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1. Dose modification dynamics of ponatinib in patients with chronic-phase chronic myeloid leukemia (CP-CML) from the PACE and OPTIC trials.

Author

Jabbour, Elias, Apperley, Jane, Cortes, Jorge, Rea, Delphine, Deininger, Michael, Abruzzese, Elisabetta, Chuah, Charles, DeAngelo, Daniel, Hochhaus, Andreas, Lipton, Jeffrey, Mauro, Michael, Nicolini, Franck, Pinilla-Ibarz, Javier, Rosti, Gianantonio, Rousselot, Philippe, Talpaz, Moshe, Vorog, Alexander, Ren, Xiaowei, Kantarjian, Hagop, and Shah, Neil Pravin

Subjects
Humans, Drug Resistance, Neoplasm, Leukemia, Myeloid, Chronic-Phase, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Imidazoles, Pyridazines, Fusion Proteins, bcr-abl, Protein Kinase Inhibitors, Antineoplastic Agents
Abstract

Ponatinib, the only approved all known-BCR::ABL1 inhibitor, is a third-generation tyrosine-kinase inhibitor (TKI) designed to inhibit BCR::ABL1 with or without any single resistance mutation, including T315I, and induced robust and durable responses at 45 mg/day in patients with CP-CML resistant to second-generation TKIs in the PACE trial. However, cardiovascular toxicities, including arterial occlusive events (AOEs), have emerged as treatment-related AEs within this class of TKIs. The OPTIC trial evaluated the efficacy and safety of ponatinib using a novel, response-based, dose-reduction strategy in patients with CP-CML whose disease is resistant to ≥2 TKIs or who harbor T315I. To assess the dose-response relationship and the effect on the safety of ponatinib, we examined the outcomes of patients with CP-CML enrolled in PACE and OPTIC who received 45 mg/day of ponatinib. A propensity score analysis was used to evaluate AOEs across both trials. Survival rates and median time to achieve ≤1% BCR::ABL1IS in OPTIC were similar or better than in PACE. The outcomes of patients with T315I mutations were robust in both trials. Patients in OPTIC had a lower exposure-adjusted incidence of AOEs compared with those in PACE. This analysis demonstrates that response-based dosing for ponatinib improves treatment tolerance and mitigates cardiovascular risk.

Published
2024

2. Asciminib monotherapy in patients with chronic-phase chronic myeloid leukemia with the T315I mutation after ≥1 prior tyrosine kinase inhibitor: 2-year follow-up results

Author

Cortes, Jorge E., Sasaki, Koji, Kim, Dong-Wook, Hughes, Timothy P., Etienne, Gabriel, Mauro, Michael J., Hochhaus, Andreas, Lang, Fabian, Heinrich, Michael C., Breccia, Massimo, Deininger, Michael, Goh, Yeow Tee, Janssen, Jeroen J.W.M., Talpaz, Moshe, de Soria, Valle Gomez Garcia, le Coutre, Philipp, DeAngelo, Daniel J., Damon, Andrea, Cacciatore, Silvia, Polydoros, Fotis, Agrawal, Nithya, and Rea, Delphine

Published
2024
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3. Correction: Dose modification dynamics of ponatinib in patients with chronic-phase chronic myeloid leukemia (CP-CML) from the PACE and OPTIC trials

Author

Jabbour, Elias, Apperley, Jane, Cortes, Jorge, Rea, Delphine, Deininger, Michael, Abruzzese, Elisabetta, Chuah, Charles, DeAngelo, Daniel J., Hochhaus, Andreas, Lipton, Jeffrey H., Mauro, Michael, Nicolini, Franck, Pinilla-Ibarz, Javier, Rosti, Gianantonio, Rousselot, Philippe, Shah, Neil P., Talpaz, Moshe, Vorog, Alexander, Ren, Xiaowei, and Kantarjian, Hagop

Published
2024
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4. Animal Models and Their Role in Imaging-Assisted Co-Clinical Trials

Author

Peehl, Donna M, Badea, Cristian T, Chenevert, Thomas L, Daldrup-Link, Heike E, Ding, Li, Dobrolecki, Lacey E, Houghton, A McGarry, Kinahan, Paul E, Kurhanewicz, John, Lewis, Michael T, Li, Shunqiang, Luker, Gary D, X., Cynthia, Manning, H Charles, Mowery, Yvonne M, O’Dwyer, Peter J, Pautler, Robia G, Rosen, Mark A, Roudi, Raheleh, Ross, Brian D, Shoghi, Kooresh I, Sriram, Renuka, Talpaz, Moshe, Wahl, Richard L, and Zhou, Rong

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Clinical Research, Clinical Trials and Supportive Activities, Biomedical Imaging, Cancer, 2.6 Resources and infrastructure (aetiology), 6.9 Resources and infrastructure (treatment evaluation), Good Health and Well Being, Animals, Mice, Humans, Neoplasms, Disease Models, Animal, Diagnostic Imaging, co-clinical trials, animal models, imaging, prostate cancer, sarcoma, colorectal cancer, osteosarcoma, pancreatic cancer, myelofibrosis, breast cancer, lung cancer
Abstract

The availability of high-fidelity animal models for oncology research has grown enormously in recent years, enabling preclinical studies relevant to prevention, diagnosis, and treatment of cancer to be undertaken. This has led to increased opportunities to conduct co-clinical trials, which are studies on patients that are carried out parallel to or sequentially with animal models of cancer that mirror the biology of the patients' tumors. Patient-derived xenografts (PDX) and genetically engineered mouse models (GEMM) are considered to be the models that best represent human disease and have high translational value. Notably, one element of co-clinical trials that still needs significant optimization is quantitative imaging. The National Cancer Institute has organized a Co-Clinical Imaging Resource Program (CIRP) network to establish best practices for co-clinical imaging and to optimize translational quantitative imaging methodologies. This overview describes the ten co-clinical trials of investigators from eleven institutions who are currently supported by the CIRP initiative and are members of the Animal Models and Co-clinical Trials (AMCT) Working Group. Each team describes their corresponding clinical trial, type of cancer targeted, rationale for choice of animal models, therapy, and imaging modalities. The strengths and weaknesses of the co-clinical trial design and the challenges encountered are considered. The rich research resources generated by the members of the AMCT Working Group will benefit the broad research community and improve the quality and translational impact of imaging in co-clinical trials.

Published
2023

5. Efficacy and safety of fedratinib in patients with myelofibrosis previously treated with ruxolitinib (FREEDOM2): results from a multicentre, open-label, randomised, controlled, phase 3 trial

Author

Harrison, Claire N, Mesa, Ruben, Talpaz, Moshe, Al-Ali, Haifa Kathrin, Xicoy, Blanca, Passamonti, Francesco, Palandri, Francesca, Benevolo, Giulia, Vannucchi, Alessandro Maria, Mediavilla, Clemence, Iurlo, Alessandra, Kim, InHo, Rose, Shelonitda, Brown, Patrick, Hernandez, Christopher, Wang, Jia, and Kiladjian, Jean-Jacques

Published
2024
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6. Targeting the mSWI/SNF complex in POU2F-POU2AF transcription factor-driven malignancies

Author

He, Tongchen, Xiao, Lanbo, Qiao, Yuanyuan, Klingbeil, Olaf, Young, Eleanor, Wu, Xiaoli S., Mannan, Rahul, Mahapatra, Somnath, Redin, Esther, Cho, Hanbyul, Bao, Yi, Kandarpa, Malathi, Ching-Yi Tien, Jean, Wang, Xiaoju, Eyunni, Sanjana, Zheng, Yang, Kim, NamHoon, Zheng, Heng, Hou, Siyu, Su, Fengyun, Miner, Stephanie J., Mehra, Rohit, Cao, Xuhong, Abbineni, Chandrasekhar, Samajdar, Susanta, Ramachandra, Murali, Dhanasekaran, Saravana M., Talpaz, Moshe, Parolia, Abhijit, Rudin, Charles M., Vakoc, Christopher R., and Chinnaiyan, Arul M.

Published
2024
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7. Safety and Efficacy of Ruxolitinib in Patients with Myelofibrosis and Low Platelet Counts (50 – 100 × 109/L): Final Analysis of an Open-Label Phase 2 Study

Author

Talpaz, Moshe, Prchal, Josef, Afrin, Lawrence, Arcasoy, Murat, Hamburg, Solomon, Clark, Jason, Kornacki, Deanna, Colucci, Philomena, and Verstovsek, Srdan

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Patient Safety, Hematology, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Anemia, Humans, Nitriles, Platelet Count, Primary Myelofibrosis, Pyrazoles, Pyrimidines, Quality of Life, Thrombocytopenia, Janus kinase inhibitor, Myeloproliferative neoplasm, Spleen volume, Total Symptom Score, Oncology and Carcinogenesis, Cardiovascular medicine and haematology, Oncology and carcinogenesis
Abstract

IntroductionTreatment options in patients with myelofibrosis (MF) presenting with thrombocytopenia are limited. Final results of the phase 2 study (NCT01348490) of ruxolitinib in patients with MF and low baseline platelet counts (50 - 100 × 109/L) are reported.Patients and methodsPatients received ruxolitinib 5 mg twice daily (BID), with optional up-titration to a maximum of 15 mg BID, provided platelet count remained ≥40 × 109/L. Assessments included spleen volume and length, Total Symptom Score (TSS), quality of life, and safety.ResultsOf 66 patients, 52 (78.8%) completed the first 24 weeks of treatment. Median (range) percentage change from baseline in spleen volume and TSS (coprimary endpoints) were -20.5% (-55.8% to 38.5%, n=51) and -39.8% (-98.6% to 226.4%, n=53), respectively; greatest median reductions were in the 10 mg BID final titrated dose group. Of patients achieving ≥35% or ≥10% reduction in spleen volume, 8/11 (72.7%) and 21/34 (61.8%), respectively, were in the 10 mg BID final titrated dose group. Thirty-seven of 65 patients (56.9%) had ≥20% improvement in TSS, and 35/66 patients (53.0%) were Patient Global Impression of Change responders. Treatment-emergent adverse events led to dose interruption in 17/66 patients (25.8%), most commonly thrombocytopenia (n=3).ConclusionA starting dose of ruxolitinib 5 mg BID with gradual up-titration and dose optimization based on hematologic parameters and response was efficacious and generally well-tolerated in patients with MF and low platelet counts. Median improvement in spleen volume and symptoms was greatest for patients receiving ruxolitinib 10 mg BID.

Published
2022

10. Asciminib monotherapy in patients with CML-CP without BCR::ABL1 T315I mutations treated with at least two prior TKIs: 4-year phase 1 safety and efficacy results

Author

Mauro, Michael J., Hughes, Timothy P., Kim, Dong-Wook, Rea, Delphine, Cortes, Jorge E., Hochhaus, Andreas, Sasaki, Koji, Breccia, Massimo, Talpaz, Moshe, Ottmann, Oliver, Minami, Hironobu, Goh, Yeow Tee, DeAngelo, Daniel J., Heinrich, Michael C., Gómez-García de Soria, Valle, le Coutre, Philipp, Mahon, Francois-Xavier, Janssen, Jeroen J. W. M., Deininger, Michael, Shanmuganathan, Naranie, Geyer, Mark B., Cacciatore, Silvia, Polydoros, Fotis, Agrawal, Nithya, Hoch, Matthias, and Lang, Fabian

Published
2023
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11. Longitudinal Assessment of Transfusion Intensity in Patients With JAK Inhibitor–Naive or –Experienced Myelofibrosis Treated With Momelotinib

Author

Harrison, Claire N., Mesa, Ruben, Talpaz, Moshe, Gupta, Vikas, Gerds, Aaron T., Perkins, Andrew, Goh, Yeow Tee, Fox, Maria Laura, McLornan, Donal, Palmer, Jeanne, Foltz, Lynda, Vannucchi, Alessandro, Koschmieder, Steffen, Passamonti, Francesco, Lee, Sung-Eun, Ellis, Catherine, Strouse, Bryan, Gonzalez Carreras, Francisco J., and Oh, Stephen T.

Published
2024
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14. ACVR1/JAK1/JAK2 inhibitor momelotinib reverses transfusion dependency and suppresses hepcidin in myelofibrosis phase 2 trial

Author

Oh, Stephen T, Talpaz, Moshe, Gerds, Aaron T, Gupta, Vikas, Verstovsek, Srdan, Mesa, Ruben, Miller, Carole B, Rivera, Candido E, Fleischman, Angela G, Goel, Swati, Heaney, Mark L, O’Connell, Casey, Arcasoy, Murat O, Zhang, Yafeng, Kawashima, Jun, Ganz, Tomas, Kowalski, Mark, and Brachmann, Carrie Baker

Subjects
Clinical Trials and Supportive Activities, Hematology, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Blood, Activin Receptors, Type I, Benzamides, Hepcidins, Humans, Janus Kinase 1, Janus Kinase 2, Primary Myelofibrosis, Pyrimidines
Abstract

Momelotinib (MMB) is a JAK1/2 and ACVR1 inhibitor with demonstrated clinical activity in all 3 hallmarks of myelofibrosis (MF): anemia, constitutional symptoms, and splenomegaly. In this phase 2 open-label translational biology study (NCT02515630) of 41 transfusion-dependent patients with MF, we explored mechanisms underlying the favorable activity of MMB on MF-associated iron-restricted anemia, including its impact on serum hepcidin levels, and markers of iron storage and availability, erythropoiesis, and inflammation. A transfusion-independent response (TI-R), defined as red blood cell transfusion independence (TI) ≥12 weeks at any time on study, occurred in 17 patients (41%; 95% confidence interval [CI], 26%-58%), including 14 patients (34%; 95% CI, 20%-51%) who achieved TI-R by week 24. In addition, 78% of TI nonresponse (TI-NR) patients achieved a ≥50% decrease in transfusion requirement for ≥8 weeks. Adverse events (AEs) were consistent with previous studies of MMB in MF, with cough, diarrhea, and nausea as the most common. Twenty-one patients experienced grade ≥3 AEs, most commonly anemia and neutropenia. Consistent with preclinical data, daily MMB treatment led to an acute and persistent decrease in blood hepcidin associated with increased iron availability and markers of erythropoiesis. Baseline characteristics associated with TI-R were lower inflammation and hepcidin as well as increased markers of erythropoiesis and bone marrow function. Overall, the study demonstrates that MMB treatment decreases hepcidin in conjunction with improving iron metabolism and erythropoiesis, suggesting a mechanistic explanation for the reduced transfusion dependency observed in transfusion-dependent MF patients treated with MMB, thereby addressing the key unmet medical need in the MF population.

Published
2020

15. Development of 2 Bromodomain and Extraterminal Inhibitors With Distinct Pharmacokinetic and Pharmacodynamic Profiles for the Treatment of Advanced Malignancies

Author

Falchook, Gerald, Rosen, Seth, LoRusso, Patricia, Watts, Justin, Gupta, Shilpa, Coombs, Catherine C, Talpaz, Moshe, Kurzrock, Razelle, Mita, Monica, Cassaday, Ryan, Harb, Wael, Peguero, Julio, Smith, David C, Piha-Paul, Sarina A, Szmulewitz, Russ, Noel, Marcus S, Yeleswaram, Swamy, Liu, Phillip, Switzky, Julie, Zhou, Gongfu, Zheng, Fred, and Mehta, Amitkumar

Subjects
Clinical Research, Patient Safety, Clinical Trials and Supportive Activities, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adolescent, Adult, Aged, Aged, 80 and over, Antineoplastic Agents, Boronic Acids, Dose-Response Relationship, Drug, Female, Humans, Male, Maximum Tolerated Dose, Middle Aged, Nausea, Neoplasms, Organic Chemicals, Proteins, Pyrimidines, Tissue Distribution, Treatment Outcome, Vomiting, Young Adult, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeBromodomain and extraterminal (BET) proteins are key epigenetic transcriptional regulators, inhibition of which may suppress oncogene expression. We report results from 2 independent first-in-human phase 1/2 dose-escalation and expansion, safety and tolerability studies of BET inhibitors INCB054329 (study INCB 54329-101; NCT02431260) and INCB057643 (study INCB 57643-101; NCT02711137).Patients and methodsPatients (≥18 years) with advanced malignancies, ≥1 prior therapy, and adequate organ functions received oral INCB054329 (monotherapy) or INCB057643 (monotherapy or in combination with standard-of-care) in 21-day cycles (or 28-day cycles depending on standard-of-care combination). Primary endpoints were safety and tolerability.ResultsSixty-nine and 134 patients received INCB054329 and INCB057643, respectively. Study INCB 54329-101 has been completed; INCB 57643-101 is currently active, but not recruiting (no patients were receiving treatment as of January 8, 2019). Terminal elimination half-life was shorter for INCB054329 versus INCB057643 (mean [SD], 2.24 [2.03] vs. 11.1 [8.27] hours). INCB054329 demonstrated higher interpatient variability in oral clearance versus INCB057643 (CV%, 142% vs. 45.5%). Most common (>20%) any-grade treatment-related adverse events were similar for both drugs (INCB054329; INCB057643): nausea (35%; 30%), thrombocytopenia (33%; 32%), fatigue (29%; 30%), decreased appetite (26%; 22%). Two confirmed complete responses and 4 confirmed partial responses with INCB057643 were reported as best responses.ConclusionsINCB057643 exhibited a more favorable PK profile versus INCB054329; exposure-dependent thrombocytopenia was observed with both drugs which limited the target inhibition that could be safely maintained. Further efforts are required to identify patient populations that can benefit most, and an optimal dosing scheme to maximize therapeutic index.

Published
2020

16. Phase 1/2 trial of glasdegib in patients with primary or secondary myelofibrosis previously treated with ruxolitinib

Author

Gerds, Aaron T, Tauchi, Tetsuzo, Ritchie, Ellen, Deininger, Michael, Jamieson, Catriona, Mesa, Ruben, Heaney, Mark, Komatsu, Norio, Minami, Hironobu, Su, Yun, Shaik, Naveed, Zhang, Xiaoxi, DiRienzo, Christine, Zeremski, Mirjana, Chan, Geoffrey, and Talpaz, Moshe

Subjects
Brain Disorders, Clinical Research, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Adolescent, Adult, Aged, Aged, 80 and over, Benzimidazoles, Chemotherapy, Adjuvant, Female, Humans, Male, Middle Aged, Nitriles, Organ Size, Phenylurea Compounds, Primary Myelofibrosis, Pyrazoles, Pyrimidines, Spleen, Treatment Outcome, Young Adult, Glasdegib, Hedgehog inhibitor, Smoothened inhibitor, Myelofibrosis, Clinical Sciences, Immunology
Abstract

Glasdegib is a potent and selective oral inhibitor of the Hedgehog pathway. We report data from the single-arm, lead-in cohort of an open-label phase 1b/2 trial of glasdegib in patients with primary/secondary myelofibrosis (MF) previously treated with at least one Janus kinase inhibitor (JAKi). Patients received glasdegib 100 mg orally once daily until there was no further clinical benefit. Primary endpoints included adverse events (AEs). Secondary endpoints included patients with spleen volume reduction (SVR) ≥35% at week 24, patients with ≥50% total symptom score (TSS) reduction, and pharmacokinetics. All 21 treated patients had one or more AE and five (23.8%) had serious AEs. Most common (>30%) AEs were dysgeusia (61.9%), muscle spasms (57.1%), alopecia (38.1%), fatigue (33.3%), and decreased appetite (33.3%). Although no patient had ≥35% SVR at week 24, one patient previously treated with ruxolitinib had an SVR of 32.9%. At week 12, two (9.5%) patients had ≥50% reduction in TSS from baseline and ˜40% had ≥20% reduction. One patient had an anaemia response. Following administration of glasdegib 100 mg once daily, the median time to peak plasma concentrations at steady-state generally occurred at 1 h post-dose. The safety profile of glasdegib monotherapy was manageable in patients with primary/secondary MF. Further study of glasdegib in combination with JAKi in a MF population may be warranted.

Published
2019

18. The genetic heterogeneity and drug resistance mechanisms of relapsed refractory multiple myeloma

Author

Vo, Josh N., Wu, Yi-Mi, Mishler, Jeanmarie, Hall, Sarah, Mannan, Rahul, Wang, Lisha, Ning, Yu, Zhou, Jin, Hopkins, Alexander C., Estill, James C., Chan, Wallace K. B., Yesil, Jennifer, Cao, Xuhong, Rao, Arvind, Tsodikov, Alexander, Talpaz, Moshe, Cole, Craig E., Ye, Jing C., Bergsagel, P. Leif, Auclair, Daniel, Cho, Hearn Jay, Robinson, Dan R., and Chinnaiyan, Arul M.

Published
2022
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20. Safety and efficacy of fedratinib in patients with myelofibrosis previously treated with ruxolitinib: primary analysis of FREEDOM trial

Author

Gupta, Vikas, primary, Yacoub, Abdulraheem, additional, Mesa, Ruben A., additional, Harrison, Claire N., additional, Vannucchi, Alessandro M., additional, Kiladjian, Jean-Jacques, additional, Deeg, Hans-Joachim, additional, Fazal, Salman, additional, Foltz, Lynda, additional, Mattison, Ryan J., additional, Miller, Carole B., additional, Parameswaran, Vinod, additional, Brown, Patrick, additional, Hernandez, Christopher, additional, Wang, Jia, additional, and Talpaz, Moshe, additional

Published
2024
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21. Updated safety and efficacy data from the phase 3 MANIFEST-2 study of pelabresib in combination with ruxolitinib for JAK inhibitor treatment-naïve patients with myelofibrosis.

Author

Rampal, Raajit, primary, Grosicki, Sebastian, additional, Chraniuk, Dominik, additional, Abruzzese, Elisabetta, additional, Bose, Prithviraj, additional, Gerds, Aaron Thomas, additional, Vannucchi, Alessandro M., additional, Palandri, Francesca, additional, Lee, Sung-Eun, additional, Gupta, Vikas, additional, Lucchesi, Alessandro, additional, Kuykendall, Andrew Tucker, additional, Mesa, Ruben A., additional, Kiladjian, Jean-Jacques, additional, Talpaz, Moshe, additional, Harris, Morgan, additional, Wu, Manlei, additional, Brown, Barbara, additional, Harrison, Claire, additional, and Mascarenhas, John, additional

Published
2024
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22. NCCN Guidelines® Insights: Systemic Mastocytosis, Version 3.2024

Author

Gotlib, Jason, primary, Gerds, Aaron T., additional, Abdelmessieh, Peter, additional, Ali, Haris, additional, Castells, Mariana, additional, Dunbar, Andrew, additional, Fein Revell, Ruth, additional, George, Tracy I., additional, Green, Steven, additional, Gundabolu, Krishna, additional, Hexner, Elizabeth, additional, Jain, Tania, additional, Jamieson, Catriona, additional, Kaesberg, Paul R., additional, Kuykendall, Andrew T., additional, Madanat, Yazan, additional, Manchanda, Naveen, additional, Masarova, Lucia, additional, May, Jori, additional, McMahon, Brandon, additional, Mohan, Sanjay R., additional, Nadiminti, Kalyan V., additional, Oh, Stephen, additional, Palmer, Jeanne, additional, Patel, Ami, additional, Patel, Anand A., additional, Podoltsev, Nikolai, additional, Rein, Lindsay, additional, Salit, Rachel, additional, Talpaz, Moshe, additional, Wadleigh, Martha, additional, Wall, Sarah, additional, Bergman, Mary Anne, additional, and Hochstetler, Cindy, additional

Published
2024
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40. Ponatinib dose-ranging study in chronic-phase chronic myeloid leukemia: a randomized, open-label phase 2 clinical trial

Author

Cortes, Jorge, Apperley, Jane, Lomaia, Elza, Moiraghi, Beatriz, Undurraga Sutton, Maria, Pavlovsky, Carolina, Chuah, Charles, Sacha, Tomasz, Lipton, Jeffrey H., Schiffer, Charles A., McCloskey, James, Hochhaus, Andreas, Rousselot, Philippe, Rosti, Gianantonio, de Lavallade, Hugues, Turkina, Anna, Rojas, Christine, Arthur, Christopher Kevin, Maness, Lori, Talpaz, Moshe, Mauro, Michael, Hall, Tracey, Lu, Vickie, Srivastava, Shouryadeep, and Deininger, Michael

Published
2021
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41. Rapid, ultra low coverage copy number profiling of cell-free DNA as a precision oncology screening strategy

Author

Hovelson, Daniel H, Liu, Chia-Jen, Wang, Yugang, Kang, Qing, Henderson, James, Gursky, Amy, Brockman, Scott, Ramnath, Nithya, Krauss, John C, Talpaz, Moshe, Kandarpa, Malathi, Chugh, Rashmi, Tuck, Missy, Herman, Kirk, Grasso, Catherine S, Quist, Michael J, Feng, Felix Y, Haakenson, Christine, Langmore, John, Kamberov, Emmanuel, Tesmer, Tim, Husain, Hatim, Lonigro, Robert J, Robinson, Dan, Smith, David C, Alva, Ajjai S, Hussain, Maha H, Chinnaiyan, Arul M, Tewari, Muneesh, Mills, Ryan E, Morgan, Todd M, and Tomlins, Scott A

Subjects
Human Genome, Cancer, Prostate Cancer, Biotechnology, Genetics, Good Health and Well Being, cell-free DNA, precision oncology, prostate cancer, whole genome sequencing, copy-number analysis, Oncology and Carcinogenesis
Abstract

Current cell-free DNA (cfDNA) next generation sequencing (NGS) precision oncology workflows are typically limited to targeted and/or disease-specific applications. In advanced cancer, disease burden and cfDNA tumor content are often elevated, yielding unique precision oncology opportunities. We sought to demonstrate the utility of a pan-cancer, rapid, inexpensive, whole genome NGS of cfDNA approach (PRINCe) as a precision oncology screening strategy via ultra-low coverage (~0.01x) tumor content determination through genome-wide copy number alteration (CNA) profiling. We applied PRINCe to a retrospective cohort of 124 cfDNA samples from 100 patients with advanced cancers, including 76 men with metastatic castration-resistant prostate cancer (mCRPC), enabling cfDNA tumor content approximation and actionable focal CNA detection, while facilitating concordance analyses between cfDNA and tissue-based NGS profiles and assessment of cfDNA alteration associations with mCRPC treatment outcomes. Therapeutically relevant focal CNAs were present in 42 (34%) cfDNA samples, including 36 of 93 (39%) mCRPC patient samples harboring AR amplification. PRINCe identified pre-treatment cfDNA CNA profiles facilitating disease monitoring. Combining PRINCe with routine targeted NGS of cfDNA enabled mutation and CNA assessment with coverages tuned to cfDNA tumor content. In mCRPC, genome-wide PRINCe cfDNA and matched tissue CNA profiles showed high concordance (median Pearson correlation = 0.87), and PRINCe detectable AR amplifications predicted reduced time on therapy, independent of therapy type (Kaplan-Meier log-rank test, chi-square = 24.9, p < 0.0001). Our screening approach enables robust, broadly applicable cfDNA-based precision oncology for patients with advanced cancer through scalable identification of therapeutically relevant CNAs and pre-/post-treatment genomic profiles, enabling cfDNA- or tissue-based precision oncology workflow optimization.

Published
2017

42. Phase 1 dose-finding study of rebastinib (DCC-2036) in patients with relapsed chronic myeloid leukemia and acute myeloid leukemia

Author

Cortes, Jorge, Talpaz, Moshe, Smith, Hedy P, Snyder, David S, Khoury, Jean, Bhalla, Kapil N, Pinilla-Ibarz, Javier, Larson, Richard, Mitchell, David, Wise, Scott C, Rutkoski, Thomas J, Smith, Bryan D, Flynn, Daniel L, Kantarjian, Hagop M, Rosen, Oliver, and Van Etten, Richard A

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Clinical Research, Hematology, Rare Diseases, 6.1 Pharmaceuticals, 6.2 Cellular and gene therapies, 5.1 Pharmaceuticals, Adult, Aged, Aged, 80 and over, Drug Monitoring, Drug Resistance, Neoplasm, Female, Fusion Proteins, bcr-abl, Humans, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Leukemia, Myeloid, Acute, Male, Maximum Tolerated Dose, Middle Aged, Mutation, Protein Kinase Inhibitors, Quinolines, Treatment Outcome, Young Adult, Cardiorespiratory Medicine and Haematology, Immunology, Cardiovascular medicine and haematology
Abstract

A vailable tyrosine kinase inhibitors for chronic myeloid leukemia bind in an adenosine 5'-triphosphate-binding pocket and are affected by evolving mutations that confer resistance. Rebastinib was identified as a switch control inhibitor of BCR-ABL1 and FLT3 and may be active against resistant mutations. A Phase 1, first-in-human, single-agent study investigated rebastinib in relapsed or refractory chronic or acute myeloid leukemia. The primary objectives were to investigate the safety of rebastinib and establish the maximum tolerated dose and recommended Phase 2 dose. Fifty-seven patients received treatment with rebastinib. Sixteen patients were treated using powder-in-capsule preparations at doses from 57 mg to 1200 mg daily, and 41 received tablet preparations at doses of 100 mg to 400 mg daily. Dose-limiting toxicities were dysarthria, muscle weakness, and peripheral neuropathy. The maximum tolerated dose was 150 mg tablets administered twice daily. Rebastinib was rapidly absorbed. Bioavailability was 3- to 4-fold greater with formulated tablets compared to unformulated capsules. Eight complete hematologic responses were achieved in 40 evaluable chronic myeloid leukemia patients, 4 of which had a T315I mutation. None of the 5 patients with acute myeloid leukemia responded. Pharmacodynamic analysis showed inhibition of phosphorylation of substrates of BCR-ABL1 or FLT3 by rebastinib. Although clinical activity was observed, clinical benefit was insufficient to justify continued development in chronic or acute myeloid leukemia. Pharmacodynamic analyses suggest that other kinases inhibited by rebastinib, such as TIE2, may be more relevant targets for the clinical development of rebastinib (clinicaltrials.gov Identifier:00827138).

Published
2017

44. Determining the recommended dose of pacritinib: results from the PAC203 dose-finding trial in advanced myelofibrosis

Author

Gerds, Aaron T., Savona, Michael R., Scott, Bart L., Talpaz, Moshe, Egyed, Miklos, Harrison, Claire N., Yacoub, Abdulraheem, Vannucchi, Alessandro, Mead, Adam J., Kiladjian, Jean-Jacques, O'Sullivan, Jennifer, García-Gutiérrez, Valentin, Bose, Prithviraj, Rampal, Raajit K., Miller, Carole B., Palmer, Jeanne, Oh, Stephen T., Buckley, Sarah A., Mould, Diane R., Ito, Kaori, Tyavanagimatt, Shanthakumar, Smith, Jennifer A., Roman-Torres, Karisse, Devineni, Sri, Craig, Adam R., and Mascarenhas, John O.

Published
2020
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45. Survival following allogeneic transplant in patients with myelofibrosis

Author

Gowin, Krisstina, Ballen, Karen, Ahn, Kwang Woo, Hu, Zhen-Huan, Ali, Haris, Arcasoy, Murat O., Devlin, Rebecca, Coakley, Maria, Gerds, Aaron T., Green, Michael, Gupta, Vikas, Hobbs, Gabriela, Jain, Tania, Kandarpa, Malathi, Komrokji, Rami, Kuykendall, Andrew T., Luber, Kierstin, Masarova, Lucia, Michaelis, Laura C., Patches, Sarah, Pariser, Ashley C., Rampal, Raajit, Stein, Brady, Talpaz, Moshe, Verstovsek, Srdan, Wadleigh, Martha, Agrawal, Vaibhav, Aljurf, Mahmoud, Angel Diaz, Miguel, Avalos, Belinda R., Bacher, Ulrike, Bashey, Asad, Beitinjaneh, Amer M., Cerny, Jan, Chhabra, Saurabh, Copelan, Edward, Cutler, Corey S., DeFilipp, Zachariah, Gadalla, Shahinaz M., Ganguly, Siddhartha, Grunwald, Michael R., Hashmi, Shahrukh K., Kharfan-Dabaja, Mohamed A., Kindwall-Keller, Tamila, Kröger, Nicolaus, Lazarus, Hillard M., Liesveld, Jane L., Litzow, Mark R., Marks, David I., Nathan, Sunita, Nishihori, Taiga, Olsson, Richard F., Pawarode, Attaphol, Rowe, Jacob M., Savani, Bipin N., Savoie, Mary Lynn, Seo, Sachiko, Solh, Melhem, Tamari, Roni, Verdonck, Leo F., Yared, Jean A., Alyea, Edwin, Popat, Uday, Sobecks, Ronald, Scott, Bart L., Nakamura, Ryotaro, Mesa, Ruben, and Saber, Wael

Published
2020
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46. Erratum to: Retrospective analysis of pacritinib in patients with myelofibrosis and severe thrombocytopenia

Author

Verstovsek, Srdan, primary, Mesa, Ruben, additional, Talpaz, Moshe, additional, Kiladjian, Jean-Jacques, additional, Harrison, Claire N., additional, Oh, Stephen T., additional, Vannucchi, Alessandro M., additional, Rampal, Raajit, additional, Scott, Bart L., additional, Buckley, Sarah A., additional, Craig, Adam R., additional, Roman-Torres, Karisse, additional, and Mascarenhas, John O., additional

Published
2024
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48. Chronic Myeloid Leukemia, Version 2.2024, NCCN Clinical Practice Guidelines in Oncology

Author

Shah, Neil P., primary, Bhatia, Ravi, additional, Altman, Jessica K., additional, Amaya, Maria, additional, Begna, Kebede H., additional, Berman, Ellin, additional, Chan, Onyee, additional, Clements, Joan, additional, Collins, Robert H., additional, Curtin, Peter T., additional, DeAngelo, Daniel J., additional, Drazer, Michael, additional, Maness, Lori, additional, Metheny, Leland, additional, Mohan, Sanjay, additional, Moore, Joseph O., additional, Oehler, Vivian, additional, Pratz, Keith, additional, Pusic, Iskra, additional, Rose, Michal G., additional, Shomali, William, additional, Smith, B. Douglas, additional, Styler, Michael, additional, Talpaz, Moshe, additional, Tanaka, Tiffany N., additional, Tantravahi, Srinivas, additional, Thompson, James, additional, Tsai, Steven, additional, Vaughn, Jennifer, additional, Welborn, Jeanna, additional, Yang, David T., additional, Sundar, Hema, additional, and Gregory, Kristina, additional

Published
2024
Full Text
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50. A randomized, double-blind study of zinpentraxin alfa in patients with myelofibrosis who were previously treated with or ineligible for ruxolitinib:stage 2 of a phase II trial

Author

Verstovsek, Srdan, Talpaz, Moshe, Wadleigh, Martha, Isidori, Alessandro, Te Boekhorst, Peter, Savona, Michael R., Bose, Prithviraj, Pozdnyakova, Olga, Mesa, Ruben, El-Galaly, Tarec C., O'Sullivan, Jennifer, Gamel, Katia, Higgins, Brian, Katakam, Sudhakar, Todorov, Boyan, Trunzer, Kerstin, Harrison, Claire N., Verstovsek, Srdan, Talpaz, Moshe, Wadleigh, Martha, Isidori, Alessandro, Te Boekhorst, Peter, Savona, Michael R., Bose, Prithviraj, Pozdnyakova, Olga, Mesa, Ruben, El-Galaly, Tarec C., O'Sullivan, Jennifer, Gamel, Katia, Higgins, Brian, Katakam, Sudhakar, Todorov, Boyan, Trunzer, Kerstin, and Harrison, Claire N.

Published
2024

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