Your search keyword '"John J. Tentler"' showing total 194 results

1. RX-5902, a novel β-catenin modulator, potentiates the efficacy of immune checkpoint inhibitors in preclinical models of triple-negative breast Cancer

Author

John J. Tentler, Julie Lang, Anna Capasso, Deog Joong Kim, Ely Benaim, Young B. Lee, Andrew Eisen, Stacey M. Bagby, Sarah J. Hartman, Betelehem W. Yacob, Brian Gittleman, Todd M. Pitts, Roberta Pelanda, S. Gail Eckhardt, and Jennifer R. Diamond

Subjects

RX-5902, Triple-negative breast cancer, p68, β-Catenin, PD-1 inhibitor, Immunotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Triple-negative breast cancer (TNBC) is an aggressive breast cancer subtype with limited systemic treatment options. RX-5902 is a novel anti-cancer agent that inhibits phosphorylated-p68 and thus attenuates nuclear β-catenin signaling. The purpose of this study was to evaluate the ability of β-catenin signaling blockade to enhance the efficacy of anti-CTLA-4 and anti-PD-1 immune checkpoint blockade in immunocompetent, preclinical models of TNBC. Methods Treatment with RX-5902, anti-PD-1, anti-CTLA-4 or the combination was investigated in BALB/c mice injected with the 4 T1 TNBC cell line. Humanized BALB/c-Rag2nullIl2rγnullSIRPαNOD (hu-CB-BRGS) mice transplanted with a human immune system were implanted with MDA-MB-231 cells. Mice were randomized into treatment groups according to human hematopoietic chimerism and treated with RX-5902, anti-PD-1 or the combination. At sacrifice, bone marrow, lymph nodes, spleen and tumors were harvested for flow cytometry analysis of human immune cells. Results The addition of RX-5902 to CTLA-4 or PD-1 inhibitors resulted in decreased tumor growth in the 4 T1 and human immune system and MDA-MB-231 xenograft models. Immunologic analyses demonstrated a significant increase in the number of activated T cells in tumor infiltrating lymphocytes (TILs) with RX-5902 treatment compared to vehicle (p

Published

2020

2. WEE1 Inhibition in Combination With Targeted Agents and Standard Chemotherapy in Preclinical Models of Pancreatic Ductal Adenocarcinoma

Author

Sarah J. Hartman, Stacey M. Bagby, Betelehem W. Yacob, Dennis M. Simmons, Morgan MacBeth, Christopher H. Lieu, S. Lindsey Davis, Alexis D. Leal, John J. Tentler, Jennifer R. Diamond, S. Gail Eckhardt, Wells A. Messersmith, and Todd M. Pitts

Subjects

pancreatic ductal adenocarcinoma, WEE1, DNA damage, 5-Fluorouracil (5-FU), irinotecan, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a highly lethal cancer with high incidences of p53 mutations. AZD1775 (adavosertib, previously MK-1775) is a small molecule WEE1 inhibitor that abrogates the G2M checkpoint and can potentially synergize with DNA damaging therapies commonly used in PDAC treatment. The purpose of this study was to identify combination partners for AZD1775, including standard chemotherapy or targeted agents, in PDAC preclinical models. Low powered preliminary screens demonstrated that two of the four PDX models responded better to the combinations of AZD1775 with irinotecan or capecitabine than to either single agent. Following the screens, two full powered PDAC PDX models of differing p53 status were tested with the combinations of AZD1775 and irinotecan or capecitabine. The combinations of AZD1775 and SN38 or 5-FU were also tested on PDAC cell lines. Cellular proliferation was measured using an IncuCyte Live Cell Imager and apoptosis was measured using a Caspase-Glo 3/7 assay. Flow cytometry was conducted to measure alterations in cell cycle distribution. Western blot analysis was used to determine the effects of the drug combinations on downstream effectors. In PDX models with mutated p53 status, there was significant tumor growth inhibition from the combination of AZD1775 with irinotecan or capecitabine (P ≤ 0.03), while PDX models with wild type p53 did not show anti-tumor synergy from the same combinations (P ≥ 0.08). The combination of AZD1775 with SN38 or 5-FU significantly decreased proliferation in all PDAC cell lines, and enhanced apoptosis in multiple cell lines. Cell cycle distribution was disrupted from the combination of AZD1775 with SN38 or 5-FU which was recorded as G2M arrest and decreased G1 phase. AZD1775 inhibited phospho-CDC2 and increased the expression of γH2AX that was either maintained or enhanced after combination with SN38 or 5-FU. The combination of AZD1775 with irinotecan/SN38 or capecitabine/5-FU showed anti-tumor effects in vivo and in vitro in PDAC models. These results support further investigation for these combination strategies to enhance outcomes for PDAC patients.

Published

2021

3. 'Omics' data integration and functional analyses link Enoyl-CoA hydratase, short chain 1 to drug refractory dilated cardiomyopathy

Author

Nzali V. Campbell, David A. Weitzenkamp, Ian L. Campbell, Ronald F. Schmidt, Chindo Hicks, Michael J. Morgan, David C. Irwin, and John J. Tentler

Subjects

drDCM, Omics, RNA-Seq, IPA, ECHS1, DBT, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Large-scale “omics” datasets have not been leveraged and integrated with functional analyses to discover potential drivers of cardiomyopathy. This study addresses the knowledge gap. Methods We coupled RNA sequence (RNA-Seq) variant detection and transcriptome profiling with pathway analysis to model drug refractory dilated cardiomyopathy (drDCM) using the BaseSpace sequencing hub and Ingenuity Pathway Analysis. We used RNA-Seq case-control datasets (n = 6 cases, n = 4 controls), exome sequence familial DCM datasets (n = 3 Italians, n = 5 Italians, n = 5 Chinese), and controls from the HapMap project (n = 5 Caucasians, and n = 5 Asians) for disease modeling and putative mutation discovery. Variant replication datasets: n = 128 cases and n = 15 controls. Source of datasets: NCBI Sequence Read Archive. Statistics: Pairwise differential expression analyses to determine differentially expressed genes and t-tests to calculate p-values. We adjusted for false discovery rates and reported q-values. We used chi-square tests to assess independence among variables, the Fisher’s Exact Tests and overlap p-values for the pathways and p-scores to rank network. Results Data revealed that ECHS1(enoyl-CoA hydratase, short chain 1(log2(foldchange) = 1.63329) hosts a mirtron, MIR3944 expressed in drDCM (FPKM = 5.2857) and not in controls (FPKM = 0). Has-miR3944-3p is a putative target of BAG1 (BCL2 associated athanogene 1(log2(foldchange) = 1.31978) and has-miR3944-5p of ITGAV (integrin subunit alpha V(log2(foldchange) = 1.46107) and RHOD (ras homolog family member D(log2(foldchange) = 1.28851). There is an association between ECHS1:11 V/A(rs10466126) and drDCM (p = 0.02496). The interaction (p = 2.82E-07) between ECHS1:75 T/I(rs1049951) and ECHS1:rs10466126 is associated with drDCM (p

Published

2018

4. A phase II clinical trial of the Aurora and angiogenic kinase inhibitor ENMD-2076 for previously treated, advanced, or metastatic triple-negative breast cancer

Author

Jennifer R. Diamond, S. G. Eckhardt, Todd M. Pitts, Adrie van Bokhoven, Dara Aisner, Daniel L. Gustafson, Anna Capasso, Sharon Sams, Peter Kabos, Kathryn Zolman, Tiffany Colvin, Anthony D. Elias, Anna M. Storniolo, Bryan P. Schneider, Dexiang Gao, John J. Tentler, Virginia F. Borges, and Kathy D. Miller

Subjects

Breast cancer, ENMD-2076, Aurora kinase inhibitor, Triple negative, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Triple-negative breast cancer (TNBC) remains an aggressive breast cancer subtype with limited treatment options. ENMD-2076 is a small-molecule inhibitor of Aurora and angiogenic kinases with proapoptotic and antiproliferative activity in preclinical models of TNBC. Methods This dual-institution, single-arm, two-stage, phase II clinical trial enrolled patients with locally advanced or metastatic TNBC previously treated with one to three prior lines of chemotherapy in the advanced setting. Patients were treated with ENMD-2076 250 mg orally once daily with continuous dosing in 4-week cycles until disease progression or unacceptable toxicity occurred. The primary endpoint was 6-month clinical benefit rate (CBR), and secondary endpoints included progression-free survival, pharmacokinetic profile, safety, and biologic correlates in archival and fresh serial tumor biopsies in a subset of patients. Results Forty-one patients were enrolled. The 6-month CBR was 16.7% (95% CI, 6–32.8%) and included two partial responses. The 4-month CBR was 27.8% (95% CI, 14–45.2%), and the average duration of benefit was 6.5 cycles. Common adverse events included hypertension, fatigue, diarrhea, and nausea. Treatment with ENMD-2076 resulted in a decrease in cellular proliferation and microvessel density and an increase in p53 and p73 expression, consistent with preclinical observations. Conclusions Single-agent ENMD-2076 treatment resulted in partial response or clinical benefit lasting more than 6 months in 16.7% of patients with pretreated, advanced, or metastatic TNBC. These results support the development of predictive biomarkers using archival and fresh tumor tissue, as well as consideration of mechanism-based combination strategies. Trial registration ClinicalTrials.gov, NCT01639248. Registered on July 12, 2012.

Published

2018

5. Antitumor activity of the polo-like kinase inhibitor, TAK-960, against preclinical models of colorectal cancer

Author

Peter J. Klauck, Stacey M. Bagby, Anna Capasso, Erica L. Bradshaw-Pierce, Heather M. Selby, Anna Spreafico, John J. Tentler, Aik Choon Tan, Jihye Kim, John J. Arcaroli, Alicia Purkey, Wells A. Messersmith, Keisuke Kuida, S. Gail Eckhardt, and Todd M. Pitts

Subjects

TAK-960, Plk1, Colorectal cancer, Patient-derived xenograft, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Polo-like kinase 1 (Plk1) is a serine/threonine kinase that is a key regulator of multiple stages of mitotic progression. Plk1 is upregulated in many tumor types including colorectal cancer (CRC) and portends a poor prognosis. TAK-960 is an ATP-competitive Plk1 inhibitor that has demonstrated efficacy across a broad range of cancer cell lines, including CRC. In this study, we investigated the activity of TAK-960 against a large collection of CRC models including 55 cell lines and 18 patient-derived xenografts. Methods Fifty-five CRC cell lines and 18 PDX models were exposed to TAK-960 and evaluated for proliferation (IC50) and Tumor Growth Inhibition Index, respectively. Additionally, 2 KRAS wild type and 2 KRAS mutant PDX models were treated with TAK-960 as single agent or in combination with cetuximab or irinotecan. TAK-960 mechanism of action was elucidated through immunoblotting and cell cycle analysis. Results CRC cell lines demonstrated a variable anti-proliferative response to TAK-960 with IC50 values ranging from 0.001 to > 0.75 μmol/L. Anti-proliferative effects were sustained after removal of drug. Following TAK-960 treatment a highly variable accumulation of mitotic (indicating cell cycle arrest) and apoptotic markers was observed. Cell cycle analysis demonstrated that TAK-960 treatment induced G2/M arrest and polyploidy. Six out of the eighteen PDX models responded to single agent TAK-960 therapy (TGII

Published

2018

6. Efficacy and Molecular Mechanisms of Differentiated Response to the Aurora and Angiogenic Kinase Inhibitor ENMD-2076 in Preclinical Models of p53-Mutated Triple-Negative Breast Cancer

Author

Anastasia A. Ionkina, John J. Tentler, Jihye Kim, Anna Capasso, Todd M. Pitts, Karen A. Ryall, Rebekah R. Howison, Peter Kabos, Carol A. Sartorius, Aik Choon Tan, S. Gail Eckhardt, and Jennifer R. Diamond

Subjects

triple negative breast cancer, ENMD-2076, targeted therapy, aurora kinase A, senescence, resistance mechanisms, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

PurposeTriple-negative breast cancer (TNBC) is a subtype associated with poor prognosis and for which there are limited therapeutic options. The purpose of this study was to evaluate the efficacy of ENMD-2076 in p53-mutated TNBC patient-derived xenograft (PDX) models and describe patterns of terminal cell fate in models demonstrating sensitivity, intrinsic resistance, and acquired resistance to ENMD-2076.Experimental designp53-mutated, TNBC PDX models were treated with ENMD-2076 and evaluated for mechanisms of sensitivity or resistance to treatment. Correlative tissue testing was performed on tumor tissue to assess for markers of proliferation, apoptosis, senescence, and pathways of resistance after treatment and at the time of acquired resistance.ResultsSensitivity to ENMD-2076 200 mg/kg daily was associated with induction of apoptosis while models exhibiting intrinsic or acquired resistance to treatment presented with a senescent phenotype. Response to ENMD-2076 was accompanied by an increase in p53 and p73 levels, even within the background of mutant p53. Treatment with ENMD-2076 resulted in a decrease in pAurA and an increase in pHH3. We observed a TNBC subtype switch from the luminal androgen receptor to the basal-like subtype at acquired resistance.ConclusionENMD-2076 has antitumor activity in preclinical models of p53-mutated TNBC. Increased levels of p53 and p73 correlated with sensitivity whereas senescence was associated with resistance to ENMD-2076. The novel finding of a TNBC subtype switch at time of acquired resistance may provide mechanistic insights into the biologic effects of selective pressure of anticancer treatments on TNBC. ENMD-2076 is currently being evaluated in a Phase 2 clinical trial in patients with metastatic, previously treated TNBC where these biologic correlates can be further explored.

Published

2017

7. Combined inhibition of MEK and Aurora A kinase in KRAS/PIK3CA double-mutant colorectal cancer models

Author

S. Lindsey eDavis, Kelli M. Robertson, Todd M. Pitts, John J. Tentler, Erica L. Bradshaw-Pierce, Peter J. Klauck, Stacey M. Bagby, Stephanie L. Hyatt, Heather M. Selby, Anna eSpreafico, Jeffrey A Ecsedy, John J. Arcaroli, Wells A. Messersmith, Aik Choon eTan, and S. Gail eEckhardt

Subjects

colorectal cancer, PIK3CA, KRAS mutation, trametinib, alisertib, MEK, Therapeutics. Pharmacology, RM1-950

Abstract

Aurora A kinase and MEK inhibitors induce different, and potentially complementary, effects on the cell cycle of malignant cells, suggesting a rational basis for utilizing these agents in combination. In this work, the combination of an Aurora A kinase and MEK inhibitor was evaluated in pre-clinical colorectal cancer models, with a focus on identifying a subpopulation in which it might be most effective. Increased synergistic activity of the drug combination was identified in colorectal cancer cell lines with concomitant KRAS and PIK3CA mutations. Anti-proliferative effects were observed upon treatment of these double-mutant cell lines with the drug combination, and tumor growth inhibition was observed in double-mutant human tumor xenografts, though effects were variable within this subset. Additional evaluation suggests that degree of G2/M delay and p53 mutation status affect apoptotic activity induced by combination therapy with an Aurora A kinase and MEK inhibitor in KRAS and PIK3CA mutant colorectal cancer. Overall, in vitro and in vivo testing was unable to identify a subset of colorectal cancer that was consistently responsive to the combination of a MEK and Aurora A kinase inhibitor.

Published

2015

8. Triple-negative breast cancer: bridging the gap from cancer genomics to predictive biomarkers

Author

S. Lindsey Davis, S. Gail Eckhardt, John J. Tentler, and Jennifer R. Diamond

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Triple-negative breast cancer (TNBC) represents a challenge clinically due to a lack of response to hormonal and HER2-targeted agents coupled with an aggressive disease course. As the biology of this breast cancer subtype is better understood, it is clear that TNBC is a heterogeneous disease and one targeted therapy is unlikely to be active in all patients. Biomarkers predictive of response to treatment are thus of great importance in TNBC. This review outlines studies evaluating biomarkers predictive of response to neoadjuvant chemotherapy and to targeted therapies in the advanced setting. The development of validated biomarkers in conjunction with novel targeted therapies represents an opportunity to improve patient outcomes in TNBC.

Published

2014

9. Supplemental Figure 3 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figure 3 shows impact of UNC2025 on cell viability.

Published

2023

10. Suppl Figure 1 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 1. Chemical structure and molecular data for TAK-733

Published

2023

11. Figure S2 from ALK Inhibitor Response in Melanomas Expressing EML4-ALK Fusions and Alternate ALK Isoforms

Author

William A. Robinson, Robert C. Doebele, Theresa Medina, Rene Gonzalez, Aik-Choon Tan, Matthew J. Rioth, Yiqun G. Shellman, John J. Tentler, Edna Chow-Maneval, Pratik Multani, Carol Amato, Allison Applegate, Keith Wells, Todd M. Pitts, Anh Le, Jennifer D. Hintzsche, Jason Christiansen, Danielle Murphy, Stacey M. Bagby, Jacqueline A. Turner, Judson Bemis, and Kasey L. Couts

Abstract

Characterization of EML4-ALK fusion variants in MB 2141

Published

2023

12. Suppl Figure 3 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 3. Immunoblot of Effector Proteins and Markers of Apoptosis in Melanoma Cell Lines

Published

2023

13. Supplemental Figure 2 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figure 2 shows impact of UNC2025 on colony forming potential.

Published

2023

14. Suppl Figure 2 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 2. Immunoblot Analysis of Effector Proteins in Melanoma Cell Lines

Published

2023

15. Supplemental Figure 4 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figure 4 shows TAM-family kinase expression in melanoma cell lines.

Published

2023

16. Suppl Table 1 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Table 1. IC50 Value Matrix

Published

2023

17. Supplementary Figure Legends from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Figure Legends

Published

2023

18. Suppl Figure 5 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 5. Immunoblot of Effector Proteins in Tumors from PDTX Mice Treated with TAK-733

Published

2023

19. Data from ALK Inhibitor Response in Melanomas Expressing EML4-ALK Fusions and Alternate ALK Isoforms

Author

William A. Robinson, Robert C. Doebele, Theresa Medina, Rene Gonzalez, Aik-Choon Tan, Matthew J. Rioth, Yiqun G. Shellman, John J. Tentler, Edna Chow-Maneval, Pratik Multani, Carol Amato, Allison Applegate, Keith Wells, Todd M. Pitts, Anh Le, Jennifer D. Hintzsche, Jason Christiansen, Danielle Murphy, Stacey M. Bagby, Jacqueline A. Turner, Judson Bemis, and Kasey L. Couts

Abstract

Oncogenic ALK fusions occur in several types of cancer and can be effectively treated with ALK inhibitors; however, ALK fusions and treatment response have not been characterized in malignant melanomas. Recently, a novel isoform of ALK (ALKATI) was reported in 11% of melanomas but the response of melanomas expressing ALKATI to ALK inhibition has not been well characterized. We analyzed 45 melanoma patient-derived xenograft models for ALK mRNA and protein expression. ALK expression was identified in 11 of 45 (24.4%) melanomas. Ten melanomas express wild-type (wt) ALK and/or ALKATI and one mucosal melanoma expresses multiple novel EML4-ALK fusion variants. Melanoma cells expressing different ALK variants were tested for response to ALK inhibitors. Whereas the melanoma expressing EML4-ALK were sensitive to ALK inhibitors in vitro and in vivo, the melanomas expressing wt ALK or ALKATI were not sensitive to ALK inhibitors. In addition, a patient with mucosal melanoma expressing ALKATI was treated with an ALK/ROS1/TRK inhibitor (entrectinib) on a phase I trial but did not respond. Our results demonstrate ALK fusions occur in malignant melanomas and respond to targeted therapy, whereas melanomas expressing ALKATI do not respond to ALK inhibitors. Targeting ALK fusions is an effective therapeutic option for a subset of melanoma patients, but additional clinical studies are needed to determine the efficacy of targeted therapies in melanomas expressing wt ALK or ALKATI. Mol Cancer Ther; 17(1); 222–31. ©2017 AACR.

Published

2023

20. Supplemental Figure 7 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figure 7 shows combined UNC2025 and vemurafenib treatment is tolerated in mice.

Published

2023

21. Supplementary Table 4 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Table 4: Combination Index (CI) Values. CI values calculated using the Chou and Talalay method from SRB proliferation data for varying concentrations of Nutlin and MLN8237 in combination. CI < 1 indicates synergy; CI = 1 additivity; CI > 1 antagonism

Published

2023

22. Suppl Figure 4 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 4. Representative PDTX Model MB1255 Treated with Vehicle or TAK-733

Published

2023

23. Data from First-in-Class Phosphorylated-p68 Inhibitor RX-5902 Inhibits β-Catenin Signaling and Demonstrates Antitumor Activity in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, John J. Tentler, S. Gail Eckhardt, Todd M. Pitts, Jihye Kim, Aik Choon Tan, Sarah J. Hartman, Brian Gittleman, Ely Benaim, Young B. Lee, Christina George, Deog Joong Kim, Julie G. Frank, Anastasia Ionkina, Betelehem W. Yacob, Naomi Currimjee, Kyrie L. Dailey, Stacey M. Bagby, and Anna Capasso

Abstract

RX-5902 is a first-in-class anticancer agent targeting phosphorylated-p68 and attenuating nuclear shuttling of β-catenin. The purpose of this study was to evaluate the efficacy of RX-5902 in preclinical models of triple-negative breast cancer (TNBC) and to explore effects on β-catenin expression. A panel of 18 TNBC cell lines was exposed to RX-5902, and changes in proliferation, apoptosis, cellular ploidy, and effector protein expression were assessed. Gene expression profiling was used in sensitive and resistant cell lines with pathway analysis to explore pathways associated with sensitivity to RX-5902. The activity of RX-5902 was confirmed in vivo in cell line and patient-derived tumor xenograft (PDX) models. RX-5902 demonstrated potent antiproliferative activity in vitro against TNBC cell lines with an average IC50 of 56 nmol/L in sensitive cell lines. RX-5902 treatment resulted in the induction of apoptosis, G2–M cell-cycle arrest, and aneuploidy in a subset of cell lines. RX-5902 was active in vivo against TNBC PDX models, and treatment resulted in a decrease in nuclear β-catenin. RX-5902 exhibited dose-proportional pharmacokinetics and plasma and tumor tissue in nude mice. Pathway analysis demonstrated an increase in the epithelial-to-mesenchymal transformation (EMT), TGFβ, and Wnt/β-catenin pathways associated with sensitivity to RX-5902. RX-5902 is active against in vitro and in vivo preclinical models of TNBC. Target engagement was confirmed with decreases in nuclear β-catenin and MCL-1 observed, confirming the proposed mechanism of action. This study supports the continued investigation of RX-5902 in TNBC and combinations with immunotherapy.

Published

2023

24. Supplementary Figure S1 from First-in-Class Phosphorylated-p68 Inhibitor RX-5902 Inhibits β-Catenin Signaling and Demonstrates Antitumor Activity in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, John J. Tentler, S. Gail Eckhardt, Todd M. Pitts, Jihye Kim, Aik Choon Tan, Sarah J. Hartman, Brian Gittleman, Ely Benaim, Young B. Lee, Christina George, Deog Joong Kim, Julie G. Frank, Anastasia Ionkina, Betelehem W. Yacob, Naomi Currimjee, Kyrie L. Dailey, Stacey M. Bagby, and Anna Capasso

Abstract

Survival curves for RX-5902 treatment and Abraxane and Vehicle control in vivo

Published

2023

25. Supplementary Figure 2 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Figure 2. Quantification of total cell counts and average cellular size at Day 15 as depicted in Fig. 4A.

Published

2023

26. Supplementary Table 1 from ALK Inhibitor Response in Melanomas Expressing EML4-ALK Fusions and Alternate ALK Isoforms

Author

William A. Robinson, Robert C. Doebele, Theresa Medina, Rene Gonzalez, Aik-Choon Tan, Matthew J. Rioth, Yiqun G. Shellman, John J. Tentler, Edna Chow-Maneval, Pratik Multani, Carol Amato, Allison Applegate, Keith Wells, Todd M. Pitts, Anh Le, Jennifer D. Hintzsche, Jason Christiansen, Danielle Murphy, Stacey M. Bagby, Jacqueline A. Turner, Judson Bemis, and Kasey L. Couts

Abstract

Primer sequences

Published

2023

27. Supplementary Table 3 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Table 3: Quantification of total cell counts and average cellular size under conditions depicted in Fig. 4A.

Published

2023

28. Supplementary Figure 4 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Figure 4. Effect of MLN8237 on Cleaved Caspase-3 in TNBC xenografts in vivo.

Published

2023

29. Supplementary Data from Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Author

Anthony D. Piscopio, Xuedong Liu, S. Gail Eckhardt, William P. Schiemann, Michael K. Wendt, James D. Winkler, John A. DeMattei, Sarah J. Hartman, Brian Gittleman, John J. Tentler, Timothy P. Newton, Betelehem W. Yacob, Jessica Pafford, Stacey M. Bagby, Andrew J. Phillips, Gan Zhang, Christopher G. Nasveschuk, Dana Ungermannova, Todd M. Pitts, and Jennifer R. Diamond

Abstract

Supplementary Data from Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Published

2023

30. Suppl Table 2 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Table 2. TAK-733 PD/ Conc. Summary, A375 tumor bearing nude mouse

Published

2023

31. Supplementary Figure 1 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Figure 1. Treatment with MLN8237 induces markers of cellular senescence in two additional CAL-51 p53 and p73 shRNA knockdown clones (p53-12, p73-26).

Published

2023

32. Suppl Table 4 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Table 4. Antitumor Activity of Orally Administered TAK-733 Against A375 Melanoma Tumor Xenografts in Female Athymic Nude Mice

Published

2023

33. Supplemental Figure 6 from Inhibition of MERTK Promotes Suppression of Tumor Growth in BRAF Mutant and BRAF Wild-Type Melanoma

Author

Douglas K. Graham, Deborah DeRyckere, H. Shelton Earp, Stephen V. Frye, Xiaodong Wang, S. Gail Eckhardt, Tal Burstyn-Cohen, Rotem Kami, William A. Robinson, Stacey M. Bagby, Jacqueline Carrico, John J. Tentler, Katherine A. Minson, and Lenka Sinik

Abstract

Supplemental Figures 6 shows efficacy of UNC2025 in a melanoma wild-type PDX mode.

Published

2023

34. Supplementary Table 2 from p53 Family Members Regulate Phenotypic Response to Aurora Kinase A Inhibition in Triple-Negative Breast Cancer

Author

Jennifer R. Diamond, S. Gail Eckhardt, Joaquin M. Espinosa, Kelly D. Sullivan, Carol A. Sartorius, Peter Kabos, Magdalena J. Glogowska, Todd M. Pitts, Timothy P. Newton, Aik Choon Tan, Anastasia A. Ionkina, and John J. Tentler

Abstract

Supplementary Table 2: Sensitivity of CAL-51 KD clones to MLN8237 in vitro.

Published

2023

35. Suppl Figure 6 from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Suppl Figure 6. Genomic Analyses of PDTX MB1374 Treated to Resistance

Published

2023

36. Data from Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Author

Anthony D. Piscopio, Xuedong Liu, S. Gail Eckhardt, William P. Schiemann, Michael K. Wendt, James D. Winkler, John A. DeMattei, Sarah J. Hartman, Brian Gittleman, John J. Tentler, Timothy P. Newton, Betelehem W. Yacob, Jessica Pafford, Stacey M. Bagby, Andrew J. Phillips, Gan Zhang, Christopher G. Nasveschuk, Dana Ungermannova, Todd M. Pitts, and Jennifer R. Diamond

Abstract

Histone deacetylases (HDACs) play critical roles in epigenomic regulation, and histone acetylation is dysregulated in many human cancers. Although HDAC inhibitors are active in T-cell lymphomas, poor isoform selectivity, narrow therapeutic indices, and a deficiency of reliable biomarkers may contribute to the lack of efficacy in solid tumors. In this article, we report the discovery and preclinical development of the novel, orally bioavailable, class-I–selective HDAC inhibitor, OKI-179. OKI-179 and its cell active predecessor OKI-005 are thioester prodrugs of the active metabolite OKI-006, a unique congener of the natural product HDAC inhibitor largazole. OKI-006, OKI-005, and subsequently OKI-179, were developed through a lead candidate optimization program designed to enhance physiochemical properties without eroding potency and selectivity relative to largazole. OKI-005 displays antiproliferative activity in vitro with induction of apoptosis and increased histone acetylation, consistent with target engagement. OKI-179 showed antitumor activity in preclinical cancer models with a favorable pharmacokinetic profile and on-target pharmacodynamic effects. Based on its potency, desirable class I HDAC inhibition profile, oral bioavailability, and efficacy against a broad range of solid tumors, OKI-179 is currently being evaluated in a first-in-human phase I clinical trial with plans for continued clinical development in solid tumor and hematologic malignancies.

Published

2023

37. Supplementary Figure Legends from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

Supplementary Figure Legends

Published

2023

38. Data from Antitumor Activity of the MEK Inhibitor TAK-733 against Melanoma Cell Lines and Patient-Derived Tumor Explants

Author

S. Gail Eckhardt, Patrick W. Vincent, Shawn M. O'Connell, Robyn Fabrey, Esha Gangolli, Todd M. Pitts, Peter J. Klauck, S. Lindsey Davis, Kelli M. Robertson, Kelsey L. Brunkow, Heather M. Selby, Aik-Choon Tan, John J. Tentler, and Lindsey N. Micel

Abstract

The goal of this study was to investigate the activity of the selective MEK1/2 inhibitor TAK-733 in both melanoma cell lines and patient-derived melanoma xenograft models. In vitro cell proliferation assays using the sulforhodamine B assay were conducted to determine TAK-733 potency and melanoma responsiveness. In vivo murine modeling with eleven patient-derived melanoma explants evaluated daily dosing of TAK-733 at 25 or 10 mg/kg. Immunoblotting was performed to evaluate on-target activity and downstream inhibition by TAK-733 in both in vitro and in vivo studies. TAK-733 demonstrated broad activity in most melanoma cell lines with relative resistance observed at IC50 > 0.1 μmol/L in vitro. TAK-733 also exhibited activity in 10 out of 11 patient-derived explants with tumor growth inhibition ranging from 0% to 100% (P < 0.001–0.03). Interestingly, BRAFV600E and NRAS mutational status did not correlate with responsiveness to TAK-733. Pharmacodynamically, pERK was suppressed in sensitive cell lines and tumor explants, confirming TAK-733–mediated inhibition of MEK1/2, although the demonstration of similar effects in the relatively resistant cell lines and tumor explants suggests that escape pathways are contributing to melanoma survival and proliferation. These data demonstrate that TAK-733 exhibits robust tumor growth inhibition and regression against human melanoma cell lines and patient-derived xenograft models, suggesting that further clinical development in melanoma is of scientific interest. Particularly interesting is the activity in BRAF wild-type models, where current approved therapy such as vemurafenib has been reported not to be active. Mol Cancer Ther; 14(2); 317–25. ©2014 AACR.

Published

2023

39. Supplementary Figure from Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Author

Anthony D. Piscopio, Xuedong Liu, S. Gail Eckhardt, William P. Schiemann, Michael K. Wendt, James D. Winkler, John A. DeMattei, Sarah J. Hartman, Brian Gittleman, John J. Tentler, Timothy P. Newton, Betelehem W. Yacob, Jessica Pafford, Stacey M. Bagby, Andrew J. Phillips, Gan Zhang, Christopher G. Nasveschuk, Dana Ungermannova, Todd M. Pitts, and Jennifer R. Diamond

Abstract

Supplementary Figure from Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Published

2023

40. Preclinical Development of the Class-I–Selective Histone Deacetylase Inhibitor OKI-179 for the Treatment of Solid Tumors

Author

Jennifer R. Diamond, Todd M. Pitts, Dana Ungermannova, Christopher G. Nasveschuk, Gan Zhang, Andrew J. Phillips, Stacey M. Bagby, Jessica Pafford, Betelehem W. Yacob, Timothy P. Newton, John J. Tentler, Brian Gittleman, Sarah J. Hartman, John A. DeMattei, James D. Winkler, Michael K. Wendt, William P. Schiemann, S. Gail Eckhardt, Xuedong Liu, and Anthony D. Piscopio

Subjects

Histone Deacetylase Inhibitors, Histones, Cancer Research, Oncology, Neoplasms, Humans, Acetylation, Histone Deacetylase 1, Histone Deacetylases, Article

Abstract

Histone deacetylases (HDACs) play critical roles in epigenomic regulation, and histone acetylation is dysregulated in many human cancers. Although HDAC inhibitors are active in T-cell lymphomas, poor isoform selectivity, narrow therapeutic indices, and a deficiency of reliable biomarkers may contribute to the lack of efficacy in solid tumors. In this article, we report the discovery and preclinical development of the novel, orally bioavailable, class-I–selective HDAC inhibitor, OKI-179. OKI-179 and its cell active predecessor OKI-005 are thioester prodrugs of the active metabolite OKI-006, a unique congener of the natural product HDAC inhibitor largazole. OKI-006, OKI-005, and subsequently OKI-179, were developed through a lead candidate optimization program designed to enhance physiochemical properties without eroding potency and selectivity relative to largazole. OKI-005 displays antiproliferative activity in vitro with induction of apoptosis and increased histone acetylation, consistent with target engagement. OKI-179 showed antitumor activity in preclinical cancer models with a favorable pharmacokinetic profile and on-target pharmacodynamic effects. Based on its potency, desirable class I HDAC inhibition profile, oral bioavailability, and efficacy against a broad range of solid tumors, OKI-179 is currently being evaluated in a first-in-human phase I clinical trial with plans for continued clinical development in solid tumor and hematologic malignancies.

Published

2022

41. Supplementary Figure 3 from Overcoming IGF1R/IR Resistance through Inhibition of MEK Signaling in Colorectal Cancer Models

Author

Stephen Leong, S. Gail Eckhardt, John J. Tentler, Heather M. Selby, Maria I. Kachaeva, Anna Spreafico, Martine C. McManus, Aik Choon Tan, Gillian N. Kulikowski, Timothy P. Newton, Todd M. Pitts, and Sara A. Flanigan

Abstract

Supplementary Figure 3 - PDF file 91K, Combination Fraction Inhibited Graphs

Published

2023

42. Supplementary Figure 3 from Predictive Biomarkers of Sensitivity to the Aurora and Angiogenic Kinase Inhibitor ENMD-2076 in Preclinical Breast Cancer Models

Author

John J. Tentler, Graham C. Fletcher, Mark R. Bray, Todd M. Pitts, Marileila Varella-Garcia, Maria I. Kachaeva, Kelsey L. Brunkow, Heather M. Selby, Timothy P. Newton, Aik Choon Tan, S. Gail Eckhardt, and Jennifer R. Diamond

Abstract

PDF file - 121K, Heatmap of the 580 differentially expressed genes between ENMD-2076-sensitive and -resistant cell lines as identified by the Significance Analysis of Microarrays (SAM) with FD

Published

2023

43. Supplementary Figure 2 from Overcoming IGF1R/IR Resistance through Inhibition of MEK Signaling in Colorectal Cancer Models

Author

Stephen Leong, S. Gail Eckhardt, John J. Tentler, Heather M. Selby, Maria I. Kachaeva, Anna Spreafico, Martine C. McManus, Aik Choon Tan, Gillian N. Kulikowski, Timothy P. Newton, Todd M. Pitts, and Sara A. Flanigan

Abstract

Supplementary Figure 2 - PDF file 153K, Bar Graphs of CI Values

Published

2023

44. Supplementary Figure Legends from Overcoming IGF1R/IR Resistance through Inhibition of MEK Signaling in Colorectal Cancer Models

Author

Stephen Leong, S. Gail Eckhardt, John J. Tentler, Heather M. Selby, Maria I. Kachaeva, Anna Spreafico, Martine C. McManus, Aik Choon Tan, Gillian N. Kulikowski, Timothy P. Newton, Todd M. Pitts, and Sara A. Flanigan

Abstract

Supplementary Figure Legends - PDF file 41K, Supplementary Figure Legends

Published

2023

45. Data from Predictive Biomarkers of Sensitivity to the Aurora and Angiogenic Kinase Inhibitor ENMD-2076 in Preclinical Breast Cancer Models

Author

John J. Tentler, Graham C. Fletcher, Mark R. Bray, Todd M. Pitts, Marileila Varella-Garcia, Maria I. Kachaeva, Kelsey L. Brunkow, Heather M. Selby, Timothy P. Newton, Aik Choon Tan, S. Gail Eckhardt, and Jennifer R. Diamond

Abstract

Purpose: The Aurora kinases are a family of conserved serine-threonine kinases with key roles in mitotic cell division. As with other promising anticancer targets, patient selection strategies to identify a responsive subtype will likely be required for successful clinical development of Aurora kinase inhibitors. The purpose of this study was to evaluate the antitumor activity of the Aurora and angiogenic kinase inhibitor ENMD-2076 against preclinical models of breast cancer with identification of candidate predictive biomarkers.Experimental Design: Twenty-nine breast cancer cell lines were exposed to ENMD-2076 and the effects on proliferation, apoptosis, and cell-cycle distribution were evaluated. In vitro activity was confirmed in MDA-MB-468 and MDA-MB-231 triple-negative breast cancer xenografts. Systematic gene expression analysis was used to identify up- and downregulated pathways in the sensitive and resistant cell lines, including within the triple-negative breast cancer subset.Results: ENMD-2076 showed antiproliferative activity against breast cancer cell lines, with more robust activity against cell lines lacking estrogen receptor expression and those without increased HER2 expression. Within the triple-negative breast cancer subset, cell lines with a p53 mutation and increased p53 expression were more sensitive to the cytotoxic and proapoptotic effects of ENMD-2076 exposure than cell lines with decreased p53 expression.Conclusions: ENMD-2076 exhibited robust anticancer activity against models of triple-negative breast cancer and the candidate predictive biomarkers identified in this study may be useful in selecting patients for Aurora kinase inhibitors in the future. Clin Cancer Res; 19(1); 291–303. ©2012 AACR.

Published

2023

46. Data from Preclinical and Dose-Finding Phase I Trial Results of Combined Treatment with a TORC1/2 Inhibitor (TAK-228) and Aurora A Kinase Inhibitor (Alisertib) in Solid Tumors

Author

Jennifer R. Diamond, Todd M. Pitts, S. Gail Eckhardt, Stephen Leong, Wells A. Messersmith, Daniel L. Gustafson, Kyrie L. Lopez, Anna Capasso, John J. Tentler, Jihye Kim, Aik-Choon Tan, Ashley E. Glode, Cindy L. O'Bryant, Bradley R. Corr, Elaine T. Lam, Joshua M. Marcus, Brian Gittleman, James D. Orth, Stacey M. Bagby, Anastasia A. Ionkina, and S. Lindsey Davis

Abstract

Purpose:The purpose of this study was to evaluate the rational combination of TORC1/2 inhibitor TAK-228 and Aurora A kinase inhibitor alisertib in preclinical models of triple-negative breast cancer (TNBC) and to conduct a phase I dose escalation trial in patients with advanced solid tumors.Experimental Design:TNBC cell lines and patient-derived xenograft (PDX) models were treated with alisertib, TAK-228, or the combination and evaluated for changes in proliferation, cell cycle, mTOR pathway modulation, and terminal cellular fate, including apoptosis and senescence. A phase I clinical trial was conducted in patients with advanced solid tumors treated with escalating doses of alisertib and TAK-228 using a 3+3 design to determine the maximum tolerated dose (MTD).Results:The combination of TAK-228 and alisertib resulted in decreased proliferation and cell-cycle arrest in TNBC cell lines. Treatment of TNBC PDX models resulted in significant tumor growth inhibition and increased apoptosis with the combination. In the phase I dose escalation study, 18 patients with refractory solid tumors were enrolled. The MTD was alisertib 30 mg b.i.d. days 1 to 7 of a 21-day cycle and TAK-228 2 mg daily, continuous dosing. The most common treatment-related adverse events were neutropenia, fatigue, nausea, rash, mucositis, and alopecia.Conclusions:The addition of TAK-228 to alisertib potentiates the antitumor activity of alisertib in vivo, resulting in increased cell death and apoptosis. The combination is tolerable in patients with advanced solid tumors and should be evaluated further in expansion cohorts with additional pharmacodynamic assessment.

Published

2023

47. Supplementary Figure S1 from Preclinical and Dose-Finding Phase I Trial Results of Combined Treatment with a TORC1/2 Inhibitor (TAK-228) and Aurora A Kinase Inhibitor (Alisertib) in Solid Tumors

Author

Jennifer R. Diamond, Todd M. Pitts, S. Gail Eckhardt, Stephen Leong, Wells A. Messersmith, Daniel L. Gustafson, Kyrie L. Lopez, Anna Capasso, John J. Tentler, Jihye Kim, Aik-Choon Tan, Ashley E. Glode, Cindy L. O'Bryant, Bradley R. Corr, Elaine T. Lam, Joshua M. Marcus, Brian Gittleman, James D. Orth, Stacey M. Bagby, Anastasia A. Ionkina, and S. Lindsey Davis

Abstract

Pharmacodynamic effects of alisertib and TAK-228 in patient tissue samples

Published

2023

48. Data from Development of an Integrated Genomic Classifier for a Novel Agent in Colorectal Cancer: Approach to Individualized Therapy in Early Development

Author

S. Gail Eckhardt, Christopher Korch, Marileila Varella-Garcia, Fred R. Hirsch, Christopher D. Coldren, Stephen Leong, Sara A. Flanigan, Amy M. Brown, John J. Tentler, Gillian N. Kulikowski, Aik Choon Tan, and Todd M. Pitts

Abstract

Background: A plethora of agents is in early stages of development for colorectal cancer (CRC), including those that target the insulin-like growth factor I receptor (IGFIR) pathway. In the current environment of numerous cancer targets, it is imperative that patient selection strategies be developed with the intent of preliminary testing in the latter stages of phase I trials. The goal of this study was to develop and characterize predictive biomarkers for an IGFIR tyrosine kinase inhibitor, OSI-906, that could be applied in CRC-specific studies of this agent.Methods: Twenty-seven CRC cell lines were exposed to OSI-906 and classified according to IC50 value as sensitive (≤1.5 μmol/L) or resistant (>5 μmol/L). Cell lines were subjected to immunoblotting and immunohistochemistry for effector proteins, IGFIR copy number by fluorescence in situ hybridization, KRAS/BRAF/phosphoinositide 3-kinase mutation status, and baseline gene array analysis. The most sensitive and resistant cell lines were used for gene array and pathway analyses, along with shRNA knockdown of highly ranked genes. The resulting integrated genomic classifier was then tested against eight human CRC explants in vivo.Results: Baseline gene array data from cell lines and xenografts were used to develop a k-top scoring pair (k-TSP) classifier, which, in combination with IGFIR fluorescence in situ hybridization and KRAS mutational status, was able to predict with 100% accuracy a test set of patient-derived CRC xenografts.Conclusions: These results indicate that an integrated approach to the development of individualized therapy is feasible and should be applied early in the development of novel agents, ideally in conjunction with late-stage phase I trials. Clin Cancer Res; 16(12); 3193–204. ©2010 AACR.

Published

2023

49. Data from Identification of Predictive Markers of Response to the MEK1/2 Inhibitor Selumetinib (AZD6244) in K-ras–Mutated Colorectal Cancer

Author

S. Gail Eckhardt, Wells A. Messersmith, John J. Arcaroli, Stephen Leong, Gillian N. Kulikowski, Sara A. Flanigan, Maria I. Kachaeva, Heather M. Selby, M. Pia Morelli, Todd M. Pitts, Anna Spreafico, Aik Choon Tan, Sujatha Nallapareddy, and John J. Tentler

Abstract

Mutant K-ras activity leads to the activation of the RAS/RAF/MEK/ERK pathway in approximately 44% of colorectal cancer (CRC) tumors. Accordingly, several inhibitors of the MEK pathway are under clinical evaluation in several malignancies including CRC. The aim of this study was to develop and characterize predictive biomarkers of response to the MEK1/2 inhibitor AZD6244 in CRC in order to maximize the clinical utility of this agent. Twenty-seven human CRC cell lines were exposed to AZD6244 and classified according to the IC50 value as sensitive (≤0.1 μmol/L) or resistant (>1 μmol/L). All cell lines were subjected to immunoblotting for effector proteins, K-ras/BRAF mutation status, and baseline gene array analysis. Further testing was done in cell line xenografts and K-ras mutant CRC human explants models to develop a predictive genomic classifier for AZD6244. The most sensitive and resistant cell lines were subjected to differential gene array and pathway analyses. Members of the Wnt signaling pathway were highly overexpressed in cell lines resistant to AZD6244 and seem to be functionally involved in mediating resistance by shRNA knockdown studies. Baseline gene array data from CRC cell lines and xenografts were used to develop a k-top scoring pair (k-TSP) classifier, which predicted with 71% accuracy which of a test set of patient-derived K-ras mutant CRC explants would respond to AZD6244, providing the basis for a patient-selective clinical trial. These results also indicate that resistance to AZD6244 may be mediated, in part, by the upregulation of the Wnt pathway, suggesting potential rational combination partners for AZD6244 in CRC. Mol Cancer Ther; 9(12); 3351–62. ©2010 AACR.

Published

2023

50. Supplementary Figure 5 from Overcoming IGF1R/IR Resistance through Inhibition of MEK Signaling in Colorectal Cancer Models

Author

Stephen Leong, S. Gail Eckhardt, John J. Tentler, Heather M. Selby, Maria I. Kachaeva, Anna Spreafico, Martine C. McManus, Aik Choon Tan, Gillian N. Kulikowski, Timothy P. Newton, Todd M. Pitts, and Sara A. Flanigan

Abstract

Supplementary Figure 5 - PDF file 116K, Caspase 3/7 Activity

Published

2023