Your search keyword '"Stephen K. Tahir"' showing total 72 results

1. Potential mechanisms of resistance to venetoclax and strategies to circumvent it

Author

Stephen K. Tahir, Morey L. Smith, Paul Hessler, Lisa Roberts Rapp, Kenneth B. Idler, Chang H. Park, Joel D. Leverson, and Lloyd T. Lam

Subjects

BCL-2, BCL-XL, MCL-1, Apoptosis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Venetoclax (ABT-199), a first-in-class orally bioavailable BCL-2-selective inhibitor, was recently approved by the FDA for use in patients with 17p-deleted chronic lymphocytic leukemia who have received prior therapy. It is also being evaluated in numerous clinical trials for treating patients with various hematologic malignancies. As with any targeted cancer therapy, it is critically important to identify potential mechanisms of resistance, both for patient stratification and developing strategies to overcome resistance, either before it develops or as it emerges. Methods In order to gain a more comprehensive insight into the nature of venetoclax resistance mechanisms, we evaluated the changes in the BCL-2 family members at the genetic and expression levels in seven different venetoclax-resistant derived leukemia and lymphoma cell lines. Results Gene and protein expression analyses identified a number of different alterations in the expression of pro- and anti-apoptotic BCL-2 family members. In the resistant derived cells, an increase in either or both the anti-apoptotic proteins BCL-XL or MCL-1, which are not targeted by venetoclax was observed, and either concomitant or exclusive with a decrease in one or more pro-apoptotic proteins. In addition, mutational analysis also revealed a mutation in the BH3 binding groove (F104L) that could potentially interfere with venetoclax-binding. Not all changes may be causally related to venetoclax resistance and may only be an epiphenomenon. For resistant cell lines showing elevations in BCL-XL or MCL-1, strong synergistic cell killing was observed when venetoclax was combined with either BCL-XL- or MCL-1-selective inhibitors, respectively. This highlights the importance of BCL-XL- and MCL-1 as causally contributing to venetoclax resistance. Conclusions Overall our study identified numerous changes in multiple resistant lines; the changes were neither mutually exclusive nor universal across the cell lines tested, thus exemplifying the complexity and heterogeneity of potential resistance mechanisms. Identifying and evaluating their contribution has important implications for both patient selection and the rational development of strategies to overcome resistance.

Published

2017

2. Rapid Colchicine Competition-Binding Scintillation Proximity Assay Using Biotin-Labeled Tubulin

Author

Stephen K. Tahir, Peter Kovar, Saul H. Rosenberg, and Shi-Chung Ng

Subjects

Biology (General), QH301-705.5

Abstract

We have developed a rapid [3H] colchicine competition-binding scintillation proximity assay (SPA) to evaluate antimitotic compounds that bind to the colchicine-binding site on tubulin. The premise of our assay is that compounds will compete with radiolabeled colchicine for the tubulin-binding domain. Biotin-labeled tubulin is incubated first with unlabeled compound and radiolabeled ligand. Streptavidin-labeled SPA beads are added, and the radiolabel associated with tubulin is directly counted with no separation steps. Under our experimental conditions, the dissociation constant of binding (Kd) for colchicine to tubulin was determined to be 1.4 μM, which was consistent with previously reported values. Assay validation was performed by competitively inhibiting [3H] colchicine binding to tubulin with known microtubule inhibitors and comparing their inhibition constants (Ki). Our SPA bead method is a powerful tool since it overcomes the disadvantage of traditional filtration techniques, as there are no separation steps. It is extremely easy to set up, multiple samples can be assayed and supply and labor costs are reduced because of the minimal volume and test reagents used.

Published

2000

3. Down-regulation of Survivin by Antisense Oligonucleotides Increases Apoptosis, Inhibits Cytokinesis and Anchorage-Independent Growth

Author

Jun Chen, Wei Wu, Stephen K. Tahir, Paul E. Kroeger, Saul H. Rosenberg, Lex M. Cowsert, Frank Bennett, Stanislaw Krajewski, Maryla Krajewska, Kate Welsh, John C. Reed, and Shi-Chung Ng

Subjects

survivin, apoptosis, antisense, oligonucleotides, cytokinesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Survivin, a member of the inhibitor of apoptosis protein (IAP) family, is detected in most common human cancers but not in adjacent normal cells. Previous studies suggest that survivin associates with the mitotic spindle and directly inhibits caspase activity. To further investigate the function of survivin, we used a survivin antisense (AS) oligonucleotide to downregulate survivin expression in normal and cancer cells. We found that inhibition of survivin expression increased apoptosis and polyploidy while decreasing colony formation in soft agar. Immunohistochemistry showed that cells without survivin can initiate the cleavage furrow and contractile ring, but cannot complete cytokinesis, thus resulting in multinucleated cells. These findings indicate that survivin plays important roles in a late stage of cytokinesis, as well as in apoptosis.

Published

2000

4. Activity of eftozanermin alfa plus venetoclax in preclinical models and patients with acute myeloid leukemia

Author

Stephen K. Tahir, Emiliano Calvo, Benedito A. Carneiro, Junichiro Yuda, Aditya Shreenivas, Mojca Jongen-Lavrencic, Eelke Gort, Kenichi Ishizawa, Daniel Morillo, Carla Biesdorf, Morey Smith, Dong Cheng, Monica Motwani, David Sharon, Tamar Uziel, Dimple A. Modi, Fritz G. Buchanan, Susan Morgan-Lappe, Bruno C. Medeiros, Darren C. Phillips, and Hematology

Subjects

SDG 3 - Good Health and Well-being, Immunology, Cell Biology, Hematology, Biochemistry

Abstract

Activation of apoptosis in malignant cells is an established strategy for controlling cancer and is potentially curative. To assess the impact of concurrently inducing the extrinsic and intrinsic apoptosis-signaling pathways in acute myeloid leukemia (AML), we evaluated activity of the TRAIL receptor agonistic fusion protein eftozanermin alfa (eftoza; ABBV-621) in combination with the B-cell lymphoma protein-2 selective inhibitor venetoclax in preclinical models and human patients. Simultaneously stimulating intrinsic and extrinsic apoptosis-signaling pathways with venetoclax and eftoza, respectively, enhanced their activities in AML cell lines and patient-derived ex vivo/in vivo models. Eftoza activity alone or plus venetoclax required death receptor 4/5 (DR4/DR5) expression on the plasma membrane but was independent of TP53 or FLT3-ITD status. The safety/tolerability of eftoza as monotherapy and in combination with venetoclax was demonstrated in patients with relapsed/refractory AML in a phase 1 clinical trial. Treatment-related adverse events were reported in 2 of 4 (50%) patients treated with eftoza monotherapy and 18 of 23 (78%) treated with eftoza plus venetoclax. An overall response rate of 30% (7/23; 4 complete responses [CRs], 2 CRs with incomplete hematologic recovery, and 1 morphologic leukemia-free state) was reported in patients who received treatment with eftoza plus venetoclax and 67% (4/6) in patients with myoblasts positive for DR4/DR5 expression; no tumor responses were observed with eftoza monotherapy. These data indicate that combination therapy with eftoza plus venetoclax to simultaneously activate the extrinsic and intrinsic apoptosis-signaling pathways may improve clinical benefit compared with venetoclax monotherapy in relapsed/refractory AML with an acceptable toxicity profile. This trial was registered at www.clinicaltrials.gov as #NCT03082209.

Published

2023

5. Supplementary Table S3 from Integrative Genomic Analysis of Small-Cell Lung Carcinoma Reveals Correlates of Sensitivity to Bcl-2 Antagonists and Uncovers Novel Chromosomal Gains

Author

Dimitri Semizarov, Rick Lesniewski, Guido Sauter, Stephen K. Tahir, Gang Wang, Mark G. Anderson, Charles Van Sant, and Edward T. Olejniczak

Abstract

Supplementary Table S3 from Integrative Genomic Analysis of Small-Cell Lung Carcinoma Reveals Correlates of Sensitivity to Bcl-2 Antagonists and Uncovers Novel Chromosomal Gains

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 Figure 2 from The Bcl-2/Bcl-XL/Bcl-w Inhibitor, Navitoclax, Enhances the Activity of Chemotherapeutic Agents In Vitro and In Vivo

Author

Steven W. Elmore, Chris Tse, Joel D. Leverson, Deepak Sampath, Heather Maecker, Saul H. Rosenberg, Scott L. Ackler, Haichao Zhang, Stephen K. Tahir, Alexander R. Shoemaker, Yu Shen, Morey Smith, Xiaoyu Lin, Paul Nimmer, Michael J. Mitten, Bernard Liu, Xiaoli Huang, Vivek Abraham, Sha Jin, and Jun Chen

Abstract

PDF file - 40K

Published

2023

8. Supplementary Figure 1 from The Bcl-2/Bcl-XL/Bcl-w Inhibitor, Navitoclax, Enhances the Activity of Chemotherapeutic Agents In Vitro and In Vivo

Author

Steven W. Elmore, Chris Tse, Joel D. Leverson, Deepak Sampath, Heather Maecker, Saul H. Rosenberg, Scott L. Ackler, Haichao Zhang, Stephen K. Tahir, Alexander R. Shoemaker, Yu Shen, Morey Smith, Xiaoyu Lin, Paul Nimmer, Michael J. Mitten, Bernard Liu, Xiaoli Huang, Vivek Abraham, Sha Jin, and Jun Chen

Abstract

PDF file - 78K

Published

2023

9. Data from Integrative Genomic Analysis of Small-Cell Lung Carcinoma Reveals Correlates of Sensitivity to Bcl-2 Antagonists and Uncovers Novel Chromosomal Gains

Author

Dimitri Semizarov, Rick Lesniewski, Guido Sauter, Stephen K. Tahir, Gang Wang, Mark G. Anderson, Charles Van Sant, and Edward T. Olejniczak

Abstract

Cancer is a highly heterogeneous disease in terms of the genetic profile and the response to therapeutics. An early identification of a genomic marker in drug discovery may help select patients that would respond to treatment in clinical trials. Here we suggest coupling compound screening with comparative genomic hybridization analysis of the model systems for early discovery of genomic biomarkers. A Bcl-2 antagonist, ABT-737, has recently been discovered and shown to induce regression of solid tumors, but its activity is limited to a fraction of small-cell lung carcinoma (SCLC) models tested. We used comparative genomic hybridization on high-density single-nucleotide polymorphism genotyping arrays to carry out a genome-wide analysis of 23 SCLC cell lines sensitive and resistant to ABT-737. The screen revealed a number of novel recurrent gene copy number abnormalities, which were also found in an independent data set of 19 SCLC tumors and confirmed by real-time quantitative PCR. A previously unknown amplification was identified on 18q and associated with the sensitivity of SCLC cell lines to ABT-737 and another Bcl-2 antagonist. The region of gain contains Bcl-2 and NOXA, two apoptosis-related genes. Expression microarray profiling showed that the genes residing in the amplified region of 18q are also overexpressed in the sensitive lines relative to the resistant lines. Fluorescence in situ hybridization analysis of tumors revealed that Bcl-2 gain is a frequent event in SCLC. Our findings suggest that 18q21-23 copy number will be a clinically relevant predictor for sensitivity of SCLC to Bcl-2 family inhibitors. The 18q21-23 genomic marker may have a broader application in cancer because Bcl-2 is associated with apoptosis evasion and chemoresistance. (Mol Cancer Res 2007;5(4):331–39)

Published

2023

10. Supplementary Table 1, Figure Legends 1-2 from The Bcl-2/Bcl-XL/Bcl-w Inhibitor, Navitoclax, Enhances the Activity of Chemotherapeutic Agents In Vitro and In Vivo

Author

Steven W. Elmore, Chris Tse, Joel D. Leverson, Deepak Sampath, Heather Maecker, Saul H. Rosenberg, Scott L. Ackler, Haichao Zhang, Stephen K. Tahir, Alexander R. Shoemaker, Yu Shen, Morey Smith, Xiaoyu Lin, Paul Nimmer, Michael J. Mitten, Bernard Liu, Xiaoli Huang, Vivek Abraham, Sha Jin, and Jun Chen

Abstract

PDF file - 77K

Published

2023

11. 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

12. Data from Identification of Expression Signatures Predictive of Sensitivity to the Bcl-2 Family Member Inhibitor ABT-263 in Small Cell Lung Carcinoma and Leukemia/Lymphoma Cell Lines

Author

Mark G. Anderson, Saul H. Rosenberg, Christin Tse, Paul E. Kroeger, Steve W. Elmore, Haichao Zhang, Paul Hessler, Viswanath Devanarayan, Mary K. Joseph, John Wass, and Stephen K. Tahir

Abstract

ABT-263 inhibits the antiapoptotic proteins Bcl-2, Bcl-xL, and Bcl-w and has single-agent efficacy in numerous small cell lung carcinoma (SCLC) and leukemia/lymphoma cell lines in vitro and in vivo. It is currently in clinical trials for treating patients with SCLC and various leukemia/lymphomas. Identification of predictive markers for response will benefit the clinical development of ABT-263. We identified the expression of Bcl-2 family genes that correlated best with sensitivity to ABT-263 in a panel of 36 SCLC and 31 leukemia/lymphoma cell lines. In cells sensitive to ABT-263, expression of Bcl-2 and Noxa is elevated, whereas expression of Mcl-1 is higher in resistant cells. We also examined global expression differences to identify gene signature sets that correlated with sensitivity to ABT-263 to generate optimal signature sets predictive of sensitivity to ABT-263. Independent cell lines were used to verify the predictive power of the gene sets and to refine the optimal gene signatures. When comparing normal lung tissue and SCLC primary tumors, the expression pattern of these genes in the tumor tissue is most similar to sensitive SCLC lines, whereas normal tissue is most similar to resistant SCLC lines. Most of the genes identified using global expression patterns are related to the apoptotic pathway; however, all but Bcl-rambo are distinct from the Bcl-2 family. This study leverages global expression data to identify key gene expression patterns for sensitivity to ABT-263 in SCLC and leukemia/lymphoma and may provide guidance in the selection of patients in future clinical trials. Mol Cancer Ther; 9(3); 545–57

Published

2023

13. Data from Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors

Author

Susan E. Morgan-Lappe, Bruce Trela, Nandini Rudra-Ganguly, Xin Lu, Enrico DiGiammarino, Li Zhou, Zhihong Liu, Nan Xu, Vivek C. Abraham, Deborah Widomski, Haichao Zhang, Morey L. Smith, Stephen K. Tahir, John Xue, Yu Xiao, Larry R. Solomon, Dong Cheng, Fritz G. Buchanan, and Darren C. Phillips

Abstract

TRAIL can activate cell surface death receptors, resulting in potent tumor cell death via induction of the extrinsic apoptosis pathway. Eftozanermin alfa (ABBV-621) is a second generation TRAIL receptor agonist engineered as an IgG1-Fc mutant backbone linked to two sets of trimeric native single-chain TRAIL receptor binding domain monomers. This hexavalent agonistic fusion protein binds to the death-inducing DR4 and DR5 receptors with nanomolar affinity to drive on-target biological activity with enhanced caspase-8 aggregation and death-inducing signaling complex formation independent of FcγR-mediated cross-linking, and without clinical signs or pathologic evidence of toxicity in nonrodent species. ABBV-621 induced cell death in approximately 36% (45/126) of solid cancer cell lines in vitro at subnanomolar concentrations. An in vivo patient-derived xenograft (PDX) screen of ABBV-621 activity across 15 different tumor indications resulted in an overall response (OR) of 29% (47/162). Although DR4 (TNFSFR10A) and/or DR5 (TNFSFR10B) expression levels did not predict the level of response to ABBV-621 activity in vivo, KRAS mutations were associated with elevated TNFSFR10A and TNFSFR10B and were enriched in ABBV-621–responsive colorectal carcinoma PDX models. To build upon the OR of ABBV-621 monotherapy in colorectal cancer (45%; 10/22) and pancreatic cancer (35%; 7/20), we subsequently demonstrated that inherent resistance to ABBV-621 treatment could be overcome in combination with chemotherapeutics or with selective inhibitors of BCL-XL. In summary, these data provide a preclinical rationale for the ongoing phase 1 clinical trial (NCT03082209) evaluating the activity of ABBV-621 in patients with cancer.Significance:This study describes the activity of a hexavalent TRAIL-receptor agonistic fusion protein in preclinical models of solid tumors that mechanistically distinguishes this molecular entity from other TRAIL-based therapeutics.

Published

2023

14. Supplementary Data from Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors

Author

Susan E. Morgan-Lappe, Bruce Trela, Nandini Rudra-Ganguly, Xin Lu, Enrico DiGiammarino, Li Zhou, Zhihong Liu, Nan Xu, Vivek C. Abraham, Deborah Widomski, Haichao Zhang, Morey L. Smith, Stephen K. Tahir, John Xue, Yu Xiao, Larry R. Solomon, Dong Cheng, Fritz G. Buchanan, and Darren C. Phillips

Abstract

Supplementary file containing all supplementary figures and tables

Published

2023

15. Supplementary Table 1 from A Small-Molecule Inhibitor of Bcl-XL Potentiates the Activity of Cytotoxic Drugs In vitro and In vivo

Author

Steven W. Elmore, Saul H. Rosenberg, Stephen W. Fesik, Haichao Zhang, Robert Warner, Baole Wang, Stephen K. Tahir, Jason Stavropoulos, Wang Shen, Weiguo Qing, Tilman Oltersdorf, Jacqueline M. O'Connor, Paul Nimmer, ShiChung Ng, Hugh Nellans, William McClellan, Kennan Marsh, Mary K. Joseph, Ken Jarvis, David J. Frost, Thomas Deckwirth, Milan Bruncko, Tony Borre, Barbara A. Belli, Joy Bauch, Anatol Oleksijew, and Alex R. Shoemaker

Abstract

Supplementary Table 1 from A Small-Molecule Inhibitor of Bcl-XL Potentiates the Activity of Cytotoxic Drugs In vitro and In vivo

Published

2023

16. Supplementary Tables 1-2 from Influence of Bcl-2 Family Members on the Cellular Response of Small-Cell Lung Cancer Cell Lines to ABT-737

Author

Christin Tse, Saul H. Rosenberg, Steve W. Elmore, Stephen W. Fesik, Shi-Chung Ng, Robert B. Warner, Jun Chen, Aparna V. Sarthy, Susan E. Morgan-Lappe, Mark G. Anderson, Xiufen Yang, and Stephen K. Tahir

Abstract

Supplementary Tables 1-2 from Influence of Bcl-2 Family Members on the Cellular Response of Small-Cell Lung Cancer Cell Lines to ABT-737

Published

2023

17. Data from A Small-Molecule Inhibitor of Bcl-XL Potentiates the Activity of Cytotoxic Drugs In vitro and In vivo

Author

Steven W. Elmore, Saul H. Rosenberg, Stephen W. Fesik, Haichao Zhang, Robert Warner, Baole Wang, Stephen K. Tahir, Jason Stavropoulos, Wang Shen, Weiguo Qing, Tilman Oltersdorf, Jacqueline M. O'Connor, Paul Nimmer, ShiChung Ng, Hugh Nellans, William McClellan, Kennan Marsh, Mary K. Joseph, Ken Jarvis, David J. Frost, Thomas Deckwirth, Milan Bruncko, Tony Borre, Barbara A. Belli, Joy Bauch, Anatol Oleksijew, and Alex R. Shoemaker

Abstract

Inhibition of the prosurvival members of the Bcl-2 family of proteins represents an attractive strategy for the treatment of cancer. We have previously reported the activity of ABT-737, a potent inhibitor of Bcl-2, Bcl-XL, and Bcl-w, which exhibits monotherapy efficacy in xenograft models of small-cell lung cancer and lymphoma and potentiates the activity of numerous cytotoxic agents. Here we describe the biological activity of A-385358, a small molecule with relative selectivity for binding to Bcl-XL versus Bcl-2 (Ki's of 0.80 and 67 nmol/L for Bcl-XL and Bcl-2, respectively). This compound efficiently enters cells and co-localizes with the mitochondrial membrane. Although A-385358 shows relatively modest single-agent cytotoxic activity against most tumor cell lines, it has an EC50 of L for survival. In addition, A-385358 enhances the in vitro cytotoxic activity of numerous chemotherapeutic agents (paclitaxel, etoposide, cisplatin, and doxorubicin) in several tumor cell lines. In A549 non–small-cell lung cancer cells, A-385358 potentiates the activity of paclitaxel by as much as 25-fold. Importantly, A-385358 also potentiated the activity of paclitaxel in vivo. Significant inhibition of tumor growth was observed when A-385358 was added to maximally tolerated or half maximally tolerated doses of paclitaxel in the A549 xenograft model. In tumors, the combination therapy also resulted in a significant increase in mitotic arrest followed by apoptosis relative to paclitaxel monotherapy. (Cancer Res 2006; 66(17): 8731-9)

Published

2023

18. Supplementary Methods, Figures 1-7, Tables 1-2 from ABT-263: A Potent and Orally Bioavailable Bcl-2 Family Inhibitor

Author

Steven W. Elmore, Saul H. Rosenberg, Stephen Fesik, Haichao Zhang, Xiufen Yang, Yu Xiao, Stephen K. Tahir, Lisa Roberts, Paul Nimmer, Michael J. Mitten, Kennan C. Marsh, Eric F. Johnson, Sha Jin, Jun Chen, Mark G. Anderson, Jessica Adickes, Alexander R. Shoemaker, and Christin Tse

Abstract

Supplementary Methods, Figures 1-7, Tables 1-2 from ABT-263: A Potent and Orally Bioavailable Bcl-2 Family Inhibitor

Published

2023

19. Data from Influence of Bcl-2 Family Members on the Cellular Response of Small-Cell Lung Cancer Cell Lines to ABT-737

Author

Christin Tse, Saul H. Rosenberg, Steve W. Elmore, Stephen W. Fesik, Shi-Chung Ng, Robert B. Warner, Jun Chen, Aparna V. Sarthy, Susan E. Morgan-Lappe, Mark G. Anderson, Xiufen Yang, and Stephen K. Tahir

Abstract

ABT-737 is a novel and potent Bcl-2 antagonist with single-agent activity against small-cell lung cancer (SCLC) cell lines. Here, we evaluated the contribution of Bcl-2 family members to the in vitro cellular response of several SCLC cell lines to ABT-737. Relatively higher levels of Bcl-2, Bcl-XL, Bim and Noxa, and lower levels of Mcl-1 characterized naïve SCLC cell lines that were sensitive to ABT-737. Conversely, a progressive decrease in the relative levels of Bcl-2 and Noxa and a progressive increase in Mcl-1 levels characterized the increased resistance of H146 cells following chronic exposure to ABT-737. Knockdown of Mcl-1 with small interfering RNA sensitized two resistant SCLC cell lines H196 and DMS114 to ABT-737 by enhancing the induction of apoptosis. Likewise, up-regulation of Noxa sensitized H196 cells to ABT-737. Combination treatment with DNA-damaging agents was extremely synergistic with ABT-737 and was associated with the down-regulation of Mcl-1 and the up-regulation of Noxa, Puma, and Bim in H196 cells. Thus, SCLC cells sensitive to ABT-737 expressed the target proteins Bcl-2 and Bcl-XL, whereas Mcl-1 and factors regulating Mcl-1 function seem to contribute to the overall resistance of SCLC cells to ABT-737. Overall, these observations provide further insight as to the mechanistic bases for ABT-737 efficacy in SCLC and will be helpful for profiling patients and aiding in the rational design of combination therapies. [Cancer Res 2007;67(3):1176–83]

Published

2023

20. Data from ABT-263: A Potent and Orally Bioavailable Bcl-2 Family Inhibitor

Author

Steven W. Elmore, Saul H. Rosenberg, Stephen Fesik, Haichao Zhang, Xiufen Yang, Yu Xiao, Stephen K. Tahir, Lisa Roberts, Paul Nimmer, Michael J. Mitten, Kennan C. Marsh, Eric F. Johnson, Sha Jin, Jun Chen, Mark G. Anderson, Jessica Adickes, Alexander R. Shoemaker, and Christin Tse

Abstract

Overexpression of the prosurvival Bcl-2 family members (Bcl-2, Bcl-xL, and Mcl-1) is commonly associated with tumor maintenance, progression, and chemoresistance. We previously reported the discovery of ABT-737, a potent, small-molecule Bcl-2 family protein inhibitor. A major limitation of ABT-737 is that it is not orally bioavailable, which would limit chronic single agent therapy and flexibility to dose in combination regimens. Here we report the biological properties of ABT-263, a potent, orally bioavailable Bad-like BH3 mimetic (Ki's of c release, and subsequent apoptosis. Oral administration of ABT-263 alone induces complete tumor regressions in xenograft models of small-cell lung cancer and acute lymphoblastic leukemia. In xenograft models of aggressive B-cell lymphoma and multiple myeloma where ABT-263 exhibits modest or no single agent activity, it significantly enhances the efficacy of clinically relevant therapeutic regimens. These data provide the rationale for clinical trials evaluating ABT-263 in small-cell lung cancer and B-cell malignancies. The oral efficacy of ABT-263 should provide dosing flexibility to maximize clinical utility both as a single agent and in combination regimens. [Cancer Res 2008;68(9):3421–8]

Published

2023

21. 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

22. Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors

Author

Deborah Widomski, Vivek C. Abraham, Darren C. Phillips, Fritz G. Buchanan, Zhihong Liu, Stephen K. Tahir, Haichao Zhang, John Xue, Nandini Rudra-Ganguly, Xin Lu, Dong Cheng, Enrico L. Digiammarino, Morey L. Smith, Yu Xiao, Larry R. Solomon, Susan E. Morgan-Lappe, Bruce Trela, Nan Xu, and Li Zhou

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, Recombinant Fusion Proteins, Cell, Antineoplastic Agents, Apoptosis, Mice, SCID, Factor IX, TNF-Related Apoptosis-Inducing Ligand, Mice, 03 medical and health sciences, 0302 clinical medicine, Mice, Inbred NOD, In vivo, Tumor Cells, Cultured, medicine, Animals, Humans, Receptor, Cell Proliferation, Chemistry, Cancer, Biological activity, medicine.disease, Xenograft Model Antitumor Assays, Fusion protein, Immunoglobulin Fc Fragments, Pancreatic Neoplasms, Receptors, TNF-Related Apoptosis-Inducing Ligand, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, Colorectal Neoplasms

Abstract

TRAIL can activate cell surface death receptors, resulting in potent tumor cell death via induction of the extrinsic apoptosis pathway. Eftozanermin alfa (ABBV-621) is a second generation TRAIL receptor agonist engineered as an IgG1-Fc mutant backbone linked to two sets of trimeric native single-chain TRAIL receptor binding domain monomers. This hexavalent agonistic fusion protein binds to the death-inducing DR4 and DR5 receptors with nanomolar affinity to drive on-target biological activity with enhanced caspase-8 aggregation and death-inducing signaling complex formation independent of FcγR-mediated cross-linking, and without clinical signs or pathologic evidence of toxicity in nonrodent species. ABBV-621 induced cell death in approximately 36% (45/126) of solid cancer cell lines in vitro at subnanomolar concentrations. An in vivo patient-derived xenograft (PDX) screen of ABBV-621 activity across 15 different tumor indications resulted in an overall response (OR) of 29% (47/162). Although DR4 (TNFSFR10A) and/or DR5 (TNFSFR10B) expression levels did not predict the level of response to ABBV-621 activity in vivo, KRAS mutations were associated with elevated TNFSFR10A and TNFSFR10B and were enriched in ABBV-621–responsive colorectal carcinoma PDX models. To build upon the OR of ABBV-621 monotherapy in colorectal cancer (45%; 10/22) and pancreatic cancer (35%; 7/20), we subsequently demonstrated that inherent resistance to ABBV-621 treatment could be overcome in combination with chemotherapeutics or with selective inhibitors of BCL-XL. In summary, these data provide a preclinical rationale for the ongoing phase 1 clinical trial (NCT03082209) evaluating the activity of ABBV-621 in patients with cancer. Significance: This study describes the activity of a hexavalent TRAIL-receptor agonistic fusion protein in preclinical models of solid tumors that mechanistically distinguishes this molecular entity from other TRAIL-based therapeutics.

Published

2021

23. Discovery of A-1331852, a First-in-Class, Potent, and Orally-Bioavailable BCL-XL Inhibitor

Author

Paul Nimmer, Erwin R. Boghaert, Robin R. Frey, Phuong N Le, Andrew J. Souers, Peter Kovar, Wenqing Gao, Deepak Sampath, Dolores Diaz, Haichao Zhang, T. Matthew Hansen, Michael J. Mitten, Stephen K. Tahir, Russell A. Judge, Edna F. Choo, Yu Xiao, Shashank Shekhar, Xiaohong Song, George Doherty, Zhi-Fu Tao, Andrew S. Judd, Wayne J. Fairbrother, Michael D. Wendt, Steven W. Elmore, Kunzer Aaron R, Le Wang, Xilu Wang, Darren C. Phillips, Morey L. Smith, John A. Flygare, John Xue, Joel D. Leverson, Milan Bruncko, Chang H. Park, and Nathaniel D. Catron

Subjects

Drug, media_common.quotation_subject, A-1331852, Design elements and principles, BCL-2, Bcl-xL, Pharmacology, 01 natural sciences, Biochemistry, BCL-XL, Drug Discovery, media_common, biology, 010405 organic chemistry, Drug discovery, Chemistry, Organic Chemistry, apoptosis, A-1155463, Featured Letter, 0104 chemical sciences, Bioavailability, 010404 medicinal & biomolecular chemistry, Orally active, structure-based drug design (SBDD), Apoptosis, biology.protein, Pharmacophore

Abstract

Herein we describe the discovery of A-1331852, a first-in-class orally active BCL-XL inhibitor that selectively and potently induces apoptosis in BCL-XL-dependent tumor cells. This molecule was generated by re-engineering our previously reported BCL-XL inhibitor A-1155463 using structure-based drug design. Key design elements included rigidification of the A-1155463 pharmacophore and introduction of sp3-rich moieties capable of generating highly productive interactions within the key P4 pocket of BCL-XL. A-1331852 has since been used as a critical tool molecule for further exploring BCL-2 family protein biology, while also representing an attractive entry into a drug discovery program.

Published

2020

24. 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

25. Quantification of BCL-2 Family Members by Flow Cytometry

Author

Morey L, Smith and Stephen K, Tahir

Subjects

Proto-Oncogene Proteins c-bcl-2, bcl-X Protein, Humans, Flow Cytometry, Cell Line

Abstract

Flow cytometry is a powerful technique for the detection and quantification of cell surface and intracellular proteins. It enables the ability to measure the expression levels of specific proteins in a cell population of interest without the need to physically separate out the cells from within a heterogeneous population by using the appropriate cell-specific markers. It also requires fewer cells than other traditional techniques such as Western blotting. Here we describe a robust and reproducible method to measure the expression levels of the BCL-2 family members, BCL-2, BCL-X

Published

2018

26. Quantification of BCL-2 Family Members by Flow Cytometry

Author

Stephen K. Tahir and Morey L. Smith

Subjects

0301 basic medicine, education.field_of_study, medicine.diagnostic_test, Intracellular protein, Bcl-2 family, Population, Cell, Bcl-xL, Computational biology, Biology, Flow cytometry, Blot, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, medicine, biology.protein, Antibody, education

Abstract

Flow cytometry is a powerful technique for the detection and quantification of cell surface and intracellular proteins. It enables the ability to measure the expression levels of specific proteins in a cell population of interest without the need to physically separate out the cells from within a heterogeneous population by using the appropriate cell-specific markers. It also requires fewer cells than other traditional techniques such as Western blotting. Here we describe a robust and reproducible method to measure the expression levels of the BCL-2 family members, BCL-2, BCL-XL, and MCL-1 by quantitative flow cytometry (QFCM) using validated antibodies.

Published

2018

27. Development of a flow cytometric method for quantification of BCL-2 family members in chronic lymphocytic leukemia and correlation with sensitivity to BCL-2 family inhibitors

Author

Brenda Chyla, Stephen K. Tahir, Evelyn McKeegan, and Morey L. Smith

Subjects

0301 basic medicine, Histology, Chronic lymphocytic leukemia, Population, Pathology and Forensic Medicine, Flow cytometry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Western blot, medicine, education, education.field_of_study, Navitoclax, medicine.diagnostic_test, biology, Cell Biology, medicine.disease, Leukemia, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Immunology, Cancer research, biology.protein, Antibody, Cytometry

Abstract

Background We have developed a quantitative fluorescence cytometry (QFCM) method that can be used to measure BCL-2 family member proteins in cell lines and clinical samples. We described the validation of antibodies, methods development and application of the assay. Method We characterized and validated antibodies to BCL-2, BCL-XL, and MCL-1 in cell lines to confirm specificity for flow cytometry. Each protein was measured in a panel of leukemia/lymphoma cell lines and B-cells from chronic lymphocytic leukemia (CLL) patients treated with the BCL-2/BCL-XL inhibitor navitoclax. The cellular activity of various BCL-2 family member inhibitors alone and in combination was determined to demonstrate utility of our assay to correlate protein levels with efficacy. Results We identified antibodies that were highly specific for each protein. The expression profile in cell lines as determined by molecules of equivalent soluble fluorochrome was comparable to western blot. Using our assay, BCL-2, BCL-XL, and MCL-1 protein levels were shown to correlate with response to BCL-2 family inhibitors in vitro and could be measured in clinical samples. Conclusions This method can quantify BCL-2 family members in a specific, highly reproducible and sensitive fashion, and requires fewer cells compared to western blot. It is particularly useful for identifying BCL-2, BCL-XL, and MCL-1 protein levels in a specific cell population within a heterogeneous population like those collected from CLL patients. These data show that our QFCM method can be used to facilitate the quantification and evaluation of biomarkers predictive of response in patients treated with BCL-2 family member inhibitors. © 2016 International Clinical Cytometry Society

Published

2016

28. The Combinatorial Activity of Eftozanermin (ABBV-621), a Novel and Potent TRAIL Receptor Agonist Fusion Protein, in Pre-Clinical Models of Hematologic Malignancies

Author

Deborah Widomski, Greg Buchanan, Dong Chen, Jason Huska, Sha Jin, Vicky Bontcheva, Haichao Zhang, Stephen K. Tahir, Susan Morgan-Lappe, Darren C. Phillips, and Morey L. Smith

Subjects

Agonist, medicine.drug_class, business.industry, Bortezomib, Immunology, Cell Biology, Hematology, Death receptor binding, Biochemistry, Pevonedistat, Apoptosis, medicine, Cancer research, Receptor clustering, Signal transduction, business, Receptor, medicine.drug

Abstract

Cell death can be initiated through activation of the extrinsic and intrinsic apoptotic signaling pathways. Tumor necrosis factor (TNF)-related apoptosis-inducing ligand (TRAIL), a member of the TNF superfamily of cytokines, preferentially triggers the extrinsic apoptotic pathway by binding as a trimer to two closely related cell surface death receptors, TRAIL-R1 (DR4) and TRAIL-R2 (DR5). Receptor trimerization leads to the formation of the death-inducing signaling complex (DISC) to recruit and activate downstream caspases that ultimately leads to apoptotic cell death. Because TRAIL signaling induces apoptosis, several TRAIL receptor agonists have been developed for the treatment of cancer. ABBV-621 is a novel, second generation TRAIL receptor agonist that is an engineered fusion protein consisting of an IgG1-Fc linked to a single chain trimer of TRAIL subunits resulting in a total of six death receptor binding sites per molecule to maximize receptor clustering that is currently being tested in Phase I clinical trials (NCT03082209). To expand upon the potential therapeutic utility of ABBV-621, we tested the combinatorial activity of ABBV-621 with numerous standard-of-care (SoC) therapeutics and targeted agents in diffuse large B-cell lymphoma (DLBCL), acute myeloid leukemia (AML) and multiple myeloma (MM) cell lines. Thein vitroresults led to selection of agents to combine with ABBV-621 forin vivostudies. In DLBCL cell line-derived xenograft (CDX) preclinical models, we observed combination activity of ABBV-621 with pevonedistat (PEV) a selective NEDD8 inhibitor. Additionally, synergistic activity was observed with ABBV-621 with either bendamustine (BED) or rituximab (RTX) alone, or BED/RTX together. In AML, we observed compelling combination activity of ABBV-621 with PEV in cell line-derived xenograft (CDX) models. In MM, combination of ABBV-621 plus bortezomib (BTZ) resulted in deeper anti-tumorigenic activity than either agent alone in several CDX models. The pre-clinical data presented here support expanding the indications and settings where ABBV-621 may have utility. A clinical trial assessing the activity of ABBV-621 in combination with bortezomib and dexamethasone in R/R MM patients is planned. 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. Disclosures Smith: AbbVie:Current Employment, Current equity holder in publicly-traded company.Jin:AbbVie:Current Employment, Current equity holder in publicly-traded company.Chen:AbbVie:Current Employment, Current equity holder in publicly-traded company.Zhang:AbbVie:Current Employment, Current equity holder in publicly-traded company.Huska:AbbVie:Current Employment, Current equity holder in publicly-traded company.Widomski:AbbVie:Current Employment, Current equity holder in publicly-traded company.Bontcheva:AbbVie:Current Employment, Current equity holder in publicly-traded company.Buchanan:AbbVie:Current Employment, Current equity holder in publicly-traded company.Morgan-Lappe:AbbVie:Current Employment, Current equity holder in publicly-traded company.Phillips:AbbVie:Current Employment, Current equity holder in publicly-traded company.Tahir:AbbVie:Current Employment, Current equity holder in publicly-traded company.

Published

2020

29. Potential mechanisms of resistance to venetoclax and strategies to circumvent it

Author

Lisa Roberts Rapp, Paul Hessler, Morey L. Smith, Lloyd T. Lam, Joel D. Leverson, Stephen K. Tahir, Chang H. Park, and Kenneth B. Idler

Subjects

0301 basic medicine, Cancer Research, Lymphoma, Chronic lymphocytic leukemia, bcl-X Protein, BCL-2, Apoptosis, Epiphenomenon, Bcl-xL, medicine.disease_cause, lcsh:RC254-282, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, BCL-XL, Cell Line, Tumor, Genetics, medicine, Humans, Cell Lineage, Sulfonamides, Mutation, Leukemia, biology, Venetoclax, business.industry, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cell killing, Proto-Oncogene Proteins c-bcl-2, Oncology, chemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Immunology, Cancer research, biology.protein, Myeloid Cell Leukemia Sequence 1 Protein, MCL-1, business, Research Article

Abstract

Background Venetoclax (ABT-199), a first-in-class orally bioavailable BCL-2-selective inhibitor, was recently approved by the FDA for use in patients with 17p-deleted chronic lymphocytic leukemia who have received prior therapy. It is also being evaluated in numerous clinical trials for treating patients with various hematologic malignancies. As with any targeted cancer therapy, it is critically important to identify potential mechanisms of resistance, both for patient stratification and developing strategies to overcome resistance, either before it develops or as it emerges. Methods In order to gain a more comprehensive insight into the nature of venetoclax resistance mechanisms, we evaluated the changes in the BCL-2 family members at the genetic and expression levels in seven different venetoclax-resistant derived leukemia and lymphoma cell lines. Results Gene and protein expression analyses identified a number of different alterations in the expression of pro- and anti-apoptotic BCL-2 family members. In the resistant derived cells, an increase in either or both the anti-apoptotic proteins BCL-XL or MCL-1, which are not targeted by venetoclax was observed, and either concomitant or exclusive with a decrease in one or more pro-apoptotic proteins. In addition, mutational analysis also revealed a mutation in the BH3 binding groove (F104L) that could potentially interfere with venetoclax-binding. Not all changes may be causally related to venetoclax resistance and may only be an epiphenomenon. For resistant cell lines showing elevations in BCL-XL or MCL-1, strong synergistic cell killing was observed when venetoclax was combined with either BCL-XL- or MCL-1-selective inhibitors, respectively. This highlights the importance of BCL-XL- and MCL-1 as causally contributing to venetoclax resistance. Conclusions Overall our study identified numerous changes in multiple resistant lines; the changes were neither mutually exclusive nor universal across the cell lines tested, thus exemplifying the complexity and heterogeneity of potential resistance mechanisms. Identifying and evaluating their contribution has important implications for both patient selection and the rational development of strategies to overcome resistance. Electronic supplementary material The online version of this article (doi:10.1186/s12885-017-3383-5) contains supplementary material, which is available to authorized users.

Published

2017

30. Discovery of a Potent and Selective BCL-XL Inhibitor with in Vivo Activity

Author

Russell A. Judge, Sha Jin, Lisa A. Hasvold, Andrew J. Souers, Guillaume Lessene, John Xue, Hans E. Purkey, Jun Chen, Chang H. Park, Sarah G. Hymowitz, Nathaniel D. Catron, Xilu Wang, Le Wang, Wayne J. Fairbrother, Brian J. Smith, Brad E. Sleebs, Erwin R. Boghaert, Kurt Deshayes, Chudi Ndubaku, Yu Xiao, Darren C. Phillips, Stephen K. Tahir, Steven W. Elmore, Michael J. Mitten, Zhi-Fu Tao, Keith G. Watson, Michael F. T. Koehler, Anatol Oleksijew, Saul H. Rosenberg, Peter Kovar, Paul Nimmer, Andrew M. Petros, Chris Tse, Morey L. Smith, Peter M. Colman, Haichao Zhang, Kerry Zobel, Joel D. Leverson, Peter E. Czabotar, and John A. Flygare

Subjects

Navitoclax, Apoptosis Inhibitor, biology, Organic Chemistry, Cancer, Bcl-xL, Pharmacology, medicine.disease, Multiple dosing, Biochemistry, chemistry.chemical_compound, chemistry, Cell culture, Apoptosis, In vivo, Drug Discovery, biology.protein, medicine

Abstract

A-1155463, a highly potent and selective BCL-XL inhibitor, was discovered through nuclear magnetic resonance (NMR) fragment screening and structure-based design. This compound is substantially more potent against BCL-XL-dependent cell lines relative to our recently reported inhibitor, WEHI-539, while possessing none of its inherent pharmaceutical liabilities. A-1155463 caused a mechanism-based and reversible thrombocytopenia in mice and inhibited H146 small cell lung cancer xenograft tumor growth in vivo following multiple doses. A-1155463 thus represents an excellent tool molecule for studying BCL-XL biology as well as a productive lead structure for further optimization.

Published

2014

31. ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets

Author

Jackie Lee, Darren C. Phillips, Sha Jin, Morey L. Smith, Yu Xiao, Heather Maecker, Nathaniel D. Catron, Saul H. Rosenberg, David C.S. Huang, Michael J. Mitten, John F. Seymour, Anatol Oleksijew, Stephen K. Tahir, Andrew J. Souers, Peter Kovar, Kylie D. Mason, Gerard M. Sullivan, Lloyd T. Lam, Chang H. Park, Sarah G. Hymowitz, Jun Chen, Scott L. Ackler, Steven W. Elmore, Rod A. Humerickhouse, Brian D. Dayton, Andrew W. Roberts, Cheol-Min Park, Sari H. Enschede, Haichao Zhang, Hong Ding, Wayne J. Fairbrother, John Xue, Kennan C. Marsh, Seong Lin Khaw, Deepak Sampath, Erwin R. Boghaert, Chris Tse, Paul Nimmer, Michael D. Wendt, Joel D. Leverson, and School of Physical and Mathematical Sciences

Subjects

Blood Platelets, Cell Survival, Chronic lymphocytic leukemia, bcl-X Protein, Antineoplastic Agents, Apoptosis, Mice, SCID, Pharmacology, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, chemistry.chemical_compound, Dogs, medicine, Animals, Humans, MCL1, Science::Chemistry::Biochemistry [DRNTU], Sulfonamides, Aniline Compounds, Navitoclax, Venetoclax, Cancer, General Medicine, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, Xenograft Model Antitumor Assays, Tumor Burden, Proto-Oncogene Proteins c-bcl-2, chemistry, Hematologic Neoplasms, Cancer cell, Female, Refractory Chronic Lymphocytic Leukemia, HeLa Cells

Abstract

Proteins in the B cell CLL/lymphoma 2 (BCL-2) family are key regulators of the apoptotic process. This family comprises proapoptotic and prosurvival proteins, and shifting the balance toward the latter is an established mechanism whereby cancer cells evade apoptosis. The therapeutic potential of directly inhibiting prosurvival proteins was unveiled with the development of navitoclax, a selective inhibitor of both BCL-2 and BCL-2-like 1 (BCL-X(L)), which has shown clinical efficacy in some BCL-2-dependent hematological cancers. However, concomitant on-target thrombocytopenia caused by BCL-X(L) inhibition limits the efficacy achievable with this agent. Here we report the re-engineering of navitoclax to create a highly potent, orally bioavailable and BCL-2-selective inhibitor, ABT-199. This compound inhibits the growth of BCL-2-dependent tumors in vivo and spares human platelets. A single dose of ABT-199 in three patients with refractory chronic lymphocytic leukemia resulted in tumor lysis within 24 h. These data indicate that selective pharmacological inhibition of BCL-2 shows promise for the treatment of BCL-2-dependent hematological cancers.

Published

2013

32. 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

33. Development of a flow cytometric method for quantification of BCL-2 family members in chronic lymphocytic leukemia and correlation with sensitivity to BCL-2 family inhibitors

Author

Morey L, Smith, Brenda, Chyla, Evelyn, McKeegan, and Stephen K, Tahir

Subjects

B-Lymphocytes, Sulfonamides, Aniline Compounds, Proto-Oncogene Proteins c-bcl-2, Drug Resistance, Neoplasm, Cell Line, Tumor, Humans, Antineoplastic Agents, Flow Cytometry, Leukemia, Lymphocytic, Chronic, B-Cell

Abstract

We have developed a quantitative fluorescence cytometry (QFCM) method that can be used to measure BCL-2 family member proteins in cell lines and clinical samples. We described the validation of antibodies, methods development and application of the assay.We characterized and validated antibodies to BCL-2, BCL-XWe identified antibodies that were highly specific for each protein. The expression profile in cell lines as determined by molecules of equivalent soluble fluorochrome was comparable to western blot. Using our assay, BCL-2, BCL-XThis method can quantify BCL-2 family members in a specific, highly reproducible and sensitive fashion, and requires fewer cells compared to western blot. It is particularly useful for identifying BCL-2, BCL-X

Published

2015

34. The Bcl-2 inhibitor ABT-263 enhances the response of multiple chemotherapeutic regimens in hematologic tumors in vivo

Author

Michael J. Mitten, Anatol Oleksijew, Steven W. Elmore, Scott L. Ackler, Marion Refici, David Frost, Christin Tse, Stephen K. Tahir, Kelly Foster, Saul H. Rosenberg, Stephen W. Fesik, Yu Xiao, and Alexander R. Shoemaker

Subjects

Cancer Research, Vincristine, Lymphoma, B-Cell, medicine.medical_treatment, Mice, SCID, CHOP, Biology, Toxicology, Mice, immune system diseases, Cell Line, Tumor, Proto-Oncogene Proteins, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Pharmacology (medical), Etoposide, Multiple myeloma, Pharmacology, Sulfonamides, Chemotherapy, Aniline Compounds, Bortezomib, Drug Synergism, medicine.disease, Xenograft Model Antitumor Assays, Lymphoma, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-bcl-2, Oncology, Cancer research, Mantle cell lymphoma, Apoptosis Regulatory Proteins, Multiple Myeloma, medicine.drug

Abstract

This study was designed to test the ability of the Bcl-2 family inhibitor ABT-263 to potentiate commonly used chemotherapeutic agents and regimens in hematologic tumor models. Models of B-cell lymphoma and multiple myeloma were tested in vitro and in vivo with ABT-263 in combination with standard chemotherapeutic regimens, including VAP, CHOP and R-CHOP, as well as single cytotoxic agents including etoposide, rituximab, bortezomib and cyclophosphamide. Alterations in Bcl-2 family member expression patterns were analyzed to define mechanisms of potentiation. ABT-263 was additive with etoposide, vincristine and VAP in vitro in the diffuse large B-cell lymphoma line (DLBCL) DoHH-2, while rituximab potentiated its activity in SuDHL-4. Bortezomib strongly synergized with ABT-263 in the mantle cell lymphoma line Granta 519. Treatment of DoHH-2 with etoposide was associated with an increase in Puma expression, while bortezomib upregulated Noxa expression in Granta 519. Combination of ABT-263 with cytotoxic agents demonstrated superior tumor growth inhibition and delay in multiple models versus cytotoxic therapy alone, along with significant improvements in tumor response rates. Inhibition of the Bcl-2 family of proteins by ABT-263 enhances the cytotoxicity of multiple chemotherapeutics in hematologic tumors and represents a promising addition to the therapeutic arsenal for treatment of these diseases.

Published

2010

35. ABT-751, a novel tubulin-binding agent, decreases tumor perfusion and disrupts tumor vasculature

Author

Bryan F. Cox, David Frost, Yanping Luo, Gerard D. Gagne, Gerard B. Fox, Saul H. Rosenberg, Gary Gordon, Vincent P. Hradil, Sherry J. Morgan, and Stephen K. Tahir

Subjects

Cancer Research, Angiogenesis Inhibitors, Drug action, Plasma protein binding, Pharmacology, Microtubules, Tubulin, In vivo, Cell Line, Tumor, Animals, Humans, Medicine, Pharmacology (medical), Sulfonamides, Binding Sites, Dose-Response Relationship, Drug, Neovascularization, Pathologic, biology, business.industry, Endothelial Cells, Neoplasms, Experimental, Actin cytoskeleton, Magnetic Resonance Imaging, Rats, Inbred F344, Rats, Endothelial stem cell, Actin Cytoskeleton, Oncology, Tubulin Binding Agent, biology.protein, Female, Endothelium, Vascular, business, Perfusion, Neoplasm Transplantation, Protein Binding

Abstract

ABT-751 is an orally bioavailable tubulin-binding agent that is currently under clinical development for cancer treatment. In preclinical studies, ABT-751 showed antitumor activity against a broad spectrum of tumor lines including those resistant to conventional chemotherapies. In this study, we investigated the antivascular properties of ABT-751 in a rat subcutaneous tumor model using dynamic contrast-enhanced magnetic resonance imaging. A single dose of ABT-751 (30 mg/kg, intravenously) induced a rapid, transient reduction in tumor perfusion. After 1 h, tumor perfusion decreased by 57% before recovering to near pretreatment levels within 6 h. In contrast, ABT-751 produced little change in muscle perfusion at either time point. To further elucidate mechanisms of drug action at the cellular level, we examined the effects of ABT-751 on endothelial cells using an in-vitro assay. ABT-751, at concentrations corresponding to plasma levels achieved in vivo, caused endothelial cell retraction and significant loss of microtubules within 1 h. The severity of these morphological changes was dose-dependent but reversible within 6 h after the discontinuation of the drug. Taken together, these results show that ABT-751 is a tubulin-binding agent with antivascular properties. Microtubule disruption and morphological changes in vascular endothelial cells may be responsible, at least in part, for the dysfunction of tumor blood vessels after ABT-751 treatment.

Published

2009

36. ABT-263: A Potent and Orally Bioavailable Bcl-2 Family Inhibitor

Author

Kennan C. Marsh, Eric F. Johnson, Sha Jin, Paul Nimmer, Saul H. Rosenberg, Christin Tse, Jessica Adickes, Haichao Zhang, Michael J. Mitten, Lisa R. Roberts, Steven W. Elmore, Alexander R. Shoemaker, Mark G. Anderson, Stephen K. Tahir, Xiufen Yang, Jun Chen, Stephen W. Fesik, and Yu Xiao

Subjects

Cancer Research, Lung Neoplasms, BH3 Mimetic ABT-737, Administration, Oral, Antineoplastic Agents, Lymphoma, Mantle-Cell, Mice, SCID, Pharmacology, Models, Biological, Antibodies, Monoclonal, Murine-Derived, Mice, chemistry.chemical_compound, Oral administration, Neoplasms, medicine, Animals, Humans, Carcinoma, Small Cell, Lung cancer, Cells, Cultured, Mice, Knockout, Sulfonamides, Aniline Compounds, Navitoclax, business.industry, Bcl-2 family, Antibodies, Monoclonal, Drug Synergism, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Thrombocytopenia, Xenograft Model Antitumor Assays, Tumor Burden, Treatment Outcome, Proto-Oncogene Proteins c-bcl-2, Oncology, chemistry, Apoptosis, Monoclonal, Rituximab, business, Obatoclax

Abstract

Overexpression of the prosurvival Bcl-2 family members (Bcl-2, Bcl-xL, and Mcl-1) is commonly associated with tumor maintenance, progression, and chemoresistance. We previously reported the discovery of ABT-737, a potent, small-molecule Bcl-2 family protein inhibitor. A major limitation of ABT-737 is that it is not orally bioavailable, which would limit chronic single agent therapy and flexibility to dose in combination regimens. Here we report the biological properties of ABT-263, a potent, orally bioavailable Bad-like BH3 mimetic (Ki's of

Published

2008

37. Influence of Bcl-2 Family Members on the Cellular Response of Small-Cell Lung Cancer Cell Lines to ABT-737

Author

Shi-Chung Ng, Susan Morgan-Lappe, Steve W. Elmore, Saul H. Rosenberg, Aparna Sarthy, Stephen K. Tahir, Robert B. Warner, Xiufen Yang, Stephen W. Fesik, Mark G. Anderson, Christin Tse, and Jun Chen

Subjects

Cancer Research, Small interfering RNA, Lung Neoplasms, BH3 Mimetic ABT-737, Down-Regulation, Apoptosis, Cell Growth Processes, Biology, Transfection, Piperazines, Carboplatin, Nitrophenols, Downregulation and upregulation, Cell Line, Tumor, Proto-Oncogene Proteins, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, Humans, Carcinoma, Small Cell, RNA, Small Interfering, neoplasms, Etoposide, Sulfonamides, Gene knockdown, Bcl-2-Like Protein 11, Biphenyl Compounds, Bcl-2 family, Membrane Proteins, Drug Synergism, Neoplasm Proteins, Up-Regulation, Proto-Oncogene Proteins c-bcl-2, Oncology, Cell culture, Immunology, Cancer research, Myeloid Cell Leukemia Sequence 1 Protein, Apoptosis Regulatory Proteins

Abstract

ABT-737 is a novel and potent Bcl-2 antagonist with single-agent activity against small-cell lung cancer (SCLC) cell lines. Here, we evaluated the contribution of Bcl-2 family members to the in vitro cellular response of several SCLC cell lines to ABT-737. Relatively higher levels of Bcl-2, Bcl-XL, Bim and Noxa, and lower levels of Mcl-1 characterized naïve SCLC cell lines that were sensitive to ABT-737. Conversely, a progressive decrease in the relative levels of Bcl-2 and Noxa and a progressive increase in Mcl-1 levels characterized the increased resistance of H146 cells following chronic exposure to ABT-737. Knockdown of Mcl-1 with small interfering RNA sensitized two resistant SCLC cell lines H196 and DMS114 to ABT-737 by enhancing the induction of apoptosis. Likewise, up-regulation of Noxa sensitized H196 cells to ABT-737. Combination treatment with DNA-damaging agents was extremely synergistic with ABT-737 and was associated with the down-regulation of Mcl-1 and the up-regulation of Noxa, Puma, and Bim in H196 cells. Thus, SCLC cells sensitive to ABT-737 expressed the target proteins Bcl-2 and Bcl-XL, whereas Mcl-1 and factors regulating Mcl-1 function seem to contribute to the overall resistance of SCLC cells to ABT-737. Overall, these observations provide further insight as to the mechanistic bases for ABT-737 efficacy in SCLC and will be helpful for profiling patients and aiding in the rational design of combination therapies. [Cancer Res 2007;67(3):1176–83]

Published

2007

38. Bcl-2 family proteins are essential for platelet survival

Author

Stephen K. Tahir, R Nelson, S J Morgan, L C Preusser, Saul H. Rosenberg, K R Hahn, Steven W. Elmore, G A Reinhart, H Zhang, Morey L. Smith, L A Iciek, Jun Chen, Paul Nimmer, R M Fryer, Chris Tse, and M C Nasarre

Subjects

Blood Platelets, Male, BH3 Mimetic ABT-737, Platelet Aggregation, Cell Survival, Apoptosis, Cell Separation, Phosphatidylserines, Cytoplasmic Granules, Exocytosis, Piperazines, Nitrophenols, chemistry.chemical_compound, Dogs, In vivo, Animals, Humans, Platelet, Platelet activation, Molecular Biology, Sulfonamides, Dose-Response Relationship, Drug, biology, Platelet Count, Cytochrome c, Biphenyl Compounds, Bcl-2 family, Cell Biology, Phosphatidylserine, Flow Cytometry, Cell biology, Liver, Proto-Oncogene Proteins c-bcl-2, Biochemistry, chemistry, biology.protein

Abstract

Platelets are relatively short-lived, anucleated cells that are essential for proper hemostasis. The regulation of platelet survival in the circulation remains poorly understood. The process of platelet activation and senescence in vivo is associated with processes similar to those observed during apoptosis in nucleated cells, including loss of mitochondrial membrane potential, caspase activation, phosphatidylserine (PS) externalization, and cell shrinkage. ABT-737, a potent antagonist of Bcl-2, Bcl-X(L), and Bcl-w, induces apoptosis in nucleated cells dependent on these proteins for survival. In vivo, ABT-737 induces a reduction of circulating platelets that is maintained during drug therapy, followed by recovery to normal levels within several days after treatment cessation. Whole body scintography utilizing ([111])Indium-labeled platelets in dogs shows that ABT-737-induced platelet clearance is primarily mediated by the liver. In vitro, ABT-737 treatment leads to activation of key apoptotic processes including cytochrome c release, caspase-3 activation, and PS externalization in isolated platelets. Despite these changes, ABT-737 is ineffective in promoting platelet activation as measured by granule release markers and platelet aggregation. Taken together, these data suggest that ABT-737 induces an apoptosis-like response in platelets that is distinct from platelet activation and results in enhanced clearance in vivo by the reticuloendothelial system.

Published

2007

39. Genomic analysis and selective small molecule inhibition identifies BCL-XL as a critical survival factor in a subset of colorectal cancer

Author

Lloyd T. Lam, Paul Hessler, John Z. Xue, Andrew J. Souers, Jun Chen, Sha Jin, Haichao Zhang, Stephen K. Tahir, and Joel D. Leverson

Subjects

Cancer Research, Programmed cell death, Colorectal cancer, Cell Survival, NOXA, bcl-X Protein, Gene Expression, Bcl-xL, BCL-XL inhibitor, BCL-XL, Cell Line, Tumor, medicine, Gene silencing, Cluster Analysis, Humans, MCL1, Benzothiazoles, biology, Research, Gene Expression Profiling, Cancer, Genomics, medicine.disease, Isoquinolines, Molecular biology, Gene expression profiling, Oncology, Proto-Oncogene Proteins c-bcl-2, Apoptosis, biology.protein, Molecular Medicine, MCL-1, Colorectal Neoplasms

Abstract

Background Defects in programmed cell death, or apoptosis, are a hallmark of cancer. The anti-apoptotic B-cell lymphoma 2 (BCL-2) family proteins, including BCL-2, BCL-XL, and MCL-1 have been characterized as key survival factors in multiple cancer types. Because cancer types with BCL2 and MCL1 amplification are more prone to inhibition of their respectively encoded proteins, we hypothesized that cancers with a significant frequency of BCL2L1 amplification would have greater dependency on BCL-XL for survival. Methods To identify tumor subtypes that have significant frequency of BCL2L1 amplification, we performed data mining using The Cancer Genome Atlas (TCGA) database. We then assessed the dependency on BCL-XL in a panel of cell lines using a selective and potent BCL-XL inhibitor, A-1155463, and BCL2L1 siRNA. Mechanistic studies on the role of BCL-XL were further undertaken via a variety of genetic manipulations. Results We identified colorectal cancer as having the highest frequency of BCL2L1 amplification across all tumor types examined. Colorectal cancer cell lines with BCL2L1 copy number >3 were more sensitive to A-1155463. Consistently, cell lines with high expression of BCL-XL and NOXA, a pro-apoptotic protein that antagonizes MCL-1 activity were sensitive to A-1155463. Silencing the expression of BCL-XL via siRNA killed the cell lines that were sensitive to A-1155463 while having little effect on lines that were resistant. Furthermore, silencing the expression of MCL-1 in resistant cell lines conferred sensitivity to A-1155463, whereas silencing NOXA abrogated sensitivity. Conclusions This work demonstrates the utility of characterizing frequent genomic alterations to identify cancer survival genes. In addition, these studies demonstrate the utility of the highly potent and selective compound A-1155463 for investigating the role of BCL-XL in mediating the survival of specific tumor types, and indicate that BCL-XL inhibition could be an effective treatment for colorectal tumors with high BCL-XL and NOXA expression.

Published

2015

40. Exploiting selective BCL-2 family inhibitors to dissect cell survival dependencies and define improved strategies for cancer therapy

Author

Wayne J. Fairbrother, Deepak Sampath, Xiaoju Max Ma, Le Wang, Haichao Zhang, Paul Nimmer, Kedar S. Vaidya, Yu Xiao, Jacqueline M. Tarrant, Anatol Oleksijew, Saul H. Rosenberg, Peter Kovar, Nghi La, Kym N Lowes, Chris Tse, Darren C. Phillips, Dolores Diaz, Erwin R. Boghaert, Jun Chen, Lisa D. Belmont, Michael J. Mitten, Steven W. Elmore, Stephen K. Tahir, Michael D. Wendt, Andrew J. Souers, John Xue, Zhi-Fu Tao, Daniel H. Albert, Morey L. Smith, Terrance J. Magoc, David C.S. Huang, Joel D. Leverson, and Sha Jin

Subjects

Neutropenia, Cell Survival, Neutrophils, Chronic lymphocytic leukemia, bcl-X Protein, Administration, Oral, Antineoplastic Agents, Docetaxel, Pharmacology, Biology, Granulopoiesis, chemistry.chemical_compound, Mice, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Benzothiazoles, Sulfonamides, Navitoclax, Aniline Compounds, Venetoclax, Gene Expression Profiling, Cancer, General Medicine, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Isoquinolines, Thrombocytopenia, Gene Expression Regulation, Neoplastic, Leukemia, Kinetics, chemistry, Proto-Oncogene Proteins c-bcl-2, Cancer research, Taxoids, Neoplasm Transplantation, medicine.drug, Granulocytes

Abstract

The BCL-2/BCL-XL/BCL-W inhibitor ABT-263 (navitoclax) has shown promising clinical activity in lymphoid malignancies such as chronic lymphocytic leukemia. However, its efficacy in these settings is limited by thrombocytopenia caused by BCL-XL inhibition. This prompted the generation of the BCL-2-selective inhibitor venetoclax (ABT-199/GDC-0199), which demonstrates robust activity in these cancers but spares platelets. Navitoclax has also been shown to enhance the efficacy of docetaxel in preclinical models of solid tumors, but clinical use of this combination has been limited by neutropenia. We used venetoclax and the BCL-XL-selective inhibitors A-1155463 and A-1331852 to assess the relative contributions of inhibiting BCL-2 or BCL-XL to the efficacy and toxicity of the navitoclax-docetaxel combination. Selective BCL-2 inhibition suppressed granulopoiesis in vitro and in vivo, potentially accounting for the exacerbated neutropenia observed when navitoclax was combined with docetaxel clinically. By contrast, selectively inhibiting BCL-XL did not suppress granulopoiesis but was highly efficacious in combination with docetaxel when tested against a range of solid tumors. Therefore, BCL-XL-selective inhibitors have the potential to enhance the efficacy of docetaxel in solid tumors and avoid the exacerbation of neutropenia observed with navitoclax. These studies demonstrate the translational utility of this toolkit of selective BCL-2 family inhibitors and highlight their potential as improved cancer therapeutics.

Published

2015

41. Clearance of systemic hematologic tumors by venetoclax (Abt-199) and navitoclax

Author

Kelly Foster, Anatol Oleksijew, Jonathan Hickson, Jerry Clarin, Sally Schlessinger, Erwin R. Boghaert, Sasmita Mishra, Jun Chen, Stephen K. Tahir, Scott L. Ackler, Andrew J. Souers, Brenda Chyla, Joel D. Leverson, Thomas McGonigal, and Morey L. Smith

Subjects

Systemic disease, Chronic lymphocytic leukemia, Apoptosis, systemic engraftment, chemistry.chemical_compound, hemic and lymphatic diseases, medicine, General Pharmacology, Toxicology and Pharmaceutics, bioluminescent imaging, Multiple myeloma, Navitoclax, Venetoclax, business.industry, Original Articles, medicine.disease, Lymphoma, Bcl-2 family proteins, drug therapy, leukemia/lymphoma, medicine.anatomical_structure, Neurology, chemistry, Immunology, Cancer research, Mantle cell lymphoma, Bone marrow, business

Abstract

The Bcl-2 family inhibitors venetoclax and navitoclax demonstrated potent antitumor activity in chronic lymphocytic leukemia patients, notably in reducing marrow load and adenopathy. Subsequent trials with venetoclax have been initiated in non-Hodgkin's lymphoma and multiple myeloma patients. Traditional preclinical models fall short either in faithfully recapitulating disease progression within such compartments or in allowing the direct longitudinal analysis of systemic disease. We show that intravenous inoculation of engineered RS4;11 (acute lymphoblastic leukemia) and Granta 519 (mantle cell lymphoma) bioluminescent reporter cell lines result in tumor engraftment of bone marrow, with additional invasion of the central nervous system in the case of Granta 519. Importantly, apoptosis induction and response of these systemically engrafted tumors to Bcl-2 family inhibitors alone or in combination with standard-of-care agents could be monitored longitudinally with optical imaging, and was more accurately reflective of the observed clinical response.

Published

2015

42. Structure-guided design of a series of MCL-1 inhibitors with high affinity and selectivity

Author

Andrew J. Souers, Lisa A. Hasvold, Elizabeth E. Fry, Xiaohong Song, Chang Park, Russell A. Judge, Steve W. Elmore, Paul Nimmer, Morey L. Smith, Milan Bruncko, Gary J. Jenkins, David Madar, Le Wang, Saul H. Rosenberg, Haichao Zhang, Chaohong Sun, George S. Sheppard, Yu Xiao, Andrew M. Petros, Peter Kovar, Chris Tse, Xilu Wang, John Xue, Joel D. Leverson, Scott A. Erickson, Stephen K. Tahir, Zhi-Fu Tao, Darren C. Phillips, Sha Jin, and Steve D. Fidanze

Subjects

Databases, Factual, Cell Survival, Cell, Antineoplastic Agents, Apoptosis, Plasma protein binding, Crystallography, X-Ray, Structure-Activity Relationship, hemic and lymphatic diseases, Drug Discovery, medicine, Tumor Cells, Cultured, Structure–activity relationship, Humans, G protein-coupled receptor, Molecular Structure, Chemistry, Kinase, medicine.disease, Small molecule, Cell biology, High-Throughput Screening Assays, Molecular Docking Simulation, Pancreatic Neoplasms, Leukemia, medicine.anatomical_structure, Cell culture, Drug Design, Cancer research, Molecular Medicine, Myeloid Cell Leukemia Sequence 1 Protein, Multiple Myeloma, Protein Binding

Abstract

Myeloid cell leukemia 1 (MCL-1) is a BCL-2 family protein that has been implicated in the progression and survival of multiple tumor types. Herein we report a series of MCL-1 inhibitors that emanated from a high throughput screening (HTS) hit and progressed via iterative cycles of structure-guided design. Advanced compounds from this series exhibited subnanomolar affinity for MCL-1 and excellent selectivity over other BCL-2 family proteins as well as multiple kinases and GPCRs. In a MCL-1 dependent human tumor cell line, administration of compound 30b rapidly induced caspase activation with associated loss in cell viability. The small molecules described herein thus comprise effective tools for studying MCL-1 biology.

Published

2015

43. An inhibitor of Bcl-2 family proteins induces regression of solid tumours

Author

Shinichi Kitada, Jacqueline M. O'Connor, John C. Reed, Wendt Michael D, Andrew M. Petros, Alexander R. Shoemaker, Anatol Oleksijew, David J. Augeri, Craig B. Thompson, Kunzer Aaron R, Jürgen Dinges, Thomas L. Deckwerth, Stanley J. Korsmeyer, Saul H. Rosenberg, Stephen K. Tahir, Barbara A. Belli, Paul Nimmer, Baole Wang, Shi Chung Ng, Steven W. Elmore, Anthony Letai, Wang Shen, Haichao Zhang, Tilman Oltersdorf, Stephen W. Fesik, Milan Bruncko, David G. Nettesheim, Robert C. Armstrong, Michael J. Mitten, Kevin J. Tomaselli, Mary K. Joseph, Philip J. Hajduk, and Chi Li

Subjects

Models, Molecular, Programmed cell death, Magnetic Resonance Spectroscopy, BH3 Mimetic ABT-737, Lymphoma, Paclitaxel, Antineoplastic Agents, Apoptosis, Piperazines, Nitrophenols, Mice, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Cell Line, Tumor, Neoplasms, Animals, Humans, Carcinoma, Small Cell, Sulfonamides, Multidisciplinary, Chemistry, Biphenyl Compounds, Bcl-2 family, Cytochromes c, Drug Synergism, Cell cycle, Mitochondria, Survival Rate, Disease Models, Animal, Proto-Oncogene Proteins c-bcl-2, Biochemistry, Cancer research, Bcl-2 Homologous Antagonist-Killer Protein, Obatoclax

Abstract

Proteins in the Bcl-2 family are central regulators of programmed cell death, and members that inhibit apoptosis, such as Bcl-X(L) and Bcl-2, are overexpressed in many cancers and contribute to tumour initiation, progression and resistance to therapy. Bcl-X(L) expression correlates with chemo-resistance of tumour cell lines, and reductions in Bcl-2 increase sensitivity to anticancer drugs and enhance in vivo survival. The development of inhibitors of these proteins as potential anti-cancer therapeutics has been previously explored, but obtaining potent small-molecule inhibitors has proved difficult owing to the necessity of targeting a protein-protein interaction. Here, using nuclear magnetic resonance (NMR)-based screening, parallel synthesis and structure-based design, we have discovered ABT-737, a small-molecule inhibitor of the anti-apoptotic proteins Bcl-2, Bcl-X(L) and Bcl-w, with an affinity two to three orders of magnitude more potent than previously reported compounds. Mechanistic studies reveal that ABT-737 does not directly initiate the apoptotic process, but enhances the effects of death signals, displaying synergistic cytotoxicity with chemotherapeutics and radiation. ABT-737 exhibits single-agent-mechanism-based killing of cells from lymphoma and small-cell lung carcinoma lines, as well as primary patient-derived cells, and in animal models, ABT-737 improves survival, causes regression of established tumours, and produces cures in a high percentage of the mice.

Published

2005

44. A-432411, a novel indolinone compound that disrupts spindle pole formation and inhibits human cancer cell growth

Author

Philip Merta, Zehan Chen, Nan-Hong Lin, Hing L. Sham, Peter Kovar, Haiying Zhang, and Stephen K. Tahir

Subjects

Cancer Research, Indoles, Time Factors, Blotting, Western, Antineoplastic Agents, Cell Separation, Spindle Apparatus, Cyclin B, Binding, Competitive, Microtubules, Spindle pole body, Microtubule polymerization, Histones, Tubulin, Microtubule, Cell Line, Tumor, CDC2 Protein Kinase, Humans, Pyrroles, Cyclin B1, Cell Proliferation, Binding Sites, Cell Death, Dose-Response Relationship, Drug, biology, Cell growth, Cell Cycle, Flow Cytometry, Immunohistochemistry, Neoplasm Proteins, Cell biology, Securin, Spindle checkpoint, Microscopy, Fluorescence, Models, Chemical, Oncology, biology.protein, Tyrosine, Endothelium, Vascular, Colchicine, Multipolar spindles, HeLa Cells

Abstract

Microtubules are among the most successful targets for anticancer therapies and for the development of new anticancer drugs. A-432411 is a novel small molecule that destabilizes microtubules at high concentration and disrupts normal spindle formation at low concentration. A-432411 is an indolinone that is structurally different from other known synthetic microtubule inhibitors. This compound is efficacious against a variety of human cancer cell lines including drug-resistant HCT-15 that overexpresses Pgp170. Biochemical studies show that A-432411 competes with the colchicine-binding site on tubulin and inhibits microtubule polymerization. Fluorescence-activated cell sorting analysis indicates that A-432411 causes G2-M arrest and induces apoptosis. Cells treated with A-432411 have increased level of phospho-histone H3 at Ser10 and decreased level of phospho-cdc2 at Tyr15. Concurrently, securin and cyclin B1 expression levels remain the same, indicating the activation of the spindle checkpoint. Immunocytochemistry and fluorescence microscopy experiments reveal that 1 μmol/L A-432411 destabilizes microtubules in cells. At 0.1 μmol/L, the compound disrupts normal spindle pole formation possibly through stabilization of microtubule dynamic. Both structural and cellular properties of A-432411 make it an attractive candidate for further development.

Published

2005

45. Aryl tetrahydropyridine inhibitors of farnesyltransferase: glycine, phenylalanine and histidine derivatives

Author

Shi-Chung Ng, Gerard M. Sullivan, Weibo Wang, Hovis M. Imade, Stephen J. O'connor, Haiying Zhang, Hing L. Sham, Stephen L. Gwaltney, Saul H. Rosenberg, Lisa A. Hasvold, Jerome Cohen, Wen-Zhen Gu, Joy Bauch, Qun Li, Stephen K. Tahir, Steve Muchmore, Charles W. Hutchins, Kennan C. Marsh, Nelson Lissa T, Clarissa G. Jakob, Vincent S. Stoll, and David Frost

Subjects

Models, Molecular, Pyridines, Stereochemistry, Phenylalanine, Farnesyltransferase, Clinical Biochemistry, Glycine, Molecular Conformation, Biological Availability, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Farnesyltranstransferase, Histidine, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Farnesyl-diphosphate farnesyltransferase, Alkyl and Aryl Transferases, biology, Aryl, Organic Chemistry, Genes, ras, Enzyme, chemistry, biology.protein, Molecular Medicine

Abstract

Inhibitors of farnesyltransferase are effective against a variety of tumors in mouse models of cancer. Clinical trials to evaluate these agents in humans are ongoing. In our effort to develop new farnesyltransferase inhibitors, we have discovered a series of aryl tetrahydropyridines that incorporate substituted glycine, phenylalanine and histidine residues. The design, synthesis, SAR and biological properties of these compounds will be discussed.

Published

2003

46. Synthesis and Biological Evaluation of 2-Indolyloxazolines as a New Class of Tubulin Polymerization Inhibitors. Discovery of A-289099 as an Orally Active Antitumor Agent

Author

Kenneth J. Barr, Laura Gehrke, Hing L. Sham, Michael A. Nukkala, Jang Lee, Shi Chung Ng, Nicolette A. Zielinski, Stephen L. Gwaltney, Michael C. Fitzgerald, Stephen K. Tahir, R. Bruce Credo, Akiyo Claiborne, Robert B. Warner, Keith W. Woods, Gang Liu, Ki H. Kim, David Frost, Yu Hua Hui, Kennan C. Marsh, Qun Li, Saul H. Rosenberg, and Peter Kovar

Subjects

Models, Molecular, Indoles, Polymers, Clinical Biochemistry, Biological Availability, Pharmaceutical Science, Antineoplastic Agents, Microtubules, Biochemistry, Chemical synthesis, Mice, chemistry.chemical_compound, Tubulin, In vivo, Drug Discovery, Tumor Cells, Cultured, Animals, Humans, Colchicine, Oxazoles, Molecular Biology, Indole test, Organic Chemistry, Stereoisomerism, In vitro, Rats, chemistry, Cell culture, Molecular Medicine, Antimitotic Agent, Drug Screening Assays, Antitumor, Lead compound

Abstract

A series of indole containing oxazolines has been discovered as a result of structural modifications of the lead compound A-105972. The compounds exert their anticancer activity through inhibition of tubulin polymerization by binding at the colchicine site. A-289099 was identified as an orally active antimitotic agent active against various cancer cell lines including those that express the MDR phenotype. The anticancer activity, pharmacokinetics, and an efficient and enantioselective synthesis of A-289099 are described.

Published

2002

47. The Bcl-2/Bcl-X(L)/Bcl-w inhibitor, navitoclax, enhances the activity of chemotherapeutic agents in vitro and in vivo

Author

Alexander R. Shoemaker, Chris Tse, Xiaoli Huang, Vivek C. Abraham, Paul Nimmer, Deepak Sampath, Scott L. Ackler, Steven W. Elmore, Stephen K. Tahir, Saul H. Rosenberg, Michael J. Mitten, Morey L. Smith, Bernard Liu, Joel D. Leverson, Yu Shen, Xiaoyu Lin, Sha Jin, Heather Maecker, Jun Chen, and Haichao Zhang

Subjects

Male, Cancer Research, bcl-X Protein, Pharmacology, Biology, medicine.disease_cause, chemistry.chemical_compound, Mice, Downregulation and upregulation, In vivo, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, medicine, Tumor Cells, Cultured, Animals, Humans, neoplasms, Sulfonamides, Navitoclax, Aniline Compounds, Drug Synergism, Hep G2 Cells, HCT116 Cells, Xenograft Model Antitumor Assays, Oncology, Docetaxel, chemistry, Proto-Oncogene Proteins c-bcl-2, Apoptosis, Cancer cell, Female, Erlotinib, Carcinogenesis, Apoptosis Regulatory Proteins, K562 Cells, medicine.drug

Abstract

The ability of a cancer cell to avoid apoptosis is crucial to tumorigenesis and can also contribute to chemoresistance. The Bcl-2 family of prosurvival proteins (Bcl-2, Bcl-XL, Bcl-w, Mcl-1, and A1) plays a key role in these processes. We previously reported the discovery of ABT-263 (navitoclax), a potent small-molecule inhibitor of Bcl-2, Bcl-XL, and Bcl-w. While navitoclax exhibits single-agent activity in tumors dependent on Bcl-2 or Bcl-XL for survival, the expression of Mcl-1 has been shown to confer resistance to navitoclax, most notably in solid tumors. Thus, therapeutic agents that can downregulate or neutralize Mcl-1 are predicted to synergize potently with navitoclax. Here, we report the activity of navitoclax in combination with 19 clinically relevant agents across a panel of 46 human solid tumor cell lines. Navitoclax broadly enhanced the activity of multiple therapeutic agents in vitro and enhanced efficacy of both docetaxel and erlotinib in xenograft models. The ability of navitoclax to synergize with docetaxel or erlotinib corresponded to an altered sensitivity of the mitochondria toward navitoclax, which was associated with the downmodulation of Mcl-1 and/or upregulation of Bim. These data provide a rationale to interrogate these combinations clinically. Mol Cancer Ther; 10(12); 2340–9. ©2011 AACR.

Published

2011

48. N-aryl-benzimidazolones as novel small molecule HSP90 inhibitors

Author

Sha Jin, Jun Chen, Saul H. Rosenberg, Hong Ding, Russell A. Judge, Chang H. Park, Xiaohong Song, Milan Bruncko, Andrew M. Petros, Jeffrey R. Huth, Cheol-Min Park, David Madar, Steven W. Elmore, Stephen K. Tahir, and Christin Tse

Subjects

animal structures, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Protein degradation, Crystallography, X-Ray, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, Protein structure, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Humans, HSP90 Heat-Shock Proteins, Binding site, Molecular Biology, Binding Sites, biology, Chemistry, Aryl, Organic Chemistry, Hsp90, Small molecule, Protein Structure, Tertiary, Enzyme inhibitor, biology.protein, Molecular Medicine, Benzimidazoles

Abstract

We describe the development of a novel series of N-aryl-benzimidazolone HSP90 inhibitors (9) targeting the N-terminal ATP-ase site. SAR development was influenced by structure-based design based around X-ray structures of ligand bound HSP90 complexes. Lead compounds exhibited high binding affinities, ATP-ase inhibition and cellular client protein degradation.

Published

2010

49. Identification of expression signatures predictive of sensitivity to the Bcl-2 family member inhibitor ABT-263 in small cell lung carcinoma and leukemia/lymphoma cell lines

Author

Paul Hessler, Viswanath Devanarayan, Mark G. Anderson, Paul E. Kroeger, John A. Wass, Stephen K. Tahir, Haichao Zhang, Steve W. Elmore, Mary K. Joseph, Christin Tse, and Saul H. Rosenberg

Subjects

Cancer Research, Lung Neoplasms, Lymphoma, Antineoplastic Agents, Biology, Biomarkers, Pharmacological, Cell Line, Tumor, Gene expression, medicine, Humans, Gene Regulatory Networks, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Sulfonamides, Aniline Compounds, Leukemia, Gene Expression Profiling, Gene signature, medicine.disease, Prognosis, Small Cell Lung Carcinoma, respiratory tract diseases, Gene expression profiling, Gene Expression Regulation, Neoplastic, Oncology, Proto-Oncogene Proteins c-bcl-2, Cell culture, Drug Resistance, Neoplasm, Multigene Family, Immunology, Cancer research

Abstract

ABT-263 inhibits the antiapoptotic proteins Bcl-2, Bcl-xL, and Bcl-w and has single-agent efficacy in numerous small cell lung carcinoma (SCLC) and leukemia/lymphoma cell lines in vitro and in vivo. It is currently in clinical trials for treating patients with SCLC and various leukemia/lymphomas. Identification of predictive markers for response will benefit the clinical development of ABT-263. We identified the expression of Bcl-2 family genes that correlated best with sensitivity to ABT-263 in a panel of 36 SCLC and 31 leukemia/lymphoma cell lines. In cells sensitive to ABT-263, expression of Bcl-2 and Noxa is elevated, whereas expression of Mcl-1 is higher in resistant cells. We also examined global expression differences to identify gene signature sets that correlated with sensitivity to ABT-263 to generate optimal signature sets predictive of sensitivity to ABT-263. Independent cell lines were used to verify the predictive power of the gene sets and to refine the optimal gene signatures. When comparing normal lung tissue and SCLC primary tumors, the expression pattern of these genes in the tumor tissue is most similar to sensitive SCLC lines, whereas normal tissue is most similar to resistant SCLC lines. Most of the genes identified using global expression patterns are related to the apoptotic pathway; however, all but Bcl-rambo are distinct from the Bcl-2 family. This study leverages global expression data to identify key gene expression patterns for sensitivity to ABT-263 in SCLC and leukemia/lymphoma and may provide guidance in the selection of patients in future clinical trials. Mol Cancer Ther; 9(3); 545–57

Published

2010

50. Cytoskeletal organization following cannabinoid treatment in undifferentiated and differentiated PC12 cells

Author

John K. Stevens, Arthur M. Zimmerman, Stephen K. Tahir, and Judy Trogadis

Subjects

Cell Survival, medicine.medical_treatment, Cytoskeletal Organization, Microfilament, Microtubules, PC12 Cells, Biochemistry, law.invention, chemistry.chemical_compound, Confocal microscopy, law, Microtubule, Image Processing, Computer-Assisted, medicine, Animals, Molecular Biology, Cytoskeleton, Cannabinoids, Cell Differentiation, Cell Biology, Rats, Cell biology, Actin Cytoskeleton, Nerve growth factor, chemistry, Cannabinol, Cannabinoid, Cannabidiol, Cell Division, medicine.drug

Abstract

Confocal microscopy in association with three-dimensional reconstruction was used to examine the changes in the microtubules and microfilaments following cannabinoid treatment of PC12 cells. Microtubules and microfilaments were disrupted in a dose-dependent manner following treatment with 10–30 μM Δ9-tetrahydrocannabinol (THC). A disruption of microtubules and microfilaments was observed following treatment with 30 μM cannabidiol and cannabinol. The amount of microtubules and microfilaments was reduced in a dose-dependent manner following treatment with 10 and 20 μM THC. Cannabidiol and cannabinol reduced the amount of microtubules and microfilaments; however, the reduction was less than that observed with THC treatment. Following the addition of nerve growth factor, differentiated PC12 cells were generally more sensitive to cannabinoid treatments than undifferentiated cells. The possible mechanisms that may account for the changes in microtubules and microfilaments following cannabinoid treatment are discussed.Key words: cannabinoids, confocal microscopy, cytoskeleton, pheochromocytoma, PC12 cells, volume reconstruction.

Published

1992