Your search keyword '"James M. Gavin"' showing total 20 results

1. A small-molecule SUMOylation inhibitor activates antitumor immune responses and potentiates immune therapies in preclinical models

Author

Keli Song, James Minissale, Richard A. Klinghoffer, James Garnsey, Katherine Galvin, Kristina Xega, Sai M Pulukuri, James M. Gavin, Xiaofeng Yang, Pooja Shah, Gary Shapiro, Cong Li, Vaishali Shinde, Eric S. Lightcap, Dennis Huszar, Zhen Lu, Stephen Grossman, Erik Koenig, Pengfei Yu, Steve Langston, Hisashi Imaichi, Serge Y. Fuchs, Mithun Khattar, Beryl A. Hatton, Yu Fu, Hongru Zhang, Dylan England, Michael Milhollen, Jessica Riceberg, and Xingyue He

Subjects

Immune system, Chemistry, Interferon, Immunity, Cancer research, medicine, SUMO protein, Sumoylation, General Medicine, Small molecule, Article, Immune therapy, medicine.drug

Abstract

SUMOylation, the covalent conjugation of small ubiquitin-like modifier (SUMO) proteins to protein substrates, has been reported to suppress type I interferon (IFN1) responses. TAK-981, a selective small molecule inhibitor of SUMOylation, pharmacologically reactivates IFN1 signaling and immune responses against cancers. In vivo treatment of wild type mice with TAK-981 upregulated IFN1 gene expression in blood cells and splenocytes. Ex vivo treatment of mouse and human dendritic cells promoted their IFN1-dependent activation, and vaccination studies in mice demonstrated stimulation of antigen cross-presentation and T cell priming in vivo. TAK-981 also directly stimulated T cell activation, driving enhanced T cell sensitivity and response to antigen ex vivo. Consistent with these observations, TAK-981 inhibited growth of syngeneic A20 and MC38 tumors in mice, dependent upon IFN1 signaling and CD8(+) T cells, and associated with increased intratumoral T and NK cell number and activation. Combination of TAK-981 with anti-PD1 or anti-CTLA4 antibodies improved the survival of mice bearing syngeneic CT26 and MC38 tumors. In conclusion, TAK-981 is a first in class SUMOylation inhibitor that promotes anti-tumor immune responses by activation of IFN1 signaling. TAK-981 is currently being studied in phase I clinical trials (NCT03648372, NCT04074330, NCT04776018 and NCT04381650) for the treatment of patients with solid tumors and lymphomas.

Published

2021

2. Mechanistic Study of Uba5 Enzyme and the Ufm1 Conjugation Pathway

Author

Kara Hoar, Jiejin Chen, Sean J. Harrison, Jingya Ma, James M. Gavin, Neil F. Bence, Wei Chen, Ping Li, Michael Sintchak, Nancy J. Bump, Qing Xu, Lawrence R. Dick, William D. Mallender, Jesse J. Chen, Alexandra E. Gould, Frank Bruzzese, and Yafang Lin

Subjects

Stereochemistry, Ubiquitin-activating enzyme, Adenylate kinase, Ubiquitin-Activating Enzymes, Ubiquitin-conjugating enzyme, Thioester, Biochemistry, Cell Line, Enzyme activator, chemistry.chemical_compound, Adenosine Triphosphate, Catalytic Domain, Humans, Protein Structure, Quaternary, Molecular Biology, Ternary complex, chemistry.chemical_classification, biology, Chemistry, Proteins, Active site, Cell Biology, Enzyme Activation, Models, Chemical, Multiprotein Complexes, Ubiquitin-Conjugating Enzymes, Enzymology, biology.protein, Adenosine triphosphate, Protein Binding

Abstract

E1 enzymes activate ubiquitin or ubiquitin-like proteins (Ubl) via an adenylate intermediate and initiate the enzymatic cascade of Ubl conjugation to target proteins or lipids. Ubiquitin-fold modifier 1 (Ufm1) is activated by the E1 enzyme Uba5, and this pathway is proposed to play an important role in the endoplasmic reticulum (ER) stress response. However, the mechanisms of Ufm1 activation by Uba5 and subsequent transfer to the conjugating enzyme (E2), Ufc1, have not been studied in detail. In this work, we found that Uba5 activated Ufm1 via a two-step mechanism and formed a binary covalent complex of Uba5∼Ufm1 thioester. This feature contrasts with the three-step mechanism and ternary complex formation in ubiquitin-activating enzyme Uba1. Uba5 displayed random ordered binding with Ufm1 and ATP, and its ATP-pyrophosphate (PPi) exchange activity was inhibited by both AMP and PPi. Ufm1 activation and Uba5∼Ufm1 thioester formation were stimulated in the presence of Ufc1. Furthermore, binding of ATP to Uba5∼Ufm1 thioester was required for efficient transfer of Ufm1 from Uba5 to Ufc1 via transthiolation. Consistent with the two-step activation mechanism, the mechanism-based pan-E1 inhibitor, adenosine 5'-sulfamate (ADS), reacted with the Uba5∼Ufm1 thioester and formed a covalent, tight-binding Ufm1-ADS adduct in the active site of Uba5, which prevented further substrate binding or catalysis. ADS was also shown to inhibit the Uba5 conjugation pathway in the HCT116 cells through formation of the Ufm1-ADS adduct. This suggests that further development of more selective Uba5 inhibitors could be useful in interrogating the roles of the Uba5 pathway in cells.

Published

2014

3. A small-molecule inhibitor of the ubiquitin activating enzyme for cancer treatment

Author

John Newcomb, James M. Gavin, Nancy J. Bump, Stephen Tirrell, Lawrence R. Dick, Saurabh Menon, Jessica Huck, Petter Veiby, Benjamin S. Amidon, Yu Yang, Marc L. Hyer, Paul D. Greenspan, Fleming Paul E, Teresa A. Soucy, Jim Brownell, Michael Sintchak, Josh Powe, Steve Langston, Mark Manfredi, Judy Shi, Jeff Ciavarri, Darshan S. Sappal, Frank Bruzzese, Mike Kuranda, Katherine Galvin, Michael Milhollen, Ping Li, Neil F. Bence, Jing Tao Wu, Claudia Rabino, Chris Claiborne, Tary Traore, Jennifer Duffy, Jessica Riceberg, Robert J. Griffin, Kara Hoar, Anya Lublinsky, Bradley Stringer, and Sai M Pulukuri

Subjects

0301 basic medicine, Proteasome Endopeptidase Complex, DNA Repair, Ubiquitin-activating enzyme, Plasma protein binding, Ubiquitin-Activating Enzymes, Sulfides, Imides, General Biochemistry, Genetics and Molecular Biology, Small Molecule Libraries, 03 medical and health sciences, Mice, Ubiquitin, Cell Line, Tumor, Neoplasms, Animals, Humans, chemistry.chemical_classification, Sulfonamides, biology, Chemistry, Nucleosides, General Medicine, Small molecule, Xenograft Model Antitumor Assays, 030104 developmental biology, Enzyme, Pyrimidines, Proteasome, Cell culture, Cancer cell, Cancer research, biology.protein, Pyrazoles, DNA Damage, Protein Binding

Abstract

The ubiquitin-proteasome system (UPS) comprises a network of enzymes that is responsible for maintaining cellular protein homeostasis. The therapeutic potential of this pathway has been validated by the clinical successes of a number of UPS modulators, including proteasome inhibitors and immunomodulatory imide drugs (IMiDs). Here we identified TAK-243 (formerly known as MLN7243) as a potent, mechanism-based small-molecule inhibitor of the ubiquitin activating enzyme (UAE), the primary mammalian E1 enzyme that regulates the ubiquitin conjugation cascade. TAK-243 treatment caused depletion of cellular ubiquitin conjugates, resulting in disruption of signaling events, induction of proteotoxic stress, and impairment of cell cycle progression and DNA damage repair pathways. TAK-243 treatment caused death of cancer cells and, in primary human xenograft studies, demonstrated antitumor activity at tolerated doses. Due to its specificity and potency, TAK-243 allows for interrogation of ubiquitin biology and for assessment of UAE inhibition as a new approach for cancer treatment.

Published

2016

4. Mechanistic Studies on Activation of Ubiquitin and Di-ubiquitin-like Protein, FAT10, by Ubiquitin-like Modifier Activating Enzyme 6, Uba6

Author

Lawrence R. Dick, Hua Liao, Neil Rollins, Xiaofeng Yang, William D. Mallender, Qing Xu, James E. Brownell, James M. Gavin, Jingyang Chen, Alexandra E. Gould, Huay-Keng Loke, Jingya Ma, Trupti Lingaraj, and Benjamin S. Amidon

Subjects

Ubiquitin-activating enzyme, Blotting, Western, Molecular Sequence Data, Ubiquitin-Activating Enzymes, Plasma protein binding, Spodoptera, Biochemistry, Mass Spectrometry, Cell Line, Substrate Specificity, Interferon-gamma, Enzyme activator, Adenosine Triphosphate, Ubiquitin, Animals, Humans, Amino Acid Sequence, Sulfhydryl Compounds, Ubiquitins, Molecular Biology, Ternary complex, Molecular Structure, biology, Tumor Necrosis Factor-alpha, Chemistry, Cell Biology, UBA1, Surface Plasmon Resonance, Adenosine Monophosphate, Ubiquitin ligase, Diphosphates, Enzyme Activation, Kinetics, Enzymology, biology.protein, Protein Binding

Abstract

Uba6 is a homolog of the ubiquitin-activating enzyme, Uba1, and activates two ubiquitin-like proteins (UBLs), ubiquitin and FAT10. In this study, biochemical and biophysical experiments were performed to understand the mechanisms of how Uba6 recognizes two distinct UBLs and catalyzes their activation and transfer. Uba6 is shown to undergo a three-step activation process and form a ternary complex with both UBLs, similar to what has been observed for Uba1. The catalytic mechanism of Uba6 is further supported by inhibition studies using a mechanism-based E1 inhibitor, Compound 1, which forms covalent adducts with both ubiquitin and FAT10. In addition, pre-steady state kinetic analysis revealed that the rates of UBL-adenylate (step 1) and thioester (step 2) formation are similar between ubiquitin and FAT10. However, distinct kinetic behaviors were also observed for ubiquitin and FAT10. FAT10 binds Uba6 with much higher affinity than ubiquitin while demonstrating lower catalytic activity in both ATP-PP(i) exchange and E1-E2 transthiolation assays. Also, Compound 1 is less potent with FAT10 as the UBL compared with ubiquitin in ATP-PP(i) exchange assays, and both a slow rate of covalent adduct formation and weak adduct binding to Uba6 contribute to the diminished potency observed for FAT10. Together with expression level analysis in IM-9 cells, this study sheds light on the potential role of cytokine-induced FAT10 expression in regulating Uba6 pathways.

Published

2012

5. An inhibitor of NEDD8-activating enzyme as a new approach to treat cancer

Author

Teresa A. Soucy, Peter G. Smith, Michael A. Milhollen, Allison J. Berger, James M. Gavin, Sharmila Adhikari, James E. Brownell, Kristine E. Burke, David P. Cardin, Stephen Critchley, Courtney A. Cullis, Amanda Doucette, James J. Garnsey, Jeffrey L. Gaulin, Rachel E. Gershman, Anna R. Lublinsky, Alice McDonald, Hirotake Mizutani, Usha Narayanan, Edward J. Olhava, Stephane Peluso, Mansoureh Rezaei, Michael D. Sintchak, Tina Talreja, Michael P. Thomas, Tary Traore, Stepan Vyskocil, Gabriel S. Weatherhead, Jie Yu, Julie Zhang, Lawrence R. Dick, Christopher F. Claiborne, Mark Rolfe, Joseph B. Bolen, and Steven P. Langston

Subjects

NEDD8 Protein, Ubiquitin-activating enzyme, Transplantation, Heterologous, Antineoplastic Agents, Cyclopentanes, Ubiquitin-Activating Enzymes, NEDD8, Mice, Ubiquitin, Cell Line, Tumor, Neoplasms, Animals, Humans, Enzyme Inhibitors, Ubiquitins, Cells, Cultured, Multidisciplinary, biology, Cullin Proteins, Cell biology, Pyrimidines, Pevonedistat, Proteasome, Cancer cell, biology.protein, Female, Neddylation, Proteasome Inhibitors, Cullin

Abstract

The clinical development of an inhibitor of cellular proteasome function suggests that compounds targeting other components of the ubiquitin-proteasome system might prove useful for the treatment of human malignancies. NEDD8-activating enzyme (NAE) is an essential component of the NEDD8 conjugation pathway that controls the activity of the cullin-RING subtype of ubiquitin ligases, thereby regulating the turnover of a subset of proteins upstream of the proteasome. Substrates of cullin-RING ligases have important roles in cellular processes associated with cancer cell growth and survival pathways. Here we describe MLN4924, a potent and selective inhibitor of NAE. MLN4924 disrupts cullin-RING ligase-mediated protein turnover leading to apoptotic death in human tumour cells by a new mechanism of action, the deregulation of S-phase DNA synthesis. MLN4924 suppressed the growth of human tumour xenografts in mice at compound exposures that were well tolerated. Our data suggest that NAE inhibitors may hold promise for the treatment of cancer.

Published

2009

6. Hydrolysis of Biological Peptides by Human Angiotensin-converting Enzyme-related Carboxypeptidase

Author

Larry Dick, Virendar K. Kaushik, Thomas F. Parsons, Peter J. Tummino, Susan L. Acton, Michael A. Patane, Kevin Godbout, Jin Tang, Elizabeth Baronas, Chad S Vickers, Frank Y. Hsieh, James M. Gavin, Paul Hales, and Andrew J. Nichols

Subjects

Stereochemistry, Peptide, Carboxypeptidases, Peptidyl-Dipeptidase A, Biochemistry, Catalysis, Humans, Amino Acid Sequence, Molecular Biology, Peptide sequence, Chromatography, High Pressure Liquid, chemistry.chemical_classification, biology, Hydrolysis, Angiotensin-converting enzyme, Cell Biology, Hydrogen-Ion Concentration, Chromatography, Ion Exchange, Carboxypeptidase, Angiotensin II, Recombinant Proteins, Amino acid, Kinetics, Enzyme, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Angiotensin-converting enzyme 2, biology.protein, Spectrophotometry, Ultraviolet, Angiotensin-Converting Enzyme 2, Peptides, hormones, hormone substitutes, and hormone antagonists

Abstract

Human angiotensin-converting enzyme-related carboxypeptidase (ACE2) is a zinc metalloprotease whose closest homolog is angiotensin I-converting enzyme. To begin to elucidate the physiological role of ACE2, ACE2 was purified, and its catalytic activity was characterized. ACE2 proteolytic activity has a pH optimum of 6.5 and is enhanced by monovalent anions, which is consistent with the activity of ACE. ACE2 activity is increased approximately 10-fold by Cl(-) and F(-) but is unaffected by Br(-). ACE2 was screened for hydrolytic activity against a panel of 126 biological peptides, using liquid chromatography-mass spectrometry detection. Eleven of the peptides were hydrolyzed by ACE2, and in each case, the proteolytic activity resulted in removal of the C-terminal residue only. ACE2 hydrolyzes three of the peptides with high catalytic efficiency: angiotensin II () (k(cat)/K(m) = 1.9 x 10(6) m(-1) s(-1)), apelin-13 (k(cat)/K(m) = 2.1 x 10(6) m(-1) s(-1)), and dynorphin A 1-13 (k(cat)/K(m) = 3.1 x 10(6) m(-1) s(-1)). The ACE2 catalytic efficiency is 400-fold higher with angiotensin II () as a substrate than with angiotensin I (). ACE2 also efficiently hydrolyzes des-Arg(9)-bradykinin (k(cat)/K(m) = 1.3 x 10(5) m(-1) s(-1)), but it does not hydrolyze bradykinin. An alignment of the ACE2 peptide substrates reveals a consensus sequence of: Pro-X((1-3 residues))-Pro-Hydrophobic, where hydrolysis occurs between proline and the hydrophobic amino acid.

Published

2002

7. Identification and application of NEDD8 E1 inhibitors

Author

Frank J, Bruzzese, Michael A, Milhollen, James M, Gavin, Helen R, Josephine, and James E, Brownell

Subjects

Enzyme Activation, NEDD8 Protein, Cell Line, Tumor, Humans, Ubiquitin-Activating Enzymes, Cullin Proteins, Ubiquitins

Abstract

The NEDD8 conjugation pathway is initiated by the NEDD8 E1, also known as NEDD8 activating enzyme (NAE) or APPBP1/UBA3 (Gong, Yeh. J Biol Chem 274:12063-12042, 1999). The best described biological role for NEDD8 conjugation is to regulate the activity of the cullin RING ligase (CRL) family of ubiquitin E3 ligases (Gong, Yeh. J Biol Chem 274:12063-12042, 1999). In this way, the NEDD8 pathway regulates the turnover of a subset of ubiquitin proteasome system (UPS) substrates that are essential for cancer cell growth and survival (Soucy, Smith, Milhollen. Nature 458:732-737, 2009). We recently initiated clinical trials with a first-in-class small molecule inhibitor of NAE for the treatment of cancer (Soucy, Smith, Milhollen. Nature 458:732-737, 2009). Here we describe a biochemical and cell-based assay used to identify NAE inhibitors and monitor inhibition of the NEDD8 conjugation pathway.

Published

2012

8. Identification and Application of NEDD8 E1 Inhibitors

Author

Michael Milhollen, Frank J. Bruzzese, Helen R. Josephine, James M. Gavin, and James E. Brownell

Subjects

Enzyme activator, Ubiquitins, Biochemistry, Proteasome, Ubiquitin, biology, Chemistry, Cullin Proteins, Ubiquitin-activating enzyme, NEDD8 Activating Enzyme, biology.protein, NEDD8

Abstract

The NEDD8 conjugation pathway is initiated by the NEDD8 E1, also known as NEDD8 activating enzyme (NAE) or APPBP1/UBA3 (Gong, Yeh. J Biol Chem 274:12063-12042, 1999). The best described biological role for NEDD8 conjugation is to regulate the activity of the cullin RING ligase (CRL) family of ubiquitin E3 ligases (Gong, Yeh. J Biol Chem 274:12063-12042, 1999). In this way, the NEDD8 pathway regulates the turnover of a subset of ubiquitin proteasome system (UPS) substrates that are essential for cancer cell growth and survival (Soucy, Smith, Milhollen. Nature 458:732-737, 2009). We recently initiated clinical trials with a first-in-class small molecule inhibitor of NAE for the treatment of cancer (Soucy, Smith, Milhollen. Nature 458:732-737, 2009). Here we describe a biochemical and cell-based assay used to identify NAE inhibitors and monitor inhibition of the NEDD8 conjugation pathway.

Published

2012

9. Treatment-emergent mutations in NAEβ confer resistance to the NEDD8-activating enzyme inhibitor MLN4924

Author

Xiaofeng Yang, Michael Milhollen, Neil Bence, Mark Manfredi, Huay-Keng Loke, Erik Koenig, James E. Brownell, Mike Sintchak, Michael P. Thomas, Usha Narayanan, Qing Xu, James M. Gavin, Jessica Riceberg, Alice McDonald, Joseph B. Bolen, Benjamin S. Amidon, Peter G. Smith, Sells Todd B, Tary Traore, Jingya Ma, and Lawrence R. Dick

Subjects

Cancer Research, Mutant, Mice, Nude, Cyclopentanes, Ubiquitin-Activating Enzymes, Biology, Adduct, Protein neddylation, chemistry.chemical_compound, Mice, Rats, Nude, Cell Line, Tumor, NEDD8 Activating Enzyme, medicine, Tumor Cells, Cultured, Animals, Humans, Enzyme Inhibitors, chemistry.chemical_classification, Clinical Trials as Topic, Binding Sites, Cancer, Cell Biology, medicine.disease, Molecular biology, Xenograft Model Antitumor Assays, Rats, Enzyme, Pevonedistat, Pyrimidines, chemistry, Biochemistry, Oncology, Drug Resistance, Neoplasm, Mutation, Female, Adenosine triphosphate

Abstract

SummaryMLN4924 is an investigational small-molecule inhibitor of NEDD8-activating enzyme (NAE) in clinical trials for the treatment of cancer. MLN4924 is a mechanism-based inhibitor, with enzyme inhibition occurring through the formation of a tight-binding NEDD8-MLN4924 adduct. In cell and xenograft models of cancer, we identified treatment-emergent heterozygous mutations in the adenosine triphosphate binding pocket and NEDD8-binding cleft of NAEβ as the primary mechanism of resistance to MLN4924. Biochemical analyses of NAEβ mutants revealed slower rates of adduct formation and reduced adduct affinity for the mutant enzymes. A compound with tighter binding properties was able to potently inhibit mutant enzymes in cells. These data provide rationales for patient selection and the development of next-generation NAE inhibitors designed to overcome treatment-emergent NAEβ mutations.

Published

2011

10. Substrate-assisted inhibition of ubiquitin-like protein-activating enzymes: the NEDD8 E1 inhibitor MLN4924 forms a NEDD8-AMP mimetic in situ

Author

Anne L. Burkhardt, Michael Milhollen, Xiaofeng Yang, Huay-Keng Loke, Lawrence R. Dick, Teresa A. Soucy, Irache Visiers, Frank J. Bruzzese, Michael D. Sintchak, James J. Spelman, Steven P. Langston, Ping Li, Kristin B. Hamman, James M. Gavin, Joseph B. Bolen, Nancy Bump, Sells Todd B, Jingya Ma, Christopher F. Claiborne, Stepan Vyskocil, Courtney Cullis, Hua Liao, Mark Rolfe, Dongyun Wu, James E. Brownell, Trupti Lingaraj, and William D. Mallender

Subjects

NEDD8 Protein, Adenylate kinase, Cyclopentanes, Crystallography, X-Ray, NEDD8, Binding, Competitive, Protein neddylation, Ubiquitin, Cell Line, Tumor, NEDD8 Activating Enzyme, Humans, Enzyme Inhibitors, Molecular Biology, Ubiquitins, chemistry.chemical_classification, Binding Sites, biology, Active site, Cell Biology, Adenosine Monophosphate, Protein Structure, Tertiary, Enzyme Activation, Pevonedistat, Enzyme, Pyrimidines, chemistry, Biochemistry, biology.protein

Abstract

The NEDD8-activating enzyme (NAE) initiates a protein homeostatic pathway essential for cancer cell growth and survival. MLN4924 is a selective inhibitor of NAE currently in clinical trials for the treatment of cancer. Here, we show that MLN4924 is a mechanism-based inhibitor of NAE and creates a covalent NEDD8-MLN4924 adduct catalyzed by the enzyme. The NEDD8-MLN4924 adduct resembles NEDD8 adenylate, the first intermediate in the NAE reaction cycle, but cannot be further utilized in subsequent intraenzyme reactions. The stability of the NEDD8-MLN4924 adduct within the NAE active site blocks enzyme activity, thereby accounting for the potent inhibition of the NEDD8 pathway by MLN4924. Importantly, we have determined that compounds resembling MLN4924 demonstrate the ability to form analogous adducts with other ubiquitin-like proteins (UBLs) catalyzed by their cognate-activating enzymes. These findings reveal insights into the mechanism of E1s and suggest a general strategy for selective inhibition of UBL conjugation pathways.

Published

2009

11. Substrate-Based Design of the First Class of Angiotensin-Converting Enzyme-Related Carboxypeptidase (ACE2) Inhibitors

Author

Timothy D. Ocain, Alexandra E. Gould, Natalie A. Dales, James Brown, Emily F. Calderwood, James M. Gavin, Charles A. Minor, Bing Guan, Chad S Vickers, Virendar K. Kaushik, Paul Hales, Michael A. Patane, Peter J. Tummino, and Michael Stewart

Subjects

Stereochemistry, Angiotensin-Converting Enzyme Inhibitors, Carboxypeptidases, Peptidyl-Dipeptidase A, Biochemistry, Catalysis, Carboxypeptidase activity, Structure-Activity Relationship, Colloid and Surface Chemistry, Glutamate carboxypeptidase II, Structure–activity relationship, chemistry.chemical_classification, biology, Chemistry, Imidazoles, Rational design, Succinates, Angiotensin-converting enzyme, General Chemistry, Carboxypeptidase, Protein Structure, Tertiary, Enzyme, Drug Design, Angiotensin-converting enzyme 2, biology.protein, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists

Abstract

Angiotensin-converting enzyme-related carboxypeptidase (ACE2) is a recently identified zinc metalloprotease with carboxypeptidase activity that was identified using our genomics platform. We implemented a rational design approach to identify potent and selective ACE2 inhibitors. To this end, picomolar inhibitors of ACE2 were designed and synthesized.

Published

2002

12. Treatment Emergent Mutations in NAEβ Confer Resistance to the NEDD8-Activating Enzyme Inhibitor MLN4924 in Pre-Clinical AML and DLBCL Models

Author

Peter G. Smith, James E. Brownell, Michael P. Thomas, Erik Koenig, Usha Narayanan, James M. Gavin, Ben Amidon, Michael Milhollen, Neil Bence, Mark Manfredi, Jessica Riceberg, Larry Dick, Tary Traore, and Sells Todd B

Subjects

chemistry.chemical_classification, Programmed cell death, business.industry, Immunology, Phases of clinical research, Cell Biology, Hematology, Pharmacology, medicine.disease, Biochemistry, In vitro, Lymphoma, Leukemia, Enzyme, chemistry, Cell culture, medicine, business, Diffuse large B-cell lymphoma

Abstract

Abstract 1413 MLN4924 is an investigational small molecule inhibitor of NEDD8-activating enzyme (NAE) that has shown clinical activity in a Phase I clinical trial in Acute Myelogenous Leukemia (AML). MLN4924 is a mechanism-based inhibitor of NAE as demonstrated through the formation of a NEDD8-MLN4924 covalent adduct that is a tight-binding inhibitor of NAE. The antitumor activity of MLN4924 has been linked to two mechanisms in pre-clinical models: (1) the induction of DNA re-replication and cell death through dysregulation of Cdt-1 and (2) the inhibition of NF-κB signaling. Importantly, modulation of both pathways has been demonstrated in pharmacodynamic (PD) studies from patients administered MLN4924. To characterize potential mechanisms of resistance to MLN4924 xenograft models of AML and Diffuse Large-B cell Lymphoma (DLBCL) were used. Mice bearing HL-60 and THP-1 (AML) and OCI-Ly10 (DLBCL) xenografts were treated with MLN4924 twice weekly for 95–110 days and most animals achieved a complete tumor regression. However, four of ten HL-60, six of ten THP-1 and one of ten OCI-Ly10 xenografts became refractory and re-grew during the MLN4924 treatment period. These tumors were harvested and subjected to microarray analysis and DNA sequencing of genes required for NEDD8 activation by NAE. Mutations in NAEβ resulting in amino acid substitutions were detected in several xenografts in the ATP binding pocket (A171T) and NEDD8-binding cleft (E204K) suggesting that mutations in the target enzyme may play a role in emergence of refractory tumors. Tumors containing mutations in NAEβ were passaged into new mice and shown to be completely insensitive to MLN4924 confirming resistance. In addition, cell lines derived from the resistant xenografts were shown to be resistant to MLN4924 in vitro but remained sensitive to other chemotherapeutic agents. Biochemical analysis of NAEβ mutants revealed a slower rate of NEDD8-MLN4924 adduct formation and demonstrated that the adduct was no longer bound tightly by the mutant enzyme. Thus, treatment emergent mutations in NAEβ lead to MLN4924 resistance in pre-clinical models through reduced inhibitory potency. These data serve as the framework for understanding mechanisms of resistance to MLN4924, provide rationale for patient selection approaches and offer a strategy to overcome treatment emergent mutations that may arise in clinical studies. Disclosures: Milhollen: Millennium Pharmaceuticals: Employment. Thomas:Millennium Pharmaceuticals: Employment. Traore:Millennium Pharmaceuticals: Employment. Narayanan:Millennium Pharmaceuticals: Employment. Riceberg:Millennium Pharmaceuticals: Employment. Sells:Millennium Pharmaceuticals: Employment. Amidon:Millennium Pharmaceuticals: Employment. Manfredi:Millennium Pharmaceuticals: Employment. Bence:Millennium Pharmaceuticals: Employment. Brownell:Millennium Pharmaceuticals: Employment. Dick:Millennium Pharmaceuticals: Employment. Koenig:Millennium Pharmaceuticals, Inc: Employment. Gavin:Millennium Pharmaceuticals: Employment. Smith:Millennium Pharmaceuticals: Employment.

Published

2011

13. Abstract C82: Identification and preclinical characterization of inhibitors of the ubiquitin-activating enzymes UBA1 and UBA6

Author

Paul E. Fleming, James M. Gavin, Yu Yang, Marc Hyer, Petter Veiby, Michael Milhollen, Peter G. Smith, Tary Traore, Sai M. Pulukuri, Jeff Ciavarri, Mark Manfredi, Darshan S. Sappal, Neil Bence, James E. Brownell, Kara Hoar, Jessica Huck, Christopher F. Claiborne, Lawrence Dick, and Derek Liqiang Tou

Subjects

Cancer Research, biology, DNA damage, Ubiquitin-activating enzyme, UBA1, Cell cycle, Ubiquitin ligase, Proliferating cell nuclear antigen, Cell biology, Oncology, Biochemistry, Ubiquitin, Proteasome, biology.protein

Abstract

Millennium Pharmaceuticals, Inc. is dedicated to the discovery and development of novel oncology therapeutics in the area of protein homeostasis. Here we report the identification and characterization of compounds that target the ubiquitin activating enzymes, UBA1 and UBA6. These compounds are mechanism based inhibitors that inactivate the ubiquitin E1 enzymes by forming a ubiquitin compound adduct that remains tightly associated with the E1 adenylate binding site. Treatment of cells with these inhibitors results in cellular effects consistent with known Uba1 biology including rapid loss of E2 ubiquitin thioesters, loss of total ubiquitin conjugates, and accumulation of many ubiquitin proteasome system substrates. Following prolonged treatment, cells primarily arrest in the G2 phase of the cell cycle and ultimately undergo apoptosis. Reflecting the extensive cellular roles of ubiquitin, the compounds also impact global protein turnover, ER stress and DNA damage repair. UBA1 inhibition impairs ubiquitination of PCNA and the Fanconia Anemia protein FANCD2 leading to defective repair of UV induced DNA damage. UBA1 inhibition impacts numerous biological pathways relevant to cancer, results in apoptosis in vitro and is capable of inhibiting tumor growth in mouse xenografts in vivo. These data implicate UBA1 as a target for the treatment of cancer. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2011 Nov 12-16; San Francisco, CA. Philadelphia (PA): AACR; Mol Cancer Ther 2011;10(11 Suppl):Abstract nr C82.

Published

2011

14. Abstract C28: Treatment emergent mutations in NAEbeta confer resistance to the investigational NEDD8-activating enzyme inhibitor MLN4924

Author

Michael P. Thomas, Erik Koenig, Neil Bence, Usha Narayanan, Peter G. Smith, Sells Todd B, Mike Sintchak, Mark Manfredi, Jessica Riceberg, Michael Milhollen, Ben Amidon, Larry Dick, James E. Brownell, James M. Gavin, and Tary Traore

Subjects

chemistry.chemical_classification, Cancer Research, Bortezomib, Mutant, Biology, Topoisomerase-I Inhibitor, Pharmacology, In vitro, Enzyme, Oncology, chemistry, Cell culture, medicine, Proteasome inhibitor, Doxorubicin, medicine.drug

Abstract

MLN4924 is an investigational small molecule inhibitor of NEDD8-activating enzyme (NAE) that has shown clinical activity in Phase I clinical trials. MLN4924 is a mechanism-based inhibitor of NAE as demonstrated through the formation of a NEDD8-MLN4924 covalent adduct that is a tight-binding inhibitor of NAE. The antitumor activity of MLN4924 has been linked to two mechanisms in pre-clinical models: (1) the induction of DNA re-replication and cell death through dysregulation of Cdt-1 and (2) the inhibition of NF- B signaling. Importantly, modulation of both pathways has been demonstrated in pharmacodynamic (PD) studies from patients administered MLN4924. To characterize potential mechanisms of resistance to MLN4924, cell line and xenograft models of solid tumors were used. HCT-116 (colon), NCI-H460 (lung) and Calu-6 (lung) cells were treated with high concentrations of MLN4924 for four days after which the remaining cells were isolated and cultured in drug free media. Six HCT-116, two NCI-H460 and one Calu-6 clone were isolated and found to be at least 10-fold less sensitive to MLN4924, in most cases the isolated clones were completely insensitive indicating they were now resistant to MLN4924. However, the MLN4924 resistant clones were still sensitive to other chemotherapies including bortezomib (proteasome inhibitor), SN-38 (topoisomerase I inhibitor) and doxorubicin (anthracycline) suggesting a resistance mechanism unique to MLN4924. Co-incubation with Pgp, BCRP or MRP2 transporter inhibitors did not re-sensitize cells to MLN4924 indicating that the resistance mechanism was not related to increased drug efflux. DNA sequencing of NAE pathway genes identified heterozygous mutations in NAEbeta resulting in amino acid substitutions in the ATP binding pocket or NEDD8-binding cleft. Nude rats bearing HCT-116 xenografts were treated with the maximum tolerated dose of MLN4924 on a clinically relevant dosing regimen of Days 1, 4, 8 and 11 of a 21 day schedule. In the first cycle of therapy tumor regressions were observed but ultimately tumors regrew over subsequent cycles and were found to contain heterozygous mutations in NAEbeta. Tumors containing mutations in NAEbeta were transplanted into nude rats and shown to be insensitive to MLN4924 confirming resistance. In addition, cell lines derived from the resistant xenografts were shown to be resistant to MLN4924 in vitro but remained sensitive to other chemotherapeutic agents. Biochemical analysis of NAEbeta mutants revealed a slower rate of NEDD8-MLN4924 adduct formation and demonstrated that the adduct was no longer bound tightly by the mutant enzyme. Thus, in pre-clinical models of solid tumors treatment emergent mutations in NAEbeta lead to MLN4924 resistance. DNA sequencing of samples obtained from MLN4924 clinical trials is ongoing. These data may provide rationales for patient selection approaches with MLN4924 and the development of next generation NAE inhibitors that can be designed to overcome treatment emergent mutations found in clinical studies. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2011 Nov 12-16; San Francisco, CA. Philadelphia (PA): AACR; Mol Cancer Ther 2011;10(11 Suppl):Abstract nr C28.

Published

2011

15. A Strategy for National Survival

Author

James M. Gavin

Subjects

Politics, Economic growth, business.industry, Strategy and Management, Material resources, Economics, Distribution (economics), Military strength, business, Socioeconomic status

Abstract

In this analysis of contemporary issues facing the nation, the author suggests that a strategy for survival must go beyond military strength to include the economic status of a nation, the conditions of its domestic society, and the degree to which that nation plans for its future. The planners who formulate such a national strategy also must carefully assess the international political situation and the distribution and availability of essential material resources, such as minerals, petroleum products, and foodstuffs.

Published

1975

16. The Tactical Use of the Atomic Bomb

Author

James M. Gavin

Subjects

education.field_of_study, History, Law, Reprint, Political Science and International Relations, Population, Nuclear weapon, Adversary, China, education, Atomic Bombs

Abstract

Since the beginning of the Korean war there has been much talk about whether the use of atomic bombs could conceivably influence the course of this campaign. On several occasions vague hints have been made that the bomb could be used not only as a mass destruction weapon against large centers of population or industrial installations in the rear of the enemy (which, at present, means in Manchuria or China proper) but also as a tactical support weapon for operation in the field. We reprint below, in a slightly shortened form, an article by Major General Gavin, which contains, to our knowledge, the only discussion by a prominent military expert of the possibility of tactical use of atomic weapons. From the statements of General Lawton Collins, it may be inferred that the views of Major General Gavin have not found acceptance by our highest military authorities—at least not in application to the Korean campaign as it has been fought to date. It is conceivable that the situation might present itself in a diff...

Published

1951

17. A soldier's doubts

Author

James M. Gavin

Subjects

Sociology and Political Science, Political Science and International Relations

Published

1966

18. Journey to Berlin

Author

James M. Gavin and Andrew J. Pierre

Subjects

Sociology and Political Science, Political Science and International Relations

Published

1978

19. On to Berlin; Battle of an Airborne Commander 1943-1946

Author

James A. Huston and James M. Gavin

Subjects

Battle, History, media_common.quotation_subject, Ancient history, media_common

Published

1979

20. Forging a New Sword

Author

Telford Taylor, William R. Kintner, Joseph I. Coffey, Raymond J. Albright, and James M. Gavin

Subjects

Law

Published

1959