Your search keyword '"Wise, Scott C."' showing total 111 results

1. Phase 1 dose-finding study of rebastinib (DCC-2036) in patients with relapsed chronic myeloid leukemia and acute myeloid leukemia

Author

Cortes, Jorge, Talpaz, Moshe, Smith, Hedy P, Snyder, David S, Khoury, Jean, Bhalla, Kapil N, Pinilla-Ibarz, Javier, Larson, Richard, Mitchell, David, Wise, Scott C, Rutkoski, Thomas J, Smith, Bryan D, Flynn, Daniel L, Kantarjian, Hagop M, Rosen, Oliver, and Van Etten, Richard A

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Pediatric, Rare Diseases, Patient Safety, Hematology, Cancer, Neurosciences, Pediatric Cancer, Childhood Leukemia, Clinical Research, 6.2 Cellular and gene therapies, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Adult, Aged, Aged, 80 and over, Drug Monitoring, Drug Resistance, Neoplasm, Female, Fusion Proteins, bcr-abl, Humans, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Leukemia, Myeloid, Acute, Male, Maximum Tolerated Dose, Middle Aged, Mutation, Protein Kinase Inhibitors, Quinolines, Treatment Outcome, Young Adult, Cardiorespiratory Medicine and Haematology, Immunology, Cardiovascular medicine and haematology

Abstract

A vailable tyrosine kinase inhibitors for chronic myeloid leukemia bind in an adenosine 5'-triphosphate-binding pocket and are affected by evolving mutations that confer resistance. Rebastinib was identified as a switch control inhibitor of BCR-ABL1 and FLT3 and may be active against resistant mutations. A Phase 1, first-in-human, single-agent study investigated rebastinib in relapsed or refractory chronic or acute myeloid leukemia. The primary objectives were to investigate the safety of rebastinib and establish the maximum tolerated dose and recommended Phase 2 dose. Fifty-seven patients received treatment with rebastinib. Sixteen patients were treated using powder-in-capsule preparations at doses from 57 mg to 1200 mg daily, and 41 received tablet preparations at doses of 100 mg to 400 mg daily. Dose-limiting toxicities were dysarthria, muscle weakness, and peripheral neuropathy. The maximum tolerated dose was 150 mg tablets administered twice daily. Rebastinib was rapidly absorbed. Bioavailability was 3- to 4-fold greater with formulated tablets compared to unformulated capsules. Eight complete hematologic responses were achieved in 40 evaluable chronic myeloid leukemia patients, 4 of which had a T315I mutation. None of the 5 patients with acute myeloid leukemia responded. Pharmacodynamic analysis showed inhibition of phosphorylation of substrates of BCR-ABL1 or FLT3 by rebastinib. Although clinical activity was observed, clinical benefit was insufficient to justify continued development in chronic or acute myeloid leukemia. Pharmacodynamic analyses suggest that other kinases inhibited by rebastinib, such as TIE2, may be more relevant targets for the clinical development of rebastinib (clinicaltrials.gov Identifier:00827138).

Published

2017

2. 1455 Characterization of gene expression signatures of tumor immunogenicity and cellular proliferation from murine cancer models grownin vitroandin vivo

Author

Strickland, Kyle C, primary, Barnes, Sheri, additional, Wallen, Zachary D, additional, Nesline, Mary K, additional, Jensen, Taylor J, additional, Caveney, Brian, additional, Eisenberg, Marcia, additional, Reddy, Prasanth, additional, Severson, Eric A, additional, Wise, Scott C, additional, and Ramkissoon, Shakti, additional

Published

2023

3. Conformational control inhibition of the BCR-ABL1 tyrosine kinase, including the gatekeeper T315I mutant, by the switch-control inhibitor DCC-2036.

Author

Chan, Wayne W, Wise, Scott C, Kaufman, Michael D, Ahn, Yu Mi, Ensinger, Carol L, Haack, Torsten, Hood, Molly M, Jones, Jennifer, Lord, John W, Lu, Wei Ping, Miller, David, Patt, William C, Smith, Bryan D, Petillo, Peter A, Rutkoski, Thomas J, Telikepalli, Hanumaiah, Vogeti, Lakshminarayana, Yao, Tony, Chun, Lawrence, Clark, Robin, Evangelista, Peter, Gavrilescu, L Cristina, Lazarides, Katherine, Zaleskas, Virginia M, Stewart, Lance J, Van Etten, Richard A, and Flynn, Daniel L

Subjects

Animals, Cell Line, Tumor, Cell Proliferation: drug effects, Cell Survival: drug effects, Drug Design, Fusion Proteins, bcr-abl: antagonists & inhibitors, chemistry, Humans, Leukemia, Myelogenous, Chronic, BCR-ABL Positive: drug therapy, Male, Mice, Mice, Inbred BALB C, Mutation, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma: drug therapy, Protein Conformation, Protein Kinase Inhibitors: pharmacology, Protein-Tyrosine Kinases: antagonists & inhibitors, chemistry

Abstract

Acquired resistance to ABL1 tyrosine kinase inhibitors (TKIs) through ABL1 kinase domain mutations, particularly the gatekeeper mutant T315I, is a significant problem for patients with chronic myeloid leukemia (CML). Using structure-based drug design, we developed compounds that bind to residues (Arg386/Glu282) ABL1 uses to switch between inactive and active conformations. The lead "switch-control" inhibitor, DCC-2036, potently inhibits both unphosphorylated and phosphorylated ABL1 by inducing a type II inactive conformation, and retains efficacy against the majority of clinically relevant CML-resistance mutants, including T315I. DCC-2036 inhibits BCR-ABL1(T315I)-expressing cell lines, prolongs survival in mouse models of T315I mutant CML and B-lymphoblastic leukemia, and inhibits primary patient leukemia cells expressing T315I in vitro and in vivo, supporting its clinical development in TKI-resistant Ph(+) leukemia.

Published

2011

4. Supplementary File from The Selective Tie2 Inhibitor Rebastinib Blocks Recruitment and Function of Tie2Hi Macrophages in Breast Cancer and Pancreatic Neuroendocrine Tumors

Author

Harney, Allison S., primary, Karagiannis, George S., primary, Pignatelli, Jeanine, primary, Smith, Bryan D., primary, Kadioglu, Ece, primary, Wise, Scott C., primary, Hood, Molly M., primary, Kaufman, Michael D., primary, Leary, Cynthia B., primary, Lu, Wei-Ping, primary, Al-Ani, Gada, primary, Chen, Xiaoming, primary, Entenberg, David, primary, Oktay, Maja H., primary, Wang, Yarong, primary, Chun, Lawrence, primary, De Palma, Michele, primary, Jones, Joan G., primary, Flynn, Daniel L., primary, and Condeelis, John S., primary

Published

2023

5. Data from The Selective Tie2 Inhibitor Rebastinib Blocks Recruitment and Function of Tie2Hi Macrophages in Breast Cancer and Pancreatic Neuroendocrine Tumors

Author

Harney, Allison S., primary, Karagiannis, George S., primary, Pignatelli, Jeanine, primary, Smith, Bryan D., primary, Kadioglu, Ece, primary, Wise, Scott C., primary, Hood, Molly M., primary, Kaufman, Michael D., primary, Leary, Cynthia B., primary, Lu, Wei-Ping, primary, Al-Ani, Gada, primary, Chen, Xiaoming, primary, Entenberg, David, primary, Oktay, Maja H., primary, Wang, Yarong, primary, Chun, Lawrence, primary, De Palma, Michele, primary, Jones, Joan G., primary, Flynn, Daniel L., primary, and Condeelis, John S., primary

Published

2023

6. Supplementary Materials and Methods, Supplementary Tables 1 through 4, and Supplementary Figures 1 through 9 from Altiratinib Inhibits Tumor Growth, Invasion, Angiogenesis, and Microenvironment-Mediated Drug Resistance via Balanced Inhibition of MET, TIE2, and VEGFR2

Author

Smith, Bryan D., primary, Kaufman, Michael D., primary, Leary, Cynthia B., primary, Turner, Benjamin A., primary, Wise, Scott C., primary, Ahn, Yu Mi, primary, Booth, R. John, primary, Caldwell, Timothy M., primary, Ensinger, Carol L., primary, Hood, Molly M., primary, Lu, Wei-Ping, primary, Patt, Tristan W., primary, Patt, William C., primary, Rutkoski, Thomas J., primary, Samarakoon, Thiwanka, primary, Telikepalli, Hanumaiah, primary, Vogeti, Lakshminarayana, primary, Vogeti, Subha, primary, Yates, Karen M., primary, Chun, Lawrence, primary, Stewart, Lance J., primary, Clare, Michael, primary, and Flynn, Daniel L., primary

Published

2023

7. Data from The ABL Switch Control Inhibitor DCC-2036 Is Active against the Chronic Myeloid Leukemia Mutant BCR-ABLT315I and Exhibits a Narrow Resistance Profile

Author

Eide, Christopher A., primary, Adrian, Lauren T., primary, Tyner, Jeffrey W., primary, Mac Partlin, Mary, primary, Anderson, David J., primary, Wise, Scott C., primary, Smith, Bryan D., primary, Petillo, Peter A., primary, Flynn, Daniel L., primary, Deininger, Michael W.N., primary, O'Hare, Thomas, primary, and Druker, Brian J., primary

Published

2023

8. Supplementary Tables 1-4, Figure 1 from The ABL Switch Control Inhibitor DCC-2036 Is Active against the Chronic Myeloid Leukemia Mutant BCR-ABLT315I and Exhibits a Narrow Resistance Profile

Author

Eide, Christopher A., primary, Adrian, Lauren T., primary, Tyner, Jeffrey W., primary, Mac Partlin, Mary, primary, Anderson, David J., primary, Wise, Scott C., primary, Smith, Bryan D., primary, Petillo, Peter A., primary, Flynn, Daniel L., primary, Deininger, Michael W.N., primary, O'Hare, Thomas, primary, and Druker, Brian J., primary

Published

2023

9. Discovery of vimseltinib (DCC-3014), a highly selective CSF1R switch-control kinase inhibitor, in clinical development for the treatment of Tenosynovial Giant Cell Tumor (TGCT)

Author

Caldwell, Timothy M., primary, Ahn, Yu Mi, additional, Bulfer, Stacie L., additional, Leary, Cynthia B., additional, Hood, Molly M., additional, Lu, Wei-Ping, additional, Vogeti, Lakshminarayana, additional, Vogeti, Subha, additional, Kaufman, Michael D., additional, Wise, Scott C., additional, Le Bourdonnec, Bertrand, additional, Smith, Bryan D., additional, and Flynn, Daniel L., additional

Published

2022

10. Discovery of acyl ureas as highly selective small molecule CSF1R kinase inhibitors

Author

Caldwell, Timothy M., primary, Kaufman, Michael D., additional, Wise, Scott C., additional, Mi Ahn, Yu, additional, Hood, Molly M., additional, Lu, Wei-Ping, additional, Patt, William C., additional, Samarakoon, Thiwanka, additional, Vogeti, Lakshminarayana, additional, Vogeti, Subha, additional, Yates, Karen M., additional, Bulfer, Stacie L., additional, Le Bourdonnec, Bertrand, additional, Smith, Bryan D., additional, and Flynn, Daniel L., additional

Published

2022

11. Foraging Behavior of Matamata Turtles: The Effects of Prey Density and the Presence of a Conspecific

Author

Formanowicz,, Daniel R., Brodie,, Edmund D., and Wise, Scott C.

Published

1989

12. Vimseltinib: A Precision CSF1R Therapy for Tenosynovial Giant Cell Tumors and Diseases Promoted by Macrophages

Author

Smith, Bryan D., primary, Kaufman, Michael D., additional, Wise, Scott C., additional, Ahn, Yu Mi, additional, Caldwell, Timothy M., additional, Leary, Cynthia B., additional, Lu, Wei-Ping, additional, Tan, Gege, additional, Vogeti, Lakshminarayana, additional, Vogeti, Subha, additional, Wilky, Breelyn A., additional, Davis, Lara E., additional, Sharma, Maitreyi, additional, Ruiz-Soto, Rodrigo, additional, and Flynn, Daniel L., additional

Published

2021

13. cJun overexpression in MCF-7 breast cancer cells produces a tumorigenic, invasive and hormone resistant phenotype

Author

Smith, Leia M, Wise, Scott C, Hendricks, Denver T, Sabichi, Anita L, Bos, Timothy, Reddy, Praveen, Brown, Powel H, and Birrer, Michael J

Published

1999

14. Identification of domains of c-Jun mediating androgen receptor transactivation

Author

Wise, Scott C, Burmeister, Lori A, Zhou, Xiao-feng, Bubulya, Athanasios, Oberfield, Jennifer L, Birrer, Michael J, and Shemshedini, Lirim

Published

1998

15. Matamata Turtles Ambush but Do Not Herd Prey

Author

Wise, Scott C., Formanowicz,, Daniel R., and Brodie,, Edmund D.

Published

1989

16. Differential Activation of Peroxisome Proliferator-Activated Receptor-γ by Troglitazone and Rosiglitazone

Author

Camp, Heidi S., Li, Ou, Wise, Scott C., Hong, Yu H., Frankowski, Christy L., Shen, Xi-qiang, Vanbogelen, Ruth, and Leff, Todd

Published

2000

17. Troglitazone, an Antidiabetic Agent, Inhibits Cholesterol Biosynthesis Through a Mechanism Independent of Peroxisome Proliferator-Activated Receptor-gamma

Author

Wang, Mingham, Wise, Scott C., Leff, Todd, and Su, Ti-Zhi

Published

1999

18. Ripretinib (DCC-2618) Is a Switch Control Kinase Inhibitor of a Broad Spectrum of Oncogenic and Drug-Resistant KIT and PDGFRA Variants

Author

Smith, Bryan D., primary, Kaufman, Michael D., additional, Lu, Wei-Ping, additional, Gupta, Anu, additional, Leary, Cynthia B., additional, Wise, Scott C., additional, Rutkoski, Thomas J., additional, Ahn, Yu Mi, additional, Al-Ani, Gada, additional, Bulfer, Stacie L., additional, Caldwell, Timothy M., additional, Chun, Lawrence, additional, Ensinger, Carol L., additional, Hood, Molly M., additional, McKinley, Arin, additional, Patt, William C., additional, Ruiz-Soto, Rodrigo, additional, Su, Ying, additional, Telikepalli, Hanumaiah, additional, Town, Ajia, additional, Turner, Benjamin A., additional, Vogeti, Lakshminarayana, additional, Vogeti, Subha, additional, Yates, Karen, additional, Janku, Filip, additional, Abdul Razak, Albiruni Ryan, additional, Rosen, Oliver, additional, Heinrich, Michael C., additional, and Flynn, Daniel L., additional

Published

2019

19. A suspected delayed hemolytic transfusion reaction mediated by anti-Joa

Author

Jajosky, Ryan P., Lumm, Wendy C., Wise, Scott C., Bollag, Roni J., and Shikle, James F.

Subjects

Medical Laboratory Technology

Published

2019

20. Abstract 5667: High-throughput analysis of MAPK and JAK-STAT signaling in CT26 tumors using a combination of immunophenotyping and phospho-flow cytometry

Author

Draper, David, primary, Wong, Alden, additional, Lapinski, Philip, additional, Barnes, Sheri R., additional, Franklin, Maryland Rosenfeld, additional, and Wise, Scott C., additional

Published

2018

21. The Selective Tie2 Inhibitor Rebastinib Blocks Recruitment and Function of Tie2Hi Macrophages in Breast Cancer and Pancreatic Neuroendocrine Tumors

Author

Harney, Allison S., primary, Karagiannis, George S., additional, Pignatelli, Jeanine, additional, Smith, Bryan D., additional, Kadioglu, Ece, additional, Wise, Scott C., additional, Hood, Molly M., additional, Kaufman, Michael D., additional, Leary, Cynthia B., additional, Lu, Wei-Ping, additional, Al-Ani, Gada, additional, Chen, Xiaoming, additional, Entenberg, David, additional, Oktay, Maja H., additional, Wang, Yarong, additional, Chun, Lawrence, additional, De Palma, Michele, additional, Jones, Joan G., additional, Flynn, Daniel L., additional, and Condeelis, John S., additional

Published

2017

22. Abstract 5624: Characterization of proliferation in multiple T-cell subsets in the CT26 murine colon carcinoma model by multi-color flow cytometry

Author

Thayer, Matt, primary, Wong, Alden, additional, Draper, David, additional, Saims, Dan, additional, and Wise, Scott C., additional

Published

2017

23. Abstract 1668: Comprehensive 10 color flow cytometry analysis of the neuroblastoma intratumoral immune response using the murine syngeneic neuro-2a tumor model

Author

Draper, David D., primary, Thayer, Matt, additional, Wong, Alden, additional, Saims, Dan, additional, and Wise, Scott C., additional

Published

2017

24. Phase 1 dose-finding study of rebastinib (DCC-2036) in patients with relapsed chronic myeloid leukemia and acute myeloid leukemia

Author

Cortes, Jorge, primary, Talpaz, Moshe, additional, Smith, Hedy P., additional, Snyder, David S., additional, Khoury, Jean, additional, Bhalla, Kapil N., additional, Pinilla-Ibarz, Javier, additional, Larson, Richard, additional, Mitchell, David, additional, Wise, Scott C., additional, Rutkoski, Thomas J., additional, Smith, Bryan D., additional, Flynn, Daniel L., additional, Kantarjian, Hagop M., additional, Rosen, Oliver, additional, and Van Etten, Richard A., additional

Published

2016

25. Abstract 3242: In depth myeloid cell characterization in the murine syngeneic CT26 colon carcinoma model by 10 color flow cytometry

Author

Thayer, Matt, primary, Draper, David, additional, Saims, Daniel, additional, Rosenfeld-Franklin, Maryland, additional, and Wise, Scott C., additional

Published

2016

26. Differential Activation of Peroxisome Proliferator-Activated Receptor-[Gamma] by Troglitazone and Rosiglitazone

Author

Camp, Heidi S., Li, Ou, Wise, Scott C., Hong, Yu H., Frankowski, Christy L., Shen, Xi-qiang, Vanbogelen, Ruth, and Leff, Todd

Subjects

Avandia (Medication) -- Physiological aspects, Troglitazone -- Physiological aspects, Hypoglycemic agents -- Physiological aspects, Thiazolidinediones -- Physiological aspects, Type 2 diabetes -- Drug therapy, Health, Drug therapy, Physiological aspects

Abstract

The antidiabetic thiazolidinediones, which include troglitazone and rosiglitazone, are ligands for the nuclear receptor peroxisome proliferator-activated receptor (PPAR)-[Gamma] and exert their antihyperglycemic effects by regulation of PPAR-[Gamma]-responsive genes. We report [...]

Published

2000

27. Altiratinib Inhibits Tumor Growth, Invasion, Angiogenesis, and Microenvironment-Mediated Drug Resistance via Balanced Inhibition of MET, TIE2, and VEGFR2

Author

Smith, Bryan D., primary, Kaufman, Michael D., additional, Leary, Cynthia B., additional, Turner, Benjamin A., additional, Wise, Scott C., additional, Ahn, Yu Mi, additional, Booth, R. John, additional, Caldwell, Timothy M., additional, Ensinger, Carol L., additional, Hood, Molly M., additional, Lu, Wei-Ping, additional, Patt, Tristan W., additional, Patt, William C., additional, Rutkoski, Thomas J., additional, Samarakoon, Thiwanka, additional, Telikepalli, Hanumaiah, additional, Vogeti, Lakshminarayana, additional, Vogeti, Subha, additional, Yates, Karen M., additional, Chun, Lawrence, additional, Stewart, Lance J., additional, Clare, Michael, additional, and Flynn, Daniel L., additional

Published

2015

28. Abstract 2690: DCC-2618 is a potent inhibitor of wild-type and mutant KIT, including refractory Exon 17 D816 KIT mutations, and exhibits efficacy in refractory GIST and AML xenograft models

Author

Smith, Bryan D., primary, Hood, Molly M., additional, Wise, Scott C., additional, Kaufman, Michael D., additional, Lu, Wei-Ping, additional, Rutkoski, Thomas, additional, Flynn, Daniel L., additional, and Heinrich, Michael C., additional

Published

2015

29. Abstract 790: Altiratinib is a potent inhibitor of TRK kinases and is efficacious in TRK-fusion driven cancer models

Author

Smith, Bryan D., primary, Leary, Cynthia B., additional, Turner, Benjamin A., additional, Kaufman, Michael D., additional, Wise, Scott C., additional, Garcia-Rendueles, Maria E. R., additional, Fagin, James A., additional, and Flynn, Daniel L., additional

Published

2015

30. Discovery of 1-(3,3-Dimethylbutyl)-3-(2-fluoro-4-methyl-5-(7-methyl-2-(methylamino)pyrido[2,3-d]pyrimidin-6-yl)phenyl)urea (LY3009120) as a Pan-RAF Inhibitor with Minimal Paradoxical Activation and Activity against BRAF or RAS Mutant Tumor Cells

Author

Henry, James R., primary, Kaufman, Michael D., additional, Peng, Sheng-Bin, additional, Ahn, Yu Mi, additional, Caldwell, Timothy M., additional, Vogeti, Lakshminarayana, additional, Telikepalli, Hanumaiah, additional, Lu, Wei-Ping, additional, Hood, Molly M., additional, Rutkoski, Thomas J., additional, Smith, Bryan D., additional, Vogeti, Subha, additional, Miller, David, additional, Wise, Scott C., additional, Chun, Lawrence, additional, Zhang, Xiaoyi, additional, Zhang, Youyan, additional, Kays, Lisa, additional, Hipskind, Philip A., additional, Wrobleski, Aaron D., additional, Lobb, Karen L., additional, Clay, Julia M., additional, Cohen, Jeffrey D., additional, Walgren, Jennie L., additional, McCann, Denis, additional, Patel, Phenil, additional, Clawson, David K., additional, Guo, Sherry, additional, Manglicmot, Danalyn, additional, Groshong, Chris, additional, Logan, Cheyenne, additional, Starling, James J., additional, and Flynn, Daniel L., additional

Published

2015

31. Abstract PR01: Rebastinib, a selective TIE2 kinase inhibitor, decreases TIE2-expressing macrophages, reduces metastasis, and increases survival in murine cancer models

Author

Flynn, Daniel L., primary, Kaufman, Michael D., additional, Leary, Cynthia B., additional, Hood, Molly M., additional, Lu, Wei-Ping, additional, Turner, Benjamin A., additional, Wise, Scott C., additional, Rudoltz, Marc S., additional, and Smith, Bryan D., additional

Published

2015

32. Abstract A53: The specific FMS kinase inhibitor, DCC-3014, durably inhibits FMS kinase in vivo and blocks cancer bone invasiveness

Author

Smith, Bryan D., primary, Kaufman, Michael D., additional, Leary, Cynthia B., additional, Hood, Molly M., additional, Lu, Wei-Ping, additional, Turner, Benjamin A., additional, Vogeti, Subha, additional, Wise, Scott C., additional, and Flynn, Daniel L., additional

Published

2015

33. Switch control pocket inhibitors of p38-MAP kinase. Durable type II inhibitors that do not require binding into the canonical ATP hinge region

Author

Ahn, Yu Mi, Clare, Michael, Ensinger, Carol L., Hood, Molly M., Lord, John W., Lu, Wei-Ping, Miller, David F., Patt, William C., Smith, Bryan D., Vogeti, Lakshminarayana, Kaufman, Michael D., Petillo, Peter A., Wise, Scott C., Abendroth, Jan, Chun, Lawrence, Clark, Robin, Feese, Michael, Kim, Hidong, Stewart, Lance, and Flynn, Daniel L.

Published

2010

34. Simultaneous Screening of Multiple Bacterial tRNA Synthetases Using an Escherichia coli S30-Based Transcription and Translation Assay

Author

Dermyer, Michael, Wise, Scott C., Braden, Timothy, Holler, Tod P., Dermyer, Michael, Wise, Scott C., Braden, Timothy, and Holler, Tod P.

Abstract

The search for novel antibiotics to combat the growing threat of resistance has led researchers to screen libraries with coupled transcription and translation systems. In these systems, a bacterial cell lysate supplies the proteins necessary for transcription and translation, a plasmid encoding a reporter protein is added as a template, and a complex mixture of amino acids and cofactors is added to supply building blocks and energy to the assay. Firefly luciferase is typically used as the reporter protein in high-throughput screens because the luminescent signal is strong and, since bacterial lysates contain no luciferase, the background is negligible. The typical coupled transcription and translation assay is sensitive to inhibitors of RNA polymerase and to compounds that bind tightly to the ribosome. We have found a way to increase the information content of the screen by making the assay more sensitive to inhibitors of tRNA synthetases. Restricting the concentration of amino acids added to the reaction mixture allows the simultaneous screening of multiple tRNA synthetase enzymes along with the classic transcription and translation targets. In addition, this assay can be used as a convenient way to determine if an antibacterial compound of unknown mechanism inhibits translation through inhibition of a tRNA synthetase, and to identify which synthetase is the target.

Published

2009

35. Abstract B145: Use of μCT imaging in the PyMT breast cancer model to monitor lung metastasis development and determine therapeutic benefit in real time.

Author

Meade, Mary Anne, primary, Balagurunathan, Deepa, additional, Bull, Chris, additional, Lister, Deanne, additional, Trachet, Erin, additional, Smith, Bryan, additional, Flynn, Daniel, additional, and Wise, Scott C., additional

Published

2013

36. Abstract B78: Rebastinib, a small molecule TIE2 kinase inhibitor, prevents primary tumor growth and lung metastasis in the PyMT breast cancer model

Author

Smith, Bryan D., primary, Hood, Molly M., additional, Kaufman, Michael D., additional, Berger, Mark, additional, Flynn, Daniel L., additional, and Wise, Scott C., additional

Published

2013

37. A Phase 1 Study of DCC-2036, a Novel Oral Inhibitor of BCR-ABL Kinase, in Patients with Philadelphia Chromosome Positive (Ph+) Leukemias Including Patients with T315I Mutation

Author

Cortes, Jorge E., primary, Talpaz, Moshe, additional, Kantarjian, Hagop M, additional, Smith, Hedy, additional, Bixby, Dale, additional, Rafferty, Usha, additional, Berger, Mark S., additional, Wise, Scott C., additional, Rutkoski, Tom J., additional, Smith, Bryan, additional, and Van Etten, Richard A., additional

Published

2011

38. Activity of Allosteric, Switch-Pocket, ABL/FLT3 Kinase Inhibitor DCC2036 Against Cultured and Primary AML Progenitors with FLT-ITD or FLT3 Kinase Domain Mutations

Author

Fiskus, Warren, primary, Smith, Catherine C., additional, Smith, Jacqueline, additional, Wise, Scott C., additional, Lasater, Elisabeth, additional, Damon, Lauren E., additional, Salerno, Sara, additional, Fleming, Allan, additional, Reyes, Ruben, additional, Ganguly, Siddhartha, additional, Berger, Mark S., additional, Rutkoski, Tom J., additional, McGuirk, Joseph, additional, Shah, Neil, additional, and Bhalla, Kapil N., additional

Published

2011

39. Targeting the KIT Activating Switch Control Pocket: A Novel Mechanism to Inhibit Mast Cell Activation and KIT D816V Neoplastic Mast Cell Proliferation

Author

Bandara, Geethani, primary, Bai, Yun, additional, Chan, Eunice Ching, additional, Maric, Irina, additional, Simakova, Olga, additional, Wise, Scott C., additional, Flynn, Daniel, additional, Metcalfe, Dean D, additional, Gilfillan, Alasdair M, additional, and Wilson, Todd M, additional

Published

2011

40. The ABL Switch Control Inhibitor DCC-2036 Is Active against the Chronic Myeloid Leukemia Mutant BCR-ABLT315I and Exhibits a Narrow Resistance Profile

Author

Eide, Christopher A., primary, Adrian, Lauren T., additional, Tyner, Jeffrey W., additional, Mac Partlin, Mary, additional, Anderson, David J., additional, Wise, Scott C., additional, Smith, Bryan D., additional, Petillo, Peter A., additional, Flynn, Daniel L., additional, Deininger, Michael W.N., additional, O'Hare, Thomas, additional, and Druker, Brian J., additional

Published

2011

41. Abstract 3594: Conformational control of FMS kinase for treatment of human malignancies

Author

Wise, Scott C., primary, Hood, Molly M., additional, Smith, Bryan D., additional, Lister, Deanne, additional, Lu, Wei-Ping, additional, Kaufman, Michael D., additional, McConville, Patrick, additional, and Flynn, Daniel L., additional

Published

2011

42. Abstract LB-300: Small molecule modulators of MET kinase for treatment of human malignancies

Author

Wise, Scott C., primary, Smith, Bryan D., additional, Hood, Molly M., additional, Kaufman, Michael D., additional, Lu, Wei-Ping, additional, and Flynn, Daniel L., additional

Published

2010

43. Examination of Edge Effects with Different Storage Conditions of Preplated Dimethyl Sulfoxide Nanospots in ChemLib 1,536- and 3,456-Well Assay-Ready Plates

Author

Turner, Benjamin A., primary, Evans, Brad P., additional, Pearson, Tania T., additional, Braden, Timothy K., additional, and Wise, Scott C., additional

Published

2008

44. DCC-2036: A Novel Switch Pocket Inhibitor of ABL Tyrosine Kinase with Therapeutic Efficacy Against BCR-ABL T315I In Vitro and in a CML Mouse Model.

Author

Van Etten, Richard A., primary, Chan, Wayne W., additional, Zaleskas, Virginia M., additional, Evangelista, Peter, additional, Lazarides, Katherine, additional, Peng, Cong, additional, Li, Shaoguang, additional, Wise, Scott C., additional, Petillo, Peter, additional, and Flynn, Daniel L., additional

Published

2007

45. Simultaneous Screening of Multiple Bacterial tRNA Synthetases Using an Escherichia coli S30-Based Transcription and Translation Assay

Author

Dermyer, Michael, primary, Wise, Scott C., additional, Braden, Timothy, additional, and Holler, Tod P., additional

Published

2007

46. c-Jun Can Mediate Androgen Receptor-induced Transactivation

Author

Bubulya, Athanasios, primary, Wise, Scott C., additional, Shen, Xi-Qiang, additional, Burmeister, Lori A., additional, and Shemshedini, Lirim, additional

Published

1996

47. VOCAL CORD DYSFUNCTION PRESENTING AS ACUTE BRONCHIAL ASTHMA

Author

Wise, Scott C., primary, OʼBrien, John, additional, and Presson, John, additional

Published

1996

48. ROCKY MOUNTAIN SPOTTED FEVER AND THE USE OF SULFONAMIDES

Author

Wise, Scott C., primary

Published

1995

49. Troglitazone, an antidiabetic agent, inhibits cholesterol biosynthesis through a mechanism independent of peroxisome proliferator-activated receptor-gamma.

Author

Minghan Wang, Wise, Scott C., Left, Todd, and Ti-Zhi Su

Subjects

*HYPOGLYCEMIC agents, *CHOLESTEROL, *BIOSYNTHESIS

Abstract

Examines the effect of troglitazone, an antidiabetic agent, in cholesterol biosynthesis through a mechanism independent of peroxisome proliferated-activated receptor (PPAR)-gamma. Inhibition of cholesterol synthesis by other PPAR-gamma activators; Effects of actinomycin D and cyclohexamide on the inhibitory effect of troglitazone on cholesterol biosynthesis.

Published

1999

50. The selective Tie2 inhibitor rebastinib blocks recruitment and function of Tie2Hi macrophages in breast cancer and neuroendocrine pancreatic tumors

Author

Harney, Allison S., Karagiannis, George S., Pignatelli, Jeanine, Smith, Bryan D., Kadioglu, Ece, Wise, Scott C., Hood, Molly M., Kaufman, Michael D., Leary, Cynthia B., Lu, Wei-Ping, Al-Ani, Gada, Chen, Xiaoming, Entenberg, David, Oktay, Maja H., Wang, Yarong, Chun, Lawrence, De Palma, Michele, Jones, Joan G., Flynn, Daniel L., and Condeelis, John S.

Subjects

embryonic structures, cardiovascular system

Abstract

Tumor-infiltrating myeloid cells promote tumor progression by mediating angiogenesis, tumor cell intravasation and metastasis, which can offset the effects of chemotherapy, radiation, and anti-angiogenic therapy. Here, we show that the kinase switch control inhibitor rebastinib inhibits Tie2, a tyrosine kinase receptor expressed on endothelial cells and pro-tumoral Tie2-expressing macrophages in mouse models of metastatic cancer. Rebastinib reduces tumor growth and metastasis in an orthotopic mouse model of metastatic mammary carcinoma through reduction of Tie2+ myeloid cell infiltration, anti-angiogenic effects, and blockade of tumor cell intravasation mediated by perivascular Tie2(hi)/VegfA(hi) macrophages in the tumor microenvironment of metastasis (TMEM). The anti-tumor effects of rebastinib enhance the efficacy of microtubule inhibiting chemotherapeutic agents, either eribulin or paclitaxel, by reducing tumor volume, metastasis, and improving overall survival. Rebastinib inhibition of angiopoietin/Tie2 signaling impairs multiple pathways in tumor progression mediated by pro-tumoral Tie2+ macrophages, including TMEM-dependent dissemination and angiopoietin/Tie2-dependent angiogenesis. Rebastinib is a promising therapy for achieving Tie2 inhibition in cancer patients.