Your search keyword '"Beresini MH"' showing total 33 results

1. Discovery of Potent, Selective, and Orally Available IRE1α Inhibitors Demonstrating Comparable PD Modulation to IRE1 Knockdown in a Multiple Myeloma Model.

Author

Braun MG, Ashkenazi A, Beveridge RE, Castanedo G, Wallweber HA, Beresini MH, Clark KR, De Bruyn T, Fu L, Gibbons P, Jiang F, Kaufman S, Kan D, Kiefer JR, Leclerc JP, Lemire A, Ly C, Segal E, Sims J, Wang W, Wei W, Zhao L, Schwarz JB, and Rudolph J

Subjects

Humans, Administration, Oral, Animals, Drug Discovery, Mice, Cell Line, Tumor, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents therapeutic use, Rats, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors therapeutic use, Protein Kinase Inhibitors pharmacokinetics, Gene Knockdown Techniques, X-Box Binding Protein 1 metabolism, X-Box Binding Protein 1 genetics, Multiple Myeloma drug therapy, Multiple Myeloma pathology, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases metabolism, Endoribonucleases antagonists & inhibitors, Endoribonucleases metabolism

Abstract

The lack of selective and safe in vivo IRE1α tool molecules has limited the evaluation of IRE1α as a viable target to treat multiple myeloma. Focus on improving the physicochemical properties of a literature compound by decreasing lipophilicity, molecular weight, and basicity allowed the discovery of a novel series with a favorable in vitro safety profile and good oral exposure. These efforts culminated in the identification of a potent and selective in vivo tool compound, G-5758 , that was well tolerated following multiday oral administration of doses up to 500 mg/kg. G-5758 demonstrated comparable pharmacodynamic effects to induced IRE1 knockdown as measured by XBP1s levels in a multiple myeloma model (KMS-11).

Published

2024

2. High-Throughput Kinetic Characterization of Irreversible Covalent Inhibitors of KRAS G12C by Intact Protein MS and Targeted MRM.

Author

Li KS, Quinn JG, Saabye MJ, Guerrero JFS, Nonomiya J, Lian Q, Phung W, Izrayelit Y, Walters BT, Gustafson A, Endres NF, Beresini MH, and Mulvihill MM

Subjects

Kinetics, Drug Discovery, Proto-Oncogene Proteins p21(ras)

Abstract

With recent advances and success in several drugs designed to treat acute and chronic diseases, targeted covalent inhibitors show a resurgence in drug discovery. As covalent inhibition is time-dependent, the preferred quantitative potency metric of irreversible inhibitors is the second-order rate constant k inact / K i , rather than IC 50 . Here, we present the development of a mass spectrometry-based platform for rapid kinetic analysis of irreversible covalent inhibitors. Using a simple liquid handling robot for automated sample preparation and a solid-phase extraction-based RapidFire-MS system for rapid MS analysis, kinetic characterization of covalent inhibitors was performed in high throughput both by intact protein analysis and targeted multiple reaction monitoring (MRM). In addition, a bimolecular reaction model was applied to extract k inact / K i in data fitting, providing tremendous flexibility in the experimental design to characterize covalent inhibitors with various properties. Using KRAS G12C inhibitors as a test case, the platform was demonstrated to be effective for studying covalent inhibitors with a wide range of k inact / K i values from single digit to 3 × 10 5 M -1 s -1 .

Published

2022

3. Activation of the IRE1 RNase through remodeling of the kinase front pocket by ATP-competitive ligands.

Author

Ferri E, Le Thomas A, Wallweber HA, Day ES, Walters BT, Kaufman SE, Braun MG, Clark KR, Beresini MH, Mortara K, Chen YA, Canter B, Phung W, Liu PS, Lammens A, Ashkenazi A, Rudolph J, and Wang W

Subjects

Adenosine Triphosphate chemistry, Allosteric Site drug effects, Crystallography, X-Ray, Endoplasmic Reticulum metabolism, Endoribonucleases chemistry, Gene Knockout Techniques, Humans, Ligands, Models, Molecular, Phosphorylation, Protein Conformation, Protein Folding, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors pharmacology, Protein Multimerization, Protein Serine-Threonine Kinases chemistry, Ribonucleases chemistry, Unfolded Protein Response, Adenosine Triphosphate metabolism, Endoribonucleases metabolism, Protein Serine-Threonine Kinases metabolism, Ribonucleases metabolism

Abstract

Inositol-Requiring Enzyme 1 (IRE1) is an essential component of the Unfolded Protein Response. IRE1 spans the endoplasmic reticulum membrane, comprising a sensory lumenal domain, and tandem kinase and endoribonuclease (RNase) cytoplasmic domains. Excess unfolded proteins in the ER lumen induce dimerization and oligomerization of IRE1, triggering kinase trans-autophosphorylation and RNase activation. Known ATP-competitive small-molecule IRE1 kinase inhibitors either allosterically disrupt or stabilize the active dimeric unit, accordingly inhibiting or stimulating RNase activity. Previous allosteric RNase activators display poor selectivity and/or weak cellular activity. In this study, we describe a class of ATP-competitive RNase activators possessing high selectivity and strong cellular activity. This class of activators binds IRE1 in the kinase front pocket, leading to a distinct conformation of the activation loop. Our findings reveal exquisitely precise interdomain regulation within IRE1, advancing the mechanistic understanding of this important enzyme and its investigation as a potential small-molecule therapeutic target.

Published

2020

4. Design of Organo-Peptides As Bipartite PCSK9 Antagonists.

Author

Burdick DJ, Skelton NJ, Ultsch M, Beresini MH, Eigenbrot C, Li W, Zhang Y, Nguyen H, Kong-Beltran M, Quinn JG, and Kirchhofer D

Subjects

Binding Sites, Crystallography, X-Ray, Drug Design, Hep G2 Cells, Humans, Molecular Structure, Peptides chemistry, Peptides metabolism, Proprotein Convertase 9 chemistry, Proprotein Convertase 9 metabolism, Protein Binding, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors metabolism, PCSK9 Inhibitors, Peptides pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

Proprotein convertase subtilisin/kexin 9 (PCSK9) has become an important therapeutic target for lipid lowering, since it regulates low-density lipoprotein cholesterol (LDL-c) levels by binding to liver LDL receptors (LDLR) and effecting their intracellular degradation. However, the development of small molecule inhibitors is hampered by the lack of attractive PCSK9 target sites. We recently discovered helical peptides that are able to bind to a cryptic groove site on PCSK9, which is situated in proximity to the main LDLR binding site. Here, we designed potent bipartite PCSK9 inhibitors by appending organic moieties to a helical groove-binding peptide to reach a hydrophobic pocket in the proximal LDLR binding region. The ultimately designed 1-amino-4-phenylcyclohexane-1-carbonyl extension improved the peptide affinity by >100-fold, yielding organo-peptide antagonists that potently inhibited PCSK9 binding to LDLR and preserved cellular LDLR. These new bipartite antagonists have reduced mass and improved potency compared to the first-generation peptide antagonists, further validating the PCSK9 groove as a viable therapeutic target site.

Published

2020

5. Disruption of IRE1α through its kinase domain attenuates multiple myeloma.

Author

Harnoss JM, Le Thomas A, Shemorry A, Marsters SA, Lawrence DA, Lu M, Chen YA, Qing J, Totpal K, Kan D, Segal E, Merchant M, Reichelt M, Ackerly Wallweber H, Wang W, Clark K, Kaufman S, Beresini MH, Laing ST, Sandoval W, Lorenzo M, Wu J, Ly J, De Bruyn T, Heidersbach A, Haley B, Gogineni A, Weimer RM, Lee D, Braun MG, Rudolph J, VanWyngarden MJ, Sherbenou DW, Gomez-Bougie P, Amiot M, Acosta-Alvear D, Walter P, and Ashkenazi A

Subjects

Aged, Animals, Bortezomib pharmacology, Endoplasmic Reticulum Stress genetics, Endoribonucleases antagonists & inhibitors, Female, Gene Expression Regulation, Neoplastic drug effects, Humans, Lenalidomide pharmacology, Male, Mice, Middle Aged, Multiple Myeloma genetics, Multiple Myeloma pathology, Protein Serine-Threonine Kinases antagonists & inhibitors, Signal Transduction drug effects, Unfolded Protein Response genetics, X-Box Binding Protein 1 genetics, Xenograft Model Antitumor Assays, Endoribonucleases genetics, Multiple Myeloma drug therapy, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases genetics

Abstract

Multiple myeloma (MM) arises from malignant immunoglobulin (Ig)-secreting plasma cells and remains an incurable, often lethal disease despite therapeutic advances. The unfolded-protein response sensor IRE1α supports protein secretion by deploying a kinase-endoribonuclease module to activate the transcription factor XBP1s. MM cells may co-opt the IRE1α-XBP1s pathway; however, the validity of IRE1α as a potential MM therapeutic target is controversial. Genetic disruption of IRE1α or XBP1s, or pharmacologic IRE1α kinase inhibition, attenuated subcutaneous or orthometastatic growth of MM tumors in mice and augmented efficacy of two established frontline antimyeloma agents, bortezomib and lenalidomide. Mechanistically, IRE1α perturbation inhibited expression of key components of the endoplasmic reticulum-associated degradation machinery, as well as secretion of Ig light chains and of cytokines and chemokines known to promote MM growth. Selective IRE1α kinase inhibition reduced viability of CD138 + plasma cells while sparing CD138 - cells derived from bone marrows of newly diagnosed or posttreatment-relapsed MM patients, in both US- and European Union-based cohorts. Effective IRE1α inhibition preserved glucose-induced insulin secretion by pancreatic microislets and viability of primary hepatocytes in vitro, as well as normal tissue homeostasis in mice. These results establish a strong rationale for developing kinase-directed inhibitors of IRE1α for MM therapy., Competing Interests: Conflict of interest statement: J.M.H., A.L.T., A.S., S.A.M., D.A.L., M. Lu, Y.-C.A.C., J.Q., K.T., D.K., E.S., M.M., M.R., H.A.W., W.W., K.C., S.K., M.H.B., S.T.L., W.S., M. Lorenzo, J.W., J.L., T.D.B., A.H., B.H., A.G., R.M.W., D.L., M.-G.B., J.R., and A.A. were employees of Genentech, Inc. during performance of this work., (Copyright © 2019 the Author(s). Published by PNAS.)

Published

2019

6. GNE-371, a Potent and Selective Chemical Probe for the Second Bromodomains of Human Transcription-Initiation-Factor TFIID Subunit 1 and Transcription-Initiation-Factor TFIID Subunit 1-like.

Author

Wang S, Tsui V, Crawford TD, Audia JE, Burdick DJ, Beresini MH, Côté A, Cummings R, Duplessis M, Flynn EM, Hewitt MC, Huang HR, Jayaram H, Jiang Y, Joshi S, Murray J, Nasveschuk CG, Pardo E, Poy F, Romero FA, Tang Y, Taylor AM, Wang J, Xu Z, Zawadzke LE, Zhu X, Albrecht BK, Magnuson SR, Bellon S, and Cochran AG

Subjects

Humans, Models, Molecular, Protein Conformation, Protein Domains, Benzimidazoles metabolism, Drug Design, Molecular Probes metabolism, Transcription Factor TFIID chemistry, Transcription Factor TFIID metabolism

Abstract

The biological functions of the dual bromodomains of human transcription-initiation-factor TFIID subunit 1 (TAF1(1,2)) remain unknown, although TAF1 has been identified as a potential target for oncology research. Here, we describe the discovery of a potent and selective in vitro tool compound for TAF1(2), starting from a previously reported lead. A cocrystal structure of lead compound 2 bound to TAF1(2) enabled structure-based design and structure-activity-relationship studies that ultimately led to our in vitro tool compound, 27 (GNE-371). Compound 27 binds TAF1(2) with an IC 50 of 10 nM while maintaining excellent selectivity over other bromodomain-family members. Compound 27 is also active in a cellular-TAF1(2) target-engagement assay (IC 50 = 38 nM) and exhibits antiproliferative synergy with the BET inhibitor JQ1, suggesting engagement of endogenous TAF1 by 27 and further supporting the use of 27 in mechanistic and target-validation studies.

Published

2018

7. Structural basis for dual-mode inhibition of the ABC transporter MsbA.

Author

Ho H, Miu A, Alexander MK, Garcia NK, Oh A, Zilberleyb I, Reichelt M, Austin CD, Tam C, Shriver S, Hu H, Labadie SS, Liang J, Wang L, Wang J, Lu Y, Purkey HE, Quinn J, Franke Y, Clark K, Beresini MH, Tan MW, Sellers BD, Maurer T, Koehler MFT, Wecksler AT, Kiefer JR, Verma V, Xu Y, Nishiyama M, Payandeh J, and Koth CM

Subjects

ATP-Binding Cassette Transporters metabolism, Allosteric Regulation drug effects, Bacterial Proteins metabolism, Binding Sites drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Escherichia coli chemistry, Hydrocarbons chemistry, Hydrocarbons metabolism, Lipopolysaccharides chemistry, Lipopolysaccharides metabolism, Lipopolysaccharides pharmacology, Models, Molecular, Protein Domains drug effects, ATP-Binding Cassette Transporters antagonists & inhibitors, ATP-Binding Cassette Transporters chemistry, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins chemistry, Quinolines chemistry, Quinolines pharmacology

Abstract

The movement of core-lipopolysaccharide across the inner membrane of Gram-negative bacteria is catalysed by an essential ATP-binding cassette transporter, MsbA. Recent structures of MsbA and related transporters have provided insights into the molecular basis of active lipid transport; however, structural information about their pharmacological modulation remains limited. Here we report the 2.9 Å resolution structure of MsbA in complex with G907, a selective small-molecule antagonist with bactericidal activity, revealing an unprecedented mechanism of ABC transporter inhibition. G907 traps MsbA in an inward-facing, lipopolysaccharide-bound conformation by wedging into an architecturally conserved transmembrane pocket. A second allosteric mechanism of antagonism occurs through structural and functional uncoupling of the nucleotide-binding domains. This study establishes a framework for the selective modulation of ABC transporters and provides rational avenues for the design of new antibiotics and other therapeutics targeting this protein family.

Published

2018

8. Mechanism-specific assay design facilitates the discovery of Nav1.7-selective inhibitors.

Author

Chernov-Rogan T, Li T, Lu G, Verschoof H, Khakh K, Jones SW, Beresini MH, Liu C, Ortwine DF, McKerrall SJ, Hackos DH, Sutherlin D, Cohen CJ, and Chen J

Subjects

Animals, High-Throughput Screening Assays, Humans, Insect Proteins, Membrane Potentials, NAV1.7 Voltage-Gated Sodium Channel drug effects, NAV1.7 Voltage-Gated Sodium Channel genetics, Rats, Veratridine, Wasp Venoms, Drug Discovery methods, Molecular Targeted Therapy, Voltage-Gated Sodium Channel Blockers analysis

Abstract

Many ion channels, including Nav1.7, Cav1.3, and Kv1.3, are linked to human pathologies and are important therapeutic targets. To develop efficacious and safe drugs, subtype-selective modulation is essential, but has been extremely difficult to achieve. We postulate that this challenge is caused by the poor assay design, and investigate the Nav1.7 membrane potential assay, one of the most extensively employed screening assays in modern drug discovery. The assay uses veratridine to activate channels, and compounds are identified based on the inhibition of veratridine-evoked activities. We show that this assay is biased toward nonselective pore blockers and fails to detect the most potent, selective voltage-sensing domain 4 (VSD4) blockers, including PF-05089771 (PF-771) and GX-936. By eliminating a key binding site for pore blockers and replacing veratridine with a VSD-4 binding activator, we directed the assay toward non-pore-blocking mechanisms and discovered Nav1.7-selective chemical scaffolds. Hence, we address a major hurdle in Nav1.7 drug discovery, and this mechanistic approach to assay design is applicable to Cav3.1, Kv1.3, and many other ion channels to facilitate drug discovery., Competing Interests: Conflict of interest statement: H.V., K.K., and C.J.C. are employees of Xenon Pharmaceuticals; and T.C.-R., T.L., G.L., S.W.J., M.H.B., C.L., D.F.O., S.J.M., D.H.H., D.S., and J.C. are employees of Genentech., (Copyright © 2018 the Author(s). Published by PNAS.)

Published

2018

9. Design and synthesis of a biaryl series as inhibitors for the bromodomains of CBP/P300.

Author

Lai KW, Romero FA, Tsui V, Beresini MH, de Leon Boenig G, Bronner SM, Chen K, Chen Z, Choo EF, Crawford TD, Cyr P, Kaufman S, Li Y, Liao J, Liu W, Ly J, Murray J, Shen W, Wai J, Wang F, Zhu C, Zhu X, and Magnuson S

Subjects

Animals, Binding Sites, Biphenyl Compounds chemical synthesis, Biphenyl Compounds metabolism, Cell Cycle Proteins, Crystallography, X-Ray, Half-Life, Humans, Hydrogen Bonding, Inhibitory Concentration 50, Mice, Microsomes, Liver metabolism, Molecular Dynamics Simulation, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins metabolism, Protein Structure, Tertiary, Rats, Structure-Activity Relationship, Transcription Factors antagonists & inhibitors, Transcription Factors metabolism, p300-CBP Transcription Factors metabolism, Biphenyl Compounds chemistry, Drug Design, p300-CBP Transcription Factors antagonists & inhibitors

Abstract

A novel, potent, and orally bioavailable inhibitor of the bromodomain of CBP, compound 35 (GNE-207), has been identified through SAR investigations focused on optimizing al bicyclic heteroarene to replace the aniline present in the published GNE-272 series. Compound 35 has excellent CBP potency (CBP IC 50  = 1 nM, MYC EC 50  = 18 nM), a selectively index of >2500-fold against BRD4(1), and exhibits a good pharmacokinetic profile., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2018

10. A Unique Approach to Design Potent and Selective Cyclic Adenosine Monophosphate Response Element Binding Protein, Binding Protein (CBP) Inhibitors.

Author

Bronner SM, Murray J, Romero FA, Lai KW, Tsui V, Cyr P, Beresini MH, de Leon Boenig G, Chen Z, Choo EF, Clark KR, Crawford TD, Jayaram H, Kaufman S, Li R, Li Y, Liao J, Liang X, Liu W, Ly J, Maher J, Wai J, Wang F, Zheng A, Zhu X, and Magnuson S

Subjects

Animals, Asparagine chemistry, Asparagine metabolism, Binding Sites, Cell Cycle Proteins, Crystallography, X-Ray, Female, Fluorescence Resonance Energy Transfer methods, Mice, Inbred Strains, Molecular Docking Simulation, Nuclear Proteins antagonists & inhibitors, Protein Domains, Pyrazoles chemistry, Pyridines chemistry, Quinolines chemistry, Transcription Factors antagonists & inhibitors, p300-CBP Transcription Factors chemistry, p300-CBP Transcription Factors metabolism, High-Throughput Screening Assays methods, p300-CBP Transcription Factors antagonists & inhibitors

Abstract

The epigenetic regulator CBP/P300 presents a novel therapeutic target for oncology. Previously, we disclosed the development of potent and selective CBP bromodomain inhibitors by first identifying pharmacophores that bind the KAc region and then building into the LPF shelf. Herein, we report the "hybridization" of a variety of KAc-binding fragments with a tetrahydroquinoline scaffold that makes optimal interactions with the LPF shelf, imparting enhanced potency and selectivity to the hybridized ligand. To demonstrate the utility of our hybridization approach, two analogues containing unique Asn binders and the optimized tetrahydroquinoline moiety were rapidly optimized to yield single-digit nanomolar inhibitors of CBP with exquisite selectivity over BRD4(1) and the broader bromodomain family.

Published

2017

11. GNE-781, A Highly Advanced Potent and Selective Bromodomain Inhibitor of Cyclic Adenosine Monophosphate Response Element Binding Protein, Binding Protein (CBP).

Author

Romero FA, Murray J, Lai KW, Tsui V, Albrecht BK, An L, Beresini MH, de Leon Boenig G, Bronner SM, Chan EW, Chen KX, Chen Z, Choo EF, Clagg K, Clark K, Crawford TD, Cyr P, de Almeida Nagata D, Gascoigne KE, Grogan JL, Hatzivassiliou G, Huang W, Hunsaker TL, Kaufman S, Koenig SG, Li R, Li Y, Liang X, Liao J, Liu W, Ly J, Maher J, Masui C, Merchant M, Ran Y, Taylor AM, Wai J, Wang F, Wei X, Yu D, Zhu BY, Zhu X, and Magnuson S

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacokinetics, CREB-Binding Protein chemistry, Dogs, Female, Forkhead Transcription Factors genetics, Forkhead Transcription Factors metabolism, HEK293 Cells, Humans, Macaca fascicularis, Male, Mice, Protein Domains, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc metabolism, Pyrazoles chemical synthesis, Pyrazoles chemistry, Pyrazoles pharmacokinetics, Pyridines chemical synthesis, Pyridines chemistry, Pyridines pharmacokinetics, RNA genetics, Rats, Sprague-Dawley, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, CREB-Binding Protein antagonists & inhibitors, Pyrazoles pharmacology, Pyridines pharmacology

Abstract

Inhibition of the bromodomain of the transcriptional regulator CBP/P300 is an especially interesting new therapeutic approach in oncology. We recently disclosed in vivo chemical tool 1 (GNE-272) for the bromodomain of CBP that was moderately potent and selective over BRD4(1). In pursuit of a more potent and selective CBP inhibitor, we used structure-based design. Constraining the aniline of 1 into a tetrahydroquinoline motif maintained potency and increased selectivity 2-fold. Structure-activity relationship studies coupled with further structure-based design targeting the LPF shelf, BC loop, and KAc regions allowed us to significantly increase potency and selectivity, resulting in the identification of non-CNS penetrant 19 (GNE-781, TR-FRET IC 50 = 0.94 nM, BRET IC 50 = 6.2 nM; BRD4(1) IC 50 = 5100 nΜ) that maintained good in vivo PK properties in multiple species. Compound 19 displays antitumor activity in an AML tumor model and was also shown to decrease Foxp3 transcript levels in a dose dependent manner.

Published

2017

12. High throughput screening identifies novel, cell cycle-arresting small molecule enhancers of transient protein expression.

Author

Meyer HJ, Turincio R, Ng S, Li J, Wilson B, Chan P, Zak M, Reilly D, Beresini MH, and Wong AW

Subjects

Animals, Antibodies genetics, Antibodies immunology, Antibody Formation immunology, CHO Cells, Cell Cycle Checkpoints drug effects, Cricetinae, Cricetulus, HEK293 Cells, Humans, Immunoglobulin G genetics, Immunoglobulin G immunology, Polyethyleneimine pharmacology, Recombinant Proteins genetics, Recombinant Proteins immunology, Small Molecule Libraries pharmacology, Transfection, Antibody Formation genetics, High-Throughput Screening Assays, Immunoglobulin G biosynthesis, Recombinant Proteins biosynthesis

Abstract

Transient gene expression in mammalian cells is an efficient process for producing recombinant proteins for various research applications to support large molecule therapeutics development. For the first time, we report a high throughput small molecule (SM) screen to identify novel compounds that increase antibody titers after polyethylenimine (PEI) transient transfection of a HEK293 cell line. After screening 31,413 SMs in a 50 μL scaled-down process, we validated 164 SMs to improve yields by up to twofold. The titer increase mediated by the SMs varied for different antibodies. SM dose optimizations resulted in almost threefold higher titers. The top 2, structurally distinct SM hits, increased antibody titers more than twofold in a 1 mL production process. Averaged across three antibodies of different expression levels, the compounds enhanced transient productivity by ∼80%. Intriguingly, both compounds arrested cells in the G2/M cell cycle phase leading to a decrease in growth and nutrient consumption, while elevating titer, nuclear plasmid DNA (pDNA) copy numbers, and mRNA levels. © 2017 American Institute of Chemical Engineers Biotechnol. Prog., 3:1579-1588, 2017., (© 2017 American Institute of Chemical Engineers.)

Published

2017

13. USP7 small-molecule inhibitors interfere with ubiquitin binding.

Author

Kategaya L, Di Lello P, Rougé L, Pastor R, Clark KR, Drummond J, Kleinheinz T, Lin E, Upton JP, Prakash S, Heideker J, McCleland M, Ritorto MS, Alessi DR, Trost M, Bainbridge TW, Kwok MCM, Ma TP, Stiffler Z, Brasher B, Tang Y, Jaishankar P, Hearn BR, Renslo AR, Arkin MR, Cohen F, Yu K, Peale F, Gnad F, Chang MT, Klijn C, Blackwood E, Martin SE, Forrest WF, Ernst JA, Ndubaku C, Wang X, Beresini MH, Tsui V, Schwerdtfeger C, Blake RA, Murray J, Maurer T, and Wertz IE

Subjects

Animals, Binding, Competitive, Cell Line, Tumor, Drug Synergism, Female, Humans, Mice, Mice, SCID, Models, Molecular, Neoplasms drug therapy, Neoplasms enzymology, Neoplasms pathology, Protein Binding, Proto-Oncogene Proteins c-mdm2 metabolism, Proto-Oncogene Proteins c-pim-1 antagonists & inhibitors, Substrate Specificity, Tumor Suppressor Protein p53 deficiency, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Ubiquitin chemistry, Ubiquitin-Specific Peptidase 7 chemistry, Ubiquitin-Specific Peptidase 7 deficiency, Ubiquitin-Specific Peptidase 7 metabolism, Aminopyridines chemistry, Aminopyridines pharmacology, Indazoles chemistry, Indazoles pharmacology, Phenols chemistry, Phenols pharmacology, Pyridines chemistry, Pyridines pharmacology, Ubiquitin metabolism, Ubiquitin-Specific Peptidase 7 antagonists & inhibitors

Abstract

The ubiquitin system regulates essential cellular processes in eukaryotes. Ubiquitin is ligated to substrate proteins as monomers or chains and the topology of ubiquitin modifications regulates substrate interactions with specific proteins. Thus ubiquitination directs a variety of substrate fates including proteasomal degradation. Deubiquitinase enzymes cleave ubiquitin from substrates and are implicated in disease; for example, ubiquitin-specific protease-7 (USP7) regulates stability of the p53 tumour suppressor and other proteins critical for tumour cell survival. However, developing selective deubiquitinase inhibitors has been challenging and no co-crystal structures have been solved with small-molecule inhibitors. Here, using nuclear magnetic resonance-based screening and structure-based design, we describe the development of selective USP7 inhibitors GNE-6640 and GNE-6776. These compounds induce tumour cell death and enhance cytotoxicity with chemotherapeutic agents and targeted compounds, including PIM kinase inhibitors. Structural studies reveal that GNE-6640 and GNE-6776 non-covalently target USP7 12 Å distant from the catalytic cysteine. The compounds attenuate ubiquitin binding and thus inhibit USP7 deubiquitinase activity. GNE-6640 and GNE-6776 interact with acidic residues that mediate hydrogen-bond interactions with the ubiquitin Lys48 side chain, suggesting that USP7 preferentially interacts with and cleaves ubiquitin moieties that have free Lys48 side chains. We investigated this idea by engineering di-ubiquitin chains containing differential proximal and distal isotopic labels and measuring USP7 binding by nuclear magnetic resonance. This preferential binding protracted the depolymerization kinetics of Lys48-linked ubiquitin chains relative to Lys63-linked chains. In summary, engineering compounds that inhibit USP7 activity by attenuating ubiquitin binding suggests opportunities for developing other deubiquitinase inhibitors and may be a strategy more broadly applicable to inhibiting proteins that require ubiquitin binding for full functional activity.

Published

2017

14. Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer.

Author

Jin L, Garcia J, Chan E, de la Cruz C, Segal E, Merchant M, Kharbanda S, Raisner R, Haverty PM, Modrusan Z, Ly J, Choo E, Kaufman S, Beresini MH, Romero FA, Magnuson S, and Gascoigne KE

Subjects

Animals, Cell Growth Processes drug effects, Cell Line, Tumor, E1A-Associated p300 Protein deficiency, E1A-Associated p300 Protein genetics, E1A-Associated p300 Protein metabolism, Female, Gene Expression, Gene Knockdown Techniques, Humans, Male, Mice, Mice, SCID, Molecular Targeted Therapy, Prostatic Neoplasms, Castration-Resistant genetics, Prostatic Neoplasms, Castration-Resistant metabolism, Prostatic Neoplasms, Castration-Resistant pathology, Protein Domains, Random Allocation, Receptors, Androgen metabolism, Signal Transduction drug effects, Transfection, Xenograft Model Antitumor Assays, E1A-Associated p300 Protein antagonists & inhibitors, Prostatic Neoplasms, Castration-Resistant drug therapy, Small Molecule Libraries pharmacology

Abstract

Resistance invariably develops to antiandrogen therapies used to treat newly diagnosed prostate cancers, but effective treatments for castration-resistant disease remain elusive. Here, we report that the transcriptional coactivator CBP/p300 is required to maintain the growth of castration-resistant prostate cancer. To exploit this vulnerability, we developed a novel small-molecule inhibitor of the CBP/p300 bromodomain that blocks prostate cancer growth in vitro and in vivo Molecular dissection of the consequences of drug treatment revealed a critical role for CBP/p300 in histone acetylation required for the transcriptional activity of the androgen receptor and its target gene expression. Our findings offer a preclinical proof of concept for small-molecule therapies to target the CBP/p300 bromodomain as a strategy to treat castration-resistant prostate cancer. Cancer Res; 77(20); 5564-75. ©2017 AACR ., (©2017 American Association for Cancer Research.)

Published

2017

15. Discovery of a cryptic peptide-binding site on PCSK9 and design of antagonists.

Author

Zhang Y, Ultsch M, Skelton NJ, Burdick DJ, Beresini MH, Li W, Kong-Beltran M, Peterson A, Quinn J, Chiu C, Wu Y, Shia S, Moran P, Di Lello P, Eigenbrot C, and Kirchhofer D

Subjects

Binding Sites, Enzyme Inhibitors isolation & purification, Humans, Molecular Docking Simulation, Peptide Library, Peptides isolation & purification, Enzyme Inhibitors metabolism, PCSK9 Inhibitors, Peptides metabolism, Proprotein Convertase 9 metabolism

Abstract

Proprotein convertase subtilisin/kexin type 9 (PCSK9) regulates plasma LDL cholesterol (LDL-c) levels by promoting the degradation of liver LDL receptors (LDLRs). Antibodies that inhibit PCSK9 binding to the EGF(A) domain of the LDLR are effective in lowering LDL-c. However, the discovery of small-molecule therapeutics is hampered by difficulty in targeting the relatively flat EGF(A)-binding site on PCSK9. Here we demonstrate that it is possible to target this site, based on the finding that the PCSK9 P' helix displays conformational flexibility. As a consequence, the vacated N-terminal groove of PCSK9, which is adjacent to the EGF(A)-binding site, is in fact accessible to small peptides. In phage-display experiments, the EGF(A)-mimicking peptide Pep2-8 was used as an anchor peptide for the attachment of an extension peptide library directed toward the groove site. Guided by structural information, we further engineered the identified groove-binding peptides into antagonists, which encroach on the EGF(A)-binding site and inhibit LDLR binding.

Published

2017

16. Discovery of a Potent and Selective in Vivo Probe (GNE-272) for the Bromodomains of CBP/EP300.

Author

Crawford TD, Romero FA, Lai KW, Tsui V, Taylor AM, de Leon Boenig G, Noland CL, Murray J, Ly J, Choo EF, Hunsaker TL, Chan EW, Merchant M, Kharbanda S, Gascoigne KE, Kaufman S, Beresini MH, Liao J, Liu W, Chen KX, Chen Z, Conery AR, Côté A, Jayaram H, Jiang Y, Kiefer JR, Kleinheinz T, Li Y, Maher J, Pardo E, Poy F, Spillane KL, Wang F, Wang J, Wei X, Xu Z, Xu Z, Yen I, Zawadzke L, Zhu X, Bellon S, Cummings R, Cochran AG, Albrecht BK, and Magnuson S

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Dogs, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Female, Humans, Madin Darby Canine Kidney Cells, Mice, Mice, Nude, Models, Molecular, Molecular Structure, Pyrazoles chemical synthesis, Pyrazoles chemistry, Pyridones chemical synthesis, Pyridones chemistry, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Drug Discovery, Pyrazoles pharmacology, Pyridones pharmacology, p300-CBP Transcription Factors antagonists & inhibitors

Abstract

The single bromodomain of the closely related transcriptional regulators CBP/EP300 is a target of much recent interest in cancer and immune system regulation. A co-crystal structure of a ligand-efficient screening hit and the CBP bromodomain guided initial design targeting the LPF shelf, ZA loop, and acetylated lysine binding regions. Structure-activity relationship studies allowed us to identify a more potent analogue. Optimization of permeability and microsomal stability and subsequent improvement of mouse hepatocyte stability afforded 59 (GNE-272, TR-FRET IC 50 = 0.02 μM, BRET IC 50 = 0.41 μM, BRD4(1) IC 50 = 13 μM) that retained the best balance of cell potency, selectivity, and in vivo PK. Compound 59 showed a marked antiproliferative effect in hematologic cancer cell lines and modulates MYC expression in vivo that corresponds with antitumor activity in an AML tumor model.

Published

2016

17. Diving into the Water: Inducible Binding Conformations for BRD4, TAF1(2), BRD9, and CECR2 Bromodomains.

Author

Crawford TD, Tsui V, Flynn EM, Wang S, Taylor AM, Côté A, Audia JE, Beresini MH, Burdick DJ, Cummings R, Dakin LA, Duplessis M, Good AC, Hewitt MC, Huang HR, Jayaram H, Kiefer JR, Jiang Y, Murray J, Nasveschuk CG, Pardo E, Poy F, Romero FA, Tang Y, Wang J, Xu Z, Zawadzke LE, Zhu X, Albrecht BK, Magnuson SR, Bellon S, and Cochran AG

Subjects

Binding Sites drug effects, Cell Cycle Proteins, Dose-Response Relationship, Drug, Fluorescence Resonance Energy Transfer, Fluorometry, Histone Acetyltransferases metabolism, Humans, Ligands, Models, Molecular, Molecular Conformation, Nuclear Proteins metabolism, Pyridones chemical synthesis, Pyridones chemistry, Pyrroles chemical synthesis, Pyrroles chemistry, Structure-Activity Relationship, TATA-Binding Protein Associated Factors metabolism, Transcription Factor TFIID metabolism, Transcription Factors metabolism, Histone Acetyltransferases antagonists & inhibitors, Nuclear Proteins antagonists & inhibitors, Pyridones pharmacology, Pyrroles pharmacology, TATA-Binding Protein Associated Factors antagonists & inhibitors, Transcription Factor TFIID antagonists & inhibitors, Transcription Factors antagonists & inhibitors, Water chemistry

Abstract

The biological role played by non-BET bromodomains remains poorly understood, and it is therefore imperative to identify potent and highly selective inhibitors to effectively explore the biology of individual bromodomain proteins. A ligand-efficient nonselective bromodomain inhibitor was identified from a 6-methyl pyrrolopyridone fragment. Small hydrophobic substituents replacing the N-methyl group were designed directing toward the conserved bromodomain water pocket, and two distinct binding conformations were then observed. The substituents either directly displaced and rearranged the conserved solvent network, as in BRD4(1) and TAF1(2), or induced a narrow hydrophobic channel adjacent to the lipophilic shelf, as in BRD9 and CECR2. The preference of distinct substituents for individual bromodomains provided selectivity handles useful for future lead optimization efforts for selective BRD9, CECR2, and TAF1(2) inhibitors.

Published

2016

18. Fragment-Based Discovery of a Selective and Cell-Active Benzodiazepinone CBP/EP300 Bromodomain Inhibitor (CPI-637).

Author

Taylor AM, Côté A, Hewitt MC, Pastor R, Leblanc Y, Nasveschuk CG, Romero FA, Crawford TD, Cantone N, Jayaram H, Setser J, Murray J, Beresini MH, de Leon Boenig G, Chen Z, Conery AR, Cummings RT, Dakin LA, Flynn EM, Huang OW, Kaufman S, Keller PJ, Kiefer JR, Lai T, Li Y, Liao J, Liu W, Lu H, Pardo E, Tsui V, Wang J, Wang Y, Xu Z, Yan F, Yu D, Zawadzke L, Zhu X, Zhu X, Sims RJ 3rd, Cochran AG, Bellon S, Audia JE, Magnuson S, and Albrecht BK

Abstract

CBP and EP300 are highly homologous, bromodomain-containing transcription coactivators involved in numerous cellular pathways relevant to oncology. As part of our effort to explore the potential therapeutic implications of selectively targeting bromodomains, we set out to identify a CBP/EP300 bromodomain inhibitor that was potent both in vitro and in cellular target engagement assays and was selective over the other members of the bromodomain family. Reported here is a series of cell-potent and selective probes of the CBP/EP300 bromodomains, derived from the fragment screening hit 4-methyl-1,3,4,5-tetrahydro-2H-benzo[b][1,4]diazepin-2-one.

Published

2016

19. Compound Transfer by Acoustic Droplet Ejection Promotes Quality and Efficiency in Ultra-High-Throughput Screening Campaigns.

Author

Dawes TD, Turincio R, Jones SW, Rodriguez RA, Gadiagellan D, Thana P, Clark KR, Gustafson AE, Orren L, Liimatta M, Gross DP, Maurer T, and Beresini MH

Subjects

Acoustics, Biomedical Technology instrumentation, Data Interpretation, Statistical, Drug Evaluation, Preclinical instrumentation, High-Throughput Screening Assays instrumentation, Small Molecule Libraries, Software, Solutions, Biomedical Technology methods, Drug Evaluation, Preclinical methods, High-Throughput Screening Assays methods

Abstract

Acoustic droplet ejection (ADE) as a means of transferring library compounds has had a dramatic impact on the way in which high-throughput screening campaigns are conducted in many laboratories. Two Labcyte Echo ADE liquid handlers form the core of the compound transfer operation in our 1536-well based ultra-high-throughput screening (uHTS) system. Use of these instruments has promoted flexibility in compound formatting in addition to minimizing waste and eliminating compound carryover. We describe the use of ADE for the generation of assay-ready plates for primary screening as well as for follow-up dose-response evaluations. Custom software has enabled us to harness the information generated by the ADE instrumentation. Compound transfer via ADE also contributes to the screening process outside of the uHTS system. A second fully automated ADE-based system has been used to augment the capacity of the uHTS system as well as to permit efficient use of previously picked compound aliquots for secondary assay evaluations. Essential to the utility of ADE in the high-throughput screening process is the high quality of the resulting data. Examples of data generated at various stages of high-throughput screening campaigns are provided. Advantages and disadvantages of the use of ADE in high-throughput screening are discussed., (© 2015 Society for Laboratory Automation and Screening.)

Published

2016

20. Development of a Potent, Specific CDK8 Kinase Inhibitor Which Phenocopies CDK8/19 Knockout Cells.

Author

Koehler MF, Bergeron P, Blackwood EM, Bowman K, Clark KR, Firestein R, Kiefer JR, Maskos K, McCleland ML, Orren L, Salphati L, Schmidt S, Schneider EV, Wu J, and Beresini MH

Abstract

Beginning with promiscuous COT inhibitors, which were found to inhibit CDK8, a series of 6-aza-benzothiophene containing compounds were developed into potent, selective CDK8 inhibitors. When cocrystallized with CDK8 and cyclin C, these compounds exhibit an unusual binding mode, making a single hydrogen bond to the hinge residue A100, a second to K252, and a key cation-π interaction with R356. Structure-based drug design resulted in tool compounds 13 and 32, which are highly potent, kinase selective, permeable compounds with a free fraction >2% and no measurable efflux. Despite these attractive properties, these compounds exhibit weak antiproliferative activity in the HCT-116 colon cancer cell line. Further examination of the activity of 32 in this cell line revealed that the compound reduced phosphorylation of the known CDK8 substrate STAT1 in a manner identical to a CDK8 knockout clone, illustrating the complex effects of inhibition of CDK8 kinase activity in proliferation in these cells.

Published

2016

21. Small-Molecule Library Subset Screening as an Aid for Accelerating Lead Identification.

Author

Beresini MH, Liu Y, Dawes TD, Clark KR, Orren L, Schmidt S, Turincio R, Jones SW, Rodriguez RA, Thana P, Hascall D, Gross DP, and Skelton NJ

Subjects

Chemistry, Pharmaceutical methods, Dose-Response Relationship, Drug, Drug Discovery, Inhibitory Concentration 50, Ligands, Reproducibility of Results, Drug Evaluation, Preclinical methods, High-Throughput Screening Assays methods, Small Molecule Libraries chemistry

Abstract

Several small-compound library subsets (14,000 to 56,000) have been established to complement screening of a larger Genentech corporate library (~1,300,000). Two validation sets (~1% of the total library) containing compounds representative of the main library were chosen by selection of plates or individual compounds. Use of these subsets guided selection of assay configuration, validated assay reproducibility, and provided estimates of hit rates expected from our full library. A larger diversity subset representing the scaffold diversity of the full library (3.4% of the total) was designed for screening more challenging targets with limited reagent availability or low-throughput assays. Retrospective analysis of this subset showed hit rates similar to those of the main library while recovering a higher proportion of hit scaffolds. Finally, a property-restricted diversity set called the "in-between library" was established to identify ligand-efficient compounds of molecular size between those typically found in fragment and high-throughput screening libraries. It was screened at fivefold higher concentrations than the main library to facilitate identification of less potent yet ligand-efficient compounds. Taken together, this work underscores the value of generating multiple purpose-focused, diversity-based library subsets that are designed using computational approaches coupled with internal screening data analyses to accelerate the lead discovery process., (© 2014 Society for Laboratory Automation and Screening.)

Published

2014

22. Case studies of minimizing nonspecific inhibitors in HTS campaigns that use assay-ready plates.

Author

Liu Y, Beresini MH, Johnson A, Mintzer R, Shah K, Clark K, Schmidt S, Lewis C, Liimatta M, Elliott LO, Gustafson A, and Heise CE

Subjects

Animals, Caspase 6 chemistry, Cattle, Computer Simulation, Drug Evaluation, Preclinical, False Positive Reactions, Humans, Models, Theoretical, Peptide Hydrolases metabolism, Protein Kinases metabolism, Serum Albumin chemistry, Small Molecule Libraries analysis, gamma-Globulins chemistry, Drug Discovery methods, High-Throughput Screening Assays methods, Peptide Hydrolases chemistry, Protein Kinases chemistry

Abstract

Identifying chemical lead matter by high-throughput screening (HTS) has been a common practice in early stage drug discovery. Evolution of small-molecule library composition to include more drug-like molecules with desirable physical chemical properties combined with improving assay technologies has vastly enhanced the capability of HTS. However, HTS campaigns can still be plagued by false positives arising from nonspecific inhibitors. The generation of assay-ready plates has permitted an incremental advancement to the speed and efficiency of HTS but has the potential to enhance the occurrence of nonspecific inhibitors. A subtle change in the order of reagent addition to the assay-ready plates can greatly alleviate false-positive inhibition. Our case studies with six different kinase and protease targets reveal that this type of inhibition affects targets regardless of enzyme class and is unpredictable based on protein construct or inhibitor chemical scaffold. These case studies support a model where a diversity set of compounds should be tested first for hit rates as a function of order of addition, carrier protein, and relevant mechanistic studies prior to launch of the HTS campaign.

Published

2012

23. Competition between intercellular adhesion molecule-1 and a small-molecule antagonist for a common binding site on the alphal subunit of lymphocyte function-associated antigen-1.

Author

Keating SM, Clark KR, Stefanich LD, Arellano F, Edwards CP, Bodary SC, Spencer SA, Gadek TR, Marsters JC Jr, and Beresini MH

Subjects

Allosteric Regulation, Binding Sites, Binding, Competitive, Cross-Linking Reagents, Enzyme-Linked Immunosorbent Assay, Humans, Immunoglobulin G metabolism, Intercellular Adhesion Molecule-1 genetics, Kidney metabolism, Ligands, Lymphocyte Function-Associated Antigen-1 genetics, Peptide Fragments chemistry, Peptide Fragments genetics, Protein Structure, Tertiary, Protein Subunits, Recombinant Fusion Proteins antagonists & inhibitors, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Intercellular Adhesion Molecule-1 chemistry, Intercellular Adhesion Molecule-1 metabolism, Lymphocyte Function-Associated Antigen-1 chemistry, Lymphocyte Function-Associated Antigen-1 metabolism, Peptide Fragments metabolism

Abstract

The lymphocyte function-associated antigen-1 (LFA-1) binding of a unique class of small-molecule antagonists as represented by compound 3 was analyzed in comparison to that of soluble intercellular adhesion molecule-1 (sICAM-1) and A-286982, which respectively define direct and allosteric competitive binding sites within LFA-1's inserted (I) domain. All three molecules antagonized LFA-1 binding to ICAM-1-Immunoglobulin G fusion (ICAM-1-Ig) in a competition ELISA, but only compound 3 and sICAM-1 inhibited the binding of a fluorescein-labeled analog of compound 3 to LFA-1. Compound 3 and sICAM-1 displayed classical direct competitive binding behavior with ICAM-1. Their antagonism of LFA-1 was surmountable by both ICAM-1-Ig and a fluorescein-labeled compound 3 analog. The competition of both sICAM-1 and compound 3 with ICAM-1-Ig for LFA-1 resulted in equivalent and linear Schild plots with slopes of 1.24 and 1.26, respectively. Cross-linking studies with a photoactivated analog of compound 3 localized the high-affinity small-molecule binding site to the N-terminal 507 amino acid segment of the alpha chain of LFA-1, a region that includes the I domain. In addition, cells transfected with a variant of LFA-1 lacking this I domain showed no significant binding of a fluorescein-labeled analog of compound 3 or ICAM-1-Ig. These results demonstrate that compound 3 inhibits the LFA-1/ICAM-1 binding interaction in a directly competitive manner by binding to a high-affinity site on LFA-1. This binding site overlaps with the ICAM-1 binding site on the alpha subunit of LFA-1, which has previously been localized to the I domain.

Published

2006

24. Phosphate ester serum albumin affinity tags greatly improve peptide half-life in vivo.

Author

Zobel K, Koehler MF, Beresini MH, Caris LD, and Combs D

Subjects

Animals, Anticoagulants pharmacokinetics, Blood Proteins metabolism, Half-Life, Humans, Injections, Intravenous, Peptides pharmacokinetics, Phosphates, Protein Binding, Rabbits, Time Factors, Anticoagulants chemistry, Organophosphates chemistry, Peptides chemistry, Serum Albumin chemistry

Abstract

A series of phosphate ester based small molecules designed to bind tightly to serum albumin were applied to the amino terminus of an anticoagulant peptide in an effort to increase its protein binding in vivo. The tagged peptides exhibited high affinity for both rabbit and human serum albumin when passed through liquid chromatographic columns with serum albumins incorporated into the stationary phase. The peptides were then administered intravenously to rabbits and found to have a greater than 50-fold increase in plasma half life. The highest affinity peptides showed a reduction in bioactivity consistent with their sequestration away from their protein target in the presence of 0.1% rabbit serum albumin.

Published

2003

25. Solid-phase synthesis of dual alpha4beta1/alpha4beta7 integrin antagonists: two scaffolds with overlapping pharmacophores.

Author

Castanedo GM, Sailes FC, Dubree NJ, Nicholas JB, Caris L, Clark K, Keating SM, Beresini MH, Chiu H, Fong S, Marsters JC Jr, Jackson DY, and Sutherlin DP

Subjects

Combinatorial Chemistry Techniques, Drug Design, Enzyme-Linked Immunosorbent Assay, Indicators and Reagents, Integrin alpha4beta1 chemistry, Integrins chemistry, Models, Molecular, Molecular Conformation, Structure-Activity Relationship, Integrin alpha4beta1 antagonists & inhibitors, Integrins antagonists & inhibitors

Abstract

Two structural classes of dual alpha4beta1/alpha4beta7 integrin antagonists were investigated via solid-phase parallel synthesis. Using an acylated amino acid backbone, lead compounds containing biphenylalanine or tyrosine carbamate scaffolds were optimized for inhibition of alpha4beta1/VCAM and alpha4beta7/MAdCAM. A comparison of the structure-activity relationships in the inhibition of the alpha4beta7/MAdCAM interaction for substituted amines employed in both scaffolds suggests a similar binding mode for the compounds.

Published

2002

26. Albumin affinity tags increase peptide half-life in vivo.

Author

Koehler MF, Zobel K, Beresini MH, Caris LD, Combs D, Paasch BD, and Lazarus RA

Subjects

Animals, Anticoagulants pharmacokinetics, Chromatography, Liquid, Dose-Response Relationship, Drug, Factor VIIa metabolism, Half-Life, Humans, Peptides pharmacokinetics, Protein Binding, Rabbits, Spectrophotometry, Ultraviolet, Affinity Labels chemistry, Albumins chemistry, Anticoagulants chemistry, Peptides chemistry

Abstract

Small organic molecules that bind tightly to serum albumin were applied to the amino terminus of an anticoagulant peptide in an effort to increase its protein binding in vivo. The tagged peptides were evaluated for their ability to be retained on liquid chromatographic columns with serum albumins incorporated into the stationary phase. Those which demonstrated significant affinity were administered intravenously to rabbits and found to have significantly increased plasma half-lives. Novel affinity tags were identified by appending a focused library of compounds to a model tetrapeptide and evaluating the resulting compounds' ability to bind to the serum albumin columns. The most promising were synthesized as the full length peptides and again evaluated in vivo. They were found to have still longer half-lives than the first generation compounds.

Published

2002

27. Selective alpha4beta7 integrin antagonists and their potential as antiinflammatory agents.

Author

Dubree NJ, Artis DR, Castanedo G, Marsters J, Sutherlin D, Caris L, Clark K, Keating SM, Beresini MH, Chiu H, Fong S, Lowman HB, Skelton NJ, and Jackson DY

Subjects

Alanine chemistry, Amino Acid Substitution, Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cell Adhesion Molecules, Chemotaxis, Leukocyte drug effects, Colitis pathology, Enzyme-Linked Immunosorbent Assay, Immunoglobulins chemistry, Integrins chemistry, Intestines pathology, Lymph Nodes drug effects, Lymph Nodes pathology, Lymphocytes drug effects, Lymphocytes pathology, Mice, Molecular Mimicry, Mucoproteins chemistry, Oligopeptides chemistry, Oligopeptides pharmacology, Peptide Library, Peptides, Cyclic chemistry, Peptides, Cyclic pharmacology, Receptors, Lymphocyte Homing chemistry, Structure-Activity Relationship, Vascular Cell Adhesion Molecule-1 chemistry, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Integrins antagonists & inhibitors, Oligopeptides chemical synthesis, Peptide Fragments chemistry, Peptides, Cyclic chemical synthesis

Abstract

The accumulation of leukocytes in various tissues contributes to the pathogenesis of numerous human autoimmune diseases. The integrin alpha4beta7, expressed on the surface of B and T lymphocytes, plays an essential role in lymphocyte trafficking throughout the gastrointestinal (GI) tract via interaction with its primary ligand, mucosal addressin cell adhesion molecule (MAdCAM). Elevated MAdCAM expression in the intestines and liver has been linked to GI-associated autoimmune disorders, including Crohn's disease, ulcerative colitis, and hepatitis C. Monoclonal antibodies that block the interaction of alpha4beta7 with MAdCAM inhibit lymphocyte homing to murine intestines without effecting migration to peripheral organs; this suggests that alpha4beta7-selective antagonists might be useful as GI specific antiinflammatory agents. Here, we report the discovery of highly potent and selective alpha4beta7 antagonists affinity selected from a random peptide-phage library. Subsequent optimization of initial peptide leads afforded alpha4beta7-selective heptapeptide inhibitors that competitively inhibit binding to MAdCAM in vitro and inhibit lymphocyte homing to murine intestines in vivo. Substitution of a single carboxylate moiety alters selectivity for alpha4beta7 by more than 500-fold to afford a potent and selective alpha4beta1 antagonist. The antagonists described here are the first peptides to demonstrate potency and selectivity for alpha4beta7 compared to other integrins.

Published

2002

28. Generation of an LFA-1 antagonist by the transfer of the ICAM-1 immunoregulatory epitope to a small molecule.

Author

Gadek TR, Burdick DJ, McDowell RS, Stanley MS, Marsters JC Jr, Paris KJ, Oare DA, Reynolds ME, Ladner C, Zioncheck KA, Lee WP, Gribling P, Dennis MS, Skelton NJ, Tumas DB, Clark KR, Keating SM, Beresini MH, Tilley JW, Presta LG, and Bodary SC

Subjects

Amino Acid Sequence, Animals, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal metabolism, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclosporine pharmacology, Dermatitis, Irritant drug therapy, Dinitrofluorobenzene, Drug Design, Enzyme-Linked Immunosorbent Assay, Epitopes, Female, Humans, Immunoglobulin Fab Fragments immunology, Immunoglobulin Fab Fragments pharmacology, Immunosuppressive Agents chemical synthesis, Immunosuppressive Agents chemistry, Immunosuppressive Agents metabolism, Intercellular Adhesion Molecule-1 chemistry, Lymphocyte Culture Test, Mixed, Lymphocyte Function-Associated Antigen-1 immunology, Mice, Mice, Inbred BALB C, Molecular Mimicry, Mutagenesis, Protein Structure, Secondary, Structure-Activity Relationship, Thiophenes chemistry, Thiophenes metabolism, beta-Alanine analogs & derivatives, beta-Alanine chemistry, beta-Alanine metabolism, Immunosuppressive Agents pharmacology, Intercellular Adhesion Molecule-1 immunology, Intercellular Adhesion Molecule-1 metabolism, Lymphocyte Function-Associated Antigen-1 metabolism, Thiophenes chemical synthesis, Thiophenes pharmacology, beta-Alanine chemical synthesis, beta-Alanine pharmacology

Abstract

The protein-protein interaction between leukocyte functional antigen-1 (LFA-1) and intercellular adhesion molecule-1 (ICAM-1) is critical to lymphocyte and immune system function. Here, we report on the transfer of the contiguous, nonlinear epitope of ICAM-1, responsible for its association with LFA-1, to a small-molecule framework. These LFA-1 antagonists bound LFA-1, blocked binding of ICAM-1, and inhibited a mixed lymphocyte reaction (MLR) with potency significantly greater than that of cyclosporine A. Furthermore, in comparison to an antibody to LFA-1, they exhibited significant anti-inflammatory effects in vivo. These results demonstrate the utility of small-molecule mimics of nonlinear protein epitopes and the protein epitopes themselves as leads in the identification of novel pharmaceutical agents.

Published

2002

29. Transfer of a protein binding epitope to a minimal designed peptide.

Author

Quan C, Skelton NJ, Clark K, Jackson DY, Renz ME, Chiu HH, Keating SM, Beresini MH, Fong S, and Artis DR

Subjects

Binding Sites, Binding, Competitive, Integrin alpha4beta1, Magnetic Resonance Spectroscopy, Methotrexate chemistry, Models, Molecular, Peptide Fragments chemistry, Structure-Activity Relationship, Vascular Cell Adhesion Molecule-1 chemistry, Epitopes chemistry, Integrins metabolism, Peptides, Cyclic chemistry, Protein Binding, Receptors, Lymphocyte Homing metabolism

Abstract

Results from protein mutagenesis and x-ray crystallographic studies of the multidomain protein Vascular Cell Adhesion Molecule (VCAM) were used to design cyclic octapeptides that retain the critical structural and binding elements of the epitope of VCAM in the interaction with the integrin alpha 4 beta 1 (VLA-4). Changes in the activities of peptide analogues correlated with the relative activities of protein mutants of VCAM, and predicted the properties of two new mutants that bound alpha 4 beta 1 with improved affinity vs wild type protein. The nmr structures of two peptides revealed a high degree of similarity to the structure of the VCAM binding epitope. These results demonstrate that a compact binding epitope identified via protein structure-function studies may be transferred to a synthetically accessible small peptide with the key structure-activity relationships intact.

Published

1998

30. Alpha-subunit of farnesyltransferase is phosphorylated in vivo: effect of protein phosphatase-1 on enzymatic activity.

Author

Kumar A, Beresini MH, Dhawan P, and Mehta KD

Subjects

Animals, Antibody Specificity, Cell Line, Cytosol enzymology, Enzyme Inhibitors pharmacology, Farnesyltranstransferase, Immunoblotting, Immunoglobulin G, Kinetics, Macromolecular Substances, Marine Toxins, Oxazoles pharmacology, PC12 Cells, Phosphates metabolism, Phosphoprotein Phosphatases antagonists & inhibitors, Phosphorylation, Protein Phosphatase 1, Rats, Transferases chemistry, Transferases isolation & purification, Alkyl and Aryl Transferases, Phosphoprotein Phosphatases metabolism, Transferases metabolism

Abstract

Farnesyltransferase is a heterodimer consisting of a 49 kDa alpha-subunit and a 46 kDa beta-subunit. In this report, we demonstrate that the endogenous heterodimeric farnesyltransferase protein is phosphorylated at the alpha-subunit in vivo and phosphorylation plays a role in the regulation of farnesyltransferase activity. In vivo 32P-labeling of PC-12 cells followed by immunoprecipitation with specific anti rat alpha-subunit IgG showed a labeled alpha-subunit protein band at an expected molecular mass of 49 kDa. Treatment of PC-12 cells with protein phosphatase inhibitor, Calyculin A, resulted in a decrease in FTase activity, and phophoserine/phosphothreonine-specific protein phosphatase-1 treatment of PC-12 and GM37 cell extracts resulted in 100% and 375% increase in farnesyltransferase activity, respectively, compared to untreated extracts.

Published

1996

31. Evaluation of EMIT Cyclosporine Assay for use with whole blood.

Author

Beresini MH, Davalian D, Alexander S, Toton-Quinn R, Barnett B, Cerelli MJ, Hu MW, Berger DE, Blohm WP, and Jaklitsch A

Subjects

Calibration, Chromatography, High Pressure Liquid, Drug Stability, Hematocrit, Humans, Microchemistry, Organ Transplantation, Quality Control, Radioimmunoassay, Sensitivity and Specificity, Cyclosporine blood, Enzyme Multiplied Immunoassay Technique statistics & numerical data, Reagent Kits, Diagnostic statistics & numerical data

Abstract

We evaluated the EMIT Cyclosporine Assay, designed for specific quantification of cyclosporine (CsA) in whole blood. The assay was run on the Roche Cobas Mira or Cobas Mira S analyzer. Analytical recovery from both normal donor whole blood and transplant patients' samples was within 17% of the standards. Measurement of diluted out-of-range samples also yielded excellent recovery (101-105%). Within-run, between-run, and total CVs were < or = 8.1%, 10.9%, and 12.1%, respectively. The detection limit was < 32 micrograms/L. The assay was linear from 0 to 500 micrograms/L. No significant cross-reactivity was observed for CsA metabolites AM1, AM19, and AM4N. Slight cross-reactivity occurred with metabolite AM9; 670 micrograms/L AM9 increased the measured CsA concentration by 49 micrograms/L. High concentrations of bilirubin, uric acid, triglycerides, and cholesterol, as well as 54 commonly coadministered drugs did not interfere with CsA quantification. Similarly, neither extreme values of hematocrit nor choice of anticoagulant affected CsA recovery. Sample extract stability was > 4 h, and assay calibration was stable for at least 2 weeks. Patients' samples analyzed by the EMIT assay showed strong correlation with both HPLC and 125I-RIA (r > 0.97). We conclude that the EMIT Cyclosporine Assay provides a convenient, accurate, and precise method for specific quantification of CsA in whole blood.

Published

1993

32. Synergistic induction of polypeptides by tumor necrosis factor and interferon-gamma in cells sensitive or resistant to tumor necrosis factor: assessment by computer based analysis of two-dimensional gels using the PDQUEST system.

Author

Beresini MH, Sugarman BJ, Shepard HM, and Epstein LB

Subjects

Cell Division, Drug Synergism, Female, Humans, Recombinant Proteins, Tumor Cells, Cultured, Uterine Cervical Neoplasms, Computer Systems, Electrophoresis, Gel, Two-Dimensional, Interferon-gamma pharmacology, Protein Biosynthesis, Tumor Necrosis Factor-alpha pharmacology

Abstract

Tumor necrosis factor (TNF) synergistically enhanced the antiproliferative activity of interferon-gamma (IFN-gamma) in both TNF-sensitive and TNF-resistant variants of the cervical carcinoma line, ME-180. TNF alone had no apparent effect on the levels of synthesis of individual proteins in either of these variant cell lines as assessed by computerized two-dimensional gel analysis of cell lysates using the PDQUEST system. However, IFN-gamma enhanced the levels of 18 polypeptides and suppressed the levels of 10 polypeptides in both cell lines. When used in combination in both cell lines, TNF and IFN-gamma induced the synthesis of 10 polypeptides that were not induced by either agent alone. These synergistically induced polypeptides may be crucial to the mechanism of the synergistic antiproliferative action of TNF and IFN-gamma in ME-180 cells.

Published

1990

33. Overlapping polypeptide induction in human fibroblasts in response to treatment with interferon-alpha, interferon-gamma, interleukin 1 alpha, interleukin 1 beta, and tumor necrosis factor.

Author

Beresini MH, Lempert MJ, and Epstein LB

Subjects

Biological Products pharmacology, Cell Division drug effects, Cytokines, Cytopathogenic Effect, Viral, Electrophoresis, Agar Gel, Fibroblasts drug effects, Humans, Fibroblasts metabolism, Interferon Type I pharmacology, Interferon-gamma pharmacology, Interleukin-1 pharmacology, Peptide Biosynthesis, Tumor Necrosis Factor-alpha pharmacology

Abstract

Cytokine-induced polypeptides were identified in whole cell lysates of human fibroblasts by computer-based analysis of two-dimensional gels with the use of the PDQuest System. Treatment with interferon-alpha (IFN-alpha) and interferon-gamma (IFN-gamma) enhanced the synthesis of 12 and 28 polypeptides, respectively. Exposure to interleukin 1 alpha (IL-1 alpha) or interleukin 1 beta (IL-1 beta) resulted in the increased synthesis of seven identical polypeptides. Treatment with tumor necrosis factor (TNF) at 100 U/ml led to enhanced expression of seven polypeptides, whereas exposure to TNF at 1000 U/ml increased the levels of these seven plus two additional polypeptides. The antiviral and antiproliferative effects of these cytokines in strain 153 fibroblasts were also assessed. Both IFN-alpha and IFN-gamma exhibited antiviral activity, whereas both IL-1 and TNF stimulated fibroblast growth. IFN-gamma was alone in inhibiting proliferation. Thus, although these cytokines exhibit low degrees of structural homology, they share some common functions, and a number of polypeptides were induced in common by two or more of these agents. The greatest similarities in polypeptide induction occur between IFN-alpha and IFN-gamma and between the IL-1s and TNF. However, polypeptides were also induced in common by IFN-alpha and TNF, IFN-gamma and IL-1, and IFN-gamma and TNF. These similarities in polypeptide induction may reflect the overlapping functions of these cytokines and may be indicative of common biochemical pathways in their mechanisms of action.

Published

1988