Your search keyword '"Richardson, Paul G."' showing total 32 results

1. Allocation and validation of the second revision of the International Staging System in the ICARIA-MM and IKEMA studies.

Author

Richardson, Paul G., Perrot, Aurore, Mikhael, Joseph, Martin, Thomas, Beksac, Meral, Spicka, Ivan, Capra, Marcelo, D'Agostino, Mattia, Sonneveld, Pieter, Bisht, Kamlesh, Fukao, Taro, Zhang, Rick, Tada, Keisuke, Tekle, Christina, Macé, Sandrine, Klippel, Zandra, van de Velde, Helgi, and Moreau, Philippe

Abstract

The International Staging System for multiple myeloma recently underwent a second revision (R2-ISS) to include gain/amplification of 1q21 and account for the additive prognostic significance of multiple high-risk features. The phase 3 ICARIA-MM (isatuximab–pomalidomide–dexamethasone vs. pomalidomide–dexamethasone) and IKEMA (isatuximab–carfilzomib–dexamethasone vs. carfilzomib–dexamethasone) studies provide large datasets for retrospectively validating the prognostic value of the R2-ISS in relapsed/refractory multiple myeloma. Of 609 pooled patients, 68 (11.2%) were reclassified as R2-ISS stage I, 136 (22.3%) as R2-ISS stage II, 204 (33.5%) as R2-ISS stage III, 55 (9.0%) as stage IV, and 146 (24.0%) "Not classified". Median progression-free survival was shorter among those reclassified as R2-ISS stage II (HR 1.52, 95% CI 0.979–2.358), stage III (HR 2.59, 95% CI 1.709–3.923), and stage IV (HR 3.51, 95% CI 2.124–5.784) versus stage I. Adding isatuximab led to longer progression-free survival versus doublet therapy (adjusted HR 0.544 [95% CI 0.436–0.680]), with a consistent treatment effect observed across all R2-ISS stages. This is the first study to validate the R2-ISS with novel agents, including anti-CD38 monoclonal antibodies, and to show that R2-ISS, as a prognostic scoring system, can be applied to patients with relapsed/refractory multiple myeloma. [ABSTRACT FROM AUTHOR]

Published

2024

2. Progression-free survival as a surrogate endpoint in myeloma clinical trials: an evolving paradigm.

Author

Pawlyn, Charlotte, Schjesvold, Fredrik H., Cairns, David A., Wei, L. J., Davies, Faith, Nadeem, Omar, Abdulhaq, Haifaa, Mateos, Maria-Victoria, Laubach, Jacob, Weisel, Katja, Ludwig, Heinz, Rajkumar, S. Vincent, Sonneveld, Pieter, Jackson, Graham, Morgan, Gareth, and Richardson, Paul G.

Subjects

CLINICAL trials, MULTIPLE myeloma, PROGRESSION-free survival, OVERALL survival, SUBGROUP analysis (Experimental design)

Abstract

Measurement of overall survival (OS) remains the gold standard for interpreting the impact of new therapies for multiple myeloma in phase 3 trials. However, as outcomes have improved, it is increasingly challenging to use OS as the primary endpoint if timely approval of novel agents is to be ensured to enable maximum benefit for patients. Surrogate endpoints of OS, such as progression-free survival (PFS) and response to treatment, have contributed to approval decisions by the Food and Drug Administration (FDA) and European Medicines Agency as endpoints demonstrating clinical benefit, and the FDA has recently supported the use of minimal residual disease (MRD) as an accelerated approval endpoint in multiple myeloma. This review aims to address situations in which the use of PFS as a surrogate endpoint warrants careful interpretation especially for specific subgroups of patients and considers ways to ensure that studies can be designed to account for possible discordance between PFS and OS. The utility of subgroup analyses, including the potential for those not pre-specified, to identify target populations for new agents is also discussed. [ABSTRACT FROM AUTHOR]

Published

2024

3. Anti-CD38 antibody therapy for patients with relapsed/refractory multiple myeloma: differential mechanisms of action and recent clinical trial outcomes.

Author

Leleu, Xavier, Martin, Thomas, Weisel, Katja, Schjesvold, Fredrik, Iida, Shinsuke, Malavasi, Fabio, Manier, Salomon, Chang-Ki Min, Ocio, Enrique M., Pawlyn, Charlotte, Perrot, Aurore, Quach, Hang, Richter, Joshua, Spicka, Ivan, Yong, Kwee, Richardson, Paul G., and Chang-Ki Min

Subjects

MULTIPLE myeloma treatment, CELL physiology

Abstract

CD38 is a transmembrane glycoprotein that functions both as a receptor and an ectoenzyme, playing key roles in the regulation of calcium signaling and migration of immune cells to tumor microenvironments. High expression on multiple myeloma (MM) cells and limited expression on normal cells makes CD38 an ideal target for the treatment of MM patients. Two monoclonal antibodies directed at CD38, isatuximab and daratumumab, are available for use in patients with relapsed and/or refractory MM (RRMM); daratumumab is also approved in newly diagnosed MM and light-chain amyloidosis. Clinical experience has shown that anti-CD38 antibody therapy is transforming treatment of MM owing to its anti-myeloma efficacy and manageable safety profile. Isatuximab and daratumumab possess similarities and differences in their mechanisms of action, likely imparted by their binding to distinct, non-overlapping epitopes on the CD38 molecule. In this review, we present the mechanistic properties of these two antibodies and outline available evidence on their abilities to induce adaptive immune responses and modulate the bone marrow niche in MM. Further, we discuss differences in regulatory labeling between these two agents and analyze recent key clinical trial results, including evidence in patients with underlying renal impairment and other poor prognostic factors. Finally, we describe the limited existing evidence for the use of isatuximab or daratumumab after disease progression on prior anti-CD38 mono- or combination therapy, highlighting the need for additional clinical evaluations to define optimal anti-CD38 antibody therapy selection and sequencing in RRMM. [ABSTRACT FROM AUTHOR]

Published

2022

4. Gaps and opportunities in the treatment of relapsed-refractory multiple myeloma: Consensus recommendations of the NCI Multiple Myeloma Steering Committee.

Author

Kumar, Shaji, Baizer, Lawrence, Callander, Natalie S., Giralt, Sergio A., Hillengass, Jens, Freidlin, Boris, Hoering, Antje, Richardson, Paul G., Schwartz, Elena I., Reiman, Anthony, Lentzsch, Suzanne, McCarthy, Philip L., Jagannath, Sundar, Yee, Andrew J., Little, Richard F., and Raje, Noopur S.

Subjects

MULTIPLE myeloma, STEM cell transplantation, ALKYLATING agents, DOSAGE forms of drugs, OVERALL survival, PLASMACYTOMA

Abstract

A wide variety of new therapeutic options for Multiple Myeloma (MM) have recently become available, extending progression-free and overall survival for patients in meaningful ways. However, these treatments are not curative, and patients eventually relapse, necessitating decisions on the appropriate choice of treatment(s) for the next phase of the disease. Additionally, an important subset of MM patients will prove to be refractory to the majority of the available treatments, requiring selection of effective therapies from the remaining options. Immunomodulatory agents (IMiDs), proteasome inhibitors, monoclonal antibodies, and alkylating agents are the major classes of MM therapies, with several options in each class. Patients who are refractory to one agent in a class may be responsive to a related compound or to a drug from a different class. However, rules for selection of alternative treatments in these situations are somewhat empirical and later phase clinical trials to inform those choices are ongoing. To address these issues the NCI Multiple Myeloma Steering Committee formed a relapsed/refractory working group to review optimal treatment choices, timing, and sequencing and provide recommendations. Additional issues considered include the role of salvage autologous stem cell transplantation, risk stratification, targeted approaches for genetic subsets of MM, appropriate clinical trial endpoints, and promising investigational agents. This report summarizes the deliberations of the working group and suggests potential avenues of research to improve the precision, timing, and durability of treatments for Myeloma. [ABSTRACT FROM AUTHOR]

Published

2022

5. Is the Endothelium the Missing Link in the Pathophysiology and Treatment of COVID-19 Complications?

Author

Castro, Pedro, Palomo, Marta, Moreno-Castaño, Ana Belen, Fernández, Sara, Torramadé-Moix, Sergi, Pascual, Georgina, Martinez-Sanchez, Julia, Richardson, Edward, Téllez, Adrián, Nicolas, Josep M., Carreras, Enric, Richardson, Paul G., Badimon, Juan José, Escolar, Gines, and Diaz-Ricart, Maribel

Abstract

Patients with COVID-19 present a wide spectrum of disease severity, from asymptomatic cases in the majority to serious disease leading to critical care and even death. Clinically, four different scenarios occur within the typical disease timeline: first, an incubation and asymptomatic period; second, a stage with mild symptoms due mainly to the virus itself; third, in up to 20% of the patients, a stage with severe symptoms where a hyperinflammatory response with a cytokine storm driven by host immunity induces acute respiratory distress syndrome; and finally, a post-acute sequelae (PASC) phase, which present symptoms that can range from mild or annoying to actually quite incapacitating. Although the most common manifestation is acute respiratory failure of the lungs, other organs are also frequently involved. The clinical manifestations of the COVID-19 infection support a key role for endothelial dysfunction in the pathobiology of this condition. The virus enters into the organism via its interaction with angiotensin-converting enzyme 2-receptor that is present prominently in the alveoli, but also in endothelial cells, which can be directly infected by the virus. Cytokine release syndrome can also drive endothelial damage independently. Consequently, a distinctive feature of SARS-CoV-2 infection is vascular harm, with severe endothelial injury, widespread thrombosis, microangiopathy, and neo-angiogenesis in response to endothelial damage. Therefore, endothelial dysfunction seems to be the pathophysiological substrate for severe COVID-19 complications. Biomarkers of endothelial injury could constitute strong indicators of disease progression and severity. In addition, the endothelium could represent a very attractive target to both prevent and treat these complications. To establish an adequate therapy, the underlying pathophysiology and corresponding clinical stage should be clearly identified. In this review, the clinical features of COVID-19, the central role of the endothelium in COVID-19 and in other pathologies, and the potential of specific therapies aimed at protecting the endothelium in COVID-19 patients are addressed. [ABSTRACT FROM AUTHOR]

Published

2022

6. Daratumumab plus lenalidomide/bortezomib/dexamethasone in Black patients with transplant-eligible newly diagnosed multiple myeloma in GRIFFIN.

Author

Nooka, Ajay K., Kaufman, Jonathan L., Rodriguez, Cesar, Jakubowiak, Andrzej, Efebera, Yvonne, Reeves, Brandi, Wildes, Tanya, Holstein, Sarah A., Anderson Jr, Larry D., Badros, Ashraf, Shune, Leyla, Chari, Ajai, Pei, Huiling, Cortoos, Annelore, Patel, Sharmila, Bartlett, J. Blake, Vermeulen, Jessica, Lin, Thomas S., Richardson, Paul G., and Voorhees, Peter

Subjects

BLACK people, MULTIPLE myeloma, DARATUMUMAB, LENALIDOMIDE, PLASMACYTOMA, BORTEZOMIB

Abstract

Among White patients, TEAEs leading to treatment discontinuation occurred in 19.3% ( I n i = 16) and 23.0% ( I n i = 17) of D-RVd and RVd patients, respectively. TEAEs leading to treatment discontinuations in Black patients occurred in 35.7% ( I n i = 5) of D-RVd patients and 27.8% ( I n i = 5) of RVd patients. MRD-negativity (10-5) rates over time are shown for (C) Black patients (D-RVd, n = 14; RVd, n = 18) and (D) White patients (D-RVd, n = 85; RVd, n = 76) in the intent-to-treat population. Median CD34 SP + sp cell yield among Black patients was 11.2 × 10 SP 6 sp /kg for the D-RVd group and 9.4 × 10 SP 6 sp /kg for the RVd group, and among White patients was 7.9 × 10 SP 6 sp /kg for the D-RVd group and 9.4 × 10 SP 6 sp /kg for the RVd group. [Extracted from the article]

Published

2022

7. Antibody interference and response kinetics of isatuximab plus pomalidomide and dexamethasone in multiple myeloma.

Author

Hulin, Cyrille, Beksac, Meral, Goodman, Hugh J., Spicka, Ivan, Alegre, Adrian, Prince, Miles, Campana, Frank, Finn, Greg, Le-Guennec, Solenn, Macé, Sandrine, Muccio, Stéphane, Tavernier, Alexandra, Rouchon, Marie-Claude, and Richardson, Paul G.

Subjects

MULTIPLE myeloma, ANTIBODY formation, DEXAMETHASONE, BONE marrow examination, BLOOD protein electrophoresis

Abstract

In conclusion, eight patients in the Isa-Pd arm, including patients with adverse prognostic characteristics, were MRD negative and were progression-free and alive at primary analysis; 1-year OS rate was 100%. The kinetics of response were faster in patients receiving Isa-Pd with a median time to first response of 1.9 months compared with 3.0 months in those receiving Pd. MRD-negative samples at a sensitivity level of 10 SP -5 sp were detected in 8/14 Isa-Pd patients and 0/2 Pd patients. Mass spectrometry results indicated that interference of Isa with IFE resulted in a 7.1% underestimation of CR in the Isa-Pd arm in patients with RRMM. [Extracted from the article]

Published

2021

8. Association between response kinetics and outcomes in relapsed/refractory multiple myeloma: analysis from TOURMALINE-MM1

Author

Millennium Pharmaceuticals, Garderet, Laurent, Laubach, Jacob P., Stoppa, Anne-Marie, Hari, Parameswaran, Cavo, Michele, Ludwig, Heinz, Mateos, Maria Victoria, Luptakova, Katarina, Lin, Jianchang, Yung, Godwin, Velde, Helgi van de, Berg, Deborah, Moreau, Philippe, Richardson, Paul G., Millennium Pharmaceuticals, Garderet, Laurent, Laubach, Jacob P., Stoppa, Anne-Marie, Hari, Parameswaran, Cavo, Michele, Ludwig, Heinz, Mateos, Maria Victoria, Luptakova, Katarina, Lin, Jianchang, Yung, Godwin, Velde, Helgi van de, Berg, Deborah, Moreau, Philippe, and Richardson, Paul G.

Abstract

The association between depth of response in multiple myeloma (MM) and long-term outcomes is well recognized [1,2,3]. Thus, clinicians and patients are often encouraged by a rapid decrease of M-protein when treatment is initiated, and achieving ≥very-good partial response (VGPR) by 4 months of initial diagnosis has been associated with decreased mortality [4]. However, little is known about the association between response kinetics and outcomes. While some reports suggest that early responders may have compromised long-term outcomes compared with late responders [5, 6], these studies were limited, confined to frontline setting only, and based in the era prior to novel-agent availability.

Published

2018

9. Predictive biomarkers with isatuximab plus pomalidomide and dexamethasone in relapsed/refractory multiple myeloma.

Author

Richardson, Paul G., Facon, Thierry, Bensinger, William I., Leleu, Xavier, Campana, Frank, Macé, Sandrine, Chiron, Marielle, van de Velde, Helgi, and Mikhael, Joseph

Subjects

DEXAMETHASONE, MULTIPLE myeloma treatment

Published

2021

10. Phase 1 study of the protein deubiquitinase inhibitor VLX1570 in patients with relapsed and/or refractory multiple myeloma.

Author

Rowinsky, Eric K., Paner, Agne, Berdeja, Jesus G., Paba-Prada, Claudia, Venugopal, Parameswaran, Porkka, Kimmo, Gullbo, Joachim, Linder, Stig, Loskog, Angelica, Richardson, Paul G., and Landgren, Ola

Subjects

ANTINEOPLASTIC agents, CANCER patients, CLINICAL trials, DRUG dosage, DRUG toxicity, INTRAVENOUS therapy, MULTIPLE myeloma, PATIENT safety, DISEASE relapse, PROTEASE inhibitors, TREATMENT effectiveness

Abstract

Summary: This phase 1 study sought to characterize the safety, tolerability, and pharmacokinetic behavior of VLX1570, a small molecule inhibitor of the deubiquitinases (DUBs) that remove sterically bulky ubiquitin chains from proteins during processing in the19S regulatory subunit of the proteasome, in patients with relapsed and refractory multiple myeloma (MM). Fourteen patients were treated with escalating doses of VLX1570 ranging from 0.05 to 1.2 mg/kg as a brief intravenous (IV) infusion on Days 1, 2, 8, 9, 15, and 16 of a 28-day cycle. Due to its poor aqueous solubility, VLX1570 was formulated in polyethylene glycol, polyoxyethylated castor oil, and polysorbate 80 and administered as a brief intravenous (IV) infusion via a central venous catheter. Anti-myeloma effects were noted at doses at or above 0.6 mg/kg, however, two patients treated at the 1.2 mg/kg dose level experienced severe, abrupt, and progressive respiratory insufficiency, which was associated with diffuse pulmonary infiltrates on imaging studies, similar to those rarely noted with bortezomib and other inhibitors of the 20S proteasome, culminating in death. Although the contribution of VLX1570's formulation to the pulmonary toxicity could not be ruled out, the severity and precipitous nature of the toxicity and the steep relationship between dose and toxicity, the study was discontinued. Despite the severe pulmonary toxicity noted with VLX1570, efforts directed at identifying DUB inhibitors with greater therapeutic indices appear warranted based on the unique mechanism of action, robustness of preclinical antitumor activity, and activity of the DUB inhibitors in MM resistant to PIs targeting the 20S proteasome subunit. [ABSTRACT FROM AUTHOR]

Published

2020

11. Single-agent belantamab mafodotin for relapsed/refractory multiple myeloma: analysis of the lyophilised presentation cohort from the pivotal DREAMM-2 study.

Author

Richardson, Paul G., Lee, Hans C., Abdallah, Al-Ola, Cohen, Adam D., Kapoor, Prashant, Voorhees, Peter M., Hoos, Axel, Wang, Karrie, Baron, January, Piontek, Trisha, Byrne, Julie, Richmond, Scott, Jewell, Roxanne C., Opalinska, Joanna, Gupta, Ira, and Lonial, Sagar

Abstract

DREAMM-2 (NCT03525678) is an ongoing global, open-label, phase 2 study of single-agent belantamab mafodotin (belamaf; GSK2857916), a B-cell maturation antigen-targeting antibody-drug conjugate, in a frozen-liquid presentation in patients with relapsed/refractory multiple myeloma (RRMM). Alongside the main study, following identical inclusion/exclusion criteria, a separate patient cohort was enrolled to receive belamaf in a lyophilised presentation (3.4 mg/kg, every 3 weeks) until disease progression/unacceptable toxicity. Primary outcome was independent review committee-assessed overall response rate (ORR). Twenty-five patients were enrolled; 24 received ≥1 dose of belamaf. As of 31 January 2020, ORR was 52% (95% CI: 31.3–72.2); 24% of patients achieved very good partial response. Median duration of response was 9.0 months (2.8–not reached [NR]); median progression-free survival was 5.7 months (2.2–9.7); median overall survival was not reached (8.7 months–NR). Most common grade 3/4 adverse events were keratopathy (microcyst-like corneal epithelial changes, a pathological finding seen on eye examination [75%]), thrombocytopenia (21%), anaemia (17%), hypercalcaemia and hypophosphatemia (both 13%), neutropenia and blurred vision (both 8%). Pharmacokinetics supported comparability of frozen-liquid and lyophilised presentations. Single-agent belamaf in a lyophilised presentation (intended for future use) showed a deep and durable clinical response and acceptable safety profile in patients with heavily pre-treated RRMM. [ABSTRACT FROM AUTHOR]

Published

2020

12. Veno-occlusive disease/sinusoidal obstruction syndrome in patients with prior gemtuzumab ozogamicin: literature analysis of survival after defibrotide treatment.

Author

Richardson, Paul G. and Corbacioglu, Selim

Subjects

HEPATIC veno-occlusive disease, HEMATOPOIETIC stem cells, CYTOKINES, CANCER chemotherapy, CALICHEAMICIN, MONOCLONAL antibodies

Published

2020

13. Influence of Disease and Patient Characteristics on Daratumumab Exposure and Clinical Outcomes in Relapsed or Refractory Multiple Myeloma.

Author

Yan, Xiaoyu, Clemens, Pamela L., Puchalski, Thomas, Lonial, Sagar, Lokhorst, Henk, Voorhees, Peter M., Usmani, Saad, Richardson, Paul G., Plesner, Torben, Liu, Kevin, Orlowski, Robert Z., Losic, Nedjad, Jansson, Richard, Ahmadi, Tahamtan, Lantz, Kristen, Ruixo, Juan Jose Perez, Zhou, Honghui, and Xu, Xu Steven

Subjects

MULTIPLE myeloma treatment, IMMUNOGLOBULIN G, DRUG efficacy, THERAPEUTIC use of monoclonal antibodies, HEALTH outcome assessment, MULTIPLE myeloma diagnosis, RESEARCH, CLINICAL trials, RESEARCH methodology, MONOCLONAL antibodies, EVALUATION research, MEDICAL cooperation, DISEASE relapse, TREATMENT effectiveness, COMPARATIVE studies, RESEARCH funding, MULTIPLE myeloma, BIOTRANSFORMATION (Metabolism), DRUG resistance in cancer cells

Abstract

Objective: The aim of this study was to understand the influence of disease and patient characteristics on exposure to daratumumab, an immunoglobulin Gκ (IgGκ) monoclonal antibody, and clinical outcomes in relapsed or refractory multiple myeloma (MM).Patients and Methods: Baseline myeloma type, albumin levels, renal/hepatic function, age, sex, race, weight, Eastern Cooperative Oncology Group (ECOG) status, refractory status, and number of prior therapies were evaluated using data from two clinical studies-GEN501 (N = 104) and SIRIUS (N = 124).Results: Daratumumab clearance was approximately 110% higher in IgG myeloma patients than non-IgG myeloma patients, leading to significantly lower exposure in IgG myeloma patients based on maximum trough serum concentrations (p < 0.0001). However, the overall response rate was similar for IgG and non-IgG myeloma patients (odds ratio 1.08, 95% confidence interval 0.54-2.17, p = 0.82). For a given exposure, the drug effect was significantly higher (approximately two times) in IgG versus non-IgG patients (p = 0.03). The influence of other patient and disease characteristics on daratumumab exposure was minimal and no significant effect on efficacy was observed (p ≥ 0.1). The incidences of infections and overall grade 3 or higher adverse events in subpopulations were generally consistent with that of the overall population.Conclusion: Due to competition with the MM-produced IgG M-protein for neonatal Fc receptor protection from clearance, IgG-based monoclonal antibodies in general may have significantly higher clearance and lower concentrations in IgG MM patients compared with non-IgG MM patients. Careful evaluation of the impact of exposure and patient and disease characteristics on safety and efficacy is warranted for all IgG-based monoclonal antibodies used in MM. [ABSTRACT FROM AUTHOR]

Published

2018

14. Dose and Schedule Selection of the Oral Proteasome Inhibitor Ixazomib in Relapsed/Refractory Multiple Myeloma: Clinical and Model-Based Analyses.

Author

Gupta, Neeraj, Yang, Huyuan, Hanley, Michael, Zhang, Steven, Liu, Rachael, Kumar, Shaji, Richardson, Paul, Skacel, Tomas, Venkatakrishnan, Karthik, Hanley, Michael J, and Richardson, Paul G

Abstract

Background: The oral proteasome inhibitor ixazomib has been approved by regulatory authorities around the world, including in the United States and the European Union, for the treatment of patients with multiple myeloma (MM) who have received at least one prior therapy, based on the pivotal phase III TOURMALINE-MM1 study.Objective: The objective of this study was to quantitatively characterize the benefit-risk profile of ixazomib in relapsed/refractory MM in support of the approved dose and schedule.Methods: We report early-phase study data and exposure-response analyses of TOURMALINE-MM1 data that support the selection of the recommended ixazomib dose and schedule.Results: Single-agent ixazomib studies showed a favorable efficacy/safety profile with weekly versus twice-weekly dosing; a phase I/II study of ixazomib in combination with lenalidomide and dexamethasone (IRd) identified a weekly ixazomib dose that offered an acceptable efficacy/safety profile. In IRd exposure-response analyses from TOURMALINE-MM1, ixazomib systemic exposure was not a significant predictor of progression-free survival or probability of response. Significant associations were observed between ixazomib exposure and the probability of grade ≥3 anemia and thrombocytopenia, and grade ≥2 diarrhea, fatigue, nausea, peripheral neuropathy, and rash. Additionally, higher ixazomib exposure was associated with lower lenalidomide relative dose intensity.Conclusions: These analyses support a favorable benefit-risk profile for weekly ixazomib 4.0 mg on days 1, 8, and 15 of 28-day cycles, which was selected for the phase III TOURMALINE registration program.Trial Registration Numbers: ClinicalTrials.gov NCT00932698, NCT00963820, NCT01217957, NCT01564537. [ABSTRACT FROM AUTHOR]

Published

2017

15. Pulmonary and Hepatic Complications of Hematopoietic Cell Transplantation.

Author

Yanik, Gregory A., Cooke, Kenneth R., Ho, Vincent T., and Richardson, Paul G.

Published

2014

16. Resistance to Proteasome Inhibitors in Multiple Myeloma.

Author

Cottini, Francesca, Guidetti, Anna, Prada, Claudia Paba, Hideshima, Teru, Maglio, Michelle, Varga, Cindy, Chauhan, Dharminder, Laubach, Jacob, Anderson, Kenneth C., and Richardson, Paul G.

Published

2014

17. Preclinical Activities of Bortezomib in MM, the Bone Marrow Microenvironment and Pharmacogenomics.

Author

Hideshima, Teru, Richardson, Paul G., and Anderson, Kenneth C.

Abstract

The intracellular protein degradation system is critical for many cellular processes, including cell cycle regulation. The proteasomes are intracellular protein complexes that degrade polyubiquitinated proteins. Bortezomib (Velcade®) is a boronic acid dipeptide that directly binds to enzymatic complex to block chimotrypsin-like activity of proteasome and is the first FDA-approved proteasome inhibitor for multiple myeloma (MM) treatment. Bortezomib blocks degradation of multi-proteins, including regulators of cell cycle, anti-apoptosis, and inflammation, as well as immune surveillance. In MM cells, bortezomib directly induces cell stress response followed by activation of c-Jun NH2 terminal kinase/stress- activated protein kinase and triggers cell cycle arrest, followed by caspase-dependent apoptosis. Bortezomib also modulates activities of non-MM cellular components, including stromal cells and osteoblasts in the bone marrow milieu. Importantly, combination treatment strategies, including histone deacetylase inhibitors, Akt inhibitor, lenalidomide, heat shock protein 90 inhibitors, and aurora kinase inhibitors demonstrate significant anti-MM activities both in preclinical and clinical studies. [ABSTRACT FROM AUTHOR]

Published

2011

18. Bortezomib-Induced Peripheral Neuropathy in Multiple Myeloma: Principles of Identification and Management.

Author

Laubach, Jacob P. and Richardson, Paul G.

Abstract

The first-in-class proteasome inhibitor bortezomib is a potent anti-myeloma drug that now figures prominently in the management of patients with both newly diagnosed and relapsed multiple myeloma. With current studies evaluating its efficacy as part of conditioning prior to and maintenance therapy following autologous stem cell transplantation, it is likely that its role in the management of the disease will expand further. Peripheral neuropathy was recognized as a toxicity associated with bortezomib at an early point in the clinical development of the agent, and further study has provided considerable insight regarding this issue. It is critical that clinicians recognize and appropriately manage bortezomib-induced PN to optimize care for patients. This chapter focuses on the identification, characterization, and management of bortezomib-induced peripheral neuropathy. [ABSTRACT FROM AUTHOR]

Published

2011

19. Rescue of Hippo coactivator YAP1 triggers DNA damage-induced apoptosis in hematological cancers.

Author

Cottini, Francesca, Hideshima, Teru, Xu, Chunxiao, Sattler, Martin, Dori, Martina, Agnelli, Luca, ten Hacken, Elisa, Bertilaccio, Maria Teresa, Antonini, Elena, Neri, Antonino, Ponzoni, Maurilio, Marcatti, Magda, Richardson, Paul G, Carrasco, Ruben, Kimmelman, Alec C, Wong, Kwok-Kin, Caligaris-Cappio, Federico, Blandino, Giovanni, Kuehl, W Michael, and Anderson, Kenneth C

Subjects

ONCOGENES, DNA damage, APOPTOSIS, CELL death, CANCER cells

Abstract

Oncogene-induced DNA damage elicits genomic instability in epithelial cancer cells, but apoptosis is blocked through inactivation of the tumor suppressor p53. In hematological cancers, the relevance of ongoing DNA damage and the mechanisms by which apoptosis is suppressed are largely unknown. We found pervasive DNA damage in hematologic malignancies, including multiple myeloma, lymphoma and leukemia, which leads to activation of a p53-independent, proapoptotic network centered on nuclear relocalization of ABL1 kinase. Although nuclear ABL1 triggers cell death through its interaction with the Hippo pathway coactivator YAP1 in normal cells, we show that low YAP1 levels prevent nuclear ABL1-induced apoptosis in these hematologic malignancies. YAP1 is under the control of a serine-threonine kinase, STK4. Notably, genetic inactivation of STK4 restores YAP1 levels, triggering cell death in vitro and in vivo. Our data therefore identify a new synthetic-lethal strategy to selectively target cancer cells presenting with endogenous DNA damage and low YAP1 levels. [ABSTRACT FROM AUTHOR]

Published

2014

20. Tumor cell-specific bioluminescence platform to identify stroma-induced changes to anticancer drug activity.

Author

McMillin, Douglas W., Delmore, Jake, Weisberg, Ellen, Negri, Joseph M., Geer, D. Corey, Klippel, Steffen, Mitsiades, Nicholas, Schlossman, Robert L., Munshi, Nikhil C., Kung, Andrew L., Griffin, James D., Richardson, Paul G., Anderson, Kenneth C., and Mitsiades, Constantine S.

Subjects

TUMORS, CANCER cells, BIOLUMINESCENCE, ANTIGEN presenting cells, DRUG resistance in cancer cells, DRUG therapy

Abstract

Conventional anticancer drug screening is typically performed in the absence of accessory cells of the tumor microenvironment, which can profoundly alter antitumor drug activity. To address this limitation, we developed the tumor cell–specific in vitro bioluminescence imaging (CS-BLI) assay. Tumor cells (for example, myeloma, leukemia and solid tumors) stably expressing luciferase are cultured with nonmalignant accessory cells (for example, stromal cells) for selective quantification of tumor cell viability, in presence versus absence of stromal cells or drug treatment. CS-BLI is high-throughput scalable and identifies stroma-induced chemoresistance in diverse malignancies, including imatinib resistance in leukemic cells. A stroma-induced signature in tumor cells correlates with adverse clinical prognosis and includes signatures for activated Akt, Ras, NF-κB, HIF-1α, myc, hTERT and IRF4; for biological aggressiveness; and for self-renewal. Unlike conventional screening, CS-BLI can also identify agents with increased activity against tumor cells interacting with stroma. One such compound, reversine, shows more potent activity in an orthotopic model of diffuse myeloma bone lesions than in conventional subcutaneous xenografts. Use of CS-BLI, therefore, enables refined screening of candidate anticancer agents to enrich preclinical pipelines with potential therapeutics that overcome stroma-mediated drug resistance and can act in a synthetic lethal manner in the context of tumor-stroma interactions. [ABSTRACT FROM AUTHOR]

Published

2010

21. The evolution and impact of therapy in multiple myeloma.

Author

Laubach, Jacob P., Richardson, Paul G., and Anderson, Kenneth C.

Abstract

Multiple myeloma is a clonal B-cell malignancy characterized by aberrant expression of plasma cells wtihin the bone marrow, and is associated with the well known clinical manifestations anemia, bone disease, renal dysfunction, hypercalcemia, and recurrent infections. For many years, melphalan and prednisone represented the standard of care in multiple myeloma therapy, with stem cell transplantation reserved for selected patients. Treatment of the disease has evolved rapidly over the past decade, however, with the development and utilization of thalidomide, lenalidomide, and bortezomib. As a result of these developments, clinical outcomes have improved significantly. This review highlights important historic landmarks as well as more recent events that have played an important role in the evolution of myeloma therapy. [ABSTRACT FROM AUTHOR]

Published

2010

22. Understanding multiple myeloma pathogenesis in the bone marrow to identify new therapeutic targets.

Author

Hideshima, Teru, Mitsiades, Constantine, Tonon, Giovanni, Richardson, Paul G., and Anderson, Kenneth C.

Subjects

MULTIPLE myeloma, CARCINOGENESIS, BONE marrow diseases, PLASMA cell diseases, HUMAN cytogenetics, TUMOR treatment

Abstract

Multiple myeloma is a plasma cell malignancy characterized by complex heterogeneous cytogenetic abnormalities. The bone marrow microenvironment promotes multiple myeloma cell growth and resistance to conventional therapies. Although multiple myeloma remains incurable, novel targeted agents, used alone or in combination, have shown great promise to overcome conventional drug resistance and improve patient outcome. Recent oncogenomic studies have further advanced our understanding of the molecular pathogenesis of multiple myeloma, providing the framework for new prognostic classification and identifying new therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2007

23. Management Strategies for Relapsed Multiple Myeloma.

Author

Richardson, Paul G., Schlossman, Robert, Munshi, Nikhil, and Anderson, Kenneth

Subjects

*MULTIPLE myeloma, *TUMOR treatment, *CANCER relapse, *DISEASE relapse, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Multiple myeloma is the second most common hematologic malignancy after non-Hodgkin lymphoma. Numerous treatments for this disease are available, but despite high overall response rates, relapse occurs in almost all patients, and survival has typically been no more than 5 years. Treatment options for relapsed patients include pulsed dexamethasone; cyclophosphamide-based therapy; doxorubicin-based regimens; melphalan and prednisone; thalidomide with or without dexamethasone; bortezomib; and high-dose chemotherapy supported by autologous or allogeneic stem cell transplantation. Relapsed disease is more difficult to treat, and patients characteristically become resistant to therapy. As a result of the numerous potential complications of multiple myeloma, including fatigue, bone pain, renal dysfunction, increased susceptibility to infection, and spinal cord compression, quality of life has a significant role in the choice of therapy. New strategies in the treatment of relapsed disease are focusing on therapy that is targeted to various cell-signaling pathways and microenvironmental interactions involved in the pathogenesis of multiple myeloma. As they become available, these strategies are showing promise in the treatment of both relapsed and refractory disease, the most recent being the potent thalidomide analog lenalidomide. Research efforts are also concentrated on improving front-line therapy to reduce the rate of relapse so that, ultimately, survival may be extended and patient outcome improved. [ABSTRACT FROM AUTHOR]

Published

2006

24. Emerging Therapies for Multiple Myeloma.

Author

Podar, Klaus, Hideshima, Teru, Yu-Tzu Tai, Richardson, Paul G., Chauhan, Dharminder, and Anderson, Kenneth C.

Subjects

MULTIPLE myeloma treatment, B cell lymphoma, PLASMA cells, IMMUNODEFICIENCY, THALIDOMIDE

Abstract

Multiple myeloma (MM) is a malignancy of plasma cells within the bone marrow characterized by bone loss, renal disease, and immunodeficiency. Recent advances in the understanding of MM pathogenesis have improved established conventional cytotoxic therapy as well as transplantation regimens. Despite these advances, median overall survival is only 3–5 years. Therefore new therapies are urgently needed. Besides thalidomide, whose antimyeloma activity has only recently been defined, a plethora of novel agents, including the thalidomide-derived immunomodulatory drugs and bortezomib, have been identified to directly target the tumor cell or its microenvironment, and thereby inhibit MM cell growth and survival, and to overcome drug resistance. After validation of their preclinical anti-MM activity, several clinical trials are now ongoing to test the efficacy of these novel therapeutics, administered alone or in combination with conventional or other novel therapeutics and bone marrow transplantation. This article reviews the development of MM therapy, from its initial description approximately 150 years ago to the novel therapy regimens of recent years, highlighting that MM may soon become a chronic disease. [ABSTRACT FROM AUTHOR]

Published

2006

25. Molecular characterization of PS-341 (bortezomib) resistance: implications for overcoming resistance using lysophosphatidic acid acyltransferase (LPAAT)-ßinhibitors.

Author

Hideshima, Teru, Chauhan, Dharminder, Ishitsuka, Kenji, Yasui, Hiroshi, Raje, Noopur, Kumar, Shaji, Podar, Klaus, Mitsiades, Constantine, Hideshima, Hiromasa, Bonham, Lynn, Munshi, Nikhil C, Richardson, Paul G, Singer, Jack W, and Anderson, Kenneth C

Subjects

APOPTOSIS, CELL death, MONOCLONAL gammopathies, ANTHRACYCLINES, LYSOPHOSPHOLIPIDS, ACYLTRANSFERASES

Abstract

PS-341 (bortezomib, Velcade™) is a promising novel agent for treatment of advanced multiple myeloma (MM); however, 65%of patients with relapsed refractory disease in a phase II study do not respond to PS-341. We have previously shown that lysophosphatidic acid acyltransferase (LPAAT)-ßinhibitor CT-32615 triggers caspase-dependent apoptosis, and can overcome resistance to conventional therapeutics (i.e., dexamethasone, doxorubicin, melphalan) in MM cells. In this study, we therefore determined whether CT-32615 could also overcome resistance to PS-341. We first characterized molecular mechanisms of resistance to PS-341 in DHL-4 cells. DHL-4 cells express low levels of caspase-3 and caspase-8; furthermore, no cleavage in caspase-8, caspase-9, caspase-3, poly ADP-ribose polymerase (PARP), or DNA fragmentation factor 45 was triggered by PS-341 treatment. We have previously shown that PS-341 treatment triggers phosphorylation of c-Jun NH2-terminal kinase (JNK), which subsequently induces caspase-dependent apoptosis; conversely, JNK inhibition blocks PS-341-induced apoptosis. We here show that phosphorylation of SEK-1, JNK, and c-Jun are not induced by PS-341 treatment, suggesting that PS-341 does not trigger a stress response in DHL-4 cells. Importantly, CT-32615 inhibits growth of DHL-4 cells in a time- and dose-dependent fashion: a transient G2/M cell cycle arrest induced by CT-32615 is mediated via downregulation of cdc25c and cdc2. CT-32615 triggered swelling and lysis of DHL-4 cells, without caspase/PARP cleavage or TUNEL-positivity, suggesting a necrotic response. Our studies therefore demonstrate that LPAAT-ßinhibitor CT-32615 triggers necrosis, even in PS-341-resistant DHL-4 cells, providing the framework for its evaluation to overcome clinical PS-341 resistance and improve patient outcome.Oncogene (2005) 24, 3121-3129. doi:10.1038/sj.onc.1208522 Published online 21 February 2005 [ABSTRACT FROM AUTHOR]

Published

2005

26. p38 MAPK inhibition enhances PS-341 (bortezomib)-induced cytotoxicity against multiple myeloma cells.

Author

Hideshima, Teru, Podar, Klaus, Chauhan, Dharminder, Ishitsuka, Kenji, Mitsiades, Constantine, Tai, Yu-Tzu, Hamasaki, Makoto, Raje, Noopur, Hideshima, Hiromasa, Schreiner, George, Nguyen, Aaron N, Navas, Tony, Munshi, Nikhil C, Richardson, Paul G, Higgins, Linda S, and Anderson, Kenneth C

Subjects

HYBRIDOMAS, PLASMACYTOMA, PATIENTS, MONOCLONAL gammopathies, PROTEIN kinases, CELLS

Abstract

Although PS-341 (bortezomib) is a promising agent to improve multiple myeloma (MM) patient outcome, 65%of patients with relapsed and refractory disease do not respond. We have previously shown that heat shock protein (Hsp)27 is upregulated after PS-341 treatment, that overexpression of Hsp27 confers PS-341 resistance, and that inhibition of Hsp27 overcomes PS-341 resistance. Since Hsp27 is a downstream target of p38 mitogen-activated protein kinase (MAPK)/MAPK-mitogen-activated protein kinase-2 (MAPKAPK2), we hypothesized that inhibition of p38 MAPK activity could augment PS-341 cytotoxicity by downregulating Hsp27. Although p38 MAPK inhibitor SCIO-469 (Scios Inc, CA, USA) alone did not induce significant growth inhibition, it blocked baseline and PS-341-triggered phosphorylation of p38 MAPK as well as upregulation of Hsp27, associated with enhanced cytotoxicity in MM.1S cells. Importantly, SCIO-469 enhanced phosphorylation of c-Jun NH2-terminal kinase (JNK) and augmented cleavage of caspase-8 and poly(ADP)-ribose polymerase. Moreover, SCIO-469 downregulated PS-341-induced increases in G2/M-phase cells, associated with downregulation of p21Cip1 expression. Importantly, SCIO-469 treatment augmented cytotoxicity of PS-341 even against PS-341-resistant cell lines and patient MM cells. These studies therefore provide the framework for clinical trials of SCIO-469 to enhance sensitivity and overcome resistance to PS-341, thereby improving patient outcome in MM.Oncogene (2004) 23, 8766-8776. doi:10.1038/sj.onc.1208118 Published online 11 October 2004 [ABSTRACT FROM AUTHOR]

Published

2004

27. Proteasome Inhibition: A Novel Approach to Anticancer Therapy.

Author

Richardson, Paul G., Hideshima, Teru, and Anderson, Kenneth C.

Subjects

*CANCER treatment, *PROTEASE inhibitors, *PROTEINS, *APOPTOSIS, *MULTIPLE myeloma

Abstract

Proteasome inhibition is a new approach under investigation for cancer therapy. Protein degradation by the proteasome is a fundamental metabolic process. Inhibition of the proteasome has been shown to result in cell-cycle arrest and programmed cell death. Bortezomib (Velcade®; formerly PS-341, Millennium Pharmaceuticals, Inc, Cambridge, Massachusetts) is the first proteasome inhibitor to enter clinical trials and is approved for the treatment of multiple myeloma in patients who have received at least two prior therapies and progressed on their last therapy. It is also being investigated for the treatment of a range of other cancers, both solid and hematologic. In preclinical studies, bortezomib causes apoptosis in cancer cells and seems to enhance the cytotoxicity of other conventional tumoricidal agents in human tumor cell lines, murine tumor models, and human xenograft models. In addition to targeting cancer cells directly, there is growing evidence that proteasome inhibition interferes with protective interactions between cancer cells and the bone marrow and may also act to prevent tumor-associated angiogenesis. Preliminary data suggest that bortezomib inhibits proteasome activity in a dose-dependent and reversible manner, and has manageable toxicities. A phase II trial in relapsed and refractory multiple myeloma patients indicated that patients experienced substantial anticancer activity when treated with bortezomib monotherapy. [ABSTRACT FROM AUTHOR]

Published

2004

28. Proteasome inhibitor PS-341 abrogates IL-6 triggered signaling cascades via caspase-dependent downregulation of gp130 in multiple myeloma.

Author

Hideshima, Teru, Chauhan, Dharminder, Hayashi, Toshiaki, Akiyama, Masaharu, Mitsiades, Nicholas, Mitsiades, Constantine, Podar, Klaus, Munshi, Nikhil C., Richardson, Paul G., and Anderson, Kenneth C.

Subjects

PHOSPHORYLATION, PROTEIN kinases, INTERLEUKIN-6, CELLS, DRUG resistance, BONE marrow, IMMUNE system, CYTOKINES

Abstract

Proteasome inhibitor PS-341 is one of the most promising novel agents against multiple myeloma (MM). We have previously shown that PS-341 inhibits IL-6 triggered phosphorylation of extracellular signal-regulated kinases (ERK) 1/2 (also known as p42/44 mitogen-activated protein kinases) in MM cells. In this study, we further examined whether clinically achievable concentrations of PS-341 could inhibit IL-6 triggered signaling cascades in MM. We found that PS-341 inhibited not only ERK, but also signal transducers and activators of transcription (STAT) 3 as well as Akt phosphorylation. Since gp130 (CD130) dimerizes and is phosphorylated after IL-6 binding to gp80 (IL-6 receptor), we hypothesized that gp130 could be involved in PS-341-induced blockade of signaling cascades mediating MM cell growth, survival, and drug resistance in the bone marrow (BM) microenvironment. In this study, we first demonstrate that PS-341 induces downregulation of gp130 in a time- and dose-dependent manner in vitro, prior to MM cell death. Conversely, downregulation of gp130 is completely abrogated by the pan-caspase inhibitor Z-VAD-FMK, suggesting that downregulation of gp130 is mediated via caspase activation. Z-VAD-FMK also abrogates the inhibitory effect of PS-341 on IL-6-triggered signaling cascades. Importantly, we demonstrate that phosphorylation of ERK, STAT3, and Akt in MM.1S cells induced by either exogenous IL-6 or by binding of MM cells to BM stromal cells is abrogated by PS-341. These studies, therefore, define another novel mechanism whereby PS-341 can overcome the growth and survival advantage in MM cells conferred by the BM milieu. Importantly, this effect on cytokine-induced gp130 signaling cascades may account, at least in part, for the remarkable preclinical sensitivity and clinical responses achieved in MM with PS-341 treatment.Oncogene (2003) 22, 8386-8393. doi:10.1038/sj.onc.1207170 [ABSTRACT FROM AUTHOR]

Published

2003

29. Activation of NF-KB and upregulation of intracellular anti-apoptotic proteins via the IGF-1/Akt signaling in human multiple myeloma cells: therapeutic implications.

Author

Mitsiades, Constantine S., Mitsiades, Nicholas, Poulaki, Vassiliki, Schlossman, Robert, Akiyama, Masaharu, Chauhan, Dharminder, Hideshima, Teru, Treon, Steven P., Munshi, Nikhil C., Richardson, Paul G., and Anderson, Kenneth C.

Subjects

SOMATOMEDIN, PHOSPHORYLATION, MYELOMA proteins

Abstract

Presents a study that demonstrated the functions of insulin-like growth factor-1. Inducement of phosphorylation of the FKHRL-1 Forkhead transcription factor; Upregulation of a series of intracellular anti-apoptotic proteins; Effect on Apo2L/TRAIL-sensitivity of multiple myeloma cells.

Published

2002

30. The KDM3A-KLF2-IRF4 axis maintains myeloma cell survival.

Author

Ohguchi, Hiroto, Hideshima, Teru, Bhasin, Manoj K., Gorgun, Gullu T., Santo, Loredana, Cea, Michele, Samur, Mehmet K., Mimura, Naoya, Suzuki, Rikio, Tai, Yu-Tzu, Carrasco, Ruben D., Raje, Noopur, Richardson, Paul G., Munshi, Nikhil C., Harigae, Hideo, Sanda, Takaomi, Sakai, Juro, and Anderson, Kenneth C.

Published

2016

31. Thalidomide maintenance in multiple myeloma.

Author

Laubach, Jacob P., Richardson, Paul G., and Anderson, Kenneth C.

Abstract

The article focuses on the efficacy of thalidomide maintenance therapy to treat patients diagnosed with multiple myeloma. It relates the study of A. Spencer and colleagues focuses on the adoption of the thalidomide-based maintenance therapy on the autologous stem cells transplantation (ASCT). It states that the study suggests that maintenance therapy with thalidomide-corticosteroid combination should be applied in patients who undergone ASCT.

Published

2009

32. Lenalidomide plus dexamethasone is efficacious in patients with relapsed or refractory multiple myeloma.

Author

Munshi, Nikhil C., Mitsiades, Constantine, Richardson, Paul G., and Anderson, Kenneth C.

Abstract

The article discusses research on the use of lenalidomide and dexamethasone in patient with relapsed or refractory multiple myeloma. It references a study by M. Dimopoulos published in a 2007 issue of the "New England Journal of Medicine." According to the study, patients treated with lenalidomide and dexamethasone posted longer time for their diseases to progress compared to those given placebo and dexamethasone.

Published

2008