Your search keyword '"Daniel H Albert"' showing total 158 results

1. PRL-3, a metastasis associated tyrosine phosphatase, is involved in FLT3-ITD signaling and implicated in anti-AML therapy.

Author

Jianbiao Zhou, Chonglei Bi, Wee-Joo Chng, Lip-Lee Cheong, Shaw-Cheng Liu, Sylvia Mahara, Kian-Ghee Tay, Qi Zeng, Jie Li, Ke Guo, Cheng Peow Bobby Tan, Hanry Yu, Daniel H Albert, and Chien-Shing Chen

Subjects

Medicine, Science

Abstract

Combination with other small molecule drugs represents a promising strategy to improve therapeutic efficacy of FLT3 inhibitors in the clinic. We demonstrated that combining ABT-869, a FLT3 inhibitor, with SAHA, a HDAC inhibitor, led to synergistic killing of the AML cells with FLT3 mutations and suppression of colony formation. We identified a core gene signature that is uniquely induced by the combination treatment in 2 different leukemia cell lines. Among these, we showed that downregulation of PTP4A3 (PRL-3) played a role in this synergism. PRL-3 is downstream of FLT3 signaling and ectopic expression of PRL-3 conferred therapeutic resistance through upregulation of STAT (signal transducers and activators of transcription) pathway activity and anti-apoptotic Mcl-1 protein. PRL-3 interacts with HDAC4 and SAHA downregulates PRL-3 via a proteasome dependent pathway. In addition, PRL-3 protein was identified in 47% of AML cases, but was absent in myeloid cells in normal bone marrows. Our results suggest such combination therapies may significantly improve the therapeutic efficacy of FLT3 inhibitors. PRL-3 plays a potential pathological role in AML and it might be a useful therapeutic target in AML, and warrant clinical investigation.

Published

2011

2. Supplemental Figure 4 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

Dose-dependent induction of G1 arrest and senescence by ABBV-075.

Published

2023

3. Figure S2 from Selective Inhibition of the Second Bromodomain of BET Family Proteins Results in Robust Antitumor Activity in Preclinical Models of Acute Myeloid Leukemia

Author

Yu Shen, Marina Konopleva, Warren M. Kati, Keith F. McDaniel, Daniel H. Albert, Michael Boyiadzis, Kathleen A. Dorritie, Neal C. Goodwin, Jenny Rowe, Terrance J. Magoc, Sriram S. Shanmugavelandy, Gaurav Mehta, Debra C. Ferguson, Lina Han, Antonio Cavazos, Qi Zhang, Tamar Uziel, Paul Hessler, Weiguo Feng, Zheng Zha, Xin Lu, Lloyd T. Lam, Vinitha M. Kuruvilla, Emily J. Faivre, Richard J. Bellin, Joshua P. Plotnik, Mai H. Bui, Xiaoli Huang, Xiaoyu Lin, Tianyu Cai, and Lu Zhang

Abstract

Figure S2. ABBV-744 retains strong transcription regulatory activities in AML cells and it did not alter the baseline expression of representative IFN-r or PMA responsive genes.

Published

2023

4. Supplemental Figure 6 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

Characterization of MDV_R cell line with acquired resistance to Enzalutamide.

Published

2023

5. Table S1 from Selective Inhibition of the Second Bromodomain of BET Family Proteins Results in Robust Antitumor Activity in Preclinical Models of Acute Myeloid Leukemia

Author

Yu Shen, Marina Konopleva, Warren M. Kati, Keith F. McDaniel, Daniel H. Albert, Michael Boyiadzis, Kathleen A. Dorritie, Neal C. Goodwin, Jenny Rowe, Terrance J. Magoc, Sriram S. Shanmugavelandy, Gaurav Mehta, Debra C. Ferguson, Lina Han, Antonio Cavazos, Qi Zhang, Tamar Uziel, Paul Hessler, Weiguo Feng, Zheng Zha, Xin Lu, Lloyd T. Lam, Vinitha M. Kuruvilla, Emily J. Faivre, Richard J. Bellin, Joshua P. Plotnik, Mai H. Bui, Xiaoli Huang, Xiaoyu Lin, Tianyu Cai, and Lu Zhang

Abstract

Primary patient sample information

Published

2023

6. Supplementary Figures 1-3 from Vulnerability of Small-Cell Lung Cancer to Apoptosis Induced by the Combination of BET Bromodomain Proteins and BCL2 Inhibitors

Author

Tamar Uziel, Yu Shen, Daniel H. Albert, Warren M. Kati, Anahita Bhathena, Terry Magoc, Michael Mitten, Stephen K. Tahir, Sha Jin, Richard J. Bellin, Denise M. Wilcox, Xiaoli Huang, Ziping Yang, Emily J. Faivre, Xiaoyu Lin, and Lloyd T. Lam

Abstract

Suppl. Figure 1. Caspase inhibitor prevents caspase 3/7 activity; Suppl. Figure 2. Levels of BIM, BAD, BAX and BAK silencing by siRNA; Suppl. Figure 3. mRNA and protein expression of BCL2 and BCLxl upon treatment with ABBV-075.

Published

2023

7. Supplementary Data from Selective Inhibition of the Second Bromodomain of BET Family Proteins Results in Robust Antitumor Activity in Preclinical Models of Acute Myeloid Leukemia

Author

Yu Shen, Marina Konopleva, Warren M. Kati, Keith F. McDaniel, Daniel H. Albert, Michael Boyiadzis, Kathleen A. Dorritie, Neal C. Goodwin, Jenny Rowe, Terrance J. Magoc, Sriram S. Shanmugavelandy, Gaurav Mehta, Debra C. Ferguson, Lina Han, Antonio Cavazos, Qi Zhang, Tamar Uziel, Paul Hessler, Weiguo Feng, Zheng Zha, Xin Lu, Lloyd T. Lam, Vinitha M. Kuruvilla, Emily J. Faivre, Richard J. Bellin, Joshua P. Plotnik, Mai H. Bui, Xiaoli Huang, Xiaoyu Lin, Tianyu Cai, and Lu Zhang

Abstract

Supplementary figure and table legends

Published

2023

8. Supplemental Figure 5 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

AR-dependent prostate cancer cell lines are dependent on BET.

Published

2023

9. Data from Selective Inhibition of the Second Bromodomain of BET Family Proteins Results in Robust Antitumor Activity in Preclinical Models of Acute Myeloid Leukemia

Author

Yu Shen, Marina Konopleva, Warren M. Kati, Keith F. McDaniel, Daniel H. Albert, Michael Boyiadzis, Kathleen A. Dorritie, Neal C. Goodwin, Jenny Rowe, Terrance J. Magoc, Sriram S. Shanmugavelandy, Gaurav Mehta, Debra C. Ferguson, Lina Han, Antonio Cavazos, Qi Zhang, Tamar Uziel, Paul Hessler, Weiguo Feng, Zheng Zha, Xin Lu, Lloyd T. Lam, Vinitha M. Kuruvilla, Emily J. Faivre, Richard J. Bellin, Joshua P. Plotnik, Mai H. Bui, Xiaoli Huang, Xiaoyu Lin, Tianyu Cai, and Lu Zhang

Abstract

Dual bromodomain BET inhibitors that bind with similar affinities to the first and second bromodomains across BRD2, BRD3, BRD4, and BRDT have displayed modest activity as monotherapy in clinical trials. Thrombocytopenia, closely followed by symptoms characteristic of gastrointestinal toxicity, have presented as dose-limiting adverse events that may have prevented escalation to higher dose levels required for more robust efficacy. ABBV-744 is a highly selective inhibitor for the second bromodomain of the four BET family proteins. In contrast to the broad antiproliferative activities observed with dual bromodomain BET inhibitors, ABBV-744 displayed significant antiproliferative activities largely although not exclusively in cancer cell lines derived from acute myeloid leukemia and androgen receptor positive prostate cancer. Studies in acute myeloid leukemia xenograft models demonstrated antitumor efficacy for ABBV-744 that was comparable with the pan-BET inhibitor ABBV-075 but with an improved therapeutic index. Enhanced antitumor efficacy was also observed with the combination of ABBV-744 and the BCL-2 inhibitor, venetoclax compared with monotherapies of either agent alone. These results collectively support the clinical evaluation of ABBV-744 in AML (Clinical Trials.gov identifier: NCT03360006).

Published

2023

10. Supplemental Table 1 from HEXIM1 as a Robust Pharmacodynamic Marker for Monitoring Target Engagement of BET Family Bromodomain Inhibitors in Tumors and Surrogate Tissues

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Lisa A. Roberts-Rapp, Daniel H. Albert, Paul Hessler, Tamar Uziel, Xiaoli Huang, and Xiaoyu Lin

Abstract

290 genes that were modulated by MS417 in both NCI-H1299 and MiaPaCa-2 cells.

Published

2023

11. Supplemental Table 3 from HEXIM1 as a Robust Pharmacodynamic Marker for Monitoring Target Engagement of BET Family Bromodomain Inhibitors in Tumors and Surrogate Tissues

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Lisa A. Roberts-Rapp, Daniel H. Albert, Paul Hessler, Tamar Uziel, Xiaoli Huang, and Xiaoyu Lin

Abstract

Expression change of 25 potential BET inhibitor responsive genes in NCI-H1299, MiaPaCa-2, and MX-1 cells treated with DMSO or 0.5 μM MS417 for 6 hours.

Published

2023

12. Supplemental Figure 1 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

ABBV-075 inhibits AR-dependent transcription and growth.

Published

2023

13. Supplemental Figure 2 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

ABBV-075 inhibits ETS family member ETV1 target gene transcription.

Published

2023

14. Supplemental Figures 1-4; Supplemental Tables 2,4,5 from HEXIM1 as a Robust Pharmacodynamic Marker for Monitoring Target Engagement of BET Family Bromodomain Inhibitors in Tumors and Surrogate Tissues

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Lisa A. Roberts-Rapp, Daniel H. Albert, Paul Hessler, Tamar Uziel, Xiaoli Huang, and Xiaoyu Lin

Abstract

Supplemental Figure 1. Chemical structure and biochemical potency of BET inhibitors used in this study. Supplemental Figure 2. Rapid reversal of PD marker responses upon BET inhibitor washout in OPM-2 cells. Supplemental Figure 3. In vivo antitumor efficacies of ABBV-075 in the OPM-2 model at the 0.25 mg/kg, qdx21 and 1 mg/kg, qdx21 dose levels. Supplemental Figure 4. Identification of potential PD markers in skin. Supplemental Table 2. Common pathways regulated by MS417 in NCI-H1299 and MiaPaCa-2 cells Supplemental Table 4.Correlation of EC50s of MS417 and ABBV-075 in regulating PD makers vs. their anti-proliferative EC50s in OPM-2 cells. Supplemental Table 5. Identification of potential PD markers in whole blood.

Published

2023

15. Supplemental Figure 3 from Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Yu Shen, Warren Kati, Keith McDaniel, Daniel H. Albert, Tamar Uziel, Wei He, Maricel Torrent, Paul Hessler, Xiaoyu Lin, Denise Wilcox, and Emily J. Faivre

Abstract

AR-dependent recruitment of BRD4 to ARE-enhancers.

Published

2023

16. Supplementary Figure Legends from Vulnerability of Small-Cell Lung Cancer to Apoptosis Induced by the Combination of BET Bromodomain Proteins and BCL2 Inhibitors

Author

Tamar Uziel, Yu Shen, Daniel H. Albert, Warren M. Kati, Anahita Bhathena, Terry Magoc, Michael Mitten, Stephen K. Tahir, Sha Jin, Richard J. Bellin, Denise M. Wilcox, Xiaoli Huang, Ziping Yang, Emily J. Faivre, Xiaoyu Lin, and Lloyd T. Lam

Abstract

Supplemental figure legends

Published

2023

17. Supplemental figure 14 to 17 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

High level of concomitant Bim and Bcl-2 expression correlates with sensitivity to ABBV-075-induced apoptosis

Published

2023

18. Supplemental table 4 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Apoptosis induction by MS417 across cancer cell lines

Published

2023

19. Supplemental figure 13 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Restoration of Myc expression under BET inhibitor treatment failed to rescue cells from apoptosis or cell cycle arrest

Published

2023

20. Data from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

ABBV-075 is a potent and selective BET family bromodomain inhibitor that recently entered phase I clinical trials. Comprehensive preclinical characterization of ABBV-075 demonstrated broad activity across cell lines and tumor models, representing a variety of hematologic malignancies and solid tumor indications. In most cancer cell lines derived from solid tumors, ABBV-075 triggers prominent G1 cell-cycle arrest without extensive apoptosis. In this study, we show that ABBV-075 efficiently triggers apoptosis in acute myeloid leukemia (AML), non-Hodgkin lymphoma, and multiple myeloma cells. Apoptosis induced by ABBV-075 was mediated in part by modulation of the intrinsic apoptotic pathway, exhibiting synergy with the BCL-2 inhibitor venetoclax in preclinical models of AML. In germinal center diffuse large B-cell lymphoma, BCL-2 levels or venetoclax sensitivity predicted the apoptotic response to ABBV-075 treatment. In vivo combination studies uncovered surprising benefits of low doses of ABBV-075 coupled with bortezomib and azacitidine treatment, despite the lack of in vitro synergy between ABBV-075 and these agents. The in vitro/in vivo activities of ABBV-075 described here may serve as a useful reference to guide the development of ABBV-075 and other BET family inhibitors for cancer therapy. Cancer Res; 77(11); 2976–89. ©2017 AACR.

Published

2023

21. Supplemental figure 10 & 11 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

ABBV-075 inhibits Bcl-XL transcription and displace BRD4 from Bcl-XL regulatory regions

Published

2023

22. Supplemental table 3 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Apoptosis induction by ABBV-075 across cancer cell lines

Published

2023

23. 'Supplemental figure 2 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Induction of apoptosis across cancer cell lines and CD34 normal cells

Published

2023

24. Supplemental table 1 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Anti-proliferative activity of ABBV-075 across cancer cell lines

Published

2023

25. Supplemental figure 7 & 8 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

BET inhibitor causes cell cycle arrest and triggers senescence in solid tumor cells

Published

2023

26. Supplemental figure legends from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

supplemental figure legends

Published

2023

27. Supplemental figure 6 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Expression of exogenous Bcl-XL rescues ABBV-075 induced apoptosis but not cell cycle arrest

Published

2023

28. Supplemental figure 4 & 5 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

Down regulation of Bcl-XL by MS417 and ABBV-075

Published

2023

29. Supplemental figure 9 from Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Yu Shen, Warren M. Kati, Keith F. McDaniel, Saul H. Rosenberg, Steven W. Elmore, Guowei Fang, Fred Kohlhapp, Xin Lu, Tamar Uziel, Lisa Hasvold, Dachun Liu, John K. Pratt, Steve Fidanze, Le Wang, George S. Sheppard, Cherrie K. Donawho, Denise Wilcox, Xiaoli Huang, Scott E. Warder, Emily J. Faivre, Lloyd T. Lam, Leiming Li, Daniel H. Albert, Xiaoyu Lin, and Mai H. Bui

Abstract

ABBV-075 inhibits genes that are important for cell cycle

Published

2023

30. Balancing Properties with Carboxylates: A Lead Optimization Campaign for Selective and Orally Active CDK9 Inhibitors

Author

Andrew J. Souers, Wei Qiu, Thomas D. Penning, Darren C. Phillips, Xiaoqin Liu, Rick F. Clark, Joel D. Leverson, Amanda M. Olson, Chunqiu Lai, Daniel H. Albert, Gui-Dong Zhu, Yunsong Tong, Peter Kovar, Kenton L. Longenecker, Anthony Mastracchio, Morey L. Smith, Bailin Shaw, Alan S. Florjancic, Stephen K. Tahir, and Donald J. Osterling

Subjects

Serine, In vivo, Oral administration, Chemistry, Kinase, Organic Chemistry, Drug Discovery, Toxicity, Cyclin-dependent kinase 9, Dosing, Pharmacology, Pharmacophore, Biochemistry

Abstract

[Image: see text] Cyclin-dependent kinase 9 (CDK9) is a serine/threonine kinase involved in the regulation of transcription elongation. An inhibition of CDK9 downregulates a number of short-lived proteins responsible for tumor maintenance and survival, including the antiapoptotic BCL-2 family member MCL-1. As pan-CDK inhibitors under development have faced dosing and toxicity challenges in the clinical setting, we generated selective CDK9 inhibitors that could be amenable to an oral administration. Here, we report the lead optimization of a series of azaindole-based inhibitors. To overcome early challenges with promiscuity and cardiovascular toxicity, carboxylates were introduced into the pharmacophore en route to compounds such as 14 and 16. These CDK9 inhibitors demonstrated a reduced toxicity, adequate pharmacokinetic properties, and a robust in vivo efficacy in mice upon oral dosing.

Published

2021

31. Co-clinical Modeling of the Activity of the BET Inhibitor Mivebresib (ABBV-075) in AML

Author

Daniel H, Albert, Neal C, Goodwin, Angela M, Davies, Jenny, Rowe, Gerold, Feuer, Michael, Boyiadzis, Kathleen A, Dorritie, Maria, Mancini, Regina, Gandour-Edwards, Brian A, Jonas, Gautam, Borthakur, Ibrahim, Aldoss, David A, Rizzieri, Olatoyosi, Odenike, Thomas, Prebet, Sanjana, Singh, Relja, Popovic, Y U, Shen, Keith F, McDaniel, Warren M, Kati, Dimple A, Modi, Monica, Motwani, Johannes E, Wolff, and David J, Frost

Subjects

Myeloid, Cancer Research, Pediatric Research Initiative, Pyridones, Childhood Leukemia, Pediatric Cancer, Clinical Sciences, Mice, SCID, Acute, SCID, General Biochemistry, Genetics and Molecular Biology, Cell Line, BRT inhibitors, Mice, Rare Diseases, AML, Mice, Inbred NOD, Cell Line, Tumor, Animals, Humans, Oncology & Carcinogenesis, co-clinical PDX models, Cancer, Pharmacology, Pediatric, Sulfonamides, Tumor, Leukemia, Hematology, Leukemia, Myeloid, Acute, Orphan Drug, 5.1 Pharmaceuticals, Inbred NOD, Development of treatments and therapeutic interventions, Mivebresib, Key Words, Research Article

Abstract

Background/Aim: The therapeutic potential of bromodomain and extra-terminal motif (BET) inhibitors in hematological cancers has been well established in preclinical and early-stage clinical trials, although as of yet, no BET-targeting agent has achieved approval. To add insight into potential response to mivebresib (ABBV-075), a broad-spectrum BET inhibitor, co-clinical modeling of individual patient biopsies was conducted in the context of a Phase I trial in acute myeloid leukemia (AML). Materials and Methods: Co-clinical modeling involves taking the patient’s biopsy and implanting it in mice with limited passage so that it closely retains the original characteristics of the malignancy and allows comparisons of response between animal model and clinical data. Procedures were developed, initially with neonate NOD/Shi-scid-IL2rγnull (NOG) mice and then optimized with juvenile NOG-EXL as host mice, eventually resulting in a robust rate of engraftment (16 out of 26, 62%). Results: Results from the co-clinical AML patient-derived xenograft (PDX) modeling (6 with >60% inhibition of bone marrow blasts) were consistent with the equivalent clinical data from patients receiving mivebresib in monotherapy, and in combination with venetoclax. The modeling system also demonstrated the activity of a novel BD2-selective BET inhibitor (ABBV-744) in the preclinical AML setting. Both agents were also highly effective in inhibiting blast counts in the spleen (10/10 and 5/6 models, respectively). Conclusion: These findings confirm the validity of the model system in the co-clinical setting, establish highly relevant in vivo models for the discovery of cancer therapy, and indicate the therapeutic value of BET inhibitors for AML and, potentially, myelofibrosis treatment.

Published

2022

32. Discovery of N-Ethyl-4-[2-(4-fluoro-2,6-dimethyl-phenoxy)-5-(1-hydroxy-1-methyl-ethyl)phenyl]-6-methyl-7-oxo-1H-pyrrolo[2,3-c]pyridine-2-carboxamide (ABBV-744), a BET Bromodomain Inhibitor with Selectivity for the Second Bromodomain

Author

Daniel H. Albert, Wei Qiu, Chang H. Park, Steven D. Fidanze, Lisa A. Hasvold, Maricel Torrent, Ganesh Rajaraman, Xiaoli Huang, Peter Kovar, Keith F. McDaniel, Xiaoyu Lin, George S. Sheppard, Le Wang, John K. Pratt, Lu Zhang, Mai Bui, Yu Shen, Kenton L. Longenecker, Warren M. Kati, Dachun Liu, Denise Wilcox, Terrance J. Magoc, and Emily J. Faivre

Subjects

0303 health sciences, BRD4, medicine.drug_class, Stereochemistry, chemical and pharmacologic phenomena, hemic and immune systems, Carboxamide, 01 natural sciences, 0104 chemical sciences, Bromodomain, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, chemistry, Drug Discovery, Pyridine, medicine, Molecular Medicine, Selectivity, 030304 developmental biology

Abstract

The BET family of proteins consists of BRD2, BRD3, BRD4, and BRDt. Each protein contains two distinct bromodomains (BD1 and BD2). BET family bromodomain inhibitors under clinical development for on...

Published

2020

33. Identification of VEGF Signaling Inhibition-Induced Glomerular Injury in Rats through Site-Specific Urinary Biomarkers

Author

Kenneth Kowalkowski, Keith B. Glaser, Wayne R. Buck, Yi Yang, Rita Ciurlionis, Eric A. G. Blomme, and Daniel H. Albert

Subjects

Male, Vascular Endothelial Growth Factor A, Pathology, medicine.medical_specialty, Urinalysis, QH301-705.5, Urinary system, Podocyte foot, Laser Capture Microdissection, Glomerulus (kidney), Article, Catalysis, Rats, Sprague-Dawley, Inorganic Chemistry, chemistry.chemical_compound, Albumins, Animals, Medicine, urinary biomarkers, Physical and Theoretical Chemistry, Biology (General), Protein Kinase Inhibitors, Molecular Biology, QD1-999, Spectroscopy, Laser capture microdissection, vascular endothelial growth factor, glomerular injury, medicine.diagnostic_test, business.industry, Organic Chemistry, Cancer, General Medicine, medicine.disease, Rats, Computer Science Applications, Vascular endothelial growth factor, Disease Models, Animal, Chemistry, Receptors, Vascular Endothelial Growth Factor, medicine.anatomical_structure, chemistry, Kidney Diseases, Signal transduction, beta 2-Microglobulin, business, Biomarkers, Signal Transduction

Abstract

Cancer therapies targeting the vascular endothelial growth factor (VEGF) signaling pathway can lead to renal damage by disrupting the glomerular ultrafiltration apparatus. The objective of the current study was to identify sensitive biomarkers for VEGF inhibition-induced glomerular changes in rats. Male Sprague-Dawley rats were administered an experimental VEGF receptor (VEGFR) inhibitor, ABT-123, for seven days to investigate the correlation of several biomarkers with microscopic and ultrastructural changes. Glomeruli obtained by laser capture microdissection were also subjected to gene expression analysis to investigate the underlying molecular events of VEGFR inhibition in glomerulus. ABT-123 induced characteristic glomerular ultrastructural changes in rats, including fusion of podocyte foot processes, the presence of subendothelial electron-dense deposits, and swelling and loss of fenestrations in glomerular endothelium. The subtle morphological changes cannot be detected with light microscopy or by changes in standard clinical chemistry and urinalysis. However, urinary albumin increased 44-fold as early as Day three. Urinary β2-microglobulin levels were also increased. Other urinary biomarkers that are typically associated with tubular injury were not significantly impacted. Such patterns in urinary biomarkers can provide valuable diagnostic insight to VEGF inhibition therapy-induced glomeruli injuries.

Published

2021

34. Selective inhibition of the BD2 bromodomain of BET proteins in prostate cancer

Author

Denise Wilcox, Vasudha Sehgal, Daniel H. Albert, John K. Pratt, Keith F. McDaniel, Xin Lu, Chaohong Sun, Dachun Liu, Joshua P. Plotnik, Srinivasa R. Mantena, Emily J. Faivre, Lisa A. Hasvold, George S. Sheppard, Xiaoli Huang, Le Wang, Lance J Bigelow, Stacey Fossey, Steve D. Fidanze, Lloyd T. Lam, Chang H. Park, Sanjay C. Panchal, Warren M. Kati, John J. Nicolette, Richard J. Bellin, Gaurav Mehta, Xiaoyu Lin, Mai H. Bui, Lu Zhang, Paul Hessler, Maricel Torrent, Tamar Uziel, Saul H. Rosenberg, Yu Shen, and Kenton L. Longenecker

Subjects

Male, BRD4, Transcription, Genetic, Pyridines, Cell Cycle Proteins, BET inhibitor, Mice, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Protein Domains, Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, Pyrroles, Receptor, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, Chemistry, Prostatic Neoplasms, medicine.disease, Xenograft Model Antitumor Assays, Rats, Bromodomain, Gene Expression Regulation, Neoplastic, Enhancer Elements, Genetic, Histone, Receptors, Androgen, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Chromatin immunoprecipitation, Transcription Factors

Abstract

Proteins of the bromodomain and extra-terminal (BET) domain family are epigenetic readers that bind acetylated histones through their bromodomains to regulate gene transcription. Dual-bromodomain BET inhibitors (DbBi) that bind with similar affinities to the first (BD1) and second (BD2) bromodomains of BRD2, BRD3, BRD4 and BRDt have displayed modest clinical activity in monotherapy cancer trials. A reduced number of thrombocytes in the blood (thrombocytopenia) as well as symptoms of gastrointestinal toxicity are dose-limiting adverse events for some types of DbBi1–5. Given that similar haematological and gastrointestinal defects were observed after genetic silencing of Brd4 in mice6, the platelet and gastrointestinal toxicities may represent on-target activities associated with BET inhibition. The two individual bromodomains in BET family proteins may have distinct functions7–9 and different cellular phenotypes after pharmacological inhibition of one or both bromodomains have been reported10,11, suggesting that selectively targeting one of the bromodomains may result in a different efficacy and tolerability profile compared with DbBi. Available compounds that are selective to individual domains lack sufficient potency and the pharmacokinetics properties that are required for in vivo efficacy and tolerability assessment10–13. Here we carried out a medicinal chemistry campaign that led to the discovery of ABBV-744, a highly potent and selective inhibitor of the BD2 domain of BET family proteins with drug-like properties. In contrast to the broad range of cell growth inhibition induced by DbBi, the antiproliferative activity of ABBV-744 was largely, but not exclusively, restricted to cell lines of acute myeloid leukaemia and prostate cancer that expressed the full-length androgen receptor (AR). ABBV-744 retained robust activity in prostate cancer xenografts, and showed fewer platelet and gastrointestinal toxicities than the DbBi ABBV-07514. Analyses of RNA expression and chromatin immunoprecipitation followed by sequencing revealed that ABBV-744 displaced BRD4 from AR-containing super-enhancers and inhibited AR-dependent transcription, with less impact on global transcription compared with ABBV-075. These results underscore the potential value of selectively targeting the BD2 domain of BET family proteins for cancer therapy. ABBV-744, a selective inhibitor of the BD2 domains of BET family proteins, is effective against prostate cancer in mouse xenograft models, with lower toxicities than the dual-bromodomain BET inhibitor ABBV-075.

Published

2020

35. A novel CDK9 inhibitor increases the efficacy of venetoclax (ABT-199) in multiple models of hematologic malignancies

Author

Jennifer R. Devlin, Andrew J. Souers, Morey L. Smith, John Xue, Stephen K. Tahir, Daniel H. Albert, Thomas D. Penning, Rick F. Clark, Ricky W. Johnstone, Jake Shortt, Sha Jin, Marina Konopleva, Yunsong Tong, Joel D. Leverson, Darren C. Phillips, Xiaoxian Zhao, Haichao Zhang, Eric D. Hsi, Jun Chen, Gareth P. Gregory, and Qi Zhang

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, Cell Survival, Antineoplastic Agents, Apoptosis, Tumor initiation, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cyclin-dependent kinase, In vivo, Cell Line, Tumor, hemic and lymphatic diseases, Tumor Cells, Cultured, Animals, Humans, Protein Kinase Inhibitors, Sulfonamides, biology, Kinase, Venetoclax, Drug Synergism, Hematology, Bridged Bicyclo Compounds, Heterocyclic, Cyclin-Dependent Kinase 9, Xenograft Model Antitumor Assays, 030104 developmental biology, Cell killing, Oncology, chemistry, Hematologic Neoplasms, 030220 oncology & carcinogenesis, biology.protein, Cancer research

Abstract

MCL-1 is one of the most frequently amplified genes in cancer, facilitating tumor initiation and maintenance and enabling resistance to anti-tumorigenic agents including the BCL-2 selective inhibitor venetoclax. The expression of MCL-1 is maintained via P-TEFb-mediated transcription, where the kinase CDK9 is a critical component. Consequently, we developed a series of potent small-molecule inhibitors of CDK9, exemplified by the orally active A-1592668, with CDK selectivity profiles that are distinct from related molecules that have been extensively studied clinically. Short-term treatment with A-1592668 rapidly downregulates RNA pol-II (Ser 2) phosphorylation resulting in the loss of MCL-1 protein and apoptosis in MCL-1-dependent hematologic tumor cell lines. This cell death could be attenuated by either inhibiting caspases or overexpressing BCL-2 protein. Synergistic cell killing was also observed between A-1592668 or the related analog A-1467729, and venetoclax in a number of hematologic cell lines and primary NHL patient samples. Importantly, the CDK9 inhibitor plus venetoclax combination was well tolerated in vivo and demonstrated efficacy superior to either agent alone in mouse models of lymphoma and AML. These data indicate that CDK9 inhibitors could be highly efficacious in tumors that depend on MCL-1 for survival or when used in combination with venetoclax in malignancies dependent on MCL-1 and BCL-2.

Published

2019

36. Selective Inhibition of the Second Bromodomain of BET Family Proteins Results in Robust Antitumor Activity in Preclinical Models of Acute Myeloid Leukemia

Author

Marina Konopleva, Tamar Uziel, Xiaoli Huang, Weiguo Feng, Xiaoyu Lin, Warren M. Kati, Lloyd T. Lam, Vinitha Mary Kuruvilla, Mai H. Bui, Emily J. Faivre, Tianyu Cai, Jenny Rowe, Daniel H. Albert, Richard J. Bellin, Lu Zhang, Zheng Zha, Sriram S. Shanmugavelandy, Paul Hessler, Michael Boyiadzis, Gaurav Mehta, Antonio Cavazos, Keith F. McDaniel, Joshua P. Plotnik, Terrance J. Magoc, Xin Lu, Debra Ferguson, Yu Shen, Lina Han, Neal Goodwin, Qi Zhang, and Kathleen A. Dorritie

Subjects

Cancer Research, BRD4, Pyridines, Androgen Receptor Positive, Antineoplastic Agents, Apoptosis, Mice, SCID, BET inhibitor, Prostate cancer, chemistry.chemical_compound, Mice, Therapeutic index, Mice, Inbred NOD, medicine, Tumor Cells, Cultured, Animals, Humans, Pyrroles, Cell Proliferation, Sulfonamides, Venetoclax, business.industry, Myeloid leukemia, Proteins, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Xenograft Model Antitumor Assays, Bromodomain, Leukemia, Myeloid, Acute, Oncology, chemistry, Proto-Oncogene Proteins c-bcl-2, Cancer research, Drug Therapy, Combination, Female, business

Abstract

Dual bromodomain BET inhibitors that bind with similar affinities to the first and second bromodomains across BRD2, BRD3, BRD4, and BRDT have displayed modest activity as monotherapy in clinical trials. Thrombocytopenia, closely followed by symptoms characteristic of gastrointestinal toxicity, have presented as dose-limiting adverse events that may have prevented escalation to higher dose levels required for more robust efficacy. ABBV-744 is a highly selective inhibitor for the second bromodomain of the four BET family proteins. In contrast to the broad antiproliferative activities observed with dual bromodomain BET inhibitors, ABBV-744 displayed significant antiproliferative activities largely although not exclusively in cancer cell lines derived from acute myeloid leukemia and androgen receptor positive prostate cancer. Studies in acute myeloid leukemia xenograft models demonstrated antitumor efficacy for ABBV-744 that was comparable with the pan-BET inhibitor ABBV-075 but with an improved therapeutic index. Enhanced antitumor efficacy was also observed with the combination of ABBV-744 and the BCL-2 inhibitor, venetoclax compared with monotherapies of either agent alone. These results collectively support the clinical evaluation of ABBV-744 in AML (Clinical Trials.gov identifier: NCT03360006).

Published

2021

37. Discovery of

Author

George S, Sheppard, Le, Wang, Steven D, Fidanze, Lisa A, Hasvold, Dachun, Liu, John K, Pratt, Chang H, Park, Kenton, Longenecker, Wei, Qiu, Maricel, Torrent, Peter J, Kovar, Mai, Bui, Emily, Faivre, Xiaoli, Huang, Xiaoyu, Lin, Denise, Wilcox, Lu, Zhang, Yu, Shen, Daniel H, Albert, Terrance J, Magoc, Ganesh, Rajaraman, Warren M, Kati, and Keith F, McDaniel

Subjects

Pyridines, Cell Cycle Proteins, Mice, SCID, Xenograft Model Antitumor Assays, Protein Structure, Secondary, Protein Structure, Tertiary, Mice, Protein Domains, Drug Discovery, Animals, Humans, Female, Pyrroles, HeLa Cells, Transcription Factors

Abstract

The BET family of proteins consists of BRD2, BRD3, BRD4, and BRDt. Each protein contains two distinct bromodomains (BD1 and BD2). BET family bromodomain inhibitors under clinical development for oncology bind to each of the eight bromodomains with similar affinities. We hypothesized that it may be possible to achieve an improved therapeutic index by selectively targeting subsets of the BET bromodomains. Both BD1 and BD2 are highly conserved across family members (70% identity), whereas BD1 and BD2 from the same protein exhibit a larger degree of divergence (∼40% identity), suggesting selectivity between BD1 and BD2 of all family members would be more straightforward to achieve. Exploiting the Asp144/His437 and Ile146/Val439 sequence differences (BRD4 BD1/BD2 numbering) allowed the identification of compound

Published

2020

38. Discovery and optimization of novel constrained pyrrolopyridone BET family inhibitors

Author

Keith F. McDaniel, Andrew Bogdan, Lisa A. Hasvold, Ana L. Aguirre, Denise Wilcox, Xiaoyu Lin, Le Wang, Mai H. Bui, Leiming Li, Warren M. Kati, Terrance J. Magoc, James H. Holms, Dachun Liu, Steven D. Fidanze, Justin D. Dietrich, Charles W. Hutchins, Ganesh Rajaraman, Yu Shen, George S. Sheppard, Rongqi Wang, Daniel H. Albert, Chang H. Park, Jasmina Marjanovic, Robert A. Mantei, Xiaoli Huang, Peter Kovar, Yujia Dai, and John K. Pratt

Subjects

0301 basic medicine, Pyridones, Transplantation, Heterologous, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Cell Cycle Proteins, Computational biology, Molecular Dynamics Simulation, Crystallography, X-Ray, Biochemistry, Mice, Structure-Activity Relationship, 03 medical and health sciences, Protein structure, In vivo, Cell Line, Tumor, Microsomes, Drug Discovery, Animals, Humans, Structure–activity relationship, Binding site, Molecular Biology, Tumor xenograft, Cell Proliferation, Binding Sites, Chemistry, Organic Chemistry, Nuclear Proteins, Protein Structure, Tertiary, Bromodomain, Transplantation, 030104 developmental biology, Molecular Medicine, Multiple Myeloma, Half-Life, Transcription Factors

Abstract

Novel conformationally constrained BET bromodomain inhibitors have been developed. These inhibitors were optimized in two similar, yet distinct chemical series, the 6-methyl-1H-pyrrolo[2,3-c]pyridin-7(6H)-ones (A) and the 1-methyl-1H-pyrrolo[2,3-c]pyridin-7(6H)-ones (B). Each series demonstrated excellent activity in binding and cellular assays, and lead compounds from each series demonstrated significant efficacy in in vivo tumor xenograft models.

Published

2018

39. Discovery of N-(4-(2,4-Difluorophenoxy)-3-(6-methyl-7-oxo-6,7-dihydro-1H-pyrrolo[2,3-c]pyridin-4-yl)phenyl)ethanesulfonamide (ABBV-075/Mivebresib), a Potent and Orally Available Bromodomain and Extraterminal Domain (BET) Family Bromodomain Inhibitor

Author

Ganesh Rajaraman, Leiming Li, Daniel H. Albert, Ruth L. Martin, Terrance J. Magoc, Todd N. Soltwedel, Denise Wilcox, Xiaoli Huang, Chang H. Park, Steven W. Elmore, George S. Sheppard, Charles W. Hutchins, Dachun Liu, Chaohong C. Sun, Guowei Fang, Le Wang, Wenqing Gao, Robert A. Mantei, Rongqi Wang, Emily J. Faivre, Steven D. Fidanze, John K. Pratt, Xiaoyu Lin, Mai H. Bui, Shekman Wong, Scott E. Warder, Jianwei J. Shen, Rohinton P. Edalji, Lisa A. Hasvold, Warren M. Kati, Keith F. McDaniel, and Yu Shen

Subjects

0301 basic medicine, Pyridones, Proton Magnetic Resonance Spectroscopy, Pharmacology, Mass Spectrometry, Mice, Structure-Activity Relationship, 03 medical and health sciences, Pharmacokinetics, In vivo, Cell Line, Tumor, Drug Discovery, Fluorescence Resonance Energy Transfer, Animals, Humans, Structure–activity relationship, Potency, Asparagine, Chromatography, High Pressure Liquid, Sulfonamides, Chemistry, Drug discovery, Proteins, Bromodomain, 030104 developmental biology, Molecular Medicine, Drug metabolism, Half-Life

Abstract

The development of bromodomain and extraterminal domain (BET) bromodomain inhibitors and their examination in clinical studies, particularly in oncology settings, has garnered substantial recent interest. An effort to generate novel BET bromodomain inhibitors with excellent potency and drug metabolism and pharmacokinetics (DMPK) properties was initiated based upon elaboration of a simple pyridone core. Efforts to develop a bidentate interaction with a critical asparagine residue resulted in the incorporation of a pyrrolopyridone core, which improved potency by 9-19-fold. Additional structure-activity relationship (SAR) efforts aimed both at increasing potency and improving pharmacokinetic properties led to the discovery of the clinical candidate 63 (ABBV-075/mivebresib), which demonstrates excellent potency in biochemical and cellular assays, advantageous exposures and half-life both in animal models and in humans, and in vivo efficacy in mouse models of cancer progression and inflammation.

Published

2017

40. Preclinical Characterization of BET Family Bromodomain Inhibitor ABBV-075 Suggests Combination Therapeutic Strategies

Author

Xiaoli Huang, Lisa A. Hasvold, Guowei Fang, Yu Shen, Denise Wilcox, Cherrie K. Donawho, George S. Sheppard, Le Wang, Fred Kohlhapp, Dachun Liu, Tamar Uziel, Leiming Li, Lloyd T. Lam, Daniel H. Albert, Scott E. Warder, Steven W. Elmore, Saul H. Rosenberg, Xiaoyu Lin, Xin Lu, Mai H. Bui, Keith F. McDaniel, Warren M. Kati, Emily J. Faivre, John K. Pratt, and Steve D. Fidanze

Subjects

0301 basic medicine, Cancer Research, Pyridones, Azacitidine, Apoptosis, Pharmacology, Biology, Transfection, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, medicine, Humans, Multiple myeloma, Sulfonamides, Bortezomib, Venetoclax, Cancer, Myeloid leukemia, Androgen Antagonists, Drug Synergism, medicine.disease, Lymphoma, Bromodomain, 030104 developmental biology, Oncology, chemistry, Cancer research, medicine.drug

Abstract

ABBV-075 is a potent and selective BET family bromodomain inhibitor that recently entered phase I clinical trials. Comprehensive preclinical characterization of ABBV-075 demonstrated broad activity across cell lines and tumor models, representing a variety of hematologic malignancies and solid tumor indications. In most cancer cell lines derived from solid tumors, ABBV-075 triggers prominent G1 cell-cycle arrest without extensive apoptosis. In this study, we show that ABBV-075 efficiently triggers apoptosis in acute myeloid leukemia (AML), non-Hodgkin lymphoma, and multiple myeloma cells. Apoptosis induced by ABBV-075 was mediated in part by modulation of the intrinsic apoptotic pathway, exhibiting synergy with the BCL-2 inhibitor venetoclax in preclinical models of AML. In germinal center diffuse large B-cell lymphoma, BCL-2 levels or venetoclax sensitivity predicted the apoptotic response to ABBV-075 treatment. In vivo combination studies uncovered surprising benefits of low doses of ABBV-075 coupled with bortezomib and azacitidine treatment, despite the lack of in vitro synergy between ABBV-075 and these agents. The in vitro/in vivo activities of ABBV-075 described here may serve as a useful reference to guide the development of ABBV-075 and other BET family inhibitors for cancer therapy. Cancer Res; 77(11); 2976–89. ©2017 AACR.

Published

2017

41. Exploitation of Castration-Resistant Prostate Cancer Transcription Factor Dependencies by the Novel BET Inhibitor ABBV-075

Author

Xiaoyu Lin, Daniel H. Albert, Paul Hessler, Wei He, Denise Wilcox, Maricel Torrent, Tamar Uziel, Emily J. Faivre, Warren M. Kati, Keith F. McDaniel, and Yu Shen

Subjects

Male, 0301 basic medicine, Cancer Research, BRD4, Transcription, Genetic, Pyridones, Antineoplastic Agents, Enhancer RNAs, Biology, Ligands, urologic and male genital diseases, BET inhibitor, Inhibitory Concentration 50, Mice, 03 medical and health sciences, Protein Domains, Transcription (biology), Cell Line, Tumor, Nitriles, Phenylthiohydantoin, Animals, Humans, Enhancer, Molecular Biology, Transcription factor, Cell Proliferation, Sulfonamides, Androgen Antagonists, Dihydrotestosterone, Chromatin, Bromodomain, Gene Expression Regulation, Neoplastic, Androgen receptor, Prostatic Neoplasms, Castration-Resistant, Enhancer Elements, Genetic, Phenotype, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, Receptors, Androgen, Benzamides, Cancer research, Signal Transduction, Transcription Factors

Abstract

Competitive inhibitors of acetyl-lysine binding to the bromodomains of the BET (bromodomain and extra terminal) family are being developed for the treatment of solid and hematologic malignancies. The function of BET family member BRD4 at enhancers/superenhancers has been shown to sustain signal-dependent or pathogenic gene expression programs. Here, the hypothesis was tested that the transcription factor drivers of castration-resistant prostate cancer (CRPC) clinical progression, including the androgen receptor (AR), are critically dependent on BRD4 and thus represent a sensitive solid tumor indication for the BET inhibitor ABBV-075. DHT-stimulated transcription of AR target genes was inhibited by ABBV-075 without significant effect on AR protein expression. Furthermore, ABBV-075 disrupted DHT-stimulated recruitment of BET family member BRD4 to gene-regulatory regions cooccupied by AR, including the well-established PSA and TMPRSS2 enhancers. Persistent BET inhibition disrupted the composition and function of AR-occupied enhancers as measured by a reduction in AR and H3K27Ac ChIP signal and inhibition of enhancer RNA transcription. ABBV-075 displayed potent antiproliferative activity in multiple models of resistance to second-generation antiandrogens and inhibited the activity of the AR splice variant AR-V7 and ligand-binding domain gain-of-function mutations, F877L and L702H. ABBV-075 was also a potent inhibitor of MYC and the TMPRSS2-ETS fusion protein, important parallel transcription factor drivers of CRPC. Implications: The ability of BET family inhibitor ABBV-075 to inhibit transcription activation downstream of the initiating events of transcription factors like AR and TMPRSS2:ETS fusion proteins provides a promising therapeutic option for CRPC patients who have developed resistance to second-generation antiandrogens. Mol Cancer Res; 15(1); 35–44. ©2016 AACR.

Published

2017

42. Phase 1 dose escalation trial of ilorasertib, a dual Aurora/VEGF receptor kinase inhibitor, in patients with hematologic malignancies

Author

Lisa Roberts-Rapp, Peter Ansell, Guillermo Garcia-Manero, Martha Arellano, Wijith Munasinghe, Hao Xiong, Brian Oliver, Emily A. Knight, Qin Qin, Raoul Tibes, Justin L. Ricker, Hagop M. Kantarjian, Mark D. McKee, Daniel H. Albert, Hanna Jean Khoury, and Tapan M. Kadia

Subjects

Male, Maximum Tolerated Dose, Azacitidine, Aurora inhibitor, Aminopyridines, Antineoplastic Agents, Pharmacology, Article, chemistry.chemical_compound, Aurora kinase, Growth factor receptor, Aurora Kinases, Antineoplastic Combined Chemotherapy Protocols, Humans, Medicine, Pharmacology (medical), Protein Kinase Inhibitors, Aged, Acute leukemia, business.industry, Phenylurea Compounds, Vascular endothelial growth factor, Receptors, Vascular Endothelial Growth Factor, Oncology, chemistry, Hematologic Neoplasms, Female, business, Tyrosine kinase, medicine.drug, Proto-oncogene tyrosine-protein kinase Src

Abstract

Background Ilorasertib (ABT-348) is a novel inhibitor of Aurora kinase, vascular endothelial growth factor (VEGF) and platelet-derived growth factor receptors, and the Src families of tyrosine kinases. Ilorasertib alone or in combination with azacitidine demonstrated activity in preclinical models in various hematological malignancies, indicating that pan-Aurora kinase and multiple kinase inhibition may have preferential antileukemic activity. This phase 1 trial determined the safety, pharmacokinetics, and preliminary antitumor activity of ilorasertib alone or combined with azacitidine in advanced hematologic malignancies. Patients and methods Fifty-two patients (median age, 67 years; 35 % with >4 prior regimens) with acute myelogenous leukaemia (AML; n = 38), myelodysplastic syndrome (n = 12), or chronic myelomonocytic leukaemia (n = 2) received 3 or 6 doses of ilorasertib per 28-day cycle and were assigned to arm A (once-weekly oral), B (twice-weekly oral), C (once-weekly oral plus azacitidine), or D (once-weekly intravenous) treatment. Results Maximum tolerated doses were not determined; the recommended phase 2 oral monotherapy doses were 540 mg once weekly and 480 mg twice weekly. The most common grade 3/4 adverse events were hypertension (28.8 %), hypokalemia (15.4 %), anemia (13.5 %), and hypophosphatemia (11.5 %). Oral ilorasertib pharmacokinetics appeared dose proportional, with a 15-hour half-life and no interaction with azacitidine. Ilorasertib inhibited biomarkers for Aurora kinase and VEGF receptors, and demonstrated clinical responses in 3 AML patients. Conclusions Ilorasertib exhibited acceptable safety and pharmacokinetics at or below the recommended phase 2 dose, displayed evidence of dual Aurora kinase and VEGF receptor kinase inhibition, and activity in AML.

Published

2015

43. Fragment-Based, Structure-Enabled Discovery of Novel Pyridones and Pyridone Macrocycles as Potent Bromodomain and Extra-Terminal Domain (BET) Family Bromodomain Inhibitors

Author

Keith F. McDaniel, Carol K. Wada, Terrance J. Magoc, Warren M. Kati, Dachun Liu, Chaohong Sun, Lisa A. Hasvold, Le Wang, Robert A. Mantei, John K. Pratt, Yu Shen, Michael D. Wendt, T. Matthew Hansen, Charles W. Hutchins, Andrew M. Petros, Robin R. Frey, Denise Wilcox, Xiaoyu Lin, Chang H. Park, Rongqi Wang, Xiaoli Huang, Robert D. Hubbard, Peter Kovar, William J. McClellan, James H. Holms, George S. Sheppard, Leiming Li, Ganesh Rajaraman, Daniel H. Albert, Sanjay C. Panchal, Scott E. Warder, Steven D. Fidanze, Todd N. Soltwedel, and Steven W. Elmore

Subjects

0301 basic medicine, BRD4, Macrocyclic Compounds, Stereochemistry, Pyridones, Crystallography, X-Ray, 01 natural sciences, 03 medical and health sciences, Structure-Activity Relationship, Drug Discovery, Potency, Structure–activity relationship, Animals, Molecular Structure, 010405 organic chemistry, Chemistry, Drug discovery, Fragment (computer graphics), Cell based assays, 0104 chemical sciences, Bromodomain, Rats, 030104 developmental biology, Biochemistry, Molecular Medicine, Tumor growth inhibition

Abstract

Members of the BET family of bromodomain containing proteins have been identified as potential targets for blocking proliferation in a variety of cancer cell lines. A two-dimensional NMR fragment screen for binders to the bromodomains of BRD4 identified a phenylpyridazinone fragment with a weak binding affinity (1, Ki = 160 μM). SAR investigation of fragment 1, aided by X-ray structure-based design, enabled the synthesis of potent pyridone and macrocyclic pyridone inhibitors exhibiting single digit nanomolar potency in both biochemical and cell based assays. Advanced analogs in these series exhibited high oral exposures in rodent PK studies and demonstrated significant tumor growth inhibition efficacy in mouse flank xenograft models.

Published

2017

44. Methylpyrrole inhibitors of BET bromodomains

Author

Lisa A. Hasvold, Steven W. Elmore, Nirupama B. Soni, Leiming Li, Yu Shen, George S. Sheppard, Terrance J. Magoc, Carol K. Wada, Dachun Liu, Sanjay C. Panchal, Scott E. Warder, Chaohong Sun, Keith F. McDaniel, Lauren Smithee, Xiaoyu Lin, Daniel H. Albert, Xiaoli Huang, Chang H. Park, Le Wang, Peter Kovar, F. Greg Buchanan, Warren M. Kati, Robert A. Mantei, Robbert Hubbard, Andrew M. Petros, Steven D. Fidanze, Denise Wilcox, and John K. Pratt

Subjects

0301 basic medicine, BRD4, Stereochemistry, Clinical Biochemistry, Transplantation, Heterologous, Pharmaceutical Science, Antineoplastic Agents, Molecular Dynamics Simulation, Crystallography, X-Ray, Biochemistry, 03 medical and health sciences, Mice, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Animals, Humans, Mouse tumor, Pyrroles, Molecular Biology, Cell Proliferation, Binding Sites, Chemistry, Organic Chemistry, Nuclear Proteins, Combinatorial chemistry, Bromodomain, 030104 developmental biology, Drug Design, Molecular Medicine, Multiple Myeloma, Half-Life, Transcription Factors

Abstract

An NMR fragment screen for binders to the bromodomains of BRD4 identified 2-methyl-3-ketopyrroles 1 and 2. Elaboration of these fragments guided by structure-based design provided lead molecules with significant activity in a mouse tumor model. Further modifications to the methylpyrrole core provided compounds with improved properties and enhanced activity in a mouse model of multiple myeloma.

Published

2017

45. HEXIM1 as a Robust Pharmacodynamic Marker for Monitoring Target Engagement of BET Family Bromodomain Inhibitors in Tumors and Surrogate Tissues

Author

Xiaoyu Lin, Tamar Uziel, Paul Hessler, Warren M. Kati, Daniel H. Albert, Lisa Roberts-Rapp, Yu Shen, Keith F. McDaniel, and Xiaoli Huang

Subjects

0301 basic medicine, Cancer Research, Biopsy, chemical and pharmacologic phenomena, Antineoplastic Agents, Biology, BET inhibitor, 03 medical and health sciences, Mice, In vivo, Cell Line, Tumor, Neoplasms, Animals, Cluster Analysis, Humans, Gene, Whole blood, Dose-Response Relationship, Drug, Gene Expression Profiling, Nuclear Proteins, RNA-Binding Proteins, hemic and immune systems, Xenograft Model Antitumor Assays, In vitro, Bromodomain, Gene expression profiling, Gene Expression Regulation, Neoplastic, Disease Models, Animal, 030104 developmental biology, Oncology, Organ Specificity, Immunology, Cancer cell, Cancer research, Female, Biomarkers, Transcription Factors

Abstract

An increasing number of BET family protein inhibitors have recently entered clinical trials. It has been reported that attempts of monitoring target engagement of the BET bromodomain inhibitor OTX015 using literature-described putative pharmacodynamic markers, such as c-Myc, BRD2, etc., failed to detect pharmacodynamic marker responses in AML patients treated at active dose and those with clinical responses. Here, we report the identification and characterization of HEXIM1 and other genes as robust pharmacodynamic markers for BET inhibitors. Global gene expression profiling studies were carried out using cancer cells and surrogate tissues, such as whole blood and skin, to identify genes that are modulated by BET family proteins. Candidate markers were further characterized for concentration- and time-dependent responses to the BET inhibitor ABBV-075 in vitro and in vivo. HEXIM1 was found to be the only gene that exhibited robust and consistent modulation by BET inhibitors across multiple cancer indications and surrogate tissues. Markers such as SERPINI1, ZCCHC24, and ZMYND8 were modulated by ABBV-075 and other BET inhibitors across cancer cell lines and xenograft tumors but not in blood and skin. Significant downregulation of c-Myc, a well-publicized target of BET inhibitors, was largely restricted to hematologic cancer cell lines. Incorporating well-characterized pharmacodynamic markers, such as HEXIM1 and other genes described here, can provide a better understanding of potential efficacy and toxicity associated with inhibiting BET family proteins and informs early clinical decisions on BET inhibitor development programs. Mol Cancer Ther; 16(2); 388–96. ©2016 AACR.

Published

2016

46. Vulnerability of Small-Cell Lung Cancer to Apoptosis Induced by the Combination of BET Bromodomain Proteins and BCL2 Inhibitors

Author

Lloyd T. Lam, Terry Magoc, Denise Wilcox, Michael J. Mitten, Xiaoyu Lin, Warren M. Kati, Tamar Uziel, Daniel H. Albert, Emily J. Faivre, Anahita Bhathena, Xiaoli Huang, Richard J. Bellin, Stephen K. Tahir, Yu Shen, Sha Jin, and Ziping Yang

Subjects

0301 basic medicine, Cancer Research, Lung Neoplasms, Pyridones, bcl-X Protein, Apoptosis, Mice, SCID, Biology, medicine.disease_cause, BET inhibitor, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, medicine, Biomarkers, Tumor, Animals, Humans, Lung cancer, neoplasms, Sulfonamides, Bcl-2-Like Protein 11, Venetoclax, Proteins, hemic and immune systems, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Molecular biology, Small Cell Lung Carcinoma, Xenograft Model Antitumor Assays, respiratory tract diseases, Bromodomain, 030104 developmental biology, Treatment Outcome, Oncology, chemistry, Proto-Oncogene Proteins c-bcl-2, Cell culture, 030220 oncology & carcinogenesis, Female, Growth inhibition, Carcinogenesis

Abstract

Ten percent to 15% of all lung cancers are small-cell lung cancer (SCLC). SCLC usually grows and metastasizes before it is diagnosed and relapses rapidly upon treatment. Unfortunately, no new targeted agent has been approved in the past 30 years for patients with SCLC. The BET (bromodomain and extraterminal) proteins bind acetylated histones and recruit protein complexes to promote transcription initiation and elongation. BET proteins have been shown to regulate expression of key genes in oncogenesis, such as MYC, CCND2, and BCL2L1. Here, we demonstrate that approximately 50% of SCLC cell lines are exquisitely sensitive to growth inhibition by the BET inhibitor, ABBV-075. The majority of these SCLC cell lines underwent apoptosis in response to ABBV-075 treatment via induction of caspase-3/7 activity. ABBV-075 enhanced the expression of proapoptotic protein BIM and downregulated antiapoptotic proteins BCL2 and BCLxl to a lesser extent. Furthermore, BET inhibition increased BCL2–BIM complex, thus priming the cells for apoptosis. Indeed, strong synergy was observed both in vitro and in vivo when cotreating the cells with BET inhibitor and the BH3-mimetic, BCL2 inhibitor venetoclax (ABT-199). ABBV-075 interaction with venetoclax positively correlated with BCL2 expression. Taken together, our studies provide a rationale for treating SCLC with BET and BCL2 inhibitors in tumors with high BCL2 protein expression. Mol Cancer Ther; 16(8); 1511–20. ©2017 AACR.

Published

2016

47. Preclinical Characterization of ABT-348, a Kinase Inhibitor Targeting the Aurora, Vascular Endothelial Growth Factor Receptor/Platelet-Derived Growth Factor Receptor, and Src Kinase Families

Author

Patrick A. Marcotte, Jun Guo, Michael R. Michaelides, Steven K. Davidsen, David R. Reuter, Junling Li, Yanping Luo, Lori J. Pease, Chris Tse, Terrance J. Magoc, Ru-Qi Wei, Paul Tapang, Eric F. Johnson, Cherrie K. Donawho, Zehan Chen, Amanda M. Olson, Donald J. Osterling, Daniel H. Albert, Michael L. Curtin, Keith B. Glaser, Jennifer J. Bouska, Mai H. Bui, and Robin R. Frey

Subjects

Male, Time Factors, Aminopyridines, Antineoplastic Agents, Mice, SCID, Protein Serine-Threonine Kinases, Histones, Mice, chemistry.chemical_compound, Growth factor receptor, Aurora Kinases, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells, Animals, Aurora Kinase B, Humans, Receptors, Platelet-Derived Growth Factor, Pharmacology, Mice, Inbred BALB C, Leukemia, Experimental, Dose-Response Relationship, Drug, Molecular Structure, biology, Phenylurea Compounds, Autophosphorylation, Xenograft Model Antitumor Assays, Molecular biology, Vascular endothelial growth factor, Vascular endothelial growth factor A, Receptors, Vascular Endothelial Growth Factor, src-Family Kinases, chemistry, NIH 3T3 Cells, biology.protein, Molecular Medicine, Female, Tyrosine kinase, Platelet-derived growth factor receptor, Proto-oncogene tyrosine-protein kinase Src

Abstract

ABT-348 [1-(4-(4-amino-7-(1-(2-hydroxyethyl)-1H-pyrazol-4-yl)thieno[3,2-c]pyridin-3-yl)phenyl)-3-(3-fluorophenyl)urea] is a novel ATP-competitive multitargeted kinase inhibitor with nanomolar potency (IC(50)) for inhibiting binding and cellular autophosphorylation of Aurora B (7 and 13 nM), C (1 and 13 nM), and A (120 and 189 nM). Cellular activity against Aurora B is reflected by inhibition of phosphorylation of histone H3, induction of polyploidy, and inhibition of proliferation of a variety of leukemia, lymphoma, and solid tumor cell lines (IC(50) = 0.3-21 nM). In vivo inhibition of Aurora B was confirmed in an engrafted leukemia model by observing a decrease in phosphorylation of histone H3 that persisted in a dose-dependent manner for 8 h and correlated with plasma concentration of ABT-348. Evaluation of ABT-348 across a panel of 128 kinases revealed additional potent binding activity (K(i) < 30 nM) against vascular endothelial growth factor receptor (VEGFR)/platelet-derived growth factor receptor (PDGFR) families and the Src family of cytoplasmic tyrosine kinases. VEGFR/PDGFR binding activity correlated with inhibition of autophosphorylation in cells and inhibition of vascular endothelial growth factor (VEGF)-stimulated endothelial cell proliferation (IC(50) ≤ 0.3 nM). Evidence of on-target activity in vivo was provided by the potency for blocking VEGF-mediated vascular permeability and inducing plasma placental growth factor. Activity against the Src kinase family was evident in antiproliferative activity against BCR-ABL chronic myeloid leukemia cells and cells expressing the gleevec-resistant BCR-ABL T315I mutation. On the basis of its unique spectrum of activity, ABT-348 was evaluated and found effective in representative solid tumor [HT1080 and pancreatic carcinoma (MiaPaCa), tumor stasis] and hematological malignancy (RS4;11, regression) xenografts. These results provide the rationale for clinical assessment of ABT-348 as a therapeutic agent in the treatment of cancer.

Published

2012

48. Abstract 4960: First-in-class, highly BDII-selective BET family inhibitor ABBV-744 displays potent anti-tumor activity in androgen receptor positive prostate cancer models and an improved tolerability profile

Author

Vasudha Sehgal, Xin Lu, Yu Shen, Tamar Uziel, Keith F. McDaniel, Warren M. Kati, Mai Ha-Bui, Emily J. Faivre, Gaurav Mehta, Paul Hessler, Denise Wilcox, and Daniel H. Albert

Subjects

0301 basic medicine, Cancer Research, BRD4, 010405 organic chemistry, business.industry, Androgen Receptor Positive, medicine.disease, 01 natural sciences, 0104 chemical sciences, Bromodomain, Androgen receptor, BET inhibitor, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 030104 developmental biology, Oncology, chemistry, LNCaP, Cancer research, Enzalutamide, Medicine, business

Abstract

First generation BET inhibitors, including ABBV-075, bind with nearly equimolar affinity to two highly conserved bromodomains (BDI and BDII) in the N-terminus of BRD2, BRD3, BRD4, and BRDt. These “pan” inhibitors compete with the natural acetylated lysine substrates of BDI and BDII to displace BET family proteins from chromatin. In so doing, pan-BET inhibitors generally block transcription and induce potent anti-tumor activity across a wide range of pre-clinical models. Consequently, numerous phase I clinical trials have been initiated with pan-BET inhibitors. The initial reports of responses in the leading indication of AML have been encouraging; however, thrombocytopenia and other dose limiting toxicities may prevent realization of a therapeutic dose in most solid tumor indications. We hypothesized that selective inhibition of BDII but not BDI of BET family proteins would improve tolerability while retaining efficacy. Medicinal chemistry efforts produced ABBV-744, a potent inhibitor specific for BDII of BRD2/3/4, with >250x differential binding preference for BDII over BDI and excellent drug-like properties. In striking contrast to the broad range of cell growth inhibition effected by pan BET inhibitor ABBV-075, BDII-selective ABBV-744 anti-proliferative activity was largely but not exclusively restricted to AML and androgen receptor (AR) positive prostate cancer cell line models, including models of Enzalutamide resistance. RNA-Seq and qPCR revealed that ABBV-744 was a potent and selective inhibitor of the AR transcription pathway. ChIP-Seq and ChIP-qPCR revealed a BDII-inhibitor displacement of BRD4 from AR-occupied enhancers and promoters, consistent with a BRD4 BDII-specific dependency of AR to sustain an oncogenic gene expression program. In vivo, doses of ABBV-744 at fractions of its MTD in LNCaP and MDA-PCa-2b xenograft models induced tumor growth inhibition that was comparable to that observed with ABBV-075 when dosed at its MTD. Together, these in vitro and in vivo results provide proof of concept that selective BDII BET family inhibitors may have improved tolerability relative to pan-BET inhibitors while maintaining tumor growth inhibition in AR positive prostate cancer. The design, study conduct, and financial support for this research were provided by AbbVie. AbbVie participated in the interpretation of data, review, and approval of the publication. Citation Format: Emily J. Faivre, Denise Wilcox, Mai Ha-Bui, Paul Hessler, Vasudha Sehgal, Xin Lu, Tamar Uziel, Gaurav Mehta, Daniel H. Albert, Keith McDaniel, Warren Kati, Yu Shen. First-in-class, highly BDII-selective BET family inhibitor ABBV-744 displays potent anti-tumor activity in androgen receptor positive prostate cancer models and an improved tolerability profile [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 4960.

Published

2018

49. Abstract 1150: Acute myeloid leukemia human/mouse co-clinical trial feasibility study optimized in human transgenic IL-3/GMCSF NOD/Shi-scid-IL2rγnull mice

Author

Michael Boyiadzis, Kathleen A. Dorritie, Jenny Rowe, Keith F. McDaniel, Regina F Gandour-Edwards, Neal Goodwin, Warren M. Kati, David J. Frost, Angela M. Davies, Mark D. McKee, Daniel H. Albert, Maria Cecilia Mancini, and Gerold Feuer

Subjects

Cancer Research, business.industry, CD33, Myeloid leukemia, Cancer, Nod, medicine.disease, Peripheral blood mononuclear cell, medicine.anatomical_structure, Oncology, Immunology, Splenocyte, Cytarabine, medicine, Bone marrow, business, medicine.drug

Abstract

Acute myeloid leukemia (AML) co-clinical modeling has been optimized with peripheral blood mononuclear cells (PBMCs) collected from low volume (14 mL) patient samples to establish an algorithm for efficiently co-clinically modeling AML patients. Methods: PBMCs were ficoll gradient purified and viably cryopreserved. Intrahepatic (i.h.) inoculation of AML PBMCs in neonate NOD/Shi-scid-IL2rγnull (NOG) mice and intravenous (i.v.) inoculation in both juvenile NOG mice and juvenile human transgenic IL-3/GMCSF NOD/Shi-scid-IL2rγnull mice (NOG-EXL) were evaluated. Bone marrow (BM) aspirates, splenocytes and PBMCs from mice were evaluated by fluorescence-activated cell sorting (FACS) at 12 weeks post AML inoculation for engraftment as determined by % ratio of human CD33+ cells to total CD45+ cells (human + murine cells). Humerus bones from inoculated animals were also evaluated by human CD33 immunohistochemistry (IHC). Results: Cells from 2/6 AML patient samples (CTG-2224 and CTG-2357) successfully engrafted into neonate mice. Animals were dosed with vehicle, cytarabine, ABBV-075 (clinical trial-staged BET family bromodomain (BD) inhibitor), or ABBV-744 (a preclinical BDII selective inhibitor) and evaluated for tumor burden six weeks post drug treatment initiation. ABBV-075 and ABBV-744 treated animals had lower tumor burden in the CTG-2224 model, 17% (p Citation Format: Neal C. Goodwin, Daniel H. Albert, Angela M. Davies, Jenny Rowe, Gerold Feuer, Michael Boyiadzis, Kathleen A. Dorritie, Maria Mancini, Regina Gandour-Edwards, Warren M. Kati, Mark D. McKee, Keith F. McDaniel, David J. Frost. Acute myeloid leukemia human/mouse co-clinical trial feasibility study optimized in human transgenic IL-3/GMCSF NOD/Shi-scid-IL2rγnull mice [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 1150.

Published

2018

50. Abstract 800: ABBV-744, a first-in-class and highly selective inhibitor of the second bromodomain of BET family proteins, displays robust activities in preclinical models of acute myelogenous leukemia

Author

Xiaoli Huang, Terrance J. Magoc, Debra Ferguson, Emily J. Faivre, Xiaoyu Lin, Paul Hessler, Richard J. Bellin, Warren M. Kati, Daniel H. Albert, Lloyd T. Lam, Mai Ha Bui, Tamar Uziel, Denise Wilcox, Keith F. McDaniel, and Yu Shen

Subjects

0301 basic medicine, Cancer Research, BRD4, business.industry, Cancer, medicine.disease, Bromodomain, BET inhibitor, 03 medical and health sciences, Leukemia, Myelogenous, Prostate cancer, 030104 developmental biology, Oncology, Tolerability, Cancer research, Medicine, business

Abstract

Many small-molecule inhibitors that target both bromodomains of the BET family proteins (pan BET inhibitors) are undergoing studies in clinical trials. Emerging data are beginning to suggest that clinical responses to these pan BET inhibitors in subsets of hematologic malignancies may be modest and short lived, perhaps due, at least in part, to tolerability issues that limit dosing levels. We hypothesized that selective inhibition of four of the eight bromodomains in BET family proteins might retain the anticancer activities in certain tumor subsets while alleviating some of the tolerability liabilities of pan BET inhibitors, thus possibly providing better therapeutic benefits. ABBV-744 is a highly selective inhibitor for the second bromodomain (BDII) of the four BET family proteins, exhibiting greater than 300-fold more potent binding affinity to the BDII bromodomain of BRD4 relative to the first bromodomain (BDI) of BRD4. In contrast to the broad antiproliferative activities observed with pan BET inhibitors, ABBV-744 only displayed significant antiproliferative activities in a limited number of cancer cell lines, including AML and androgen receptor (AR)-positive prostate cancer. Studies in AML xenograft models demonstrated antitumor efficacy for ABBV-744 that was comparable to the pan-BET inhibitor ABBV-075 but with improved tolerability. Taken together, these results suggest that ABBV-744 could be a promising second-generation BET inhibitor for AML therapy. Affiliation: Oncology Discovery, AbbVie Inc., 1 North Waukegan Rd., North Chicago, IL 60064. Disclosures: All authors are employees of AbbVie. The design, study conduct, and financial support for this research were provided by AbbVie. AbbVie participated in the interpretation of data, review, and approval of the publication. Citation Format: Xiaoyu Lin, Xiaoli Huang, Richard Bellin, Emily Faivre, Paul Hessler, Lloyd Lam, Mai Ha Bui, Denise Wilcox, Tamar Uziel, Debra C. Ferguson, Terrance J. Magoc, Daniel H. Albert, Keith F. McDaniel, Warren Kati, Yu Shen. ABBV-744, a first-in-class and highly selective inhibitor of the second bromodomain of BET family proteins, displays robust activities in preclinical models of acute myelogenous leukemia [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 800.

Published

2018