Your search keyword '"Alicia Allred"' showing total 5 results

1. Combined BRAF and MEK Inhibition in Melanoma with BRAF V600 Mutations

Author

Peng Sun, Kevin B. Kim, Howard A. Burris, Omid Hamid, Jeffrey A. Sosman, Jonathan Cebon, Alicia Allred, Peter F. Lebowitz, Gerald S. Falchook, Richard F. Kefford, Karl D. Lewis, Daniele Ouellet, Keith T. Flaherty, J. R. Infante, Lynn M. Schuchter, Adil Daud, Rene Gonzalez, Georgina V. Long, Jeffrey S. Weber, Nageatte Ibrahim, Igor Puzanov, Ragini Kudchadkar, Ajay Singh, Alain Algazi, Shonda M Little, and Kiran Patel

Subjects

Male, Medical and Health Sciences, Gastroenterology, chemistry.chemical_compound, Oximes, Antineoplastic Combined Chemotherapy Protocols, Vemurafenib, Melanoma, 6.2 Cellular and gene therapies, Cancer, Trametinib, Hazard ratio, Imidazoles, Binimetinib, General Medicine, Middle Aged, 6.1 Pharmaceuticals, Combination, Drug Therapy, Combination, Female, medicine.drug, Proto-Oncogene Proteins B-raf, Adult, medicine.medical_specialty, Fever, Combination therapy, Pyridones, MAP Kinase Signaling System, Clinical Trials and Supportive Activities, Pyrimidinones, Article, Disease-Free Survival, Drug Therapy, Clinical Research, General & Internal Medicine, Internal medicine, medicine, Humans, Aged, Mitogen-Activated Protein Kinase Kinases, Cobimetinib, business.industry, Evaluation of treatments and therapeutic interventions, Dabrafenib, medicine.disease, Surgery, chemistry, Mutation, business

Abstract

BackgroundResistance to therapy with BRAF kinase inhibitors is associated with reactivation of the mitogen-activated protein kinase (MAPK) pathway. To address this problem, we conducted a phase 1 and 2 trial of combined treatment with dabrafenib, a selective BRAF inhibitor, and trametinib, a selective MAPK kinase (MEK) inhibitor.MethodsIn this open-label study involving 247 patients with metastatic melanoma and BRAF V600 mutations, we evaluated the pharmacokinetic activity and safety of oral dabrafenib (75 or 150 mg twice daily) and trametinib (1, 1.5, or 2 mg daily) in 85 patients and then randomly assigned 162 patients to receive combination therapy with dabrafenib (150 mg) plus trametinib (1 or 2 mg) or dabrafenib monotherapy. The primary end points were the incidence of cutaneous squamous-cell carcinoma, survival free of melanoma progression, and response. Secondary end points were overall survival and pharmacokinetic activity.ResultsDose-limiting toxic effects were infrequently observed in patients receiving combination therapy with 150 mg of dabrafenib and 2 mg of trametinib (combination 150/2). Cutaneous squamous-cell carcinoma was seen in 7% of patients receiving combination 150/2 and in 19% receiving monotherapy (P=0.09), whereas pyrexia was more common in the combination 150/2 group than in the monotherapy group (71% vs. 26%). Median progression-free survival in the combination 150/2 group was 9.4 months, as compared with 5.8 months in the monotherapy group (hazard ratio for progression or death, 0.39; 95% confidence interval, 0.25 to 0.62; P

Published

2012

2. Phase I Study of GSK461364, a Specific and Competitive Polo-like Kinase 1 Inhibitor, in Patients with Advanced Solid Malignancies

Author

Jorge Barriuso, Sarah P. Blagden, Mohammed M. Dar, Andre T. Brunetto, Thomas A. Lampkin, Richard H. Wilson, David Olmos, Hanine Medani, Alicia Allred, Timothy A. Yap, Deborah A. Smith, Anne B. Taegtmeyer, Douglas Barker, Yan Degenhardt, Johann S. de Bono, Rohini Sharma, and Sharon C. Murray

Subjects

Adult, Male, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Cmax, Antineoplastic Agents, Cell Cycle Proteins, Thiophenes, Adenocarcinoma, Protein Serine-Threonine Kinases, Neutropenia, Binding, Competitive, Gastroenterology, Substrate Specificity, Pharmacokinetics, Neoplasms, Proto-Oncogene Proteins, Internal medicine, medicine, Humans, Protein Kinase Inhibitors, Aged, Aged, 80 and over, business.industry, Cancer, Middle Aged, Esophageal cancer, medicine.disease, Surgery, Clinical trial, Oncology, Pharmacodynamics, Disease Progression, Benzimidazoles, Female, Cancer biomarkers, Colorectal Neoplasms, business

Abstract

Purpose: GSK461364 is an ATP-competitive inhibitor of polo-like kinase 1 (Plk1). A phase I study of two schedules of intravenous GSK461364 was conducted. Experimental Design: GSK461364 was administered in escalating doses to patients with solid malignancies by two schedules, either on days 1, 8, and 15 of 28-day cycles (schedule A) or on days 1, 2, 8, 9, 15, and 16 of 28-day cycles (schedule B). Assessments included pharmacokinetic and pharmacodynamic profiles, as well as marker expression studies in pretreatment tumor biopsies. Results: Forty patients received GSK461364: 23 patients in schedule A and 17 in schedule B. Dose-limiting toxicities (DLT) in schedule A at 300 mg (2 of 7 patients) and 225 mg (1 of 8 patients) cohorts included grade 4 neutropenia and/or grade 3–4 thrombocytopenia. In schedule B, DLTs of grade 4 pulmonary emboli and grade 4 neutropenia occurred at 7 or more days at 100 mg dose level. Venous thrombotic emboli (VTE) and myelosuppression were the most common grade 3–4, drug-related events. Pharmacokinetic data indicated that AUC (area under the curve) and Cmax (maximum concentration) were proportional across doses, with a half-life of 9 to 13 hours. Pharmacodynamic studies in circulating tumor cells revealed an increase in phosphorylated histone H3 (pHH3) following drug administration. A best response of prolonged stable disease of more than 16 weeks occurred in 6 (15%) patients, including 4 esophageal cancer patients. Those with prolonged stable disease had greater expression of Ki-67, pHH3, and Plk1 in archived tumor biopsies. Conclusions: The final recommended phase II dose for GSK461364 was 225 mg administered intravenously in schedule A. Because of the high incidence (20%) of VTE, for further clinical evaluation, GSK461364 should involve coadministration of prophylactic anticoagulation. Clin Cancer Res; 17(10); 3420–30. ©2011 AACR.

Published

2011

3. Efficacy and tolerability in an open-label phase I/II study of MEK inhibitor trametinib (T), BRAF inhibitor dabrafenib (D), and anti-EGFR antibody panitumumab (P) in combination in patients (pts) with BRAF V600E mutated colorectal cancer (CRC)

Author

Johanna C. Bendell, Chloe E. Atreya, René Bernards, Yuehui Wu, Jan H.M. Schellens, Monica Motwani, Eric Van Cutsem, Thierry André, William Y. Go, Benjamin B. Suttle, Ryan B. Corcoran, Sabine Tejpar, Keith W. Orford, Alicia Allred, Michael S. Gordon, Axel Hoos, Josep Tabernero, and Roger Sidhu

Subjects

Trametinib, Cancer Research, endocrine system diseases, Colorectal cancer, business.industry, MEK inhibitor, Melanoma, Dabrafenib, Pharmacology, medicine.disease, digestive system diseases, enzymes and coenzymes (carbohydrates), Oncology, Tolerability, medicine, Cancer research, Panitumumab, In patient, skin and connective tissue diseases, business, neoplasms, medicine.drug

Abstract

3515 Background: BRAF V600 mutations occur in 5–10% of CRC and confer poor prognosis. Unlike in BRAF mutant (BRAFm) melanoma, BRAF and MEK inhibitors show limited activity in BRAFm CRC. Preclinical...

Published

2014

4. BRAF V600 mutant colorectal cancer (CRC) expansion cohort from the phase I/II clinical trial of BRAF inhibitor dabrafenib (GSK2118436) plus MEK inhibitor trametinib (GSK1120212)

Author

Jennifer Luan, Scott Kopetz, Shonda M Little, Wells A. Messersmith, Eunice L. Kwak, Razelle Kurzrock, Omid Hamid, Ryan B. Corcoran, Gerald S. Falchook, Adrienne A Brenner, David P. Ryan, Peng Sun, Alicia Allred, Jeffrey R. Infante, Kiran Patel, and Alan P. Venook

Subjects

Trametinib, Oncology, Cancer Research, Chemotherapy, medicine.medical_specialty, business.industry, Colorectal cancer, medicine.medical_treatment, MEK inhibitor, Mutant, Dabrafenib, medicine.disease, digestive system diseases, Clinical trial, Internal medicine, Cohort, medicine, business, neoplasms, medicine.drug

Abstract

3528 Background: BRAF V600 mutations occur in 10-15% of CRC and may predict lack of response to standard chemotherapy and anti-EGFR treatment. There have been no significant recent changes in the treatment of CRC. Novel therapeutic strategies for BRAF mutant CRC are critically needed. To collect preliminary efficacy data, an expansion cohort of 25 BRAF mutant CRC patients (pts) was included in part 2 of a phase I/II study evaluating the combination of dabrafenib (BRAFi) and trametinib (MEKi). Methods: Eligible pts had BRAF V600 mutant CRC, measurable disease per RECIST 1.1, and previous treatment with anti-cancer therapies. Pts were treated with established dose of dabrafenib (150mg BID) and trametinib (2mg QD). Results: Data for 23 pts are available at data cut-off: median age 54 years, 74% female, ECOG performance status 0 (48%) or 1 (52%). 39% had received prior EGFR inhibitor treatment. 74% had received ≥ 2 prior chemotherapy regimens; 48% had ≥ 1 biologic therapy. 48% had ≥ 3 metastatic sites. Three of the 23 pts were non-evaluable at data cut-off as they had not reached the first restaging assessment. Among the 20 evaluable pts, 1 (5%) achieved partial response and 10 (50%) stable disease. Minor responses (>10% to

Published

2012

5. Phase I/II study to assess safety, pharmacokinetics, and efficacy of the oral MEK 1/2 inhibitor GSK1120212 (GSK212) dosed in combination with the oral BRAF inhibitor GSK2118436 (GSK436)

Author

Jeffrey S. Weber, Keith T. Flaherty, J. R. Infante, Sheng-Bin Peng, B. Yi, Peter F. Lebowitz, Arthur Clements, D. P. Lawrence, H. A. Burris, Ragini Kudchadkar, Richard F. Kefford, Daniele Ouellet, Kiran Patel, Alicia Allred, K. B. Kim, Gerald Steven Falchook, R. Kurzrock, Johanna C. Bendell, Geoffrey I. Shapiro, and Georgina V. Long

Subjects

Drug, BRAF Inhibitor GSK2118436, Cancer Research, business.industry, media_common.quotation_subject, MEK inhibitor, Melanoma, Pharmacology, medicine.disease, Salivary duct carcinoma, Oncology, Pharmacokinetics, Cancer cell, Medicine, Dosing, business, media_common

Abstract

CRA8503 Background: In preclinical models, the BRAF/MEK inhibitor (i) combination GSK436/GSK212 has demonstrated enhanced activity against BRAF-mutant cancer cells compared to either drug alone, delayed emergence of GSK436 resistance, and prevented proliferative skin lesions attributable to BRAFi exposure. Methods: Eligible patients (pts) had BRAF V600 mutation positive solid tumors. Part 1: pharmacokinetic (PK) drug-drug interaction (DDI) study. Part 2: Dose escalation of continuous daily dosing of the combination followed by expansion cohorts; Part 3: Randomized phase II trial in untreated stage IV melanoma. Results: 45 pts have received ≥ 1 dose of GSK212 + GSK436, including 43 melanoma (all BRAFi naïve), 1 NSCLC and 1 salivary duct carcinoma. PK results of 7 pts in Part 1 showed no effect of GSK212 on single dose of GSK436. There was no clinically meaningful DDI between GSK436 and GSK212 after repeat dosing of the combination (Part 2). GSK436 was dosed 75-150 mg BID in combination with GSK212 1.0, 1.5, 2.0 mg QD. The recommended dose was 2 mg QD GSK212 in combination with 150 mg BID GSK436. At 1.5 mg GSK212, there was one DLT, a recurrent grade (G) 2 neutrophilic panniculitis. The only G4 adverse event (AE) was a sepsis-like syndrome with fever/hypotension. G3 AEs included generalized rash (n=2, 4%) and neutropenia (n=2, 4%). Skin toxicity ≥ G2 occurred in 9 (20%) pts; of these, G2 rash (n=4, 8%) and G2 macular rash (n=1, 2%). No cutaneous squamous cell carcinoma (SCC) or hyperproliferative skin lesions have occurred at any dose level. Other common G2 toxicities were pyrexia (n=5, 11%), vomiting (n=2, 4%) and fatigue (n=2, 4%). Of 16 evaluable pts in Part 2, 13 pts had PR and 3 SD for an ORR of 81% (95% CI 54.4%-96.0%) and all but 2 pts remain on study. In 10 evaluable pts who received 150 mg BID GSK436 + ≥1 mg QD GSK212, 9 pts had PR and 1 SD. Conclusions: GSK212 at 2 mg QD combines safely with GSK436 150 mg BID, no SCC thus far and decreased frequency of rash compared to previous trials of single agent GSK436 and GSK212, respectively. The preliminary anti-tumor activity warrants further investigation; the randomized phase II trial (Part 3) is accruing.

Published

2011