Your search keyword '"Sean Caenepeel"' showing total 23 results

1. AMG 757, a Half-Life Extended, DLL3-Targeted Bispecific T-Cell Engager, Shows High Potency and Sensitivity in Preclinical Models of Small-Cell Lung Cancer

Author

Jinghui Zhan, Christopher Murawsky, Petra Deegen, Jonathan Werner, Oliver Homann, Siyuan Liu, Melissa Thomas, Angela Coxon, Keegan Cooke, Pedro J. Beltran, Joshua T. Pearson, Juan Estrada, Fei Lee, Tobias Raum, Julie M. Bailis, Matthias Friedrich, Jude Canon, Jennitte Stevens, Giffin Michael John, Sean Caenepeel, Yajing Yang, Paul E. Hughes, and Edward K. Lobenhofer

Subjects

0301 basic medicine, Cancer Research, Lung Neoplasms, T-Lymphocytes, T cell, Antineoplastic Agents, Apoptosis, Mice, SCID, Mice, 03 medical and health sciences, 0302 clinical medicine, Mice, Inbred NOD, Antibodies, Bispecific, Tumor Cells, Cultured, Animals, Humans, Medicine, Potency, Lung cancer, Cell Proliferation, business.industry, Intracellular Signaling Peptides and Proteins, Antibodies, Monoclonal, Membrane Proteins, Half-life, medicine.disease, Small Cell Lung Carcinoma, Xenograft Model Antitumor Assays, respiratory tract diseases, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Oncology, Tolerability, Cell culture, 030220 oncology & carcinogenesis, Pharmacodynamics, Cancer research, Female, Non small cell, business

Abstract

Purpose: Small-cell lung cancer (SCLC) is an aggressive neuroendocrine tumor with a high relapse rate, limited therapeutic options, and poor prognosis. We investigated the antitumor activity of AMG 757, a half-life extended bispecific T-cell engager molecule targeting delta-like ligand 3 (DLL3)—a target that is selectively expressed in SCLC tumors, but with minimal normal tissue expression. Experimental Design: AMG 757 efficacy was evaluated in SCLC cell lines and in orthotopic and patient-derived xenograft (PDX) mouse SCLC models. Following AMG 757 administration, changes in tumor volume, pharmacodynamic changes in tumor-infiltrating T cells (TILs), and the spatial relationship between the appearance of TILs and tumor histology were examined. Tolerability was assessed in nonhuman primates (NHPs). Results: AMG 757 showed potent and specific killing of even those SCLC cell lines with very low DLL3 expression ( Conclusions: AMG 757 has a compelling safety and efficacy profile in preclinical studies making it a viable option for targeting DLL3-expressing SCLC tumors in the clinical setting.

Published

2021

2. Dual Inhibition of Angiopoietin-TIE2 and MET Alters the Tumor Microenvironment and Prolongs Survival in a Metastatic Model of Renal Cell Carcinoma

Author

Remi Adelaiye-Ogala, Karen Rex, Li Shen, Swathi Ramakrishnan, Roberto Pili, May Elbanna, Ashley Orillion, Eric Ciamporcero, Sean Caenepeel, Sreenivasulu Chintala, Sheng-Yu Ku, Nur P. Damayanti, Kiersten Marie Miles, and Angela Coxon

Subjects

Male, 0301 basic medicine, Cancer Research, Combination therapy, Mice, SCID, Article, Angiopoietin-2, Angiopoietin, Mice, 03 medical and health sciences, 0302 clinical medicine, Renal cell carcinoma, Cell Line, Tumor, Tumor Microenvironment, medicine, Carcinoma, Animals, Humans, Neoplasm Metastasis, Carcinoma, Renal Cell, Tumor microenvironment, biology, business.industry, medicine.disease, Survival Analysis, Primary tumor, Angiopoietin receptor, Clear cell renal cell carcinoma, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, business

Abstract

Receptor tyrosine kinase inhibitors have shown clinical benefit in clear cell renal cell carcinoma (ccRCC), but novel therapeutic strategies are needed. The angiopoietin/Tie2 and MET pathways have been implicated in tumor angiogenesis, metastases, and macrophage infiltration. In our study, we used trebananib, an angiopoietin 1/2 inhibitor, and a novel small-molecule MET kinase inhibitor in patient-derived xenograft (PDX) models of ccRCC. Our goal was to assess the ability of these compounds to alter the status of tumor-infiltrating macrophages, inhibit tumor growth and metastases, and prolong survival. Seven-week-old SCID mice were implanted subcutaneously or orthotopically with human ccRCC models. One month postimplantation, mice were treated with angiopoietin 1/2 inhibitor trebananib (AMG 386), MET kinase inhibitor, or combination. In our metastatic ccRCC PDX model, RP-R-02LM, trebananib alone, and in combination with a MET kinase inhibitor, significantly reduced lung metastases and M2 macrophage infiltration (P = 0.0075 and P = 0.0205, respectively). Survival studies revealed that treatment of the orthotopically implanted RP-R-02LM tumors yielded a significant increase in survival in both trebananib and combination groups. In addition, resection of the subcutaneously implanted primary tumor allowed for a significant survival advantage to the combination group compared with vehicle and both single-agent groups. Our results show that the combination of trebananib with a MET kinase inhibitor significantly inhibits the spread of metastases, reduces infiltrating M2-type macrophages, and prolongs survival in our highly metastatic ccRCC PDX model, suggesting a potential use for this combination therapy in treating patients with ccRCC.

Published

2020

3. Discovery and in Vivo Evaluation of Macrocyclic Mcl-1 Inhibitors Featuring an α-Hydroxy Phenylacetic Acid Pharmacophore or Bioisostere

Author

Gwenaella Rescourio, Ana Z. Gonzalez, Salman Jabri, Brian Belmontes, Gordon Moody, Doug Whittington, Xin Huang, Sean Caenepeel, Mario Cardozo, Alan C. Cheng, David Chow, Hannah Dou, Adrie Jones, Ron C. Kelly, Yihong Li, Mike Lizarzaburu, Mei-Chu Lo, Rommel Mallari, Cesar Meleza, Yosup Rew, Scott Simonovich, Daqing Sun, Simon Turcotte, Xuelei Yan, Simon G. Wong, Evelyn Yanez, Manuel Zancanella, Jonathan Houze, Julio C. Medina, Paul E. Hughes, and Sean P. Brown

Subjects

Sulfonamides, Administration, Oral, Biological Availability, Mice, Nude, Antineoplastic Agents, Hydrogen Bonding, Crystallography, X-Ray, Xenograft Model Antitumor Assays, Rats, Sprague-Dawley, Structure-Activity Relationship, Drug Stability, Cell Line, Tumor, Drug Design, Drug Discovery, Animals, Humans, Myeloid Cell Leukemia Sequence 1 Protein, Molecular Medicine, Female, Multiple Myeloma, Phenylacetates

Abstract

Overexpression of the antiapoptotic protein Mcl-1 provides a survival advantage to some cancer cells, making inhibition of this protein an attractive therapeutic target for the treatment of certain types of tumors. Herein, we report our efforts toward the identification of a novel series of macrocyclic Mcl-1 inhibitors featuring an α-hydroxy phenylacetic acid pharmacophore or bioisostere. This work led to the discovery of

Published

2019

4. Targeting MCL-1 in hematologic malignancies: Rationale and progress

Author

Andrew H. Wei, Sean Caenepeel, Khalid Mezzi, Paul E. Hughes, Andrew Spencer, Roland B. Walter, Phuong Khanh Morrow, Zach McIver, David S. Siegel, Andrew W. Roberts, Aaron S. Rosenberg, and Anthony S. Stein

Subjects

medicine.medical_specialty, Myeloid, Chronic lymphocytic leukemia, Antineoplastic Agents, Article, chemistry.chemical_compound, immune system diseases, Internal medicine, hemic and lymphatic diseases, medicine, Animals, Humans, Molecular Targeted Therapy, neoplasms, Multiple myeloma, Hematology, business.industry, Venetoclax, Myeloid leukemia, medicine.disease, Up-Regulation, Myeloid Cell Leukemia Sequence 1 Protein, Gene Expression Regulation, Neoplastic, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Oncology, chemistry, Hematologic Neoplasms, Cancer research, business, Multiple Myeloma, Signal Transduction

Abstract

Myeloid cell leukemia sequence 1 (MCL-1) is an antiapoptotic protein that plays a key role in promoting cell survival in multiple myeloma (MM), acute myeloid leukemia (AML), and non-Hodgkin lymphoma (NHL). Overexpression of MCL-1 is associated with treatment resistance and poor prognosis; thus, MCL-1 inhibitors are rational therapeutic options for malignancies depending on MCL-1. Several MCL-1 inhibitors have entered clinical trials, including AZD5991, S64315, AMG 176, and AMG 397. A key area of investigation is whether MCL-1 inhibitors will complement the activity of BCL-2 inhibitors, such as venetoclax, and synergistically enhance anti-tumor efficacy when given in combination with other anti-cancer drugs. Another important question is whether a safe therapeutic window can be found for this new class of inhibitors. In summary, inhibition of MCL-1 shows potential as a treatment for hematologic malignancies and clinical evaluation of MCL-1 inhibitors is currently underway.

Published

2019

5. Targeted Therapy and Checkpoint Immunotherapy Combinations for the Treatment of Cancer

Author

Lawren C. Wu, Paul E. Hughes, and Sean Caenepeel

Subjects

Vascular Endothelial Growth Factor A, 0301 basic medicine, MAPK/ERK pathway, Angiogenesis, T-Lymphocytes, medicine.medical_treatment, Programmed Cell Death 1 Receptor, Immunology, B7-H1 Antigen, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Immune system, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Animals, Humans, Immunology and Allergy, Medicine, Combined Modality Therapy, CTLA-4 Antigen, Molecular Targeted Therapy, Extracellular Signal-Regulated MAP Kinases, business.industry, Antibodies, Monoclonal, Cancer, Immunotherapy, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Signal transduction, business, Signal Transduction

Abstract

Many advances in the treatment of cancer have been driven by the development of targeted therapies that inhibit oncogenic signaling pathways and tumor-associated angiogenesis, as well as by the recent development of therapies that activate a patient's immune system to unleash antitumor immunity. Some targeted therapies can have effects on host immune responses, in addition to their effects on tumor biology. These immune-modulating effects, such as increasing tumor antigenicity or promoting intratumoral T cell infiltration, provide a rationale for combining these targeted therapies with immunotherapies. Here, we discuss the immune-modulating effects of targeted therapies against the MAPK and VEGF signaling pathways, and how they may synergize with immunomodulatory antibodies that target PD1/PDL1 and CTLA4. We critically examine the rationale in support of these combinations in light of the current understanding of the underlying mechanisms of action of these therapies. We also discuss the available preclinical and clinical data for these combination approaches and their implications regarding mechanisms of action. Insights from these studies provide a framework for considering additional combinations of targeted therapies and immunotherapies for the treatment of cancer.

Published

2016

6. Preclinical Evaluation of AMG 337, a Highly Selective Small Molecule MET Inhibitor, in Hepatocellular Carcinoma

Author

Ying He, Ouhong Wang, Yanni Zhang, Zhiqiang Du, En-Tzu Tang, Eric Huang, Hui Zhou, Karen Rex, Wenge Zhong, Yuqing Shen, Mingqiang Zhang, Angela Coxon, Sean Caenepeel, Jacqueline Huang, and Liaoyuan Hu

Subjects

0301 basic medicine, Cancer Research, Carcinoma, Hepatocellular, Cell Survival, Pyridones, Administration, Oral, Antineoplastic Agents, Pharmacology, Small Molecule Libraries, Mice, 03 medical and health sciences, 0302 clinical medicine, In vivo, Cell Line, Tumor, medicine, Carcinoma, Animals, Humans, Viability assay, Cell Proliferation, Cell growth, Chemistry, Liver Neoplasms, Gene Amplification, Cancer, Proto-Oncogene Proteins c-met, Triazoles, medicine.disease, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Hepatocyte growth factor, Signal Transduction, medicine.drug

Abstract

Aberrant hepatocyte growth factor (HGF)/MET signaling has been implicated in hepatocarcinogenesis, suggesting that MET may serve as an attractive therapeutic target in hepatocellular carcinoma. We sought to investigate the in vitro and in vivo antitumor activity of AMG 337, a potent and highly selective small molecule MET kinase inhibitor, in preclinical models of hepatocellular carcinoma. The antiproliferative activity of AMG 337 was evaluated across a panel of hepatocellular carcinoma cell lines in a viability assay. Daily oral administration was used to evaluate the in vivo antitumor activity of AMG 337 in two patient-derived xenograft (PDX) models of hepatocellular carcinoma (LI0612 and LI1078). AMG 337 exerted potent antiproliferative activity against 2 of 40 hepatocellular carcinoma cell lines, namely, MHCC97H (IC50, 0.015 μmol/L) and HCCLM3 (IC50, 0.025 μmol/L). Both sensitive cell lines showed MET amplification (MET/CEN-7 >2.0) assessed by FISH, and high MET expression (3+ IHC) assessed by IHC. AMG 337 potently inhibited p-MET in all cell lines with detectable levels of total MET. However, the dose-dependent inhibition of downstream effectors of HGF/MET signaling, including p-GAB1, p-AKT, and p-ERK, was limited to those cell lines sensitive to AMG 337 in a viability assay (MHCC97H and HCCLM3). AMG 337 significantly inhibited tumor growth at all doses tested in the MET-amplified and MET-high–expressing hepatocellular carcinoma PDX model LI0612 and had no effect on tumor growth in the non-MET–amplified and MET-low–expressing hepatocellular carcinoma PDX model LI1078. AMG 337 represents a promising and novel therapeutic strategy for targeting hepatocellular carcinomas with a dependence on HGF/MET signaling. Mol Cancer Ther; 15(6); 1227–37. ©2016 AACR.

Published

2016

7. Selective MET Kinase Inhibition in MET-Dependent Glioma Models Alters Gene Expression and Induces Tumor Plasticity

Author

Isabelle Dussault, Arend Heerschap, Angela Coxon, Houshang Amiri, William P.J. Leenders, Tessa J. J. de Bitter, Anna C. Navis, Wiljan Hendriks, Paul N. Span, Pieter Wesseling, Corina N. A. M. van den Heuvel, Karen Rex, Kiek Verrijp, and Sean Caenepeel

Subjects

0301 basic medicine, Cancer Research, Cabozantinib, Cell Survival, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Aminopyridines, Biology, Receptor tyrosine kinase, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Paracrine signalling, Mice, 0302 clinical medicine, Growth factor receptor, In vivo, Glioma, Cell Line, Tumor, Urological cancers Radboud Institute for Molecular Life Sciences [Radboudumc 15], Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, Animals, Humans, Molecular Biology, Protein Kinase Inhibitors, Cell Proliferation, Women's cancers Radboud Institute for Molecular Life Sciences [Radboudumc 17], Brain Neoplasms, Sequence Analysis, RNA, Gene Expression Profiling, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Phosphorylation, Pyrazoles, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19], HT29 Cells

Abstract

Contains fulltext : 181795.pdf (Publisher’s version ) (Closed access) The receptor tyrosine kinase (RTK) MET represents a promising tumor target in a subset of glioblastomas. Most RTK inhibitors available in the clinic today, including those inhibiting MET, affect multiple targets simultaneously. Previously, it was demonstrated that treatment with cabozantinib (MET/VEGFR2/RET inhibitor) prolonged survival of mice carrying orthotopic patient-derived xenografts (PDX) of the MET-addicted glioblastoma model E98, yet did not prevent development of recurrent and cabozantinib-resistant tumors. To exclude VEGFR2 inhibition-inflicted blood-brain barrier normalization and diminished tumor distribution of the drug, we have now investigated the effects of the novel MET-selective inhibitor Compound A in the orthotopic E98 xenograft model. In vitro, Compound A proved a highly potent inhibitor of proliferation of MET-addicted cell lines. In line with its target selectivity, Compound A did not restore the leaky blood-brain barrier and was more effective than cabozantinib in inhibiting MET phosphorylation in vivo Compound A treatment significantly prolonged survival of mice carrying E98 tumor xenografts, but did not prevent eventual progression. Contrasting in vitro results, the Compound A-treated xenografts displayed high levels of AKT phosphorylation despite the absence of phosphorylated MET. Profiling by RNA sequencing showed that in vivo transcriptomes differed significantly from those in control xenografts.Implications: Collectively, these findings demonstrate the plasticity of paracrine growth factor receptor signaling in vivo and urge for prudency with in vitro drug-testing strategies to validate monotherapies. Mol Cancer Res; 15(11); 1587-97. (c)2017 AACR.

Published

2017

8. MAPK pathway inhibition induces MET and GAB1 levels, priming BRAF mutant melanoma for rescue by hepatocyte growth factor

Author

Keegan Cooke, Blanca Homet Moreno, Sean Caenepeel, Sarah Wadsworth, Giulia Parisi, Lidia Robert, Angela Coxon, Antoni Ribas, Richard Kendall, Paul E. Hughes, Elaina Cajulis, Guo Huang, and Pedro J. Beltran

Subjects

0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, MAPK/ERK pathway, Indoles, medicine.medical_treatment, Nude, Drug Resistance, GAB1, Apoptosis, Targeted therapy, Mice, 0302 clinical medicine, HGF, Cancer, Sulfonamides, Tumor, Hepatocyte Growth Factor, Melanoma, Adaptor Proteins, Dipeptides, Proto-Oncogene Proteins c-met, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Benzamides, MET, Hepatocyte growth factor, Female, Development of treatments and therapeutic interventions, Tyrosine kinase, Research Paper, medicine.drug, Proto-Oncogene Proteins B-raf, Combination therapy, Pyridones, MAP Kinase Signaling System, Oncology and Carcinogenesis, Mice, Nude, Antineoplastic Agents, Cell Line, BRAF, resistance, 03 medical and health sciences, Cell Line, Tumor, medicine, melanoma, Animals, Humans, neoplasms, Protein Kinase Inhibitors, Adaptor Proteins, Signal Transducing, business.industry, Diphenylamine, Signal Transducing, Triazoles, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, Vemurafenib, Drug Resistance, Neoplasm, Immunology, Cancer research, Neoplasm, business

Abstract

Therapeutic resistance is a major obstacle to achieving durable clinical responses with targeted therapies, highlighting a need to elucidate the underlying mechanisms responsible for resistance and identify strategies to overcome this challenge. An emerging body of data implicates the tyrosine kinase MET in mediating resistance to BRAF inhibitors in BRAFV600E mutant melanoma. In this study we observed a dominant role for the HGF/MET axis in mediating resistance to BRAF and MEK inhibitors in models of BRAFV600E and NRAS mutant melanoma. In addition, we showed that MAPK pathway inhibition induced rapid increases in MET and GAB1 levels, providing novel mechanistic insight into how BRAFV600E mutant melanoma is primed for HGF-mediated rescue. We also determined that tumor-derived HGF, not systemic HGF, may be required to convey resistance to BRAF inhibition in vivo and that resistance could be reversed following treatment with AMG 337, a selective MET inhibitor. In summary, these findings support the clinical evaluation of MET-directed targeted therapy to circumvent resistance to BRAF and MEK inhibitors in BRAFV600E mutant melanoma. In addition, the induction of MET following treatment with BRAF and MEK inhibitors has the potential to serve as a predictive biomarker for identifying patients best suited for MET inhibitor combination therapy.

Published

2017

9. MDM2 antagonists synergize broadly and robustly with compounds targeting fundamental oncogenic signaling pathways

Author

Tao Osgood, Julie A. Lofgren, Marc Payton, Rebecca Robertson, Sean Caenepeel, Dongyin Yu, Jude Canon, Cheng Su, Adrie Jones, Jebediah Ledell, Chetan Deshpande, Jonathan D. Oliner, Xiaoning Zhao, Paul E. Hughes, and Anne Y. Saiki

Subjects

Drug, MAPK/ERK pathway, Cell Survival, media_common.quotation_subject, Gene Expression, synergy, Apoptosis, Drug resistance, Biology, PI3K, MDM2, Cell Line, Tumor, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Humans, Viability assay, PI3K/AKT/mTOR pathway, Cell Proliferation, media_common, FOXM1, Rational design, Drug Synergism, Proto-Oncogene Proteins c-mdm2, MAPK, MEK, Oncology, Targeted drug delivery, biology.protein, Cancer research, Mdm2, Drug Screening Assays, Antitumor, Signal Transduction, Priority Research Paper

Abstract

While MDM2 inhibitors hold great promise as cancer therapeutics, drug resistance will likely limit their efficacy as single agents. To identify drug combinations that might circumvent resistance, we screened for agents that could synergize with MDM2 inhibition in the suppression of cell viability. We observed broad and robust synergy when combining MDM2 antagonists with either MEK or PI3K inhibitors. Synergy was not limited to cell lines harboring MAPK or PI3K pathway mutations, nor did it depend on which node of the PI3K axis was targeted. MDM2 inhibitors also synergized strongly with BH3 mimetics, BCR-ABL antagonists, and HDAC inhibitors. MDM2 inhibitor-mediated synergy with agents targeting these mechanisms was much more prevalent than previously appreciated, implying that clinical translation of these combinations could have far-reaching implications for public health. These findings highlight the importance of combinatorial drug targeting and provide a framework for the rational design of MDM2 inhibitor clinical trials.

Published

2014

10. The Role of MDM2 Amplification and Overexpression in Tumorigenesis

Author

Jonathan D. Oliner, Anne Y. Saiki, and Sean Caenepeel

Subjects

0301 basic medicine, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, law.invention, 03 medical and health sciences, Mice, 0302 clinical medicine, law, Gene duplication, medicine, SNP, Animals, Humans, neoplasms, Mice, Knockout, Gene Amplification, Proto-Oncogene Proteins c-mdm2, medicine.disease, 030104 developmental biology, Cell Transformation, Neoplastic, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Mdm2, Suppressor, Sarcoma, Tumor Suppressor Protein p53, Carcinogenesis, Nuclear localization sequence, Perspectives

Abstract

Mouse double minute 2 (MDM2) is a critical negative regulator of the tumor suppressor p53, playing a key role in controlling its transcriptional activity, protein stability, and nuclear localization. MDM2 expression is up-regulated in numerous cancers, resulting in a loss of p53-dependent activities, such as apoptosis and cell-cycle arrest. Genetic amplification and inheritance of MDM2 promoter single-nucleotide polymorphisms (SNPs) are the two best-studied mechanisms for up-regulating MDM2 activity. This article provides an overview of these events in human cancer, highlighting the frequent occurrence of MDM2 amplification in sarcoma and the role of SNP309 and SNP285 in regulating MDM2 expression and cancer risk. The availability of large-scale genomic profiling datasets, like those from The Cancer Genome Atlas Research Network, have provided the opportunity to evaluate the consequences of MDM2 amplification and SNP inheritance across high-quality tumor samples from diverse cancer indications.

Published

2016

11. Synthesis and structure–activity relationships of dual PI3K/mTOR inhibitors based on a 4-amino-6-methyl-1,3,5-triazine sulfonamide scaffold

Author

Yunxin Bo, Tisha San Miguel, Nobuko Nishimura, Jian Jiang, Douglas A. Whittington, Paul E. Hughes, Sean Caenepeel, Mark H. Norman, John D. McCarter, Erin L. Mullady, Daniel J. Freeman, Kevin Yang, Ryan Wurz, Longbin Liu, Raju Subramanian, Kristin L. Andrews, Ling Wang, Liping H. Pettus, and Nancy Zhang

Subjects

Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Pharmacology, Crystallography, X-Ray, Biochemistry, Mice, Phosphatidylinositol 3-Kinases, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Neoplasms, Drug Discovery, Animals, Humans, Structure–activity relationship, Phosphorylation, Protein Kinase Inhibitors, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Sulfonamides, Binding Sites, Phosphoinositide 3-kinase, biology, Triazines, Akt/PKB signaling pathway, Chemistry, TOR Serine-Threonine Kinases, Cellular Assay, Organic Chemistry, Rats, Molecular Docking Simulation, biology.protein, Molecular Medicine, Female, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Phosphoinositide 3-kinase (PI3K) is an important target in oncology due to the deregulation of the PI3K/Akt signaling pathway in a wide variety of tumors. A series of 4-amino-6-methyl-1,3,5-triazine sulfonamides were synthesized and evaluated as inhibitors of PI3K. The synthesis, in vitro biological activities, pharmacokinetic and in vivo pharmacodynamic profiling of these compounds are described. The most promising compound from this investigation (compound 3j) was found to be a pan class I PI3K inhibitor with a moderate (>10-fold) selectivity over the mammalian target of rapamycin (mTOR) in the enzyme assay. In a U87 MG cellular assay measuring phosphorylation of Akt, compound 3j displayed low double digit nanomolar IC(50) and exhibited good oral bioavailability in rats (F(oral)=63%). Compound 3j also showed a dose dependent reduction in the phosphorylation of Akt in a U87 tumor pharmacodynamic model with a plasma EC(50)=193 nM (91 ng/mL).

Published

2012

12. Structure-Based Design of a Novel Series of Potent, Selective Inhibitors of the Class I Phosphatidylinositol 3-Kinases

Author

Yunxin Y. Bo, Leeanne Zalameda, Kevin Yang, Fang-Tsao Hong, Longbin Liu, Anthony B. Reed, Kristin L. Andrews, Tisha San Miguel, Brian A. Lanman, Paul E. Hughes, Noel D'angelo, Brad Herberich, Jian Jiang, Victor J. Cee, Claire L. M. Jackson, Ryan Wurz, Nobuko Nishimura, Raju Subramanian, Seifu Tadesse, Nancy Zhang, John D. McCarter, Daniel J. Freeman, Ling Wang, Nuria A. Tamayo, Erin L. Mullady, Mark H. Norman, Liping H. Pettus, Tian Wu, Douglas A. Whittington, Sean Caenepeel, Adrian L. Smith, and Shon Booker

Subjects

Models, Molecular, Indazoles, Class I Phosphatidylinositol 3-Kinases, Pyridines, Biological Availability, Mice, Nude, Crystallography, X-Ray, Piperazines, Mice, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Drug Discovery, Animals, Humans, Structure–activity relationship, Sulfones, Phosphatidylinositol, PI3K/AKT/mTOR pathway, Sulfonamides, Triazines, Akt/PKB signaling pathway, Chemistry, Kinase, TOR Serine-Threonine Kinases, Xenograft Model Antitumor Assays, Rats, Cell biology, Pyrimidines, Biochemistry, Purines, Drug Design, Microsomes, Liver, Pyrazoles, Molecular Medicine, Female, Signal transduction, Proto-Oncogene Proteins c-akt, Signal Transduction, Phosphoinositide-dependent kinase-1

Abstract

A highly selective series of inhibitors of the class I phosphatidylinositol 3-kinases (PI3Ks) has been designed and synthesized. Starting from the dual PI3K/mTOR inhibitor 5, a structure-based approach was used to improve potency and selectivity, resulting in the identification of 54 as a potent inhibitor of the class I PI3Ks with excellent selectivity over mTOR, related phosphatidylinositol kinases, and a broad panel of protein kinases. Compound 54 demonstrated a robust PD-PK relationship inhibiting the PI3K/Akt pathway in vivo in a mouse model, and it potently inhibited tumor growth in a U-87 MG xenograft model with an activated PI3K/Akt pathway.

Published

2012

13. Phospshoinositide 3-Kinase (PI3K)/Mammalian Target of Rapamycin (mTOR) Dual Inhibitors: Discovery and Structure–Activity Relationships of a Series of Quinoline and Quinoxaline Derivatives

Author

Ling Wang, Leeanne Zalameda, Hongyu Liao, Kristin L. Andrews, Yunxin Bo, Nobuko Nishimura, Paul E. Hughes, John D. McCarter, Erin L. Mullady, Tisha San Miguel, Douglas A. Whittington, Sean Caenepeel, Nancy Zhang, Daniel J. Freeman, Mark H. Norman, Shon Booker, Aaron C. Siegmund, Nuria A. Tamayo, Marian C. Bryan, Raju Subramanian, Kevin Yang, and Longbin Liu

Subjects

Male, Models, Molecular, Protein Conformation, Biological Availability, In Vitro Techniques, Pharmacology, Crystallography, X-Ray, PI3K signaling, Rats, Sprague-Dawley, Mice, Phosphatidylinositol 3-Kinases, Structure-Activity Relationship, chemistry.chemical_compound, Quinoxaline, In vivo, Quinoxalines, Drug Discovery, medicine, Animals, Humans, Phosphorylation, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Kinase, Chemistry, TOR Serine-Threonine Kinases, Quinoline, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Rats, Liver, Quinolines, Molecular Medicine, Protein Binding

Abstract

The phosphoinositide 3-kinase (PI3K) family catalyzes the ATP-dependent phosphorylation of the 3'-hydroxyl group of phosphatidylinositols and plays an important role in cell growth and survival. There is abundant evidence demonstrating that PI3K signaling is dysregulated in many human cancers, suggesting that therapeutics targeting the PI3K pathway may have utility for the treatment of cancer. Our efforts to identify potent, efficacious, and orally available PI3K/mammalian target of rapamycin (mTOR) dual inhibitors resulted in the discovery of a series of substituted quinolines and quinoxalines derivatives. In this report, we describe the structure-activity relationships, selectivity, and pharmacokinetic data of this series and illustrate the in vivo pharmacodynamic and efficacy data for a representative compound.

Published

2011

14. Pyridyl-pyrimidine benzimidazole derivatives as potent, selective, and orally bioavailable inhibitors of Tie-2 kinase

Author

Alan C. Cheng, Karina Romero, Jasmine Lin, Hanh Nho Nguyen, Yihong Zhou, Paul E. Hughes, Vinod F. Patel, Stephanie D. Geuns-Meyer, Philip R. Olivieri, James Bready, Annette Bak, Sean Caenepeel, Joseph L. Kim, Holly L. Deak, Alexander M. Long, Angela Coxon, Steve Bellon, Douglas A. Whittington, Victor J. Cee, Brian L. Hodous, Yan Gu, Ling Wang, Jenne Fretland, Christopher Mohr, and Xin Huang

Subjects

Models, Molecular, Benzimidazole, Pyrimidine, Angiogenesis, Clinical Biochemistry, Administration, Oral, Biological Availability, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, chemistry.chemical_compound, Pathological Angiogenesis, Drug Discovery, Humans, Transferase, Protein Kinase Inhibitors, Molecular Biology, Kinase, Organic Chemistry, Receptor, TIE-2, Small molecule, Bioavailability, chemistry, Molecular Medicine, Benzimidazoles, HeLa Cells

Abstract

Selective small molecule inhibitors of Tie-2 kinase are important tools for the validation of Tie-2 signaling in pathological angiogenesis. Reported herein is the optimization of a nonselective scaffold into a potent and highly selective inhibitor of Tie-2 kinase.

Published

2009

15. Broad Antitumor Activity in Breast Cancer Xenografts by Motesanib, a Highly Selective, Oral Inhibitor of Vascular Endothelial Growth Factor, Platelet-Derived Growth Factor, and Kit Receptors

Author

Stephen Kaufman, Robert Radinsky, James B. Rottman, Vinod F. Patel, Douglas Saffran, Paul E. Hughes, Sean Caenepeel, Tammy L. Bush, Brian Belmontes, Karen Rex, Anthony Polverino, Angela Coxon, Richard Kendall, and Andrew Tasker

Subjects

Niacinamide, Vascular Endothelial Growth Factor A, Oncology, Cancer Research, medicine.medical_specialty, Indoles, Platelet-derived growth factor, Angiogenesis, Oligonucleotides, Mice, Nude, Angiogenesis Inhibitors, Mice, Random Allocation, chemistry.chemical_compound, Growth factor receptor, Cell Line, Tumor, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Motesanib, Animals, Humans, Growth factor receptor inhibitor, Cell Proliferation, Platelet-Derived Growth Factor, Dose-Response Relationship, Drug, business.industry, Body Weight, Mammary Neoplasms, Experimental, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Vascular endothelial growth factor, Proto-Oncogene Proteins c-kit, chemistry, Cancer research, Female, business, Tamoxifen, medicine.drug

Abstract

Purpose: Angiogenesis plays a critical role in breast cancer development and progression. Vascular endothelial growth factor (VEGF) is a potent angiogenic factor that regulates endothelial cell proliferation and survival. We investigated the effects of motesanib, a novel, oral inhibitor of VEGF receptors 1, 2, and 3; platelet-derived growth factor receptor; and Kit receptor, on the growth of xenografts representing various human breast cancer subtypes. Experimental Design: Athymic nude mice were implanted with MCF-7 (luminal) or MDA-MB-231 (mesenchymal) tumor fragments or Cal-51 (mixed/progenitor) tumor cells. Once tumors were established, animals were randomized to receive increasing doses of motesanib alone or motesanib plus cytotoxic chemotherapy (docetaxel, doxorubicin, or tamoxifen). Results: Across all three xenograft models, motesanib treatment resulted in significant dose-dependent reductions in tumor growth, compared with vehicle-treated controls, and in marked reductions in viable tumor fraction and blood vessel density. No significant effect on body weight was observed with compound treatment compared with control-treated animals. Motesanib did not affect the proliferation of tumor cells in vitro. There was a significantly greater reduction in xenograft tumor growth when motesanib was combined with docetaxel (MDA-MB-231 tumors) or with the estrogen receptor modulator tamoxifen (MCF-7 tumors), compared with either treatment alone, but not when combined with doxorubicin (Cal-51 tumors). Conclusions: Treatment with motesanib alone or in combination with chemotherapy inhibits tumor growth in vivo in various models of human breast cancer. These data suggest that motesanib may have broad utility in the treatment of human breast cancer.

Published

2008

16. Alkynylpyrimidine Amide Derivatives as Potent, Selective, and Orally Active Inhibitors of Tie-2 Kinase

Author

Joseph L. Kim, Paul E. Hughes, Brian K. Albrecht, Jenne Fretland, Paul Gallant, David C. Mcgowan, Huilin Zhao, Steve Bellon, Michael Morrison, Victor J. Cee, Vinod F. Patel, Sean Caenepeel, Stephanie D. Geuns-Meyer, Alexander M. Long, Anthony Polverino, James Bready, Ling Wang, Doug Hoffman, Brian L. Hodous, Yan Gu, Paul E. Rose, Angela Coxon, David Powers, Rebecca E. Johnson, Maurice Emery, Richard Kendall, Philip R. Olivieri, and Stuart C. Chaffee

Subjects

Male, Angiogenesis, Angiogenesis Inhibitors, In Vitro Techniques, Receptor tyrosine kinase, Cell Line, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, Adenosine Triphosphate, Vasculogenesis, Drug Discovery, Animals, Humans, Phosphorylation, Receptor, Lung, Binding Sites, biology, Kinase, Chemistry, Autophosphorylation, Stereoisomerism, Blood Proteins, Amides, Receptor, TIE-2, Rats, Pyrimidines, Biochemistry, Alkynes, Microsomes, Liver, biology.protein, Cancer research, Molecular Medicine, Female, Signal transduction, Protein Binding

Abstract

The recognition that aberrant angiogenesis contributes to the pathology of inflammatory diseases, cancer, and myocardial ischemia has generated considerable interest in the molecular mechanisms that regulate blood vessel growth. The receptor tyrosine kinase Tie-2 is expressed primarily by vascular endothelial cells and is critical for embryonic vasculogenesis. Interference with the Tie-2 pathway by diverse blocking agents such as soluble Tie-2 receptors, anti-Tie-2 intrabodies, anti-Ang-2 antibodies, and peptide-Fc conjugates has been shown to suppress tumor growth in xenograft studies. An alternative strategy for interfering with the Tie-2 signaling pathway involves direct inhibition of the kinase functions of the Tie-2 receptor. Herein we describe the development of alkynylpyrimidine amide derivatives as potent, selective, and orally available ATP-competitive inhibitors of Tie-2 autophosphorylation.

Published

2007

17. Evolution of a Highly Selective and Potent 2-(Pyridin-2-yl)-1,3,5-triazine Tie-2 Kinase Inhibitor

Author

Brian K. Albrecht, Paul E. Rose, James Bready, Yan Gu, Joseph L. Kim, Angela Coxon, Paul Tempest, Rebecca E. Johnson, Vinod F. Patel, Paul Gallant, Brian L. Hodous, Stephanie D. Geuns-Meyer, Huilin Zhao, Maurice Emery, Ling Wang, Victor J. Cee, Jenne Fretland, Paul E. Hughes, Richard Kendall, Douglas A. Whittington, Philip R. Olivieri, Doug Hoffman, Stuart C. Chaffee, Steve Bellon, Michael Morrison, Sean Caenepeel, Alexander M. Long, and Anthony Polverino

Subjects

Male, Models, Molecular, Pyridines, Angiogenesis, Administration, Oral, Angiogenesis Inhibitors, Crystallography, X-Ray, Receptor tyrosine kinase, Rats, Sprague-Dawley, Neovascularization, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Animals, Humans, Phosphorylation, Triazine, Binding Sites, Molecular Structure, Nicotinamide, biology, Triazines, Kinase, Blood Proteins, Receptor, TIE-2, Vascular Endothelial Growth Factor Receptor-2, Angiopoietin receptor, Rats, Biochemistry, chemistry, Benzamides, Injections, Intravenous, Cancer research, biology.protein, Molecular Medicine, Female, medicine.symptom, Signal transduction, Injections, Intraperitoneal, Protein Binding

Abstract

Inhibition of angiogenesis is a promising and clinically validated approach for limiting tumor growth and survival. The receptor tyrosine kinase Tie-2 is expressed almost exclusively in the vascular endothelium and is required for developmental angiogenesis and vessel maturation. However, the significance of Tie-2 signaling in tumor angiogenesis is not well understood. In order to evaluate the therapeutic utility of inhibiting Tie-2 signaling, we developed a series of potent and orally bioavailable small molecule Tie-2 kinase inhibitors with selectivity over other kinases, especially those that are believed to be important for tumor angiogenesis. Our earlier work provided pyridinyl pyrimidine 6 as a potent, nonselective Tie-2 inhibitor that was designed on the basis of X-ray cocrystal structures of KDR inhibitors 34 (triazine) and 35 (nicotinamide). Lead optimization resulted in pyridinyl triazine 63, which exhibited30-fold selectivity over a panel of kinases, good oral exposure, and in vivo inhibition of Tie-2 phosphorylation.

Published

2007

18. In Vitro and In Vivo Activity of AMG 337, a Potent and Selective MET Kinase Inhibitor, in MET-Dependent Cancer Models

Author

Martin A. Broome, Jean-Christophe Harmange, Jodi Moriguchi, Hue T. Kha, Benny Amore, Michael A. Damore, Robert Radinsky, Richard Kendall, Teresa L. Burgess, Angela Coxon, Deborah Choquette, Karen Rex, Yihong Zhang, Daniel M. Baker, Jonathan Werner, Paul E. Hughes, Yajing Yang, Isabelle Dussault, Paula Kaplan-Lefko, and Sean Caenepeel

Subjects

0301 basic medicine, MAPK/ERK pathway, Cancer Research, Cell Survival, MAP Kinase Signaling System, Antineoplastic Agents, Pharmacology, 03 medical and health sciences, Mice, Necrosis, Phosphatidylinositol 3-Kinases, 0302 clinical medicine, In vivo, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Receptor, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cell Proliferation, Dose-Response Relationship, Drug, Kinase, Chemistry, Gene Amplification, Proto-Oncogene Proteins c-met, Xenograft Model Antitumor Assays, Disease Models, Animal, 030104 developmental biology, Oncology, Mechanism of action, Cell culture, 030220 oncology & carcinogenesis, Phosphorylation, Female, medicine.symptom, Signal Transduction

Abstract

The MET receptor tyrosine kinase is involved in cell growth, survival, and invasion. Clinical studies with small molecule MET inhibitors have shown the role of biomarkers in identifying patients most likely to benefit from MET-targeted therapy. AMG 337 is an oral, small molecule, ATP-competitive, highly selective inhibitor of the MET receptor. Herein, we describe AMG 337 preclinical activity and mechanism of action in MET-dependent tumor models. These studies suggest MET is the only therapeutic target for AMG 337. In an unbiased tumor cell line proliferation screen (260 cell lines), a closely related analogue of AMG 337, Compound 5, exhibited activity in 2 of 260 cell lines; both were MET-amplified. Additional studies examining the effects of AMG 337 on the proliferation of a limited panel of cell lines with varying MET copy numbers revealed that high-level focal MET amplification (>12 copies) was required to confer MET oncogene addiction and AMG 337 sensitivity. One MET-amplified cell line, H1573 (>12 copies), was AMG 337 insensitive, possibly because of a downstream G12A KRAS mutation. Mechanism-of-action studies in sensitive MET-amplified cell lines demonstrated that AMG 337 inhibited MET and adaptor protein Gab-1 phosphorylation, subsequently blocking the downstream PI3K and MAPK pathways. AMG 337 exhibited potency in pharmacodynamic assays evaluating MET signaling in tumor xenograft models; >90% inhibition of Gab-1 phosphorylation was observed at 0.75 mg/kg. These findings describe the preclinical activity and mechanism of action of AMG 337 in MET-dependent tumor models and indicate its potential as a novel therapeutic for the treatment of MET-dependent tumors. Mol Cancer Ther; 15(7); 1568–79. ©2016 AACR.

Published

2015

19. The mouse kinome: Discovery and comparative genomics of all mouse protein kinases

Author

Sean Caenepeel, Glen Charydczak, Gerard Manning, Tony Hunter, and Sucha Sudarsanam

Subjects

Retroelements, Pseudogene, MAPK7, MAP2K2, Mouse Protein, Biology, Evolution, Molecular, Mice, Species Specificity, MAP2K1, Animals, Humans, Kinome, MAPK1, Conserved Sequence, Genetics, Comparative genomics, Multidisciplinary, Base Sequence, Chromosome Mapping, Genomics, Biological Sciences, Phenotype, Mutation, Databases, Nucleic Acid, Protein Kinases

Abstract

We have determined the full protein kinase (PK) complement (kinome) of mouse. This set of 540 genes includes many novel kinases and corrections or extensions to >150 published sequences. The mouse has orthologs for 510 of the 518 human PKs. Nonorthologous kinases arise only by retrotransposition and gene decay. Orthologous kinase pairs vary in sequence conservation along their length, creating a map of functionally important regions for every kinase pair. Many species-specific sequence inserts exist and are frequently alternatively spliced, allowing for the creation of evolutionary lineage-specific functions. Ninety-seven kinase pseudogenes were found, all distinct from the 107 human kinase pseudogenes. Chromosomal mapping links 163 kinases to mutant phenotypes and unlocks the use of mouse genetics to determine functions of orthologous human kinases.

Published

2004

20. Identifying the determinants of response to MDM2 inhibition

Author

Michael Boedigheimer, Sean Caenepeel, Jonathan D. Oliner, Anne Y. Saiki, Cheng Su, and Elissa Cosgrove

Subjects

Genetics, Gene Amplification, Proto-Oncogene Proteins c-mdm2, Mutant cell, Biology, P53 Mutation, amplification, 3. Good health, Oncology, MDM2, Cell Line, Tumor, Neoplasms, Mutational status, Humans, TP53, Tumor Suppressor Protein p53, neoplasms, Cell Proliferation, Research Paper

Abstract

// Anne Y. Saiki 1 , Sean Caenepeel 1 , Elissa Cosgrove 2, 5 , Cheng Su 3 , Michael Boedigheimer 4 , Jonathan D. Oliner 1 1 Oncology Research, Amgen, Inc., Thousand Oaks, California, USA 2 Genome Analysis Unit, Amgen, Inc., South San Francisco, California, USA 3 Biostatistics, Amgen, Inc., Seattle, Washington, USA 4 Molecular Sciences, Amgen, Inc., Thousand Oaks, California, USA 5 Department of Molecular Biology and Genetics, Cornell University, Ithaca, New York, USA Correspondence to: Jonathan D. Oliner, e-mail: jonoliner@hotmail.com Keywords: TP53 , MDM2 , amplification Received: October 28, 2014 Accepted: January 08, 2015 Published: February 03, 2015 ABSTRACT Previous reports have provided evidence that p53 mutation is a strong negative predictor of response to MDM2 inhibitors. However, this correlation is not absolute, as many p53 Mutant cell lines have been reported to respond to MDM2 inhibition, while many p53 WT cell lines have been shown not to respond. To better understand the nature of these exceptions, we screened a panel of 260 cell lines and noted similar discrepancies. However, upon extensive curation of this panel, these apparent exceptions could be eliminated, revealing a perfect correlation between p53 mutational status and MDM2 inhibitor responsiveness. It has been suggested that the MDM2 -amplified subset of p53 WT tumors might be particularly sensitive to MDM2 inhibition. To facilitate clinical testing of this hypothesis, we identified a rationally derived copy number cutoff for assignment of functionally relevant MDM2 amplification. Applying this cutoff resulted in a pan-cancer MDM2 amplification rate far lower than previously published.

Published

2014

21. Discovery and optimization of a series of benzothiazole phosphoinositide 3-kinase (PI3K)/mammalian target of rapamycin (mTOR) dual inhibitors

Author

Yang Xu, Leeanne Zalameda, Raju Subramanian, Erin L. Mullady, Michael Schrag, Kevin Yang, Daniel J. Freeman, Jian Jiang, Longbin Liu, Tian Wu, Derin C. D'amico, John D. McCarter, Noel D'angelo, Sean Caenepeel, Peter Yakowec, Ling Wang, Mark H. Norman, Robert C. Wahl, Tisha San Miguel, Jin Tang, Douglas A. Whittington, Paul E. Hughes, Shon Booker, Ning Xi, Tae-Seong Kim, Kui Chen, Nancy Zhang, and Kristin L. Andrews

Subjects

Models, Molecular, Transplantation, Heterologous, Biological Availability, Mice, Nude, Antineoplastic Agents, Crystallography, X-Ray, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Animals, Humans, Benzothiazoles, Phosphorylation, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Sulfonamides, Phosphoinositide 3-kinase, Binding Sites, biology, Drug discovery, Chemistry, Kinase, TOR Serine-Threonine Kinases, In vitro, Rats, Transplantation, Biochemistry, Benzothiazole, Liver, biology.protein, Molecular Medicine, Female, Drug Screening Assays, Antitumor, Proto-Oncogene Proteins c-akt, Neoplasm Transplantation

Abstract

Phosphoinositide 3-kinase α (PI3Kα) is a lipid kinase that plays a key regulatory role in several cellular processes. The mutation or amplification of this kinase in humans has been implicated in the growth of multiple tumor types. Consequently, PI3Kα has become a target of intense research for drug discovery. Our studies began with the identification of benzothiazole compound 1 from a high throughput screen. Extensive SAR studies led to the discovery of sulfonamide 45 as an early lead, based on its in vitro cellular potency. Subsequent modifications of the central pyrimidine ring dramatically improved enzyme and cellular potency and led to the identification of chloropyridine 70. Further arylsulfonamide SAR studies optimized in vitro clearance and led to the identification of 82 as a potent dual inhibitor of PI3K and mTOR. This molecule exhibited potent enzyme and cell activity, low clearance, and high oral bioavailability. In addition, compound 82 demonstrated tumor growth inhibition in U-87 MG, A549, and HCT116 tumor xenograft models.

Published

2011

22. Motesanib inhibits Kit mutations associated with gastrointestinal stromal tumors

Author

Anthony Polverino, Todd Juan, Paul E. Hughes, Angelo Baher, Raffi Manoukian, Sean Caenepeel, Will Baron, Andrew Tasker, Lisa Renshaw-Gegg, and Tammy L. Bush

Subjects

Niacinamide, Cancer Research, Indoles, Gastrointestinal Stromal Tumors, Blotting, Western, Oligonucleotides, CHO Cells, lcsh:RC254-282, Receptor tyrosine kinase, Mice, chemistry.chemical_compound, Cricetulus, Growth factor receptor, Cricetinae, medicine, Motesanib, Animals, Humans, Phosphorylation, Cell Proliferation, biology, Cell growth, Research, Autophosphorylation, Imatinib, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Mice, Inbred C57BL, Proto-Oncogene Proteins c-kit, Oncology, chemistry, Mutation, biology.protein, Cancer research, Female, Platelet-derived growth factor receptor, medicine.drug

Abstract

Background Activating mutations in Kit receptor tyrosine kinase or the related platelet-derived growth factor receptor (PDGFR) play an important role in the pathogenesis of gastrointestinal stromal tumors (GIST). Methods This study investigated the activity of motesanib, an inhibitor of vascular endothelial growth factor receptors (VEGFR) 1, 2, and 3; PDGFR; and Kit, against primary activating Kit mutants and mutants associated with secondary resistance to imatinib. Single- and double-mutant isoforms of Kit were evaluated for their sensitivity to motesanib or imatinib in autophosphorylation assays and in Ba/F3 cell proliferation assays. Results Motesanib inhibited Kit autophosphorylation in CHO cell lines expressing primary activating mutations in exon 9 (AYins503-504, IC50 = 18 nM) and exon 11 (V560 D, IC50 = 5 nM; Δ552-559, IC50 = 1 nM). Motesanib also demonstrated activity against kinase domain mutations conferring imatinib resistance (V560D/V654A, IC50 = 77 nM; V560D/T670I, IC50 = 277 nM; Y823 D, IC50 = 64 nM) but failed to inhibit the imatinib-resistant D816V mutant (IC50 > 3000 nM). Motesanib suppressed the proliferation of Ba/F3 cells expressing Kit mutants with IC50 values in good agreement with those observed in the autophosphorylation assays. Conclusions In conclusion, our data suggest that motesanib possesses inhibitory activity against primary Kit mutations and some imatinib-resistant secondary mutations.

Published

2010

23. The DNA sequence and biology of human chromosome 19

Author

Mary Bao Tran-Gyamfi, Ivan Ovcharenko, Trevor Hawkins, Maria Gomez, Mirian Denys, Victor V. Solovyev, Terrence S. Furey, Jamie Jett, Jeremy Schmutz, Dea Fotopulos, David Gordon, Tom Slezak, Kevin Wu, Heather Kimball, Pieter J. deJong, Catherine Medina, Vladimer Larionov, Paula McCready, Stephanine Rogers, James Retterer, John C. Detter, Diego Martinez, Richard M. Myers, Paul Predki, Stacey Black, Eva Bajorek, Chenier Caoile, Alex Rodriguez, Isaac Ho, Arthur Kobayashi, Jane Lamerdin, Xinwei She, Yunian Lou, Jane Grimwood, Kristen Kadner, Alex Copeland, Wayne Huang, Sanjay Israni, Carmen Rosa Albacete García, Gary Xie, Doug Smith, Anthony V. Carrano, Matthew Groza, Catherine A. Cleland, Matt Nolan, Paul G. Richardson, Eidelyn Gonzales, Nina Thayer, Anna Ustaszewska, Eileen Dalin, Olivier Couronne, Evan E. Eichler, Tijana Glavina, Astrid Terry, Sun-Hee Leem, Steve Lowry, Anne S. Olsen, Lucía Ramírez, Ming Tsai, Stephanie Malfatti, Hope Tice, Uffe Hellsten, David Goodstein, Martin Pollard, Daniel S. Rokhsar, Nancy Hammon, Angelica Salazar, Jenna Morgan, Yee Man Chan, Michael R. Altherr, Paramvir S. Dehal, Nu Vo, Linda K. Ashworth, Elbert Branscomb, Laurie Gordon, Julio Escobar, Anthony P. Popkie, Dave Flowers, Anca M. Georgescu, Len A. Pennacchio, Sam Pitluck, Sam Rash, Edward M. Rubin, Sean Caenepeel, Glenda Quan, Asaf Salamov, Inna Dubchak, Lisa Stubbs, Andrea Aerts, Mark Dickson, Kathryn Nelson, Mari Christensen, Lauren Haydu, Frederick Lopez, Mark C. Wagner, Jeremy Wheeler, Joan Yang, and Susan Lucas

Subjects

Genetics, Medical, Molecular Sequence Data, Biology, Evolution, Molecular, Chromosome 15, Mice, Chromosome 16, Chromosome 19, Gene Duplication, Animals, Humans, Conserved Sequence, Genetics, Base Composition, Multidisciplinary, Sequence Analysis, DNA, Physical Chromosome Mapping, Chromosome 17 (human), Alternative Splicing, Chromosome 4, Chromosome 3, Genes, Multigene Family, CpG Islands, Chromosome 21, Chromosome 22, Chromosomes, Human, Pair 19, Pseudogenes

Abstract

Chromosome 19 has the highest gene density of all human chromosomes, more than double the genome-wide average. The large clustered gene families, corresponding high G + C content, CpG islands and density of repetitive DNA indicate a chromosome rich in biological and evolutionary significance. Here we describe 55.8 million base pairs of highly accurate finished sequence representing 99.9% of the euchromatin portion of the chromosome. Manual curation of gene loci reveals 1,461 protein-coding genes and 321 pseudogenes. Among these are genes directly implicated in mendelian disorders, including familial hypercholesterolaemia and insulin-resistant diabetes. Nearly one-quarter of these genes belong to tandemly arranged families, encompassing more than 25% of the chromosome. Comparative analyses show a fascinating picture of conservation and divergence, revealing large blocks of gene orthology with rodents, scattered regions with more recent gene family expansions and deletions, and segments of coding and non-coding conservation with the distant fish species Takifugu.

Published

2003