Your search keyword '"Agus DB"' showing total 11 results

1. Phase 1/2 study of orteronel (TAK-700), an investigational 17,20-lyase inhibitor, with docetaxel-prednisone in metastatic castration-resistant prostate cancer.

Author

Petrylak DP, Gandhi JG, Clark WR, Heath E, Lin J, Oh WK, Agus DB, Carthon B, Moran S, Kong N, Suri A, Bargfrede M, and Liu G

Subjects

Aged, Aged, 80 and over, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Antineoplastic Combined Chemotherapy Protocols, Dehydroepiandrosterone Sulfate blood, Disease Progression, Disease-Free Survival, Docetaxel, Dose-Response Relationship, Drug, Humans, Imidazoles administration & dosage, Imidazoles adverse effects, Male, Middle Aged, Naphthalenes administration & dosage, Naphthalenes adverse effects, Prednisone administration & dosage, Prostate-Specific Antigen, Prostatic Neoplasms, Castration-Resistant drug therapy, Steroid 17-alpha-Hydroxylase antagonists & inhibitors, Taxoids administration & dosage, Testosterone blood, Antineoplastic Agents therapeutic use, Imidazoles therapeutic use, Naphthalenes therapeutic use, Prednisone therapeutic use, Taxoids therapeutic use

Abstract

Background: Docetaxel-prednisone (DP) is an approved therapy for metastatic castration-resistant prostate cancer (mCRPC). Orteronel (TAK-700) is an investigational, selective, non-steroidal inhibitor of 17,20-lyase, a key enzyme in androgenic hormone production. This phase 1/2 study evaluated orteronel plus DP in mCRPC patients., Methods: Adult men with chemotherapy-naïve mCRPC, serum prostate-specific antigen (PSA) ≥5 ng/mL, and serum testosterone <50 ng/dL received oral orteronel 200 or 400 mg twice-daily (BID) in phase 1 to determine the recommended dose for phase 2, plus intravenous docetaxel 75 mg/m(2) every 3 weeks, and oral prednisone 5 mg BID. Phase 2 objectives included safety, pharmacokinetics, and efficacy., Results: In phase 1 (n = 6, orteronel 200 mg; n = 8, orteronel 400 mg), there was one dose-limiting toxicity of grade 3 febrile neutropenia at 400 mg BID. This dose was evaluated further in phase 2 (n = 23). After 4 cycles, 68, 59, and 23% of patients achieved ≥30, ≥50, and ≥90% PSA reductions, respectively; median best PSA response was -77%. Seven of 10 (70%) RECIST-evaluable patients achieved objective partial responses. Median time to PSA progression and radiographic disease progression was 6.7 and 12.9 months, respectively. Dehydroepiandrosterone-sulfate (DHEA-S) and testosterone levels were rapidly and durably reduced. Common adverse events were fatigue (78%), alopecia (61%), diarrhea (48%), nausea (43%), dysgeusia (39%), and neutropenia (39%). Orteronel and docetaxel pharmacokinetics were similar alone and in combination., Conclusions: Orteronel plus DP was tolerable, with substantial reductions in PSA, DHEA-S, and testosterone levels, and evidence for measurable disease responses.

Published

2015

2. Quantitative proteomic profiling identifies protein correlates to EGFR kinase inhibition.

Author

Kani K, Faca VM, Hughes LD, Zhang W, Fang Q, Shahbaba B, Luethy R, Erde J, Schmidt J, Pitteri SJ, Zhang Q, Katz JE, Gross ME, Plevritis SK, McIntosh MW, Jain A, Hanash S, Agus DB, and Mallick P

Subjects

Animals, Cell Line, Tumor, Drug Resistance, Neoplasm, ErbB Receptors metabolism, Female, Gefitinib, Humans, Mice, Mice, Inbred BALB C, Mice, Nude, Proteomics, Quinazolines pharmacology, Reproducibility of Results, Signal Transduction drug effects, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, ErbB Receptors antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Proteome

Abstract

Clinical oncology is hampered by lack of tools to accurately assess a patient's response to pathway-targeted therapies. Serum and tumor cell surface proteins whose abundance, or change in abundance in response to therapy, differentiates patients responding to a therapy from patients not responding to a therapy could be usefully incorporated into tools for monitoring response. Here, we posit and then verify that proteomic discovery in in vitro tissue culture models can identify proteins with concordant in vivo behavior and further, can be a valuable approach for identifying tumor-derived serum proteins. In this study, we use stable isotope labeling of amino acids in culture (SILAC) with proteomic technologies to quantitatively analyze the gefitinib-related protein changes in a model system for sensitivity to EGF receptor (EGFR)-targeted tyrosine kinase inhibitors. We identified 3,707 intracellular proteins, 1,276 cell surface proteins, and 879 shed proteins. More than 75% of the proteins identified had quantitative information, and a subset consisting of 400 proteins showed a statistically significant change in abundance following gefitinib treatment. We validated the change in expression profile in vitro and screened our panel of response markers in an in vivo isogenic resistant model and showed that these were markers of gefitinib response and not simply markers of phospho-EGFR downregulation. In doing so, we also were able to identify which proteins might be useful as markers for monitoring response and which proteins might be useful as markers for a priori prediction of response., (©2012 AACR)

Published

2012

3. Safety and pharmacokinetics of high-dose gefitinib in patients with solid tumors: results of a phase I study.

Author

Gross ME, Leichman L, Lowe ES, Swaisland A, and Agus DB

Subjects

Administration, Oral, Adult, Aged, Aged, 80 and over, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Dose-Response Relationship, Drug, Female, Gefitinib, Humans, Male, Maximum Tolerated Dose, Middle Aged, Neoplasms pathology, Quinazolines adverse effects, Quinazolines pharmacokinetics, Treatment Outcome, Antineoplastic Agents administration & dosage, Neoplasms drug therapy, Quinazolines administration & dosage

Abstract

Purpose: Previous studies established the safety of continuous gefitinib 250 or 500 mg daily. It was postulated that a higher dose may have increased efficacy by inhibiting signaling in both the mitogen-activated protein kinase and AKT pathways. This study investigated the tolerability, pharmacokinetics, and antitumor activity of high-dose gefitinib in patients with refractory solid malignancies., Methods: Sequential cohorts received oral gefitinib once or twice-weekly, with dose escalation from 1,500 to 3,500 mg., Results: Twenty-three patients received gefitinib at seven dose levels (1,500, 2,000, 2,500, 3,000, and 3,500 mg once-weekly; 1,500 and 2,000 mg twice-weekly). Gefitinib was well tolerated, with no dose-limiting toxicities. The maximum tolerated dose was not reached. The most common gefitinib-related adverse events were nausea and diarrhea, vomiting, and rash. Pharmacokinetic data demonstrated no consistent increase in exposure to gefitinib with increasing dose across cohorts. Consequently, the study was stopped early and gefitinib 2,000 mg twice-weekly was the highest dose administered. One of eight patients with non-small-cell lung cancer achieved a partial response., Conclusions: Exposure to gefitinib did not increase consistently with increasing dose beyond gefitinib 1,500 mg once-weekly or twice-weekly. These data do not support further evaluation of gefitinib at high-dose schedules.

Published

2012

4. Epidermal growth factor receptor dimerization status determines skin toxicity to HER-kinase targeted therapies.

Author

Laux I, Jain A, Singh S, and Agus DB

Subjects

Antibodies, Monoclonal, Humanized, Cell Culture Techniques, Cetuximab, Dimerization, ErbB Receptors drug effects, Gefitinib, Humans, Keratinocytes physiology, Ligands, Receptor, ErbB-2 drug effects, Signal Transduction, Antibodies, Monoclonal adverse effects, Antineoplastic Agents adverse effects, ErbB Receptors physiology, Exanthema chemically induced, Exanthema physiopathology, Quinazolines adverse effects, Receptor, ErbB-2 physiology

Abstract

Skin toxicity, a common drug-related adverse event observed in cancer patients treated with epidermal growth factor receptor (EGFR)-directed therapies is rarely seen with therapies targeting HER2. This study reports the significance of the EGFR and HER2 dimerization status in skin with regard to these dermatologic side effects. We demonstrate the differential effect of HER-directed therapies on the ligand driven activation status of EGFR, HER2 and MAPK in normal human epidermal keratinocytes. EGFR-directed therapies, such as gefitinib and cetuximab, inhibited ligand-induced activation of EGFR and MAPK in human keratinocytes. Pertuzumab, an antibody interfering with functional HER2 heterodimerization, failed to block ligand-induced HER signaling in primary keratinocytes. Using a novel proximity-based dimerization assay (eTagtrade mark) we show that EGFR homodimers are the predominant HER dimer pair in normal primary kertinocytes and in normal skin tissue from 16 patients with solid malignancies. The presence of [p]EGFR and [p]MAPK, but the absence of [p]HER2, demonstrates productive signaling via EGFR but not HER2 in human skin. These data illustrate the importance of the EGFR dimerization partner in human skin and suggests that inhibition of EGFR homodimer signaling rather than EGFR/HER2 heterodimer signaling maybe the key molecular event determining dermatologic toxicity discrepancies observed between EGFR-targeted versus HER2-targeted therapies.

Published

2006

5. PPARgamma signaling: one size fits all?

Author

Jain A and Agus DB

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents therapeutic use, Cell Differentiation drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Colorectal Neoplasms drug therapy, Colorectal Neoplasms metabolism, Colorectal Neoplasms pathology, Humans, Ligands, PPAR gamma metabolism, Structure-Activity Relationship, Antineoplastic Agents pharmacology, PPAR gamma agonists, Signal Transduction drug effects

Abstract

Outcome of PPARgamma activation in cancer cells is not one-dimensional. PPARgamma signaling is dependent upon PPARgamma ligand affinity and binding characteristics, target cell context and interacting signaling networks.

Published

2004

6. Targeting the HER-kinase axis in cancer.

Author

Gross ME, Shazer RL, and Agus DB

Subjects

Animals, Clinical Trials as Topic, ErbB Receptors metabolism, Gene Expression Regulation, Humans, Ligands, Neoplasms metabolism, Receptor, ErbB-2 metabolism, Receptor, ErbB-3 metabolism, Receptor, ErbB-4, Signal Transduction, Antineoplastic Agents therapeutic use, ErbB Receptors antagonists & inhibitors, Neoplasms drug therapy, Receptor, ErbB-2 antagonists & inhibitors, Receptor, ErbB-3 antagonists & inhibitors

Abstract

The human epidermal growth factor receptor (HER) family of receptor tyrosine kinases controls critical pathways involved in the differentiation, growth, division, and motility of normal epithelial cells. Most human solid tumors are of epithelial origin. The process of malignant transformation and progression in many cancers may depend on activation of ligands and receptors that function as part of the HER-kinase pathway. This signaling axis has earned increased attention because of the development of antibodies and small-molecule tyrosine kinase inhibitors that specifically target components of the HER-kinase axis for cancer therapy. This review focuses on the basic biology underlying HER-kinase pathway activation and the current state of development for agents that target this axis. In particular, the importance of pan-HER inhibitors is discussed.

Published

2004

7. Update on HER-kinase-directed therapy in prostate cancer.

Author

Gross ME, Jo S, and Agus DB

Subjects

Adenocarcinoma enzymology, Androgens, Antibodies, Monoclonal immunology, Antibodies, Monoclonal pharmacology, Antibodies, Monoclonal, Humanized, Antineoplastic Agents pharmacology, Breast Neoplasms drug therapy, Clinical Trials as Topic, Dimerization, Disease Progression, Drug Delivery Systems, Enzyme Activation, ErbB Receptors chemistry, ErbB Receptors immunology, ErbB Receptors physiology, Female, Gene Expression Regulation, Neoplastic drug effects, Humans, Ligands, Male, Neoplasm Proteins immunology, Neoplasm Proteins physiology, Neoplasms, Hormone-Dependent enzymology, Prostatic Neoplasms enzymology, Protein Kinase Inhibitors pharmacology, Receptor, ErbB-2 antagonists & inhibitors, Receptor, ErbB-2 chemistry, Receptor, ErbB-2 physiology, Receptor, ErbB-3 antagonists & inhibitors, Receptor, ErbB-3 chemistry, Receptor, ErbB-3 physiology, Receptor, ErbB-4, Signal Transduction drug effects, Signal Transduction physiology, Trastuzumab, Adenocarcinoma drug therapy, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents therapeutic use, ErbB Receptors antagonists & inhibitors, Neoplasm Proteins antagonists & inhibitors, Prostatic Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use

Abstract

The human epidermal growth factor receptor (HER) family of receptor tyrosine kinases is part of a network of pathways that are involved in the development and progression of prostate cancer. HER-kinase receptors include epidermal growth factor receptor (EGFR), HER2, HER3, and HER4, which must combine as dimers to affect signaling. Different combinations of receptors produce different qualities and levels of pathway activation. Among HER-family receptors, HER2 activation is particularly important in breast cancer, as HER2 gene amplification is associated with a distinct clinical course and response to treatment with a HER2-directed therapy (trastuzumab). Although HER2 can be over-expressed in prostate cancer, there is no clinical data to support the use of trastuzumab for prostate cancer patients. Preclinical and clinical data show that the activation of the HER-kinase axis is important for the progression of prostate cancer to androgen-independent disease. Data points towards the importance of inhibiting multiple members of the HER-kinase family to achieve more complete blockade of this axis for cancers other than HER2-overexpressing breast cancer. Multiple pharmaceutical agents that block the HER-kinase axis are currently being tested for patients with prostate cancer. These include antibodies, tyrosine kinase inhibitors, and novel strategies which seek to decrease HER2 expression.

Published

2004

8. Inhibition of transformed cell growth and induction of cellular differentiation by pyroxamide, an inhibitor of histone deacetylase.

Author

Butler LM, Webb Y, Agus DB, Higgins B, Tolentino TR, Kutko MC, LaQuaglia MP, Drobnjak M, Cordon-Cardo C, Scher HI, Breslow R, Richon VM, Rifkind RA, and Marks PA

Subjects

Acetylation drug effects, Aminopyridines therapeutic use, Animals, Antineoplastic Agents therapeutic use, Cell Division drug effects, Cell Line, Transformed, Cyclin-Dependent Kinase Inhibitor p21, Cyclins biosynthesis, Disease Models, Animal, Enzyme Inhibitors therapeutic use, Histone Deacetylases metabolism, Histones metabolism, Humans, Hydroxamic Acids therapeutic use, Male, Mice, Mice, Inbred BALB C, Mice, Nude, Prostate-Specific Antigen blood, Prostatic Neoplasms blood, Prostatic Neoplasms drug therapy, Treatment Outcome, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Aminopyridines pharmacology, Antineoplastic Agents pharmacology, Cell Differentiation drug effects, Enzyme Inhibitors pharmacology, Histone Deacetylase Inhibitors, Hydroxamic Acids pharmacology

Abstract

Purpose: We have synthesized a series of hybrid polar compounds that induce differentiation and/or apoptosis of various transformed cells. These agents are also potent inhibitors of histone deacetylases (HDACs). Pyroxamide (suberoyl-3-aminopyridineamide hydroxamic acid) is a new member of this class of compounds that is currently under development as an anticancer agent. We investigated the activity of pyroxamide as an inducer of differentiation and/or apoptosis in transformed cells., Experimental Design and Results: Pyroxamide, at micromolar concentrations, induced terminal differentiation in murine erythroleukemia (MEL) cells and caused growth inhibition by cell cycle arrest and/or apoptosis in MEL, prostate carcinoma, bladder carcinoma, and neuroblastoma cells. Administration of pyroxamide (100 or 200 mg/kg/day) to nude mice at doses that caused little evident toxicity significantly suppressed the growth of s.c. CWR22 prostate cancer xenografts. Despite the potent growth-inhibitory effects of pyroxamide in this tumor model, serum prostate-specific antigen levels in control versus pyroxamide-treated mice were not significantly different. Pyroxamide is a potent inhibitor of affinity-purified HDAC1 (ID(50) = 100 nM) and causes the accumulation of acetylated core histones in MEL cells cultured with the agent. Human CWR22 prostate tumor xenografts from mice treated with pyroxamide (100 or 200 mg/kg/day) showed increased levels of histone acetylation and increased expression of the cell cycle regulator p21/WAF1, compared with tumors from vehicle-treated control animals., Conclusions: The findings suggest that pyroxamide may be a useful agent for the treatment of malignancy and that induction of p21/WAF1 in transformed cells by pyroxamide may contribute to the antitumor effects of this agent.

Published

2001

9. HER-2/neu as a therapeutic target in non-small cell lung cancer, prostate cancer, and ovarian cancer.

Author

Agus DB, Bunn PA Jr, Franklin W, Garcia M, and Ozols RF

Subjects

Animals, Antibodies, Monoclonal, Humanized, Carcinoma, Non-Small-Cell Lung genetics, Clinical Trials as Topic, Drug Screening Assays, Antitumor, Female, Humans, Lung Neoplasms genetics, Male, Neoplasms, Hormone-Dependent drug therapy, Neoplasms, Hormone-Dependent genetics, Ovarian Neoplasms genetics, Prognosis, Prostatic Neoplasms genetics, Trastuzumab, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Genes, erbB-2, Lung Neoplasms drug therapy, Ovarian Neoplasms drug therapy, Prostatic Neoplasms drug therapy

Abstract

HER-2/neu is overexpressed in most epithelial malignancies. Lung cancer, prostate cancer, and ovarian cancer are common epithelial tumors in which clinical trials are currently in progress to explore the potential therapeutic role for monoclonal antibodies to HER-2/neu (trastuzumab [Herceptin; Genentech, Inc, South San Francisco, CA]). In preclinical studies with tumor cell lines, trastuzumab was found to have additive and synergistic effects with some chemotherapeutic agents. Clinical trials investigating combination chemotherapy with trastuzumab and a variety of chemotherapeutic agents are already in progress in lung cancer.

Published

2000

10. Suberoylanilide hydroxamic acid, an inhibitor of histone deacetylase, suppresses the growth of prostate cancer cells in vitro and in vivo.

Author

Butler LM, Agus DB, Scher HI, Higgins B, Rose A, Cordon-Cardo C, Thaler HT, Rifkind RA, Marks PA, and Richon VM

Subjects

Animals, Antineoplastic Agents toxicity, Cell Death drug effects, Cell Division drug effects, Enzyme Inhibitors toxicity, Growth Inhibitors pharmacology, Histone Deacetylase Inhibitors, Histones metabolism, Humans, Hydroxamic Acids toxicity, Male, Mice, Mice, Inbred BALB C, Mice, Nude, Neoplasm Transplantation, Prostate-Specific Antigen blood, Prostatic Neoplasms enzymology, Prostatic Neoplasms pathology, Transplantation, Heterologous, Tumor Cells, Cultured drug effects, Vorinostat, Antineoplastic Agents pharmacology, Enzyme Inhibitors pharmacology, Hydroxamic Acids pharmacology, Prostatic Neoplasms drug therapy

Abstract

Suberoylanilide hydroxamic acid (SAHA) is the prototype of a family of hybrid polar compounds that induce growth arrest in transformed cells and show promise for the treatment of cancer. SAHA induces differentiation and/or apoptosis in certain transformed cells in culture and is a potent inhibitor of histone deacetylases. In this study, we examined the effects of SAHA on the growth of human prostate cancer cells in culture and on the growth of the CWR22 human prostate xenograft in nude mice. SAHA suppressed the growth of the LNCaP, PC-3, and TSU-Pr1 cell lines at micromolar concentrations (2.5-7.5 microM). SAHA induced dose-dependent cell death in the LNCaP cells. In mice with transplanted CWR222 human prostate tumors, SAHA (25, 50, and 100 mg/kg/day) caused significant suppression of tumor growth compared with mice receiving vehicle alone; treatment with 50 mg/kg/day resulted in a 97% reduction in the mean final tumor volume compared with controls. At this dose, there was no detectable toxicity as evaluated by weight gain and necropsy examination. Increased accumulation of acetylated core histones was detected in the CWR22 tumors within 6 h of SAHA administration. SAHA induced prostate-specific antigen mRNA expression in CWR22 prostate cancer cells, resulting in higher levels of serum prostate-specific antigen than predicted from tumor volume alone. The results suggest that hydroxamic acid-based hybrid polar compounds inhibit prostate cancer cell growth and may be useful, relatively nontoxic agents for the treatment of prostate carcinoma.

Published

2000

11. Response of prostate cancer to anti-Her-2/neu antibody in androgen-dependent and -independent human xenograft models.

Author

Agus DB, Scher HI, Higgins B, Fox WD, Heller G, Fazzari M, Cordon-Cardo C, and Golde DW

Subjects

Animals, Antibodies, Monoclonal, Humanized, Female, Humans, Immunohistochemistry, Male, Mice, Mice, Nude, Paclitaxel therapeutic use, Prostatic Neoplasms pathology, Transplantation, Heterologous, Trastuzumab, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents therapeutic use, Prostatic Neoplasms therapy, Receptor, ErbB-2 immunology

Abstract

Antibody to the Her-2/neu gene product has been shown to inhibit the growth of breast cancer cells overexpressing Her-2/neu and to have clinical utility in treating breast cancer. We studied a recombinant, humanized anti-Her-2/neu antibody (Herceptin) in preclinical models of human prostate cancer. The androgen-dependent CWR22 and LNCaP human prostate cancer xenograft models and androgen-independent sublines of CWR22 were used. Her-2/neu staining of the parental, androgen-dependent, and androgen-independent CWR22 tumors and LNCaP tumors demonstrated variable Her-2/neu expression. Herceptin was administered i.p. at a dose of 20 mg/kg twice weekly after the xenograft had been established. No effect of Herceptin on tumor growth was observed in any of the androgen-independent tumors; however, significant growth inhibition was observed in both of the androgen-dependent xenograft models, CWR22 (68% growth inhibition at the completion of the experiment; P = 0.03 for trajectories of the average tumor volume of the groups) and LNCaP (89% growth inhibition; P = 0.002). There was a significant increase in prostate-specific antigen (PSA) index (ng PSA/ml serum/mm3 tumor) in Herceptin-treated androgen-dependent groups compared with control (CWR22, 18-fold relative to pretreatment value versus 1.0-fold, P = 0.0001; LNCaP, 2.35-fold relative to pretreatment value versus 0.6-fold, P = 0.001). When paclitaxel (6.25 mg/kg s.c., five times/week) was given to animals with androgen-dependent and -independent tumors, there was growth inhibition in each group. Paclitaxel and Herceptin cotreatment led to greater growth inhibition than was seen for the agents individually. Thus, in these prostate cancer model systems, Herceptin alone has clinical activity only in the androgen-dependent tumor and has at least an additive effect on growth, in combination with paclitaxel, in both androgen-dependent and androgen-independent tumors. Response to Herceptin did not correlate with the PSA levels, because the PSA index markedly increased in the Herceptin-treated group, whereas it remained constant in the control group. These results suggest the utility of Herceptin in the treatment of human prostate cancer.

Published

1999