAD Transcription Factors Is Required for Their Stability and Function in Hippo Pathway Signaling.

Author

Noland CL, Gierke S, Schnier PD, Murray J, Sandoval WN, Sagolla M, Dey A, Hannoush RN, Fairbrother WJ, and Cunningham CN

Subjects

Adaptor Proteins, Signal Transducing metabolism, Amino Acid Sequence, Cysteine metabolism, DNA-Binding Proteins metabolism, HeLa Cells, Hippo Signaling Pathway, Humans, Lipoylation, Molecular Sequence Data, Nuclear Envelope metabolism, Phosphoproteins metabolism, Protein Binding, Protein Folding, Protein Stability, TEA Domain Transcription Factors, Transcription Factors metabolism, YAP-Signaling Proteins, DNA-Binding Proteins chemistry, Protein Processing, Post-Translational, Protein Serine-Threonine Kinases metabolism, Signal Transduction, Transcription Factors chemistry

Abstract

The Hippo signaling pathway is responsible for regulating the function of TEAD family transcription factors in metazoans. TEADs, with their co-activators YAP/TAZ, are critical for controlling cell differentiation and organ size through their transcriptional activation of genes involved in cell growth and proliferation. Dysregulation of the Hippo pathway has been implicated in multiple forms of cancer. Here, we identify a novel form of regulation of TEAD family proteins. We show that human TEADs are palmitoylated at a universally conserved cysteine, and report the crystal structures of the human TEAD2 and TEAD3 YAP-binding domains in their palmitoylated forms. These structures show a palmitate bound within a highly conserved hydrophobic cavity at each protein's core. Our findings also demonstrate that this modification is required for proper TEAD folding and stability, indicating a potential new avenue for pharmacologically regulating the Hippo pathway through the modulation of TEAD palmitoylation., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

23. Phosphorylation and linear ubiquitin direct A20 inhibition of inflammation.

Author

Wertz IE, Newton K, Seshasayee D, Kusam S, Lam C, Zhang J, Popovych N, Helgason E, Schoeffler A, Jeet S, Ramamoorthi N, Kategaya L, Newman RJ, Horikawa K, Dugger D, Sandoval W, Mukund S, Zindal A, Martin F, Quan C, Tom J, Fairbrother WJ, Townsend M, Warming S, DeVoss J, Liu J, Dueber E, Caplazi P, Lee WP, Goodnow CC, Balazs M, Yu K, Kolumam G, and Dixit VM

Subjects

Animals, Cell Death, Cysteine Endopeptidases chemistry, Cysteine Endopeptidases genetics, Female, Inflammation genetics, Inflammation pathology, Intracellular Signaling Peptides and Proteins chemistry, Intracellular Signaling Peptides and Proteins genetics, Lysine metabolism, Male, Mice, Mice, Inbred C57BL, Mutation, Phosphorylation, Polyubiquitin chemistry, Polyubiquitin metabolism, Protein Binding, Protein Kinases metabolism, Signal Transduction, Tumor Necrosis Factor alpha-Induced Protein 3, Tumor Necrosis Factor-alpha metabolism, Ubiquitination, Cysteine Endopeptidases metabolism, Inflammation metabolism, Intracellular Signaling Peptides and Proteins metabolism, Ubiquitin chemistry, Ubiquitin metabolism

Abstract

Inactivation of the TNFAIP3 gene, encoding the A20 protein, is associated with critical inflammatory diseases including multiple sclerosis, rheumatoid arthritis and Crohn's disease. However, the role of A20 in attenuating inflammatory signalling is unclear owing to paradoxical in vitro and in vivo findings. Here we utilize genetically engineered mice bearing mutations in the A20 ovarian tumour (OTU)-type deubiquitinase domain or in the zinc finger-4 (ZnF4) ubiquitin-binding motif to investigate these discrepancies. We find that phosphorylation of A20 promotes cleavage of Lys63-linked polyubiquitin chains by the OTU domain and enhances ZnF4-mediated substrate ubiquitination. Additionally, levels of linear ubiquitination dictate whether A20-deficient cells die in response to tumour necrosis factor. Mechanistically, linear ubiquitin chains preserve the architecture of the TNFR1 signalling complex by blocking A20-mediated disassembly of Lys63-linked polyubiquitin scaffolds. Collectively, our studies reveal molecular mechanisms whereby A20 deubiquitinase activity and ubiquitin binding, linear ubiquitination, and cellular kinases cooperate to regulate inflammation and cell death.

Published

2015

24. Exploiting selective BCL-2 family inhibitors to dissect cell survival dependencies and define improved strategies for cancer therapy.

Author

Leverson JD, Phillips DC, Mitten MJ, Boghaert ER, Diaz D, Tahir SK, Belmont LD, Nimmer P, Xiao Y, Ma XM, Lowes KN, Kovar P, Chen J, Jin S, Smith M, Xue J, Zhang H, Oleksijew A, Magoc TJ, Vaidya KS, Albert DH, Tarrant JM, La N, Wang L, Tao ZF, Wendt MD, Sampath D, Rosenberg SH, Tse C, Huang DC, Fairbrother WJ, Elmore SW, and Souers AJ

Subjects

Administration, Oral, Aniline Compounds therapeutic use, Animals, Antineoplastic Agents therapeutic use, Benzothiazoles chemistry, Bridged Bicyclo Compounds, Heterocyclic therapeutic use, Cell Line, Tumor, Cell Survival, Docetaxel, Gene Expression Profiling, Granulocytes metabolism, Humans, Isoquinolines chemistry, Kinetics, Mice, Neoplasm Transplantation, Neoplasms metabolism, Neutropenia chemically induced, Neutrophils drug effects, Proto-Oncogene Proteins c-bcl-2 metabolism, Sulfonamides therapeutic use, Taxoids adverse effects, Thrombocytopenia chemically induced, bcl-X Protein antagonists & inhibitors, bcl-X Protein metabolism, Gene Expression Regulation, Neoplastic, Neoplasms drug therapy, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors

Abstract

The BCL-2/BCL-XL/BCL-W inhibitor ABT-263 (navitoclax) has shown promising clinical activity in lymphoid malignancies such as chronic lymphocytic leukemia. However, its efficacy in these settings is limited by thrombocytopenia caused by BCL-XL inhibition. This prompted the generation of the BCL-2-selective inhibitor venetoclax (ABT-199/GDC-0199), which demonstrates robust activity in these cancers but spares platelets. Navitoclax has also been shown to enhance the efficacy of docetaxel in preclinical models of solid tumors, but clinical use of this combination has been limited by neutropenia. We used venetoclax and the BCL-XL-selective inhibitors A-1155463 and A-1331852 to assess the relative contributions of inhibiting BCL-2 or BCL-XL to the efficacy and toxicity of the navitoclax-docetaxel combination. Selective BCL-2 inhibition suppressed granulopoiesis in vitro and in vivo, potentially accounting for the exacerbated neutropenia observed when navitoclax was combined with docetaxel clinically. By contrast, selectively inhibiting BCL-XL did not suppress granulopoiesis but was highly efficacious in combination with docetaxel when tested against a range of solid tumors. Therefore, BCL-XL-selective inhibitors have the potential to enhance the efficacy of docetaxel in solid tumors and avoid the exacerbation of neutropenia observed with navitoclax. These studies demonstrate the translational utility of this toolkit of selective BCL-2 family inhibitors and highlight their potential as improved cancer therapeutics., (Copyright © 2015, American Association for the Advancement of Science.)

Published

2015

25. Potent and selective small-molecule MCL-1 inhibitors demonstrate on-target cancer cell killing activity as single agents and in combination with ABT-263 (navitoclax).

Author

Leverson JD, Zhang H, Chen J, Tahir SK, Phillips DC, Xue J, Nimmer P, Jin S, Smith M, Xiao Y, Kovar P, Tanaka A, Bruncko M, Sheppard GS, Wang L, Gierke S, Kategaya L, Anderson DJ, Wong C, Eastham-Anderson J, Ludlam MJ, Sampath D, Fairbrother WJ, Wertz I, Rosenberg SH, Tse C, Elmore SW, and Souers AJ

Subjects

Apoptosis Regulatory Proteins metabolism, Bcl-2-Like Protein 11, Carboxylic Acids, Cell Line, Tumor, Cell Survival drug effects, Drug Synergism, Humans, Indoles pharmacology, Membrane Proteins metabolism, Myeloid Cell Leukemia Sequence 1 Protein metabolism, Proto-Oncogene Proteins metabolism, Aniline Compounds pharmacology, Apoptosis drug effects, Myeloid Cell Leukemia Sequence 1 Protein antagonists & inhibitors, Neoplasms pathology, Small Molecule Libraries pharmacology, Sulfonamides pharmacology

Abstract

The anti-apoptotic protein MCL-1 is a key regulator of cancer cell survival and a known resistance factor for small-molecule BCL-2 family inhibitors such as ABT-263 (navitoclax), making it an attractive therapeutic target. However, directly inhibiting this target requires the disruption of high-affinity protein-protein interactions, and therefore designing small molecules potent enough to inhibit MCL-1 in cells has proven extremely challenging. Here, we describe a series of indole-2-carboxylic acids, exemplified by the compound A-1210477, that bind to MCL-1 selectively and with sufficient affinity to disrupt MCL-1-BIM complexes in living cells. A-1210477 induces the hallmarks of intrinsic apoptosis and demonstrates single agent killing of multiple myeloma and non-small cell lung cancer cell lines demonstrated to be MCL-1 dependent by BH3 profiling or siRNA rescue experiments. As predicted, A-1210477 synergizes with the BCL-2/BCL-XL inhibitor navitoclax to kill a variety of cancer cell lines. This work represents the first description of small-molecule MCL-1 inhibitors with sufficient potency to induce clear on-target cellular activity. It also demonstrates the utility of these molecules as chemical tools for dissecting the basic biology of MCL-1 and the promise of small-molecule MCL-1 inhibitors as potential therapeutics for the treatment of cancer.

Published

2015

26. Internal motions prime cIAP1 for rapid activation.

Author

Phillips AH, Schoeffler AJ, Matsui T, Weiss TM, Blankenship JW, Zobel K, Giannetti AM, Dueber EC, and Fairbrother WJ

Subjects

Humans, Kinetics, Models, Molecular, Nuclear Magnetic Resonance, Biomolecular, Protein Binding, Protein Conformation, Protein Multimerization, Protein Structure, Tertiary, Scattering, Small Angle, Ubiquitin metabolism, Ubiquitin-Activating Enzymes metabolism, Ubiquitin-Protein Ligases, X-Ray Diffraction, Inhibitor of Apoptosis Proteins chemistry, Inhibitor of Apoptosis Proteins metabolism

Abstract

Cellular inhibitor of apoptosis 1 (cIAP1) is a ubiquitin ligase with critical roles in the control of programmed cell death and NF-κB signaling. Under normal conditions, the protein exists as an autoinhibited monomer, but proapoptotic signals lead to its dimerization, activation and proteasomal degradation. This view of cIAP1 as a binary switch has been informed by static structural studies that cannot access the protein's dynamics. Here, we use NMR spectroscopy to study micro- and millisecond motions of specific domain interfaces in human cIAP1 and use time-resolved small-angle X-ray scattering to observe the global conformational changes necessary for activation. Although motions within each interface of the 'closed' monomer are insufficient to activate cIAP1, they enable associations with catalytic partners and activation factors. We propose that these internal motions facilitate rapid peptide-induced opening and dimerization of cIAP1, which undergoes a dramatic spring-loaded structural transition.

Published

2014

27. Discovery of a Potent and Selective BCL-XL Inhibitor with in Vivo Activity.

Author

Tao ZF, Hasvold L, Wang L, Wang X, Petros AM, Park CH, Boghaert ER, Catron ND, Chen J, Colman PM, Czabotar PE, Deshayes K, Fairbrother WJ, Flygare JA, Hymowitz SG, Jin S, Judge RA, Koehler MF, Kovar PJ, Lessene G, Mitten MJ, Ndubaku CO, Nimmer P, Purkey HE, Oleksijew A, Phillips DC, Sleebs BE, Smith BJ, Smith ML, Tahir SK, Watson KG, Xiao Y, Xue J, Zhang H, Zobel K, Rosenberg SH, Tse C, Leverson JD, Elmore SW, and Souers AJ

Abstract

A-1155463, a highly potent and selective BCL-XL inhibitor, was discovered through nuclear magnetic resonance (NMR) fragment screening and structure-based design. This compound is substantially more potent against BCL-XL-dependent cell lines relative to our recently reported inhibitor, WEHI-539, while possessing none of its inherent pharmaceutical liabilities. A-1155463 caused a mechanism-based and reversible thrombocytopenia in mice and inhibited H146 small cell lung cancer xenograft tumor growth in vivo following multiple doses. A-1155463 thus represents an excellent tool molecule for studying BCL-XL biology as well as a productive lead structure for further optimization.

Published

2014

28. Designer proteins to trigger cell death.

Author

Fairbrother WJ and Ashkenazi A

Subjects

Animals, Humans, Herpesvirus 4, Human chemistry, Protein Engineering, Proteins pharmacology, Viral Proteins antagonists & inhibitors

Abstract

Efforts to generate biologically active proteins by de novo computational design have been limited to creating functional sites within pre-existing scaffolds. Procko et al. use an innovative computational design approach coupled with in-vitro-targeted evolution to produce a potent polypeptide inhibitor of a viral Bcl-2-like protein. This novel inhibitor triggers apoptosis of virus-infected cells., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

29. Structure-Guided Rescaffolding of Selective Antagonists of BCL-XL.

Author

Koehler MF, Bergeron P, Choo EF, Lau K, Ndubaku C, Dudley D, Gibbons P, Sleebs BE, Rye CS, Nikolakopoulos G, Bui C, Kulasegaram S, Kersten WJ, Smith BJ, Czabotar PE, Colman PM, Huang DC, Baell JB, Watson KG, Hasvold L, Tao ZF, Wang L, Souers AJ, Elmore SW, Flygare JA, Fairbrother WJ, and Lessene G

Abstract

Because of the promise of BCL-2 antagonists in combating chronic lymphocytic leukemia (CLL) and non-Hodgkin's lymphoma (NHL), interest in additional selective antagonists of antiapoptotic proteins has grown. Beginning with a series of selective, potent BCL-XL antagonists containing an undesirable hydrazone functionality, in silico design and X-ray crystallography were utilized to develop alternative scaffolds that retained the selectivity and potency of the starting compounds.

Published

2014

30. Further insights into the effects of pre-organizing the BimBH3 helix.

Author

Okamoto T, Segal D, Zobel K, Fedorova A, Yang H, Fairbrother WJ, Huang DC, Smith BJ, Deshayes K, and Czabotar PE

Subjects

Animals, Humans, Apoptosis, Peptide Fragments chemistry, Peptide Fragments metabolism, Proto-Oncogene Proteins chemistry, Proto-Oncogene Proteins metabolism

Published

2014

31. Learning and confirming with preclinical studies: modeling and simulation in the discovery of GDC-0917, an inhibitor of apoptosis proteins antagonist.

Author

Wong H, Gould SE, Budha N, Darbonne WC, Kadel EE 3rd, La H, Alicke B, Halladay JS, Erickson R, Portera C, Tolcher AW, Infante JR, Mamounas M, Flygare JA, Hop CE, and Fairbrother WJ

Subjects

Animals, Biological Availability, Breast Neoplasms drug therapy, Breast Neoplasms metabolism, Cell Line, Tumor, Dogs, Drug Evaluation, Preclinical, Female, Half-Life, Hepatocytes drug effects, Humans, Macaca fascicularis, Male, Mice, Mice, SCID, Rats, Rats, Sprague-Dawley, Xenograft Model Antitumor Assays methods, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Inhibitor of Apoptosis Proteins metabolism, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors pharmacology

Abstract

The application of modeling and simulation techniques is increasingly common in the preclinical stages of the drug development process. GDC-0917 [(S)-1-((S)-2-cyclohexyl-2-((S)-2-(methylamino)propanamido)acetyl)-N-(2-(oxazol-2-yl)-4-phenylthiazol-5-yl)pyrrolidine-2-carboxamide] is a potent second-generation antagonist of inhibitor of apoptosis (IAP) proteins that is being developed for the treatment of various cancers. GDC-0917 has low to moderate clearance in the mouse (12.0 ml/min/kg), rat (27.0 ml/min/kg), and dog (15.3 ml/min/kg), and high clearance in the monkey (67.6 ml/min/kg). Accordingly, oral bioavailability was lowest in monkeys compared with other species. Based on our experience with a prototype molecule with similar structure, in vitro-in vivo extrapolation was used to predict a moderate clearance (11.5 ml/min/kg) in humans. The predicted human volume of distribution was estimated using simple allometry at 6.69 l/kg. Translational pharmacokinetic-pharmacodynamic (PK-PD) analysis using results from MDA-MB-231-X1.1 breast cancer xenograft studies and predicted human pharmacokinetics suggests that ED50 and ED90 targets can be achieved in humans using acceptable doses (72 mg and 660 mg, respectively) and under an acceptable time frame. The relationship between GDC-0917 concentrations and pharmacodynamic response (cIAP1 degradation) was characterized using an in vitro peripheral blood mononuclear cell immunoassay. Simulations of human GDC-0917 plasma concentration-time profile and cIAP1 degradation at the 5-mg starting dose in the phase 1 clinical trial agreed well with observations. This work shows the importance of leveraging information from prototype molecules and illustrates how modeling and simulation can be used to add value to preclinical studies in the early stages of the drug development process.

Published

2013

32. Conformational dynamics control ubiquitin-deubiquitinase interactions and influence in vivo signaling.

Author

Phillips AH, Zhang Y, Cunningham CN, Zhou L, Forrest WF, Liu PS, Steffek M, Lee J, Tam C, Helgason E, Murray JM, Kirkpatrick DS, Fairbrother WJ, and Corn JE

Subjects

Amino Acid Sequence, Endopeptidases chemistry, Models, Molecular, Protein Binding, Protein Conformation, Ubiquitin chemistry, Endopeptidases metabolism, Signal Transduction, Ubiquitin metabolism

Abstract

Ubiquitin is a highly conserved eukaryotic protein that interacts with a diverse set of partners to act as a cellular signaling hub. Ubiquitin's conformational flexibility has been postulated to underlie its multifaceted recognition. Here we use computational and library-based means to interrogate core mutations that modulate the conformational dynamics of human ubiquitin. These ubiquitin variants exhibit increased affinity for the USP14 deubiquitinase, with concomitantly reduced affinity for other deubiquitinases. Strikingly, the kinetics of conformational motion are dramatically slowed in these variants without a detectable change in either the ground state fold or excited state population. These variants can be ligated into substrate-linked chains in vitro and in vivo but cannot solely support growth in eukaryotic cells. Proteomic analyses reveal nearly identical interaction profiles between WT ubiquitin and the variants but identify a small subset of altered interactions. Taken together, these results show that conformational dynamics are critical for ubiquitin-deubiquitinase interactions and imply that the fine tuning of motion has played a key role in the evolution of ubiquitin as a signaling hub.

Published

2013

33. Bcl-2/Bcl-xL inhibition increases the efficacy of MEK inhibition alone and in combination with PI3 kinase inhibition in lung and pancreatic tumor models.

Author

Tan N, Wong M, Nannini MA, Hong R, Lee LB, Price S, Williams K, Savy PP, Yue P, Sampath D, Settleman J, Fairbrother WJ, and Belmont LD

Subjects

Aniline Compounds administration & dosage, Apoptosis drug effects, Cell Line, Tumor, Enzyme Inhibitors administration & dosage, Genes, bcl-2 genetics, Humans, Indazoles administration & dosage, Lung Neoplasms genetics, Lung Neoplasms pathology, MAP Kinase Kinase Kinases metabolism, Molecular Targeted Therapy, Pancreatic Neoplasms genetics, Pancreatic Neoplasms pathology, Phosphatidylinositol 3-Kinases metabolism, Signal Transduction drug effects, Sulfonamides administration & dosage, bcl-X Protein genetics, Lung Neoplasms drug therapy, MAP Kinase Kinase Kinases antagonists & inhibitors, Pancreatic Neoplasms drug therapy, Phosphoinositide-3 Kinase Inhibitors, bcl-X Protein antagonists & inhibitors

Abstract

Although mitogen-activated protein (MAP)-extracellular signal-regulated kinase (ERK) kinase (MEK) inhibition is predicted to cause cell death by stabilization of the proapoptotic BH3-only protein BIM, the induction of apoptosis is often modest. To determine if addition of a Bcl-2 family inhibitor could increase the efficacy of a MEK inhibitor, we evaluated a panel of 53 non-small cell lung cancer and pancreatic cancer cell lines with the combination of navitoclax (ABT-263), a Bcl-2/Bcl-xL (BCL2/BCL2L1) antagonist, and a novel MAP kinase (MEK) inhibitor, G-963. The combination is synergistic in the majority of lines, with an enrichment of cell lines harboring KRAS mutations in the high synergy group. Cells exposed to G-963 arrest in G1 and a small fraction undergo apoptosis. The addition of navitoclax to G-963 does not alter the kinetics of cell-cycle arrest, but greatly increases the percentage of cells that undergo apoptosis. The G-963/navitoclax combination was more effective than either single agent in the KRAS mutant H2122 xenograft model; BIM stabilization and PARP cleavage were observed in tumors, consistent with the mechanism of action observed in cell culture. Addition of the phosphatidylinositol 3-kinase (PI3K, PIK3CA) inhibitor GDC-0941 to this treatment combination increases cell killing compared with double- or single-agent treatment. Taken together, these data suggest the efficacy of agents that target the MAPK and PI3K pathways can be improved by combination with a Bcl-2 family inhibitor., (©2013 AACR)

Published

2013

34. Structure-guided design of a selective BCL-X(L) inhibitor.

Author

Lessene G, Czabotar PE, Sleebs BE, Zobel K, Lowes KN, Adams JM, Baell JB, Colman PM, Deshayes K, Fairbrother WJ, Flygare JA, Gibbons P, Kersten WJ, Kulasegaram S, Moss RM, Parisot JP, Smith BJ, Street IP, Yang H, Huang DC, and Watson KG

Subjects

Animals, Apoptosis, Benzothiazoles chemistry, Cell Line, Tumor, Crystallography, X-Ray, Drug Screening Assays, Antitumor, Humans, Hydrazones chemistry, Kinetics, Mice, Models, Chemical, Myeloid Cell Leukemia Sequence 1 Protein, Protein Binding, Proto-Oncogene Proteins c-bcl-2 genetics, Antineoplastic Agents pharmacology, Drug Design, bcl-X Protein antagonists & inhibitors, bcl-X Protein chemistry

Abstract

The prosurvival BCL-2 family protein BCL-X(L) is often overexpressed in solid tumors and renders malignant tumor cells resistant to anticancer therapeutics. Enhancing apoptotic responses by inhibiting BCL-X(L) will most likely have widespread utility in cancer treatment and, instead of inhibiting multiple prosurvival BCL-2 family members, a BCL-X(L)-selective inhibitor would be expected to minimize the toxicity to normal tissues. We describe the use of a high-throughput screen to discover a new series of small molecules targeting BCL-X(L) and their structure-guided development by medicinal chemistry. The optimized compound, WEHI-539 (7), has high affinity (subnanomolar) and selectivity for BCL-X(L) and potently kills cells by selectively antagonizing its prosurvival activity. WEHI-539 will be an invaluable tool for distinguishing the roles of BCL-X(L) from those of its prosurvival relatives, both in normal cells and notably in malignant tumor cells, many of which may prove to rely upon BCL-X(L) for their sustained growth.

Published

2013

35. Stabilizing the pro-apoptotic BimBH3 helix (BimSAHB) does not necessarily enhance affinity or biological activity.

Author

Okamoto T, Zobel K, Fedorova A, Quan C, Yang H, Fairbrother WJ, Huang DC, Smith BJ, Deshayes K, and Czabotar PE

Subjects

Animals, Humans, Mice, Models, Molecular, Protein Structure, Secondary, Apoptosis, Peptide Fragments chemistry, Peptide Fragments metabolism, Proto-Oncogene Proteins chemistry, Proto-Oncogene Proteins metabolism

Abstract

An attractive approach for developing therapeutic peptides is to enhance binding to their targets by stabilizing their α-helical conformation, for example, stabilized BimBH3 peptides (BimSAHB) designed to induce apoptosis. Unexpectedly, we found that such modified peptides have reduced affinity for their targets, the pro-survival Bcl-2 proteins. We attribute this loss in affinity to disruption of a network of stabilizing intramolecular interactions present in the bound state of the native peptide. Altering this network may compromise binding affinity, as in the case of the BimBH3 stapled peptide studied here. Moreover, cells exposed to these peptides do not readily undergo apoptosis, strongly indicating that BimSAHB is not inherently cell permeable.

Published

2013

36. ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets.

Author

Souers AJ, Leverson JD, Boghaert ER, Ackler SL, Catron ND, Chen J, Dayton BD, Ding H, Enschede SH, Fairbrother WJ, Huang DC, Hymowitz SG, Jin S, Khaw SL, Kovar PJ, Lam LT, Lee J, Maecker HL, Marsh KC, Mason KD, Mitten MJ, Nimmer PM, Oleksijew A, Park CH, Park CM, Phillips DC, Roberts AW, Sampath D, Seymour JF, Smith ML, Sullivan GM, Tahir SK, Tse C, Wendt MD, Xiao Y, Xue JC, Zhang H, Humerickhouse RA, Rosenberg SH, and Elmore SW

Subjects

Aniline Compounds pharmacology, Animals, Antineoplastic Agents therapeutic use, Apoptosis drug effects, Cell Survival drug effects, Dogs, Female, HeLa Cells, Humans, Mice, Mice, SCID, Proto-Oncogene Proteins c-bcl-2 chemistry, Tumor Burden, Xenograft Model Antitumor Assays, bcl-X Protein antagonists & inhibitors, Antineoplastic Agents pharmacology, Blood Platelets drug effects, Bridged Bicyclo Compounds, Heterocyclic pharmacology, Hematologic Neoplasms drug therapy, Proto-Oncogene Proteins c-bcl-2 antagonists & inhibitors, Sulfonamides pharmacology

Abstract

Proteins in the B cell CLL/lymphoma 2 (BCL-2) family are key regulators of the apoptotic process. This family comprises proapoptotic and prosurvival proteins, and shifting the balance toward the latter is an established mechanism whereby cancer cells evade apoptosis. The therapeutic potential of directly inhibiting prosurvival proteins was unveiled with the development of navitoclax, a selective inhibitor of both BCL-2 and BCL-2-like 1 (BCL-X(L)), which has shown clinical efficacy in some BCL-2-dependent hematological cancers. However, concomitant on-target thrombocytopenia caused by BCL-X(L) inhibition limits the efficacy achievable with this agent. Here we report the re-engineering of navitoclax to create a highly potent, orally bioavailable and BCL-2-selective inhibitor, ABT-199. This compound inhibits the growth of BCL-2-dependent tumors in vivo and spares human platelets. A single dose of ABT-199 in three patients with refractory chronic lymphocytic leukemia resulted in tumor lysis within 24 h. These data indicate that selective pharmacological inhibition of BCL-2 shows promise for the treatment of BCL-2-dependent hematological cancers.

Published

2013

37. Toxicity profile of small-molecule IAP antagonist GDC-0152 is linked to TNF-α pharmacology.

Author

Erickson RI, Tarrant J, Cain G, Lewin-Koh SC, Dybdal N, Wong H, Blackwood E, West K, Steigerwalt R, Mamounas M, Flygare JA, Amemiya K, Dambach D, Fairbrother WJ, and Diaz D

Subjects

Animals, Antineoplastic Agents blood, Chemokines blood, Cyclohexanes blood, Dogs, Female, Liver drug effects, Liver immunology, Liver metabolism, Liver pathology, Lung drug effects, Lung immunology, Lung metabolism, Lung pathology, Male, Pyrroles blood, Rats, Rats, Sprague-Dawley, Species Specificity, Systemic Inflammatory Response Syndrome chemically induced, Systemic Inflammatory Response Syndrome immunology, Systemic Inflammatory Response Syndrome pathology, Toxicity Tests, Tumor Necrosis Factor-alpha pharmacology, Antineoplastic Agents toxicity, Cyclohexanes toxicity, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Pyrroles toxicity, Tumor Necrosis Factor-alpha blood

Abstract

Inhibitor-of-apoptosis (IAP) proteins suppress apoptosis and are overexpressed in a variety of cancers. Small-molecule IAP antagonists are currently being tested in clinical trials as novel cancer therapeutics. GDC-0152 is a small-molecule drug that triggers tumor cell apoptosis by selectively antagonizing IAPs. GDC-0152 induces NF-κB transcriptional activity leading to expression of several chemokines and cytokines, of which tumor necrosis factor alpha (TNF-α) is the most important for single-agent tumor activity. TNF-α is a pleiotropic cytokine that drives a variety of cellular responses, comprising inflammation, proliferation, and cell survival or death depending on the cellular context. As malignant and normal cells produce TNF-α upon IAP antagonism, increased TNF-α could drive both efficacy and toxicity. The toxicity profile of GDC-0152 in dogs and rats was characterized after iv dose administration once every 2 weeks for four doses. Findings in both species consisted of a dose-related, acute, systemic inflammatory response, and hepatic injury. Laboratory findings included elevated plasma cytokines, an inflammatory leukogram, and increased liver transaminases with histopathological findings of inflammatory infiltrates and apoptosis/necrosis in multiple tissues; a toxicology profile consistent with TNF-α-mediated toxicity. Dogs exhibited more severe findings than rats, and humans did not exhibit these findings, at comparable exposures across species. Furthermore, elevations in blood neutrophil count, serum monocyte chemoattractant protein-1, and other markers of inflammation corresponded to GDC-0152 exposure and toxicity and thus may have utility as safety biomarkers.

Published

2013

38. Dogs are more sensitive to antagonists of inhibitor of apoptosis proteins than rats and humans: a translational toxicokinetic/toxicodynamic analysis.

Author

Wong H, Budha NR, West K, Blackwood E, Ware JA, Yu R, Darbonne WC, Gould SE, Steigerwalt R, Erickson R, Hop CE, LoRusso P, Eckhardt SG, Wagner A, Chan IT, Mamounas M, Flygare JA, and Fairbrother WJ

Subjects

Animals, Area Under Curve, Caspase Inhibitors pharmacokinetics, Cyclohexanes pharmacokinetics, Cytokines metabolism, Dogs, Drug Evaluation, Preclinical, Female, Half-Life, Humans, Injections, Intravenous, Male, Models, Biological, Pyrroles pharmacokinetics, Rats, Rats, Sprague-Dawley, Species Specificity, Caspase Inhibitors toxicity, Cyclohexanes toxicity, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Pyrroles toxicity

Abstract

Inhibitor of apoptosis (IAP) proteins suppress apoptosis and are overexpressed in a variety of cancers. GDC-0152 is a potent and selective IAP antagonist being developed as an anticancer agent. In preclinical safety studies, dogs were particularly sensitive to GDC-0152 showing adverse signs of a tumor necrosis factor alpha (TNF-α) driven systemic inflammatory response, related to cellular IAP degradation and activation of NFκB signaling, at lower exposures compared with rat. In addition, downstream increases in systemic levels of cytokines and chemokines, such as monocyte chemotactic protein-1 (MCP-1), were observed. A semimechanistic population toxicokinetic/toxicodynamic (TK/TD) model incorporating transit compartments was used to fit MCP-1 plasma concentrations from rats or dogs given iv GDC-0152 doses. Estimated TD parameters inferred that lower GDC-0152 plasma concentrations triggered more severe increases in plasma MCP-1 in dogs compared with rats. Human simulations performed using dog TD parameters and human pharmacokinetics predicted 300-2400% increases of MCP-1 in humans at iv doses from 0.76 to 1.48mg/kg. Similar simulations using rat TD parameters suggest little or no change. Patients given iv doses of GDC-0152 up to 1.48mg/kg iv showed no substantial increases in systemic MCP-1 or signs of a severe TNF-α driven systemic inflammatory response. Emerging clinical data reported for other IAP antagonists are consistent with our observations. Taken together, the data suggest dogs are more sensitive to IAP antagonists compared with humans and rats. This study illustrates how TK/TD analysis can be utilized to quantitatively translate and context an identified preclinical safety risk in dogs to humans.

Published

2012

39. Characterization of ML-IAP protein stability and physiological role in vivo.

Author

Varfolomeev E, Moradi E, Dynek JN, Zha J, Fedorova AV, Deshayes K, Fairbrother WJ, Newton K, Le Couter J, and Vucic D

Subjects

Adaptor Proteins, Signal Transducing antagonists & inhibitors, Adaptor Proteins, Signal Transducing genetics, Animals, Cell Line, Tumor, Eye blood supply, Female, Humans, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Inhibitor of Apoptosis Proteins genetics, Intraocular Pressure, Male, Melanoma, Mice, Mice, Mutant Strains, Neoplasm Proteins antagonists & inhibitors, Neoplasm Proteins genetics, Organ Specificity, Proteasome Endopeptidase Complex metabolism, Protein Stability, Protein Structure, Tertiary, Retina anatomy & histology, Retina physiology, Ubiquitin-Protein Ligases metabolism, Adaptor Proteins, Signal Transducing physiology, Eye metabolism, Inhibitor of Apoptosis Proteins physiology, Neoplasm Proteins physiology

Abstract

ML-IAP [melanoma IAP (inhibitor of apoptosis)] is an anti-apoptotic protein that is expressed highly in melanomas where it contributes to resistance to apoptotic stimuli. The anti-apoptotic activity and elevated expression of IAP family proteins in many human cancers makes IAP proteins attractive targets for inhibition by cancer therapeutics. Small-molecule IAP antagonists that bind with high affinities to select BIR (baculovirus IAP repeat) domains have been shown to stimulate auto-ubiquitination and rapid proteasomal degradation of c-IAP1 (cellular IAP1) and c-IAP2 (cellular IAP2). In the present paper, we report ML-IAP proteasomal degradation in response to bivalent, but not monovalent, IAP antagonists. This degradation required ML-IAP ubiquitin ligase activity and was independent of c-IAP1 or c-IAP2. Although ML-IAP is best characterized in melanoma cells, we show that ML-IAP expression in normal mammalian tissues is restricted largely to the eye, being most abundant in ciliary body epithelium and retinal pigment epithelium. Surprisingly, given this pattern of expression, gene-targeted mice lacking ML-IAP exhibited normal intraocular pressure as well as normal retinal structure and function. The results of the present study indicate that ML-IAP is dispensable for both normal mouse development and ocular homoeostasis.

Published

2012

40. Discovery of a potent small-molecule antagonist of inhibitor of apoptosis (IAP) proteins and clinical candidate for the treatment of cancer (GDC-0152).

Author

Flygare JA, Beresini M, Budha N, Chan H, Chan IT, Cheeti S, Cohen F, Deshayes K, Doerner K, Eckhardt SG, Elliott LO, Feng B, Franklin MC, Reisner SF, Gazzard L, Halladay J, Hymowitz SG, La H, LoRusso P, Maurer B, Murray L, Plise E, Quan C, Stephan JP, Young SG, Tom J, Tsui V, Um J, Varfolomeev E, Vucic D, Wagner AJ, Wallweber HJ, Wang L, Ware J, Wen Z, Wong H, Wong JM, Wong M, Wong S, Yu R, Zobel K, and Fairbrother WJ

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacokinetics, Apoptosis drug effects, Baculoviral IAP Repeat-Containing 3 Protein, Binding, Competitive, Breast Neoplasms metabolism, Breast Neoplasms pathology, Caspases metabolism, Cell Line, Tumor, Cell Survival drug effects, Clinical Trials, Phase I as Topic, Female, Humans, Inhibitor of Apoptosis Proteins metabolism, Male, Thiadiazoles chemistry, Thiadiazoles pharmacokinetics, Ubiquitin-Protein Ligases, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Breast Neoplasms drug therapy, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Thiadiazoles chemical synthesis, Thiadiazoles pharmacology

Abstract

A series of compounds were designed and synthesized as antagonists of cIAP1/2, ML-IAP, and XIAP based on the N-terminus, AVPI, of mature Smac. Compound 1 (GDC-0152) has the best profile of these compounds; it binds to the XIAP BIR3 domain, the BIR domain of ML-IAP, and the BIR3 domains of cIAP1 and cIAP2 with K(i) values of 28, 14, 17, and 43 nM, respectively. These compounds promote degradation of cIAP1, induce activation of caspase-3/7, and lead to decreased viability of breast cancer cells without affecting normal mammary epithelial cells. Compound 1 inhibits tumor growth when dosed orally in the MDA-MB-231 breast cancer xenograft model. Compound 1 was advanced to human clinical trials, and it exhibited linear pharmacokinetics over the dose range (0.049 to 1.48 mg/kg) tested. Mean plasma clearance in humans was 9 ± 3 mL/min/kg, and the volume of distribution was 0.6 ± 0.2 L/kg.

Published

2012

41. Navitoclax (ABT-263) reduces Bcl-x(L)-mediated chemoresistance in ovarian cancer models.

Author

Wong M, Tan N, Zha J, Peale FV, Yue P, Fairbrother WJ, and Belmont LD

Subjects

Aniline Compounds administration & dosage, Cell Line, Tumor, Deoxycytidine administration & dosage, Deoxycytidine analogs & derivatives, Deoxycytidine pharmacology, Drug Synergism, Female, Humans, Immunohistochemistry, Ovarian Neoplasms metabolism, Paclitaxel administration & dosage, Paclitaxel pharmacology, Sulfonamides administration & dosage, Gemcitabine, Aniline Compounds pharmacology, Antineoplastic Combined Chemotherapy Protocols pharmacology, Ovarian Neoplasms drug therapy, Sulfonamides pharmacology, bcl-X Protein metabolism

Abstract

To examine the potential of combining Bcl-2 family inhibitors with chemotherapy in ovarian cancer, we evaluated a panel of 27 ovarian cancer cell lines for response to the combination of navitoclax (formerly ABT-263) and paclitaxel or gemcitabine. The majority of cell lines exhibited a greater than additive response to either combination, as determined by the Bliss independence model, and more than 50% of the ovarian cell lines exhibited strong synergy for the navitoclax/paclitaxel combination. To identify biomarkers for tumors likely to respond to this combination, we evaluated the protein levels of intrinsic apoptosis pathway components. Bcl-x(L) seems necessary, but not sufficient, for navitoclax/paclitaxel synergy in vitro, suggesting that exclusion of patients whose tumors have low or undetectable Bcl-x(L) would enrich for patients responsive to the combination. We evaluated Bcl-x(L) levels in ovarian cancer tumor tissue from 40 patients (20 taxane responsive and 20 with poor response to taxane) and found that patients with high Bcl-x(L) were less sensitive to taxane treatment (10 of 12) Bcl-x(L) positive patients, P = 0.014). These data support the use of navitoclax in combination with taxane-based therapy in ovarian cancer patients with high levels of Bcl-x(L)., (©2012 AACR.)

Published

2012

42. The structure of the extracellular domain of the jumping translocation breakpoint protein reveals a variation of the midkine fold.

Author

Rousseau F, Pan B, Fairbrother WJ, Bazan JF, and Lingel A

Subjects

Amino Acid Sequence, Animals, Carrier Proteins chemistry, Cloning, Molecular methods, Disulfides chemistry, Humans, Membrane Proteins metabolism, Midkine, Models, Molecular, Molecular Sequence Data, Neoplasm Proteins metabolism, Nuclear Magnetic Resonance, Biomolecular methods, Protein Folding, Protein Interaction Domains and Motifs, Protein Structure, Secondary, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Translocation, Genetic genetics, Cytokines chemistry, Membrane Proteins chemistry, Membrane Proteins genetics, Neoplasm Proteins chemistry, Neoplasm Proteins genetics

Abstract

Jumping Translocation Breakpoint (JTB) is an orphan receptor that is conserved from nematodes to humans and whose gene expression in humans is strikingly upregulated in diverse types of cancers. Translocations occur frequently at the hJTB genomic locus, leading to multiple copies of a truncated JTB gene, which potentially encodes a soluble secreted ectodomain. In addition, JTB and its orthologs likely represent a unique and ancient protein family since homologs could not be identified by direct sequence comparison. In the present study, we have determined the NMR solution structure of the N-terminal ectodomain of human JTB, showing that its fold architecture is a new variant of a three-β-strand antiparallel β-meander. The JTB structure has a distant relationship to the midkine/pleiotrophin fold, particularly in the conservation of distinctive disulfide bridge patterns. The structure of this newly characterized small cysteine-rich domain suggests potential involvement of JTB in interactions with proteins or extracellular matrix and may help to uncover the elusive biological functions of this protein., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

43. Antagonists induce a conformational change in cIAP1 that promotes autoubiquitination.

Author

Dueber EC, Schoeffler AJ, Lingel A, Elliott JM, Fedorova AV, Giannetti AM, Zobel K, Maurer B, Varfolomeev E, Wu P, Wallweber HJ, Hymowitz SG, Deshayes K, Vucic D, and Fairbrother WJ

Subjects

Amino Acid Sequence, Animals, Cell Line, Cell Line, Tumor, Cloning, Molecular, Humans, Hydrophobic and Hydrophilic Interactions, Inhibitor of Apoptosis Proteins metabolism, Mice, Models, Biological, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Proteasome Endopeptidase Complex metabolism, Protein Conformation, Protein Interaction Domains and Motifs, Protein Multimerization, Protein Structure, Secondary, Scattering, Small Angle, Ubiquitin-Protein Ligases chemistry, Ubiquitin-Protein Ligases metabolism, Ubiquitinated Proteins chemistry, Ubiquitinated Proteins metabolism, Ubiquitination, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Inhibitor of Apoptosis Proteins chemistry

Abstract

Inhibitor of apoptosis (IAP) proteins are negative regulators of cell death. IAP family members contain RING domains that impart E3 ubiquitin ligase activity. Binding of endogenous or small-molecule antagonists to select baculovirus IAP repeat (BIR) domains within cellular IAP (cIAP) proteins promotes autoubiquitination and proteasomal degradation and so releases inhibition of apoptosis mediated by cIAP. Although the molecular details of antagonist-BIR domain interactions are well understood, it is not clear how this binding event influences the activity of the RING domain. Here biochemical and structural studies reveal that the unliganded, multidomain cIAP1 sequesters the RING domain within a compact, monomeric structure that prevents RING dimerization. Antagonist binding induces conformational rearrangements that enable RING dimerization and formation of the active E3 ligase.

Published

2011

44. Murine insulin growth factor-like (IGFL) and human IGFL1 proteins are induced in inflammatory skin conditions and bind to a novel tumor necrosis factor receptor family member, IGFLR1.

Author

Lobito AA, Ramani SR, Tom I, Bazan JF, Luis E, Fairbrother WJ, Ouyang W, and Gonzalez LC

Subjects

Animals, Disease Models, Animal, Humans, Insulin-Like Growth Factor I genetics, Mice, Mice, Inbred BALB C, Protein Structure, Tertiary, Psoriasis genetics, Psoriasis pathology, Receptors, Tumor Necrosis Factor genetics, Skin pathology, T-Lymphocytes metabolism, T-Lymphocytes pathology, Wounds and Injuries genetics, Wounds and Injuries pathology, Insulin-Like Growth Factor I biosynthesis, Psoriasis metabolism, Receptors, Tumor Necrosis Factor metabolism, Skin metabolism, Up-Regulation, Wounds and Injuries metabolism

Abstract

Psoriasis is a human skin condition characterized by epidermal hyperproliferation and infiltration of multiple leukocyte populations. In characterizing a novel insulin growth factor (IGF)-like (IGFL) gene in mice (mIGFL), we found transcripts of this gene to be most highly expressed in skin with enhanced expression in models of skin wounding and psoriatic-like inflammation. A possible functional ortholog in humans, IGFL1, was uniquely and significantly induced in psoriatic skin samples. In vitro IGFL1 expression was up-regulated in cultured primary keratinocytes stimulated with tumor necrosis factor α but not by other psoriasis-associated cytokines. Finally, using a secreted and transmembrane protein library, we discovered high affinity interactions between human IGFL1 and mIGFL and the TMEM149 ectodomain. TMEM149 (renamed here as IGFLR1) is an uncharacterized gene with structural similarity to the tumor necrosis factor receptor family. Our studies demonstrate that IGFLR1 is expressed primarily on the surface of mouse T cells. The connection between mIGFL and IGFLR1 receptor suggests mIGFL may influence T cell biology within inflammatory skin conditions.

Published

2011

45. Quinazoline sulfonamides as dual binders of the proteins B-cell lymphoma 2 and B-cell lymphoma extra long with potent proapoptotic cell-based activity.

Author

Sleebs BE, Czabotar PE, Fairbrother WJ, Fairlie WD, Flygare JA, Huang DC, Kersten WJ, Koehler MF, Lessene G, Lowes K, Parisot JP, Smith BJ, Smith ML, Souers AJ, Street IP, Yang H, and Baell JB

Subjects

Animals, Binding, Competitive, Cell Line, Tumor, Crystallography, X-Ray, Drug Screening Assays, Antitumor, Fibroblasts cytology, Fibroblasts drug effects, Humans, Mice, Models, Molecular, Myeloid Cell Leukemia Sequence 1 Protein, Protein Binding, Proto-Oncogene Proteins c-bcl-2 genetics, Quinazolines chemistry, Quinazolines pharmacology, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Apoptosis, Proto-Oncogene Proteins c-bcl-2 metabolism, Quinazolines chemical synthesis, Sulfonamides chemical synthesis, bcl-X Protein metabolism

Abstract

ABT-737 and ABT-263 are potent inhibitors of the BH3 antiapoptotic proteins, Bcl-x(L) and Bcl-2. This class of putative anticancer agents invariantly contains an acylsulfonamide core. We have designed and synthesized a series of novel quinazoline-based inhibitors of Bcl-2 and Bcl-x(L) that contain a heterocyclic alternative to the acylsulfonamide. These compounds exhibit submicromolar, mechanism-based activity in human small-cell lung carcinoma cell lines in the presence of 10% human serum. This comprises the first successful demonstration of a quinazoline sulfonamide core serving as an effective benzoylsulfonamide bioisostere. Additionally, these novel quinazolines comprise only the second known class of Bcl-2 family protein inhibitors to induce mechanism-based cell death.

Published

2011

46. Navitoclax enhances the efficacy of taxanes in non-small cell lung cancer models.

Author

Tan N, Malek M, Zha J, Yue P, Kassees R, Berry L, Fairbrother WJ, Sampath D, and Belmont LD

Subjects

Aniline Compounds administration & dosage, Animals, Antineoplastic Agents pharmacology, Cell Culture Techniques, Cell Cycle, Cell Lineage, Cell Survival, Green Fluorescent Proteins metabolism, Humans, Image Processing, Computer-Assisted, Mice, Mitosis, Neoplasm Transplantation, Paclitaxel administration & dosage, Sulfonamides administration & dosage, Time Factors, bcl-X Protein antagonists & inhibitors, Aniline Compounds pharmacology, Carcinoma, Non-Small-Cell Lung metabolism, Gene Expression Regulation, Neoplastic, Lung Neoplasms metabolism, Sulfonamides pharmacology, Taxoids chemistry

Abstract

Purpose: To explore the potential of navitoclax in combination with taxane-based chemotherapy in the treatment of non-small cell lung cancer (NSCLC) by defining mechanism of synergy and identifying correlative biomarkers., Experimental Design: We treated a panel of NSCLC lines with a dose matrix of paclitaxel and navitoclax (formerly ABT-263), an inhibitor of Bcl-2, Bcl-x(L), and Bcl-w (1), and evaluated synergy. We next used time-lapse microscopy to explore mechanism of synergy. Finally, we developed an immunohistochemical assay and assessed prevalence of Bcl-x(L) in NSCLC tumor tissues., Results: All cell lines exhibit greater than additive response to the combination of navitoclax and a taxane. These results were extended to mouse xenograft tumor models, in which the combination is more efficacious than either single-agent docetaxel or navitoclax. Addition of navitoclax to paclitaxel decreases the time from mitotic entry to cell death and changes cell fate from mitotic slippage to death during mitotic arrest. The relative levels of Bcl-x(L) and Mcl-1 correlate with the extent of synergy, suggesting that cancers with elevated levels of Bcl-x(L) will be relatively resistant to taxane-based therapy but could benefit from the addition of navitoclax to taxane treatment. Finally, a significant percentage of NSCLC patient samples exhibit relatively high Bcl-x(L) levels., Conclusions: The addition of navitoclax to taxane-based chemotherapy in NSCLC has the potential to increase efficacy, particularly in patients whose tumors express high levels of Bcl-x(L)., (©2011 AACR.)

Published

2011

47. Sensitivity to antitubulin chemotherapeutics is regulated by MCL1 and FBW7.

Author

Wertz IE, Kusam S, Lam C, Okamoto T, Sandoval W, Anderson DJ, Helgason E, Ernst JA, Eby M, Liu J, Belmont LD, Kaminker JS, O'Rourke KM, Pujara K, Kohli PB, Johnson AR, Chiu ML, Lill JR, Jackson PK, Fairbrother WJ, Seshagiri S, Ludlam MJ, Leong KG, Dueber EC, Maecker H, Huang DC, and Dixit VM

Subjects

Animals, Apoptosis drug effects, Cell Cycle Proteins genetics, Cell Line, Cell Line, Tumor, Cell Transformation, Neoplastic drug effects, Drug Resistance, Neoplasm, F-Box Proteins genetics, F-Box-WD Repeat-Containing Protein 7, Fibroblasts, Humans, Mice, Mitosis drug effects, Myeloid Cell Leukemia Sequence 1 Protein, Paclitaxel pharmacology, Pharmacogenetics, Phosphorylation drug effects, Polyploidy, Proteasome Endopeptidase Complex metabolism, Protein Binding drug effects, Proto-Oncogene Proteins c-bcl-2 deficiency, Proto-Oncogene Proteins c-bcl-2 genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Ubiquitin-Protein Ligases deficiency, Ubiquitin-Protein Ligases genetics, Vincristine pharmacology, Cell Cycle Proteins metabolism, F-Box Proteins metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism, Tubulin metabolism, Tubulin Modulators pharmacology, Ubiquitin-Protein Ligases metabolism

Abstract

Microtubules have pivotal roles in fundamental cellular processes and are targets of antitubulin chemotherapeutics. Microtubule-targeted agents such as Taxol and vincristine are prescribed widely for various malignancies, including ovarian and breast adenocarcinomas, non-small-cell lung cancer, leukaemias and lymphomas. These agents arrest cells in mitosis and subsequently induce cell death through poorly defined mechanisms. The strategies that resistant tumour cells use to evade death induced by antitubulin agents are also unclear. Here we show that the pro-survival protein MCL1 (ref. 3) is a crucial regulator of apoptosis triggered by antitubulin chemotherapeutics. During mitotic arrest, MCL1 protein levels decline markedly, through a post-translational mechanism, potentiating cell death. Phosphorylation of MCL1 directs its interaction with the tumour-suppressor protein FBW7, which is the substrate-binding component of a ubiquitin ligase complex. The polyubiquitylation of MCL1 then targets it for proteasomal degradation. The degradation of MCL1 was blocked in patient-derived tumour cells that lacked FBW7 or had loss-of-function mutations in FBW7, conferring resistance to antitubulin agents and promoting chemotherapeutic-induced polyploidy. Additionally, primary tumour samples were enriched for FBW7 inactivation and elevated MCL1 levels, underscoring the prominent roles of these proteins in oncogenesis. Our findings suggest that profiling the FBW7 and MCL1 status of tumours, in terms of protein levels, messenger RNA levels and genetic status, could be useful to predict the response of patients to antitubulin chemotherapeutics.

Published

2011

48. c-IAP1 and UbcH5 promote K11-linked polyubiquitination of RIP1 in TNF signalling.

Author

Dynek JN, Goncharov T, Dueber EC, Fedorova AV, Izrael-Tomasevic A, Phu L, Helgason E, Fairbrother WJ, Deshayes K, Kirkpatrick DS, and Vucic D

Subjects

Cell Line, Humans, NF-kappa B metabolism, Protein Binding, Tumor Necrosis Factor-alpha metabolism, Two-Hybrid System Techniques, Ubiquitination, Inhibitor of Apoptosis Proteins metabolism, Nuclear Pore Complex Proteins metabolism, RNA-Binding Proteins metabolism, Ubiquitin-Conjugating Enzymes metabolism

Abstract

Ubiquitin ligases are critical components of the ubiquitination process that determine substrate specificity and, in collaboration with E2 ubiquitin-conjugating enzymes, regulate the nature of polyubiquitin chains assembled on their substrates. Cellular inhibitor of apoptosis (c-IAP1 and c-IAP2) proteins are recruited to TNFR1-associated signalling complexes where they regulate receptor-stimulated NF-κB activation through their RING domain ubiquitin ligase activity. Using a directed yeast two-hybrid screen, we found several novel and previously identified E2 partners of IAP RING domains. Among these, the UbcH5 family of E2 enzymes are critical regulators of the stability of c-IAP1 protein following destabilizing stimuli such as TWEAK or CD40 signalling or IAP antagonists. We demonstrate that c-IAP1 and UbcH5 family promote K11-linked polyubiquitination of receptor-interacting protein 1 (RIP1) in vitro and in vivo. We further show that TNFα-stimulated NF-κB activation involves endogenous K11-linked ubiquitination of RIP1 within the TNFR1 signalling complex that is c-IAP1 and UbcH5 dependent. Lastly, NF-κB essential modifier efficiently binds K11-linked ubiquitin chains, suggesting that this ubiquitin linkage may have a signalling role in the activation of proliferative cellular pathways.

Published

2010

49. Antagonists of inhibitor of apoptosis proteins based on thiazole amide isosteres.

Author

Cohen F, Koehler MF, Bergeron P, Elliott LO, Flygare JA, Franklin MC, Gazzard L, Keteltas SF, Lau K, Ly CQ, Tsui V, and Fairbrother WJ

Subjects

Binding Sites, Biomimetics, Crystallography, X-Ray, Humans, Inhibitor of Apoptosis Proteins metabolism, Models, Molecular, Peptides metabolism, Amides chemistry, Amides pharmacology, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Peptides chemistry, Thiazoles chemistry, Thiazoles pharmacology

Abstract

A series of IAP antagonists based on thiazole or benzothiazole amide isosteres was designed and synthesized. These compounds were tested for binding to the XIAP-BIR3 and ML-IAP BIR using a fluorescence polarization assay. The most potent of these compounds, 19a and 33b, were found to have K(i)'s of 20-30 nM against ML-IAP and 50-60 nM against XIAP-BIR3., (2010 Elsevier Ltd. All rights reserved.)

Published

2010

50. Small-molecule pan-IAP antagonists: a patent review.

Author

Flygare JA and Fairbrother WJ

Subjects

Animals, Antineoplastic Agents chemistry, Apoptosis drug effects, Binding Sites, Humans, Inhibitor of Apoptosis Proteins genetics, Inhibitor of Apoptosis Proteins metabolism, Models, Molecular, Molecular Mimicry, Oligopeptides chemistry, Patents as Topic, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Inhibitor of Apoptosis Proteins antagonists & inhibitors, Oligopeptides pharmacology

Abstract

Importance of the Field: The inhibitor of apoptosis (IAP) proteins are critical regulators of cancer cell survival that have become important targets for therapeutic intervention in human malignancies. One strategy for targeting IAP proteins involves agents that mimic the amino terminus of the endogenous IAP protein antagonist second mitochondria-derived activator of caspases (Smac)/direct IAP-binding protein with low pI (DIABLO) and thus block critical IAP protein interactions., Areas Covered in This Review: This review of the IAP antagonist patent literature covers the period from 2000 to mid-2009. Over 50 patents and patent applications pertaining to IAP antagonists have been published over the past 10 years. In the case of several filings, only the original source is reviewed in this analysis., What the Reader Will Gain: Readers will gain an overview of IAP protein antagonist scaffolds, with representative examples including monovalent and bivalent Smac mimetics, and an understanding of their structure-activity relationships., Take Home Message: The feasibility of disrupting IAP protein interactions with pro-apoptotic proteins using monovalent and bivalent Smac-derived peptidomimetic compounds has been broadly established. Four such compounds have entered or been approved to enter human clinical trials, which will hopefully allow the utility of this potential therapeutic approach to be evaluated in cancer patients.

Published

2010