Your search keyword '"Munshi, Nikhil C"' showing total 105 results

1. Idecabtagene Vicleucel in Relapsed and Refractory Multiple Myeloma.

Author

Munshi, Nikhil C., Anderson, Larry D., Shah, Nina, Madduri, Deepu, Berdeja, JesOs, Lonial, Sagar, Raje, Noopur, Lin, Yi, Siegel, David, Oriol, Albert, Moreau, Philippe, Yakoub-Agha, Ibrahim, Delforge, Michel, Cavo, Michele, Einsele, Hermann, Goldschmidt, Hartmut, Weisel, Katja, Rambaldi, Alessandro, Reece, Donna, and Petrocca, Fabio

Subjects

*MULTIPLE myeloma, *CYTOKINE release syndrome, *DRUG efficacy, *CHIMERIC antigen receptors, *CELL analysis

Abstract

BACKGROUND Idecabtagene vicleucel (ide-cel, also called bb2121), a B-cell maturation antigen directed chimeric antigen receptor (CAR) T-cell therapy, has shown clinical activity with expected CAR T-cell toxic effects in patients with relapsed and refractory multiple myeloma. METHODS In this phase 2 study, we sought to confirm the efficacy and safety of ide-cel in patients with relapsed and refractory myeloma. Patients with disease after at least three previous regimens including a proteasome inhibitor, an immunomodulating agent, and an anti-CD38 antibody were enrolled. Patients received ide-cel target doses of 150 x 106 to 450 x 106 CAR-positive (CAR+) T cells. The primary end point was an overall response (partial response or better); a key secondary end point was a complete response or better (comprising complete and stringent complete responses). RESULTS Of 140 patients enrolled, 128 received ide-cel. At a median follow-up of 13.3 months, 94 of 128 patients (7396) had a response, and 42 of 128 (33%) had a complete response or better. Minimal residual disease (MRD)-negative status (<10-5 nucleated cells) was confirmed in 33 patients, representing 26% of all 128 patients who were treated and 79% of the 42 patients who had a complete response or better. The median progression-free survival was 8.8 months (95% confidence interval, 5.6 to 11.6). Common toxic effects among the 128 treated patients included neutropenia in 117 patients (91%), anemia in 89 (70%), and thrombocytopenia in 81 (63%). Cytokine release syndrome was reported in 107 patients (84%), including 7 (5%) who had events of grade 3 or higher. Neurotoxic effects developed in 23 patients (18%) and were of grade 3 in 4 patients (3%); no neurotoxic effects higher than grade 3 occurred. Cellular kinetic analysis confirmed CAR+ T cells in 29 of49 patients (59%) at 6 months and 4 of 11 patients (36%) at 12 months after infusion. CONCLUSIONS Ide-cel induced responses in a majority of heavily pretreated patients with refractory and relapsed myeloma; MRD-negative status was achieved in 26% of treated patients. Almost all patients had grade 3 or 4 toxic effects, most commonly hematologic toxic effects and cytokine release syndrome. (Funded by bluebird bio and Celgene, a Bristol-Myers Squibb company; KarMMa ClinicalTrials.gov number, NCT03361748.) [ABSTRACT FROM AUTHOR]

Published

2021

2. Deep Response in Multiple Myeloma: A Critical Review.

Author

Fulciniti, Mariateresa, Munshi, Nikhil C., and Martinez-Lopez, Joaquin

Subjects

*CANCER patients, *MULTIPLE myeloma, *PROGNOSIS, *TREATMENT effectiveness

Abstract

Novel and more effective treatment strategies against multiple myeloma (MM) have significantly prolonged patients’ survival and raised interest in the depth of response and its association with clinical outcome. Minimal residual disease (MRD) has emerged as one of themost relevant prognostic factors inMMand should be included in a new definition of complete response (CR). Although further standardization is still required, MRD monitoring should be applied in prospective clinical trials as a sensitive tool to compare and evaluate the efficacy of different treatment strategies, particularly in the consolidation and maintenance settings, and implement individualized therapy-monitoring approaches.Here, we review current definition of deep response in MM, advantages and limitations of current MRD assessment assays, clinical evidences for MRD monitoring as a prognostic tool for therapeutic decisions in MM, and challenges to develop uniform criteria for MRD monitoring [ABSTRACT FROM AUTHOR]

Published

2015

3. Pathogenesis beyond the cancer clone(s) in multiple myeloma.

Author

Bianchi, Giada and Munshi, Nikhil C.

Subjects

*CARCINOGENESIS, *MULTIPLE myeloma diagnosis, *MULTIPLE myeloma treatment, *MOLECULAR biology, *PLASMA cells

Abstract

Over the past 4 decades, basic research has provided crucial information regarding the cellular and molecular biology of cancer. In particular, the relevance of cancer microenvironment (including both cellular and noncellular elements) and the concept of clonal evolution and heterogeneity have emerged as important in cancer pathogenesis, immunologic escape, and resistance to therapy. Multiple myeloma (MM), a cancer of terminally differentiated plasma cells, is emblematic of the impact of cancer microenvironment and the role of clonal evolution. Although genetic and epigenetic aberrations occur in MM and evolve over time under the pressure of exogenous stimuli, they are also largely present in premalignant plasma cell dys-crasia such as monoclonal gammopathy of undetermined significance (MGUS) and smoldering multiple myeloma (SMM), suggesting that genetic mutations alone are necessary, but not sufficient, for myeloma transformation. The role of bone marrow microenvironment in mediating survival, proliferation, and resistance to therapy in myeloma is well established; and although an appealing speculation, its role in fostering the evolution of MGUS or SMM into MM is yet to be proven. In this review, we discuss MM pathogenesis with a particular emphasis on the role of bone marrow micro-environment. [ABSTRACT FROM AUTHOR]

Published

2015

4. Genomic heterogeneity in multiple myeloma.

Author

Szalat, Raphaël and Munshi, Nikhil C

Subjects

*MULTIPLE myeloma, *CANCER cell proliferation, *GENOMICS, *HUMAN genetics, *PLASMA cells, *GENE expression

Abstract

Multiple myeloma (MM) is an incurable malignancy in majority of patients characterized by clonal proliferation of plasma cells. To date, treatment is established based on general conditions and age of patients. However, MM is a heterogeneous disease, featured by various subtypes and different outcomes. Thus, the understanding of MM biology is currently a major challenge to eventually cure the disease. During the last decade, karyotype studies and gene expression profiling have identified robust prognostic markers as well as a widespread genomic landscape. More recently, studies of epigenetic, transcriptional modifications and next generation sequencing have allowed characterization of critical genes and pathways, clonal heterogeneity and mutational profiles involved in myelomagenesis. Altogether, these findings constitute important tools to develop new targeted and personalized therapies in MM. [ABSTRACT FROM AUTHOR]

Published

2015

5. THE AUTHORS REPLY.

Author

Munshi, Nikhil C., Hege, Kristen, and San-Miguel, Jesús

Subjects

*LACTATE dehydrogenase, *PLASMA cell diseases, *OVERALL survival, *FLUORESCENCE in situ hybridization

Published

2021

6. Case 13-2008.

Author

Munshi, Nikhil C., Digumarthy, Subba, and Rahemtullah, Aliyah

Subjects

*RHEUMATOID arthritis, *LYMPHOPROLIFERATIVE disorders, *CANCER patients, *PULMONARY fibrosis, *PATIENTS

Abstract

The article presents a case study of a 46 year old rheumatoid arthritis patient who had been healthy until presenting to doctors with anorexia and generalized lymphadenopathy. A discussion of various medical tests, including laboratory blood tests and computed tomography scans, which were performed on the patient, is presented. The patient's diagnosis of pulmonary fibrosis related to rheumatoid arthritis and lymphoma, and subsequent successful treatment are discussed.

Published

2008

7. CLINICAL NEPHROLOGY - EPIDEMIOLOGY - CLINICAL TRIALS Podocyte injury associated glomerulopathies induced by pamidronate.

Author

Barri, Yousri M., Munshi, Nikhil C., Sukumalchantra, Suteetat, Abulezz, Sameh R., Bonsib, Stephen M., Wallach, Jeffrey, and Walker, Patrick D.

Subjects

*GLOMERULONEPHRITIS, *DISODIUM pamidronate, *TUMORS, *THERAPEUTICS, *HISTOLOGY, *PHARMACODYNAMICS, *DRUG efficacy

Abstract

Podocyte injury associated glomerulopathies induced by pamidronate. Background. Pamidronate has been demonstrated to decrease bone-related complications in multiple myeloma and delay progression of the disease. This has led to its use in supportive and maintenance therapy of myeloma in conjunction with steroids and chemotherapy. It has also been selectively used in patients with breast cancer and other neoplasms. Methods. We report on five patients who developed glomerular disease induced by pamidronate. Pamidronate was the only drug common to all patients. Tests for hepatitis B and C and human immunodeficiency virus (HIV) were negative for all patients. The first two patients received a high dose of pamidronate for 8 weeks, whereas the other three patients were on monthly therapy for a prolonged period of time. Sources of data included chart review and pathologic analysis of kidney biopsy. Results. Three patients were female and two were males and all were Caucasian, ranging in age from 58 to 71 years. Renal biopsy findings included minimal change disease in two, focal segmental glomerulosclerosis in two, and collapsing focal segmental glomerulosclerosis in one. Immunofluorescence was essentially negative in all cases. Electron microscopy showed variable podocyte injury and extensive foot process effacement. There was no evidence of multiple myeloma-related renal disease. After the biopsy, pamidronate was discontinued and renal function stabilized in all patients except the one with the collapsing variant of focal segmental glomerulosclerosis who required hemodialysis. Three patients had resolution of proteinuria, one patient continued to have proteinuria without deterioration in renal function. Conclusion. Pamidronate has been mainly associated with collapsing focal segmental glomerulosclerosis. This report expands that relationship and adds other glomerular diseases linked with podocyte injury. Additional studies are needed to define the cause of the variability of renal histology with this agent. [ABSTRACT FROM AUTHOR]

Published

2004

8. Natural Language Processing Algorithm to Extract Multiple Myeloma Stage From Oncology Notes in the Veterans Affairs Healthcare System.

Author

Goryachev, Sergey D., Yildirim, Cenk, DuMontier, Clark, La, Jennifer, Dharne, Mayuri, Gaziano, J. Michael, Brophy, Mary T., Munshi, Nikhil C., Driver, Jane A., Do, Nhan V., and Fillmore, Nathanael R.

Subjects

*ELECTRONIC health records, *MULTIPLE myeloma, *DATA warehousing, *TUMOR classification, *PATHOLOGY

Abstract

PURPOSE: Stage in multiple myeloma (MM) is an essential measure of disease risk, but its measurement in large databases is often lacking. We aimed to develop and validate a natural language processing (NLP) algorithm to extract oncologists' documentation of stage in the national Veterans Affairs (VA) Healthcare System. METHODS: Using nationwide electronic health record (EHR) and cancer registry data from the VA Corporate Data Warehouse, we developed and validated a rule-based NLP algorithm to extract oncologist-determined MM stage. To that end, a clinician annotated MM stage within over 5,000 short snippets of clinical notes, and annotated MM stage at MM treatment initiation for 200 patients. These were allocated into snippet- and patient-level development and validation sets. We developed MM stage extraction and roll-up algorithms within the development sets. After the algorithms were finalized, we validated them using standard measures in held-out validation sets. RESULTS: We developed algorithms for three different MM staging systems that have been in widespread use (Revised International Staging System [R-ISS], International Staging System [ISS], and Durie-Salmon [DS]) and for stage reported without a clearly defined system. Precision and recall were uniformly high for MM stage at the snippet level, ranging from 0.92 to 0.99 for the different MM staging systems. Performance in identifying for MM stage at treatment initiation at the patient level was also excellent, with precision of 0.92, 0.96, 0.90, and 0.86 and recall of 0.99, 0.98, 0.94, and 0.92 for R-ISS, ISS, DS, and unclear stage, respectively. CONCLUSION: Our MM stage extraction algorithm uses rule-based NLP and data aggregation to accurately measure MM stage documented in oncology notes and pathology reports in VA's national EHR system. It may be adapted to other systems where MM stage is recorded in clinical notes. [ABSTRACT FROM AUTHOR]

Published

2024

9. Monoclonal Gammopathy of Undetermined Significance: Genetic vs Environmental Etiologies.

Author

Munshi, Nikhil C.

Subjects

*MONOCLONAL gammopathies, *PLASMA cell diseases, *DISEASE prevalence, *ETIOLOGY of diseases, *DISEASE risk factors

Abstract

The article presents the different study that asserts the prevalence and growth rate of monoclonal gamopathy of undetermined significance (MGUS). The study was administered in different population and countries with distinct environmental characteristics wherein ethnic differences and genetic factors affects the prevalence and growth rate development. The author adds that the conducted studies provides opportunity to identify and implement preventive strategies that addresses its risk factors.

Published

2007

10. Natural Language Processing Algorithm to Extract Multiple Myeloma Stage From Oncology Notes in the Veterans Affairs Healthcare System.

Author

Goryachev, Sergey D., Yildirim, Cenk, DuMontier, Clark, La, Jennifer, Dharne, Mayuri, Gaziano, J. Michael, Brophy, Mary T., Munshi, Nikhil C., Driver, Jane A., Do, Nhan V., and Fillmore, Nathanael R.

Subjects

*MULTIPLE myeloma, *TUMOR classification, *ELECTRONIC health records, *DATA extraction, *MEDICAL care, *ALGORITHMS, *NATURAL language processing

Abstract

PURPOSE: Stage in multiple myeloma (MM) is an essential measure of disease risk, but its measurement in large databases is often lacking. We aimed to develop and validate a natural language processing (NLP) algorithm to extract oncologists' documentation of stage in the national Veterans Affairs (VA) Healthcare System. METHODS: Using nationwide electronic health record (EHR) and cancer registry data from the VA Corporate Data Warehouse, we developed and validated a rule-based NLP algorithm to extract oncologist-determined MM stage. To that end, a clinician annotated MM stage within over 5,000 short snippets of clinical notes, and annotated MM stage at MM treatment initiation for 200 patients. These were allocated into snippet- and patient-level development and validation sets. We developed MM stage extraction and roll-up algorithms within the development sets. After the algorithms were finalized, we validated them using standard measures in held-out validation sets. RESULTS: We developed algorithms for three different MM staging systems that have been in widespread use (Revised International Staging System [R-ISS], International Staging System [ISS], and Durie-Salmon [DS]) and for stage reported without a clearly defined system. Precision and recall were uniformly high for MM stage at the snippet level, ranging from 0.92 to 0.99 for the different MM staging systems. Performance in identifying for MM stage at treatment initiation at the patient level was also excellent, with precision of 0.92, 0.96, 0.90, and 0.86 and recall of 0.99, 0.98, 0.94, and 0.92 for R-ISS, ISS, DS, and unclear stage, respectively. CONCLUSION: Our MM stage extraction algorithm uses rule-based NLP and data aggregation to accurately measure MM stage documented in oncology notes and pathology reports in VA's national EHR system. It may be adapted to other systems where MM stage is recorded in clinical notes. Stage is a key factor in assessment of multiple myeloma (MM) risk, but large databases lack the necessary laboratory and pathology data for staging. We developed a rules-based NLP algorithm to extract oncologist-determined MM stage from VA EHR data. The algorithm demonstrated accurate assignment of MM stage when validated against clinician annotation. [ABSTRACT FROM AUTHOR]

Published

2024

11. c‐MYC expression and maturity phenotypes are associated with outcome benefit from addition of ixazomib to lenalidomide‐dexamethasone in myeloma.

Author

Di Bacco, Alessandra, Bahlis, Nizar J., Munshi, Nikhil C., Avet‐Loiseau, Hervé, Masszi, Tamás, Viterbo, Luísa, Pour, Ludek, Ganly, Peter, Cavo, Michele, Langer, Christian, Kumar, Shaji K., Rajkumar, S. Vincent, Keats, Jonathan J., Berg, Deborah, Lin, Jianchang, Li, Bin, Badola, Sunita, Shen, Lei, Zhang, Jacob, and Esseltine, Dixie‐Lee

Subjects

*STEM cell transplantation, *RNA sequencing, *MULTIPLE myeloma, *PROGRESSION-free survival, *STEM cell treatment

Abstract

Objectives: In the TOURMALINE‐MM1 phase 3 trial in relapsed/refractory multiple myeloma, ixazomib‐lenalidomide‐dexamethasone (IRd) showed different magnitudes of progression‐free survival (PFS) benefit vs placebo‐Rd according to number and type of prior therapies, with greater benefit seen in patients with >1 prior line of therapy or 1 prior line of therapy without stem cell transplantation (SCT). Methods: RNA sequencing data were used to investigate the basis of these differences. Results: The PFS benefit of IRd vs placebo‐Rd was greater in patients with tumors expressing high c‐MYC levels (median not reached vs 11.3 months; hazard ratio [HR] 0.42; 95% CI, 0.26, 0.66; P <.001) compared with in those expressing low c‐MYC levels (median 20.6 vs 16.6 months; HR 0.75; 95% CI, 0.42, 1.2). Expression of c‐MYC in tumors varied based on the number and type of prior therapy received, with the lowest levels observed in tumors of patients who had received 1 prior line of therapy including SCT. These tumors also had higher expression levels of CD19 and CD81. Conclusions: PFS analyses suggest that lenalidomide and ixazomib target tumors with different levels of c‐MYC, CD19, and CD81 expression, thus providing a potential rationale for the differential benefits observed in the TOURMALINE‐MM1 study. This trial was registered at www.clinicaltrials.gov as: NCT01564537 [ABSTRACT FROM AUTHOR]

Published

2020

12. Corrigendum to “Genomic heterogeneity in multiple myeloma” [Curr. Opin. Genet. Dev. 30 (2015) 56–65].

Author

Szalat, Raphaël and Munshi, Nikhil C

Subjects

*MULTIPLE myeloma, *CANCER genetics, *MEDICAL periodicals, *GENETICS

Published

2016

13. Genetic Alterations in Members of the Proteasome 26S Subunit, AAA-ATPase (PSMC) Gene Family in the Light of Proteasome Inhibitor Resistance in Multiple Myeloma.

Author

Haertle, Larissa, Buenache, Natalia, Cuesta Hernández, Hipólito Nicolás, Simicek, Michal, Snaurova, Renata, Rapado, Inmaculada, Martinez, Nerea, López-Muñoz, Nieves, Sánchez-Pina, José María, Munawar, Umair, Han, Seungbin, Ruiz-Heredia, Yanira, Colmenares, Rafael, Gallardo, Miguel, Sanchez-Beato, Margarita, Piris, Miguel Angel, Samur, Mehmet Kemal, Munshi, Nikhil C., Ayala, Rosa, and Kortüm, Klaus Martin

Subjects

*THERAPEUTIC use of antineoplastic agents, *GENETIC mutation, *SEQUENCE analysis, *GENETICS, *ADENOSINE triphosphatase, *MONOCLONAL gammopathies, *RESEARCH funding, *MULTIPLE myeloma, *ENZYME inhibitors, *DRUG resistance in cancer cells, *CARRIER proteins, *CHEMICAL inhibitors

Abstract

Simple Summary: In comparison to other neoplasias, Multiple Myeloma is extremely sensitive to changes in protein homeostasis. Therefore, proteasome inhibitors are highly efficient and widely used for this disease. Genetic alterations of the PSMC genes, such as the ones shown in this manuscript, affect this Multiple Myeloma vulnerability and, therefore, play a key role in the physiopathogenesis and resistance to proteasome inhibitors. By different modes of action, those alterations are likely to increase the proteolytic capacity of cancer cells. Even though they occur in low frequencies, they can serve as biomarkers to predict and monitor a patient's response to proteasome inhibitors over time and might be useful to guide therapy. For the treatment of Multiple Myeloma, proteasome inhibitors are highly efficient and widely used, but resistance is a major obstacle to successful therapy. Several underlying mechanisms have been proposed but were only reported for a minority of resistant patients. The proteasome is a large and complex machinery. Here, we focus on the AAA ATPases of the 19S proteasome regulator (PSMC1-6) and their implication in PI resistance. As an example of cancer evolution and the acquisition of resistance, we conducted an in-depth analysis of an index patient by applying FISH, WES, and immunoglobulin-rearrangement sequencing in serial samples, starting from MGUS to newly diagnosed Multiple Myeloma to a PI-resistant relapse. The WES analysis uncovered an acquired PSMC2 Y429S mutation at the relapse after intensive bortezomib-containing therapy, which was functionally confirmed to mediate PI resistance. A meta-analysis comprising 1499 newly diagnosed and 447 progressed patients revealed a total of 36 SNVs over all six PSMC genes that were structurally accumulated in regulatory sites for activity such as the ADP/ATP binding pocket. Other alterations impact the interaction between different PSMC subunits or the intrinsic conformation of an individual subunit, consequently affecting the folding and function of the complex. Interestingly, several mutations were clustered in the central channel of the ATPase ring, where the unfolded substrates enter the 20S core. Our results indicate that PSMC SNVs play a role in PI resistance in MM. [ABSTRACT FROM AUTHOR]

Published

2023

14. RAD51 Is Implicated in DNA Damage, Chemoresistance and Immune Dysregulation in Solid Tumors.

Author

Liao, Chengcheng, Talluri, Srikanth, Zhao, Jiangning, Mu, Shidai, Kumar, Subodh, Shi, Jialan, Buon, Leutz, Munshi, Nikhil C., and Shammas, Masood A.

Subjects

*PROTEIN metabolism, *ADENOCARCINOMA, *BIOMARKERS, *SEQUENCE analysis, *GENETIC mutation, *WESTERN immunoblotting, *IMMUNE system, *PLASMIDS, *RNA, *APOPTOSIS, *CELL physiology, *GENE expression, *INTERFERONS, *CELL survival, *CELLULAR signal transduction, *BIOINFORMATICS, *GENOMICS, *TRANSFERASES, *GENE expression profiling, *DNA damage, *CELL lines, *MULTIPLE myeloma, *DRUG resistance in cancer cells, TUMOR prevention

Abstract

Simple Summary: Aims and objectives: Destabilization of genetic material can contribute to development and progression of cancer including development of drug resistance and treatment failure. We have previously shown that a protein RAD51 and its corresponding activity, which maintain stability of genetic material (DNA) in normal cells, are dysregulated in cancer. Purpose of this study was to investigate role of RAD51 and its potential as therapeutic target in cancer. Results: We demonstrate that increased level of RAD51 is associated with poor survival of esophageal, breast and colon cancer patients. Our data indicated that increased RAD51 contributes to growth as well as spontaneous and chemotherapy-induced damage and destabilization of genetic material in cancer cells. Moreover, the treatment of cancer cells with chemotherapeutic drug (cisplatin) led to activation of mechanisms which disrupt immune surveillance and maintenance of genetic material, whereas addition of RAD51 inhibitor prevented activation of such mechanisms. Conclusions: Drugs targeting RAD51 have potential to inhibit growth of cancer cells while preserving integrity of genetic material and immune system. When used in combination, these treatments can increase ability of chemotherapeutic drugs to kill cancer cells while minimizing their harmful impact on genetic material and immune system. Background: In normal cells, homologous recombination (HR) is tightly regulated and plays an important role in the maintenance of genomic integrity and stability through precise repair of DNA damage. RAD51 is a recombinase that mediates homologous base pairing and strand exchange during DNA repair by HR. Our previous data in multiple myeloma and esophageal adenocarcinoma (EAC) show that dysregulated HR mediates genomic instability. Purpose of this study was to investigate role of HR in genomic instability, chemoresistance and immune dysregulation in solid tumors including colon and breast cancers. Methods: The GEO dataset were used to investigate correlation of RAD51 expression with patient survival and expression of various immune markers in EAC, breast and colorectal cancers. RAD51 was inhibited in cancer cell lines using shRNAs and a small molecule inhibitor. HR activity was evaluated using a plasmid-based assay, DNA breaks assessed by evaluating expression of γ-H2AX (a marker of DNA breaks) and p-RPA32 (a marker of DNA end resection) using Western blotting. Genomic instability was monitored by investigating micronuclei (a marker of genomic instability). Impact of RAD51 inhibitor and/or a DNA-damaging agent was assessed on viability and apoptosis in EAC, breast and colon cancer cell lines in vitro and in a subcutaneous tumor model of EAC. Impact of RAD51 inhibitor on expression profile was monitored by RNA sequencing. Results: Elevated RAD51 expression correlated with poor survival of EAC, breast and colon cancer patients. RAD51 knockdown in cancer cell lines inhibited DNA end resection and strand exchange activity (key steps in the initiation of HR) as well as spontaneous DNA breaks, whereas its overexpression increased DNA breaks and genomic instability. Treatment of EAC, colon and breast cancer cell lines with a small molecule inhibitor of RAD51 inhibited DNA breaking agent-induced DNA breaks and genomic instability. RAD51 inhibitor potentiated cytotoxicity of DNA breaking agent in all cancer cell types tested in vitro as well as in a subcutaneous model of EAC. Evaluation by RNA sequencing demonstrated that DNA repair and cell cycle related pathways were induced by DNA breaking agent whereas their induction either prevented or reversed by RAD51 inhibitor. In addition, immune-related pathways such as PD-1 and Interferon Signaling were also induced by DNA breaking agent whereas their induction prevented by RAD51 inhibitor. Consistent with these observations, elevated RAD51 expression also correlated with that of genes involved in inflammation and other immune surveillance. Conclusions: Elevated expression of RAD51 and associated HR activity is involved in spontaneous and DNA damaging agent-induced DNA breaks and genomic instability thus contributing to chemoresistance, immune dysregulation and poor prognosis in cancer. Therefore, inhibitors of RAD51 have great potential as therapeutic agents for EAC, colon, breast and probably other solid tumors. [ABSTRACT FROM AUTHOR]

Published

2022

15. Quality of life, psychological distress, and prognostic perceptions in patients with multiple myeloma.

Author

O'Donnell, Elizabeth K., Shapiro, Yael N., Yee, Andrew J., Nadeem, Omar, Hu, Bonnie Y., Laubach, Jacob P., Branagan, Andrew R., Anderson, Kenneth C., Mo, Clifton C., Munshi, Nikhil C., Ghobrial, Irene M., Sperling, Adam S., Agyemang, Emerentia A., Burke, Jill N., Harrington, Cynthia C., Richardson, Paul G., Raje, Noopur S., and El‐Jawahri, Areej

Abstract

Background: Multiple myeloma (MM) is an incurable hematologic malignancy requiring long‐term, continuous therapy. Despite its chronic and unrelenting course, studies examining quality of life (QOL), psychological distress, and perceptions of prognosis by line of therapy are lacking. Methods: The authors conducted a cross‐sectional, multisite study of patients undergoing treatment for MM (excluding maintenance) between June 2020 and January 2021. The authors conducted purposeful sampling and recruited patients to 3 cohorts based on lines of therapy: 1) newly diagnosed receiving first‐line therapy; 2) 2 to 3 lines; and 3) 4 or more lines. Patients completed validated questionnaires to assess their QOL, fatigue, psychological distress, and perceptions of prognosis. Results: A total of 180 patients with MM were enrolled (newly diagnosed [n = 60], 2 to 3 lines [n = 60], and ≥4 lines of therapy [n = 60]). QOL, symptom burden, and fatigue scores did not differ by lines of therapy. There were no statistically significant differences in psychological distress by line of therapy. The rates of clinically significant depression, anxiety, and post‐traumatic stress disorder symptoms were 23.9% (43 of 180), 23.9% (43 of 180), and 24.4% (44 of 180), respectively. Most patients (84.7%, 149 of 176) reported that their oncologist told them their cancer was incurable, but only 30.6% (53 of 173) acknowledged that they were terminally ill, and 42.0% (73 of 174) reported that they thought their cancer was incurable. Conclusions: Patients with MM undergoing treatment experience impaired QOL and elevated psychological distress across the disease continuum, regardless of line of therapy. A substantial proportion of patients with MM have significant misperceptions about their prognosis and the curability of their illness despite reporting being informed of the prognosis by their oncologist. Lay Summary: This study discusses 180 patients with MM (newly diagnosed [n = 60], 2‐3 lines [n = 60], and ≥4 lines of therapy [n = 60]). Quality of life, symptom burden, and fatigue scores do not differ by lines of therapy. There are also no statistically significant differences in psychological distress by line of therapy.The rates of clinically significant depression, anxiety, and post‐traumatic stress disorder symptoms are 23.9%, 23.9%, and 24.4%, respectively.Most patients (84.7%) report that their oncologist told them their cancer was incurable, but only 30.6% acknowledge that they are terminally ill, and 42.0% report that they thought their cancer was incurable. Patients with multiple myeloma undergoing treatment experience impaired quality of life and elevated psychological distress across the disease continuum. Although the majority reported that their oncologist had told them that their cancer is incurable, a substantial proportion still reported that they believed their cancer was curable. [ABSTRACT FROM AUTHOR]

Published

2022

16. Chromothripsis identifies a rare and aggressive entity among newly diagnosed multiple myeloma patients.

Author

Magrangeas, Florence, Avet-Loiseau, Hervé, Munshi, Nikhil C., and Minvielle, Stéphane

Subjects

*PLASMA cells, *CELL proliferation, *GENOMICS, *NUCLEOTIDES, *GENETIC polymorphisms, *DISEASES

Abstract

Multiple myeloma (MM) develops from a premalignant plasma cell proliferative disorder, and with time can progress to a more aggressive disease in extramedullary locations. The gradually clinical evolution is supported by clonal expansion of cells that acquire genetic lesions over years. This model of cancer evolution based on ongoing genomic instability mechanism may apply to development of most MM cases. However, in a small fraction of newly diagnosed MM who relapse quickly and finally die within 2 years, the gradual model appears to be untenable. Analysis of high resolution copy number profiles obtained using single nucleotide polymorphism array data from 764 newly diagnosed MM identified large numbers of genomic rearrangements with the hallmarks of chromothripsis in 1.3% of samples. Moreover, this catastrophic event confers a poor outcome. Because chromothripsis appears to occur in a single crisis, our results suggest that high-risk MM patients use this novel way of cancer evolution. [ABSTRACT FROM AUTHOR]

Published

2011

17. MHC class I chain-related protein A antibodies and shedding are associated with the progression of multiple myeloma.

Author

Jinushi, Masahisa, Vanneman, Matthew, Munshi, Nikhil C., Yu-Tzu Tai, Prabhala, Rao H., Ritz, Jerome, Neuberg, Donna, Anderson, Kenneth C., Carrasco, Daniel Ruben, and Dranoff, Glenn

Subjects

*MULTIPLE myeloma, *IMMUNOGLOBULINS, *PLASMA cells, *B cell lymphoma, *MONOCLONAL gammopathies, *PLASMACYTOMA, *LEUCOCYTES

Abstract

Monoclonal gammopathy of undetermined significance (MGUS) is a common disorder of aging and a precursor lesion to full-blown multiple myeloma (MM). The mechanisms underlying the progression from MGUS to MM are incompletely understood but include the suppression of innate and adaptive antitumor immunity. Here, we demonstrate that NKG2D, an activating receptor on natural killer (NK) cells, CD8+ T lymphocytes, and MHC class I chain-related protein A (MICA), an NKG2D ligand induced in malignant plasma cells through DNA damage, contribute to the pathogenesis of MGUS and MM. MICA expression is increased on plasma cells from MGUS patients compared with normal donors, whereas MM patients display intermediate MICA levels and a high expression of ERp5, a protein disulfide isomerase linked to MICA shedding (sMICA). MM, but not MGUS, patients harbor circulating sMICA, which triggers the down-regulation of NKG2D and impaired lymphocyte cytotoxicity. In contrast, MGUS, but not MM, patients generate high-titer anti-MICA antibodies that antagonize the suppressive effects of sMICA and stimulate dendritic cell cross-presentation of malignant plasma cells. Bortezomib, a proteasome inhibitor with anti-MM clinical efficacy, activates the DNA damage response to augment MICA expression in some MM cells, thereby enhancing their opsonization by anti-MICA antibodies. Together, these findings reveal that the alterations in the NKG2D pathway are associated with the progression from MGUS to MM and raise the possibility that anti-MICA monoclonal antibodies might prove therapeutic for these disorders. [ABSTRACT FROM AUTHOR]

Published

2008

18. The role of the bone microenvironment in the pathophysiology and therapeutic management of multiple myeloma: Interplay of growth factors, their receptors and stromal interactions

Author

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

Subjects

*MULTIPLE myeloma, *BONE marrow, *PATHOLOGICAL physiology, *IMMUNE system

Abstract

Abstract: The close relationship between the biological behaviour of malignant cells and the local microenvironment where they reside is a feature of diverse neoplasias. Multiple myeloma (MM) is considered a main disease model for the study of such interactions and the mechanisms that can lead to bone-related clinical complications, as well as the role of these interactions in attenuating the activity of conventional anti-MM therapeutics, such as dexamethasone and cytotoxic chemotherapeutics. This review focuses on recent progress in the study of interactions of MM cells with their local microenvironment. Major emphasis is placed on how bone marrow stromal cells (BMSCs) and other normal constituents of the bone marrow milieu promote, through cell adhesion- and cytokine-mediated mechanisms, the ability of MM cells to resist conventional anti-MM therapies. The review also addresses ongoing research into these mechanisms, which has already provided several new molecular targets and corresponding therapeutic strategies, such as the proteasome inhibitor bortezomib and thalidomide derivatives (e.g. lenalidomide), for the management of myeloma. [Copyright &y& Elsevier]

Published

2006

19. CD44 v5 domain inhibition represses the polarization of Th2 cells by interfering with the IL‐4/IL‐4R signaling pathway.

Author

Yang, Chun, Lin, Jianhong, Liang, Hongyan, Xue, Li, Kwart, Ariel, Jiang, Meng, Zhao, Jianjun, Ren, Huan, Jiang, Xiaofeng, and Munshi, Nikhil C

Subjects

*TH2 cells, *CD44 antigen, *CELLULAR signal transduction, *TH1 cells, *T cells, *INTERLEUKIN-7

Abstract

The balance between T helper type 1 (Th1) and T helper type 2 (Th2) cells is critical for both innate and acquired immune reactions. However, the precise mechanisms of T helper‐cell differentiation remain unclear. As an important T‐cell activation molecule, CD44 participates in the differentiation of Th1 and Th2 cells. We demonstrated that CD44 variant exon v5 (CD44 v5) is highly expressed by induced human Th2 cells. To investigate the role of the CD44 v5 domain in Th2 cell differentiation, we treated human CD4+ T cells with anti‐CD44v5 antibody and observed that the levels of phosphorylated STAT6 and GATA3 and the secretion of interleukin‐4 (IL‐4) were significantly decreased after the treatment. We also further found that the inhibition of Th2 differentiation was caused by the degradation of the alpha chain of IL‐4 receptor (IL‐4Rα), the CD44 v5 domain colocalized with IL‐4Rα on cell surface and the degradation of IL‐4Rα increased after CD44 v5 domain blocking or ablating. Our results indicated that CD44v5 antibody treatment interrupted the interaction between CD44 v5 domain and IL‐4Rα, but the CD44 v5 domain blockage would not spoil the colocalization between IL‐4R expression and T‐cell receptor and the immunological synapse formation; similar results were also found in CD44v5‐deficient CD4+ T cells. In conclusion, we revealed the function of the CD44 v5 domain in Th2 cell differentiation; blocking or ablating the CD44 v5 domain could accelerate IL‐4Rα degradation and then induce the Th2 cell inhibition. [ABSTRACT FROM AUTHOR]

Published

2022

20. Focus on multiple myeloma

Author

Mitsiades, Constantine S., Mitsiades, Nicholas, Munshi, Nikhil C., and Anderson, Kenneth C.

Published

2004

21. Defining Multimorbidity and Its Impact in Older United States Veterans Newly Treated for Multiple Myeloma.

Author

Fillmore, Nathanael R, DuMontier, Clark, Yildirim, Cenk, La, Jennifer, Epstein, Mara M, Cheng, David, Cirstea, Diana, Yellapragada, Sarvari, Abel, Gregory A, Gaziano, J Michael, Do, Nhan, Brophy, Mary, Kim, Dae H, Munshi, Nikhil C, Driver, Jane A, and Fillmore, Nathanael

Subjects

*MULTIPLE myeloma, *COMORBIDITY, *OLDER people, *VETERANS, *OVERALL survival, *CARDIOVASCULAR diseases, *METABOLIC disorders, *MULTIPLE myeloma treatment, *RESEARCH, *RESEARCH methodology, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding

Abstract

Background: Traditional count-based measures of comorbidity are unlikely to capture the complexity of multiple chronic conditions (multimorbidity) in older adults with cancer. We aimed to define patterns of multimorbidity and their impact in older United States veterans with multiple myeloma (MM).Methods: We measured 66 chronic conditions in 5076 veterans aged 65 years and older newly treated for MM in the national Veterans Affairs health-care system from 2004 to 2017. Latent class analysis was used to identify patterns of multimorbidity among these conditions. These patterns were then assessed for their association with overall survival, our primary outcome. Secondary outcomes included emergency department visits and hospitalizations.Results: Five patterns of multimorbidity emerged from the latent class analysis, and survival varied across these patterns (log-rank 2-sided P < .001). Older veterans with cardiovascular and metabolic disease (30.9%, hazard ratio [HR] = 1.33, 95% confidence interval [CI] = 1.21 to 1.45), psychiatric and substance use disorders (9.7%, HR = 1.58, 95% CI = 1.39 to 1.79), chronic lung disease (15.9%, HR = 1.69, 95% CI = 1.53 to 1.87), and multisystem impairment (13.8%, HR = 2.25, 95% CI = 2.03 to 2.50) had higher mortality compared with veterans with minimal comorbidity (29.7%, reference). Associations with mortality were maintained after adjustment for sociodemographic variables, measures of disease risk, and the count-based Charlson Comorbidity Index. Multimorbidity patterns were also associated with emergency department visits and hospitalizations.Conclusions: Our findings demonstrate the need to move beyond count-based measures of comorbidity and consider cancer in the context of multiple chronic conditions. [ABSTRACT FROM AUTHOR]

Published

2021

22. Ciltacabtagene autoleucel, a B-cell maturation antigen-directed chimeric antigen receptor T-cell therapy in patients with relapsed or refractory multiple myeloma (CARTITUDE-1): a phase 1b/2 open-label study.

Author

Berdeja, Jesus G, Madduri, Deepu, Usmani, Saad Z, Jakubowiak, Andrzej, Agha, Mounzer, Cohen, Adam D, Stewart, A Keith, Hari, Parameswaran, Htut, Myo, Lesokhin, Alexander, Deol, Abhinav, Munshi, Nikhil C, O'Donnell, Elizabeth, Avigan, David, Singh, Indrajeet, Zudaire, Enrique, Yeh, Tzu-Min, Allred, Alicia J, Olyslager, Yunsi, and Banerjee, Arnob

Subjects

*CHIMERIC antigen receptors, *MULTIPLE myeloma, *CYTOKINE release syndrome, *OVERALL survival, *SURVIVAL rate, *LYMPHOPENIA, *RESEARCH, *IMMUNIZATION, *CLINICAL trials, *RESEARCH methodology, *CELL receptors, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies

Abstract

Background: CARTITUDE-1 aimed to assess the safety and clinical activity of ciltacabtagene autoleucel (cilta-cel), a chimeric antigen receptor T-cell therapy with two B-cell maturation antigen-targeting single-domain antibodies, in patients with relapsed or refractory multiple myeloma with poor prognosis.Methods: This single-arm, open-label, phase 1b/2 study done at 16 centres in the USA enrolled patients aged 18 years or older with a diagnosis of multiple myeloma and an Eastern Cooperative Oncology Group performance status score of 0 or 1, who received 3 or more previous lines of therapy or were double-refractory to a proteasome inhibitor and an immunomodulatory drug, and had received a proteasome inhibitor, immunomodulatory drug, and anti-CD38 antibody. A single cilta-cel infusion (target dose 0·75 × 106 CAR-positive viable T cells per kg) was administered 5-7 days after start of lymphodepletion. The primary endpoints were safety and confirmation of the recommended phase 2 dose (phase 1b), and overall response rate (phase 2) in all patients who received treatment. Key secondary endpoints were duration of response and progression-free survival. This trial is registered with ClinicalTrials.gov, NCT03548207.Findings: Between July 16, 2018, and Oct 7, 2019, 113 patients were enrolled. 97 patients (29 in phase 1b and 68 in phase 2) received a cilta-cel infusion at the recommended phase 2 dose of 0·75 × 106 CAR-positive viable T cells per kg. As of the Sept 1, 2020 clinical cutoff, median follow-up was 12·4 months (IQR 10·6-15·2). 97 patients with a median of six previous therapies received cilta-cel. Overall response rate was 97% (95% CI 91·2-99·4; 94 of 97 patients); 65 (67%) achieved stringent complete response; time to first response was 1 month (IQR 0·9-1·0). Responses deepened over time. Median duration of response was not reached (95% CI 15·9-not estimable), neither was progression-free survival (16·8-not estimable). The 12-month progression-free rate was 77% (95% CI 66·0-84·3) and overall survival rate was 89% (80·2-93·5). Haematological adverse events were common; grade 3-4 haematological adverse events were neutropenia (92 [95%] of 97 patients), anaemia (66 [68%]), leukopenia (59 [61%]), thrombocytopenia (58 [60%]), and lymphopenia (48 [50%]). Cytokine release syndrome occurred in 92 (95%) of 97 patients (4% were grade 3 or 4); with median time to onset of 7·0 days (IQR 5-8) and median duration of 4·0 days (IQR 3-6). Cytokine release syndrome resolved in all except one with grade 5 cytokine release syndrome and haemophagocytic lymphohistiocytosis. CAR T-cell neurotoxicity occurred in 20 (21%) patients (9% were grade 3 or 4). 14 deaths occurred in the study; six due to treatment-related adverse events, five due to progressive disease, and three due to treatment-unrelated adverse events.Interpretation: A single cilta-cel infusion at the target dose of 0·75 × 106 CAR-positive viable T cells per kg led to early, deep, and durable responses in heavily pretreated patients with multiple myeloma with a manageable safety profile. The data from this study formed the basis for recent regulatory submissions.Funding: Janssen Research & Development and Legend Biotech. [ABSTRACT FROM AUTHOR]

Published

2021

23. Prevalence and Outcome of COVID-19 Infection in Cancer Patients: A National Veterans Affairs Study.

Author

Fillmore, Nathanael R, La, Jennifer, Szalat, Raphael E, Tuck, David P, Nguyen, Vinh, Yildirim, Cenk, Do, Nhan V, Brophy, Mary T, and Munshi, Nikhil C

Subjects

*COVID-19, *CANCER patients, *CANCER-related mortality, *VETERANS, *OLDER patients, *RESEARCH funding

Abstract

Background: Emerging data suggest variability in susceptibility and outcome to coronavirus disease 2019 (COVID-19) infection. Identifying risk factors associated with infection and outcomes in cancer patients is necessary to develop healthcare recommendations.Methods: We analyzed electronic health records of the US Veterans Affairs Healthcare System and assessed the prevalence of COVID-19 infection in cancer patients. We evaluated the proportion of cancer patients tested for COVID-19 who were positive, as well as outcome attributable to COVID-19, and stratified by clinical characteristics including demographics, comorbidities, cancer treatment, and cancer type. All statistical tests are 2-sided.Results: Of 22 914 cancer patients tested for COVID-19, 1794 (7.8%) were positive. The prevalence of COVID-19 was similar across age. Higher prevalence was observed in African American (15.0%) compared with White (5.5%; P < .001) and in patients with hematologic malignancy compared with those with solid tumors (10.9% vs 7.8%; P < .001). Conversely, prevalence was lower in current smokers and patients who recently received cancer therapy (<6 months). The COVID-19-attributable mortality was 10.9%. Higher attributable mortality rates were observed in older patients, those with higher Charlson comorbidity score, and in certain cancer types. Recent (<6 months) or past treatment did not influence attributable mortality. Importantly, African American patients had 3.5-fold higher COVID-19-attributable hospitalization; however, they had similar attributable mortality as White patients.Conclusion: Preexistence of cancer affects both susceptibility to COVID-19 infection and eventual outcome. The overall COVID-19-attributable mortality in cancer patients is affected by age, comorbidity, and specific cancer types; however, race or recent treatment including immunotherapy do not impact outcome. [ABSTRACT FROM AUTHOR]

Published

2021

24. Integrated genomics and comprehensive validation reveal drivers of genomic evolution in esophageal adenocarcinoma.

Author

Kumar, Subodh, Buon, Leutz, Talluri, Srikanth, Roncador, Marco, Liao, Chengcheng, Zhao, Jiangning, Shi, Jialan, Chakraborty, Chandraditya, Gonzalez, Gabriel, Tai, Yu-Tzu, Prabhala, Rao, Samur, Mehmet K., Munshi, Nikhil C., and Shammas, Masood A.

Subjects

*BIOLOGICAL evolution, *ESOPHAGEAL tumors, *TUMOR growth, *DNA damage, *DATA analysis, TUMOR genetics

Abstract

Esophageal adenocarcinoma (EAC) is associated with a marked genomic instability, which underlies disease progression and development of resistance to treatment. In this study, we used an integrated genomics approach to identify a genomic instability signature. Here we show that elevated expression of this signature correlates with poor survival in EAC as well as three other cancers. Knockout and overexpression screens establish the relevance of these genes to genomic instability. Indepth evaluation of three genes (TTK, TPX2 and RAD54B) confirms their role in genomic instability and tumor growth. Mutational signatures identified by whole genome sequencing and functional studies demonstrate that DNA damage and homologous recombination are common mechanisms of genomic instability induced by these genes. Our data suggest that the inhibitors of TTK and possibly other genes identified in this study have potential to inhibit/reduce growth and spontaneous as well as chemotherapy-induced genomic instability in EAC and possibly other cancers. Subodh Kumar et al. identify a gene signature correlated with genomic instability and poor survival in esophageal adenocarcinoma (EAC), using a combination of integrative genomic analysis of patient data and laboratory validation in cell line models and mice. They find that inhibitors of some of the identified proteins, including TTK, could be used to reduce genomic evolution as well as inhibit growth of EAC cells. [ABSTRACT FROM AUTHOR]

Published

2021

25. Summary of the Third Annual Blood and Marrow Transplant Clinical Trials Network Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling.

Author

Holstein, Sarah A., Al-Kadhimi, Zaid, Costa, Luciano J., Hahn, Theresa, Hari, Parameswaran, Hillengass, Jens, Jacob, Allison, Munshi, Nikhil C., Oliva, Stefania, Pasquini, Marcelo C., Shi, Qian, Stadtmauer, Edward A., Waldvogel, Stephanie L., and McCarthy, Philip L.

Subjects

*IMMUNOLOGIC diseases, *CLINICAL trials, *BONE marrow, *BLOOD, *TRANSPLANTATION of organs, tissues, etc.

Abstract

• This is a comprehensive summary from the third annual Blood and Marrow Transplant Clinical Trials Network Myeloma Intergroup Minimal Residual Disease (MRD) and Immune Profiling (IP) workshop. • MRD is not yet established as a surrogate endpoint but is a prognostic biomarker. • Incorporation of IP as an exploratory endpoint in trial design is recommended. The third annual Blood and Marrow Transplant Clinical Trials Network (BMT CTN) Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling was held on November 29, 2018, at the American Society of Hematology (ASH) annual meeting. This workshop featured the latest research focused on minimal residual disease (MRD) assessment and immune profiling (IP) in myeloma as well as discussion of the statistical and regulatory issues intrinsic to the development of MRD as a surrogate endpoint. In this report, we provide a summary of the workshop and focus on the integration of MRD and IP assessment into trial design and clinical practice. [ABSTRACT FROM AUTHOR]

Published

2020

26. Summary of the Second Annual BMT CTN Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling.

Author

Holstein, Sarah A., Ye, J Christine, Howard, Alan, Bhutani, Manisha, Gormley, Nicole, Hahn, Theresa, Hillengass, Jens, Krishnan, Amrita, Landgren, C. Ola, Munshi, Nikhil C., Oliva, Stefania, Owen, Roger G., Pasquini, Marcelo C., Puig, Noemi, Weinhold, Niels, Weisel, Katja, and McCarthy, Philip L.

Subjects

*IMMUNOLOGIC diseases, *TRIAL practice, *STEM cell transplantation, *LONGITUDINAL method, *CLINICAL trials

Abstract

Highlights • Summary from the second annual BMT CTN Myeloma Intergroup minimal residual disease (MRD)/immune profiling (IP) workshop. • MRD is currently considered a prognostic biomarker from a regulatory perspective. • Additional prospective studies are required to develop MRD as a surrogate endpoint. • Standardization of immunophenotyping/IP studies is needed. Abstract The second annual Blood and Marrow Transplant Clinical Trials Network (BMT CTN) Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling was convened on December 7, 2017, at the American Society of Hematology (ASH) meeting. During this workshop, investigators from around the world presented their latest research involving assessment of minimal residual disease (MRD) and immune profiling (IP) in myeloma. This document summarizes the workshop presentations as well as relevant ASH abstracts and focuses on the regulatory issues involved in the integration of MRD and IP assessment in clinical trial design and practice. [ABSTRACT FROM AUTHOR]

Published

2019

27. Therapeutic vulnerability of multiple myeloma to MIR17PTi, a first-in-class inhibitor of pri-miR-17-92.

Author

Morelli, Eugenio, Biamonte, Lavinia, Federico, Cinzia, Amodio, Nicola, Di Martino, Maria Teresa, Cantafio, Maria Eugenia Gallo, Manzoni, Martina, Scionti, Francesca, Samur, Mehmet Kemal, Gullà, Annamaria, Stamato, Maria Angelica, Pitari, Maria Rita, Caracciolo, Daniele, Sesti, Settimio, Frandsen, Niels M., Rossi, Marco, Neri, Antonino, Fulciniti, Mariateresa, Munshi, Nikhil C., and Tagliaferri, Pierosandro

Subjects

*MULTIPLE myeloma treatment, *MICRORNA, *ANTISENSE DNA, *OLIGONUCLEOTIDES, *APOPTOSIS

Abstract

The microRNA(miRNA) clustermiR-17-92 is oncogenic and represents a valuable therapeutic target in c-MYC (MYC)-driven malignancies. Here, we developed novel LNA gapmeR antisense oligonucleotides (ASOs) to induce ribonuclease H-mediated degradation of MIR17HG primary transcripts and consequently prevent biogenesis of miR-17-92 miRNAs (miR-17-92s). The leading LNA ASO, MIR17PTi, impaired proliferation of several cancer cell lines (n 5 48) established from both solid and hematologic tumors by on-target antisense activity, more effectively as compared with miR-17-92 inhibitors. By focusing on multiple myeloma (MM), we found that MIR17PTi triggers apoptosis via impairment of homeostatic MYC/miR-17-92 feed-forward loops (FFLs) in patient-derivedMMcells and inducesMYC-dependent synthetic lethality. We show that alteration of a BIM-centered FFL is instrumental for MIR17PTi to induce cytotoxicity in MM cells. MIR17PTi exerts strong in vivo antitumor activity in nonobese diabetic severe combined immunodeficient mice bearing clinically relevant models of MM, with advantageous safety and pharmacokinetic profiles in nonhuman primates. Altogether, MIR17PTi is a novel pharmacological tool to be tested in early-phase clinical trials against MM and other MYC-driven malignancies. [ABSTRACT FROM AUTHOR]

Published

2018

28. A phase 2 study of modified lenalidomide, bortezomib and dexamethasone in transplant‐ineligible multiple myeloma.

Author

O'Donnell, Elizabeth K., Laubach, Jacob P., Yee, Andrew J., Chen, Tianqi, Huff, Carol Ann, Basile, Frank G., Wade, Philip M., Paba‐Prada, Claudia E., Ghobrial, Irene M., Schlossman, Robert L., Burke, Jill N., Harrington, Cynthia C., Lively, Kathleen J., Lyons, Hannah F., Munshi, Nikhil C., Anderson, Kenneth C., Trippa, Lorenzo, Richardson, Paul G., and Raje, Noopur S.

Subjects

*MULTIPLE myeloma, *CANCER chemotherapy, *BORTEZOMIB, *DEXAMETHASONE, *DRUG therapy

Abstract

Abstract: We sought a regimen that incorporates optimal novel agents and balances efficacy with toxicity in transplant‐ineligible multiple myeloma (MM) patients. Our study evaluated modified lenalidomide‐bortezomib‐dexamethasone (RVD lite) in this population and was administered over a 35‐day cycle. Lenalidomide 15 mg was given orally on days 1–21; bortezomib 1·3 mg/m2 weekly subcutaneously on days 1, 8, 15 and 22; and dexamethasone 20 mg orally was given on the day of and day after bortezomib for 9 cycles followed by 6 cycles of consolidation with lenalidomide and bortezomib. The primary objective was to evaluate the overall response rate (ORR); secondary objectives included safety, progression‐free survival (PFS) and overall survival (OS). Fifty‐three eligible patients were screened between April 2013 and May 2015; 50 received at least one dose of therapy. Median age at study entry was 73 years (range 65–91). The ORR was 86% and 66% of patients achieved a very good partial response or better. Median PFS was 35·1 months (95% confidence interval 30·9–not reached) and median OS was not reached at a median follow‐up of 30 months. Peripheral neuropathy was reported in 31 (62%) patients with only 1 patient experiencing grade 3 symptoms. RVD lite is a well‐tolerated and highly effective regimen, with robust PFS and OS, in the transplant‐ineligible MM population. [ABSTRACT FROM AUTHOR]

Published

2018

29. BMT CTN Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling: Summary and Recommendations from the Organizing Committee.

Author

Holstein, Sarah A., Avet-Loiseau, Hervé, Hahn, Theresa, Ho, Christine M., Lohr, Jens G., Munshi, Nikhil C., Paiva, Bruno, Pasquini, Marcelo C., Jr.Tario, Joseph D., Usmani, Saad Z., Wallace, Paul K., Weisel, Katja, and McCarthy, Philip L.

Subjects

*BONE marrow transplantation, *BLOOD transfusion, *HEMATOLOGY, *CLINICAL trials, *IMMUNITY, *MEDICAL societies

Abstract

The Blood and Marrow Transplant Clinical Trials Network Myeloma Intergroup Workshop on Minimal Residual Disease and Immune Profiling was convened on December 1, 2016 at the American Society of Hematology meeting to discuss the emerging data and technologies for minimal residual disease assessment and immune profiling in myeloma. Particular emphasis was placed on developing strategies to incorporate these techniques into clinical trial design. This document reviews the literature, summarizes the topics discussed in the workshop, and provides recommendations for integration of these techniques into future clinical trial design. [ABSTRACT FROM AUTHOR]

Published

2018

30. Recent common human Coronavirus infection protects against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection: A Veterans Affairs cohort study.

Author

Fillmore, Nathanael R., Szalat, Raphael E., La, Jennifer, Branch-Elliman, Westyn, Monach, Paul A., Vinh Nguyen, Samur, Mehmet K., Brophy, Mary T., Nhan V. Do, and Munshi, Nikhil C.

Subjects

*SARS-CoV-2, *COVID-19, *FRAIL elderly

Published

2022

31. Next-generation sequencing of a family with a high penetrance of monoclonal gammopathies for the identification of candidate risk alleles.

Author

Bolli, Niccolo, Barcella, Matteo, Salvi, Erika, D'Avila, Francesca, Vendramin, Antonio, De Philippis, Chiara, Munshi, Nikhil C., Avet‐Loiseau, Herve, Campbell, Peter J., Mussetti, Alberto, Carniti, Cristiana, Maura, Francesco, Barlassina, Cristina, Corradini, Paolo, and Montefusco, Vittorio

Subjects

*MONOCLONAL gammopathies, *MULTIPLE myeloma, *FAMILIAL diseases, *GENETIC mutation, *PLASMA cell diseases, *SINGLE nucleotide polymorphisms, *GENETICS, *DIAGNOSIS, *DISEASE risk factors, *ALLELES, *FAMILIES, *GENEALOGY, *GENETIC polymorphisms, *GENETIC techniques, *PARAPROTEINEMIA, *PHENOTYPES, *RELATIVE medical risk, *SEQUENCE analysis

Abstract

Background: The authors describe a family with a high penetrance of plasma cell dyscrasias, suggesting inheritance of an autosomal dominant risk allele.Methods: The authors performed whole-exome sequencing and reported on a combined approach aimed at the identification of causative variants and risk loci, using the wealth of data provided by this approach.Results: The authors identified gene mutations and single-nucleotide polymorphisms of potential significance, and pinpointed a known risk locus for myeloma as a potential area of transmissible risk in the family.Conclusions: To the authors' knowledge, the current study is the first to provide a whole-exome sequencing approach to such cases, and a framework analysis that could be applied to further understanding of the inherited risk of developing plasma cell dyscrasias. Cancer 2017;123:3701-3708. © 2017 American Cancer Society. [ABSTRACT FROM AUTHOR]

Published

2017

32. p53-related protein kinase confers poor prognosis and represents a novel therapeutic target in multiple myeloma.

Author

Teru Hideshima, Cottini, Francesca, Yoshihisa Nozawa, Hyuk-Soo Seo, Hiroto Ohguchi, Samur, Mehmet K., Cirstea, Diana, Naoya Mimura, Yoshikazu Iwasawa, Richardson, Paul G., Munshi, Nikhil C., Chauhan, Dharminder, Massefski, Walter, Teruhiro Utsugi, Dhe-Paganon, Sirano, and Anderson, Kenneth C.

Subjects

*P53 protein, *PROTEIN kinases, *MULTIPLE myeloma, *PHOSPHORYLATION, *IMMUNOLOGICAL adjuvants, *PROGNOSIS

Abstract

p53-related protein kinase (TP53RK, also known as PRPK) is an upstream kinase that phosphorylates (serine residue Ser15) and mediates p53 activity. Here we show that TP53RK confers poor prognosis in multiple myeloma (MM) patients, and, conversely, that TP53RK knockdown inhibits p53 phosphorylation and triggers MM cell apoptosis, associated with downregulation of c-Myc and E2F-1-mediated upregulation of proapoptotic Bim. We further demonstrate that TP53RK downregulation also triggers growth inhibition in p53-deficient and p53-mutant MM cell lines and identify novel downstream targets of TP53RK including ribonucleotide reductase-1, telomerase reverse transcriptase, and cyclin-dependent kinase inhibitor 2C. Our previous studies showed that immunomodulatory drugs (IMiDs) downregulate p21 and trigger apoptosis in wild-typep53 MM.1S cells, Importantly, we demonstrate by pull-down, nuclear magnetic resonance spectroscopy, differential scanning fluorimetry, and isothermal titration calorimetry that IMiDs bind and inhibit TP53RK, with biologic sequelae similar to TP53RK knockdown. Our studies therefore demonstrate that either genetic or pharmacological inhibition of TP53RK triggers MM cell apoptosis via both p53-Myc axis-dependent and axis-independent pathways, validating TP53RK as a novel therapeutic target in patients with poor-prognosis MM. [ABSTRACT FROM AUTHOR]

Published

2017

33. p53-related protein kinase confers poor prognosis and represents a novel therapeutic target in multiple myeloma.

Author

Hideshima, Teru, Cottini, Francesca, Yoshihisa Nozawa, Hyuk-Soo Seo, Hiroto Ohguchi, Samur, Mehmet K., Cirstea, Diana, Naoya Mimura, Yoshikazu Iwasawa, Richardson, Paul G., Munshi, Nikhil C., Chauhan, Dharminder, Massefski, Walter, Teruhiro Utsugi, Dhe-Paganon, Sirano, and Anderson, Kenneth C.

Subjects

*PHOSPHOTRANSFERASES, *PLASMACYTOMA, *PARAPROTEINEMIA, *MULTIPLE myeloma, *MONOCLONAL gammopathies

Abstract

p53-related protein kinase (TP53RK, also known as PRPK) is an upstream kinase that phosphorylates (serine residue Ser15) and mediates p53 activity. Here we show that TP53RK confers poor prognosis in multiple myeloma (MM) patients, and, conversely, that TP53RK knockdown inhibits p53 phosphorylation and triggers MM cell apoptosis, associated with downregulation of c-Myc and E2F-1-mediated upregulation of pro-apoptotic Bim. We further demonstrate that TP53RK downregulation also triggers growth inhibition in p53-deficient and p53-mutant MM cell lines and identify novel downstream targets of TP53RK including ribonucleotide reductase-1, telomerase reverse transcrip-tase, and cyclin-dependent kinase inhibitor 2C. Our previous studies showed that immunomodulatory drugs (IMiDs) downregulate p21 and trigger apoptosis in wild-type-p53 MM. 1S cells, Importantly, we demonstrate by pull-down, nuclear magnetic resonance spectroscopy, differential scanning f luorimetry, and isothermal titration calorimetry that IMiDs bind and inhibit TP53RK, with biologic sequelae similar to TP53RK knockdown. Our studies therefore demonstrate that either genetic or pharmacological inhibition of TP53RK triggers MM cell apoptosis via both p53-Myc axis-dependent and axis-independent pathways, validating TP53RK as a novel therapeutic target in patients with poor-prognosis MM. [ABSTRACT FROM AUTHOR]

Published

2017

34. Analysis of patient-reported experiences up to 2 years after receiving idecabtagene vicleucel (ide-cel, bb2121) for relapsed or refractory multiple myeloma: Longitudinal findings from the phase 2 KarMMa trial.

Author

Delforge, Michel, Otero, Paula Rodríguez, Shah, Nina, Moshkovich, Olga, Braverman, Julia, Dhanda, Devender S., Lanar, Sally, Devlen, Jennifer, Miera, Matthew, Gerould, Heather, Campbell, Timothy B., and Munshi, Nikhil C.

Subjects

*MULTIPLE myeloma, *PATIENTS' attitudes, *PATIENT experience, *CHIMERIC antigen receptors, *QUALITY of life

Abstract

To understand the long-term experience of patients receiving ide-cel chimeric antigen receptor T (CAR T) cell therapy for relapsed or refractory multiple myeloma in the pivotal phase 2 KarMMa trial. This qualitative study analyzed semi-structured patient interviews 6–24 months after ide-cel infusion. Thematic analysis with quantitative and longitudinal analyses explored patient perceptions of ide-cel treatment experience, advantages and disadvantages, and long-term health-related quality of life impact. Patient journeys were developed from narrative analysis of perceived treatment benefits with known remission length. Interviews with 45 patients 6–24 months postinfusion were analyzed; all reported ≥ 1 ide-cel treatment advantage, most often related to efficacy (n = 42/45, 93%), few or no side effects (n = 35/45, 78%), and avoidance of other treatments (n = 34/45, 76%). Patients generally reported 6-month improvements in physical health, functioning, emotional well-being, social life, and outlook on the future; these improvements mostly remained "stable" through 18 and 24 months. The most common patient journeys comprised physical, functioning, or emotional benefit with remission < 2 years. Longitudinal analysis of patient experiences showed sustained benefits and preference for ide-cel up to 24 months after treatment. Trial Registration Number and Date: NCT03361748. December 5, 2017. [Display omitted] • Patients preferred ide-cel to other treatments for efficacy and side effect profile. • Despite impactful side effects, patients still considered ide-cel advantageous. • Quality-of-life improved 6 months after treatment and stabilized through 24 months. • Patients would repeat their ide-cel treatment and recommend ide-cel to others. [ABSTRACT FROM AUTHOR]

Published

2023

35. Osteoclasts promote immune suppressive microenvironment in multiple myeloma: therapeutic implication.

Author

Gang An, Acharya, Chirag, Xiaoyan Feng, Wen, Kenneth, Zhong, Mike, Li Zhang, Munshi, Nikhil C., Lugui Qiu, Yu-Tzu Tai, and Anderson, Kenneth C.

Subjects

*OSTEOCLASTS, *MYELOMA proteins, *BONE marrow, *CELL proliferation, *CELL-mediated cytotoxicity

Abstract

The number and activity of osteoclasts (OCs) are strongly enhanced by myeloma cells, leading to significant bone lesions in patients with multiple myeloma (MM). Mechanisms remain elusive as to whether myeloma-supporting OCs also induce suppressive immune bone marrow (BM) microenvironment. Here, we first show that OCs significantly protect MM cells against T-cell–mediated cytotoxicity via direct inhibition of proliferating CD4+ and CD8+ T cells. The immune checkpoint molecules programmed death ligand 1 (PD-L1), Galectin-9, herpesvirus entry mediator (HVEM), and CD200, as well as T-cell metabolism regulators indoleamine 2, 3-dioxygenase (IDO), and CD38 are significantly upregulated during osteoclastogenesis. Importantly, the levels of these molecules, except CD38, are higher in OCs than in MM cells. Anti–PD-L1 monoclonal antibody (mAb) and IDO inhibitor partly overcome OC-inhibited T-cell responses against MM cells, confirming their roles in OC-suppressed MM cell lysis by cytotoxic T cells. In addition, Galectin-9 and a proliferation-induced ligand (APRIL), secreted by OCs, are significantly upregulated during osteoclastogenesis. Galectin-9 specifically induces apoptosis of T cells while sparing monocytes and MM cells. APRIL induces PD-L1 expression in MM cells, providing additional immune inhibition by OCs. Moreover, CD38 is significantly upregulated during osteoclastogenesis. When targeted by an anti-CD38 mAb, suppressive T-cell function by OCs is alleviated, associated with downregulation of HVEM and IDO. Taken together, these results define the expression of multiple immune proteins and cytokines in OCs essential for suppressive MM BM milieu. These results further support the combination of targeting these molecules to improve anti-MM immunity. [ABSTRACT FROM AUTHOR]

Published

2016

36. DNA repair of myeloma plasma cells correlates with clinical outcome: the effect of the nonhomologous end-joining inhibitor SCR7.

Author

Gkotzamanidou, Maria, Terpos, Evangelos, Bamia, Christina, Munshi, Nikhil C., Dimopoulos, Meletios A., and Souliotis, Vassilis L.

Subjects

*DNA repair, *BIOCHEMICAL genetics, *PLASMA cells, *MYELOMA proteins, *APOPTOSIS

Abstract

DNArepair activity ofmalignant cells seems to influencetherapeuticoutcomeandpatients' survival. Herein, we investigated the mechanistic basis for the link between DNA repair efficiency and response to antimyeloma therapy. Nucleotide excision repair (NER), interstrand cross-links repair (ICL/R), double-strand breaks repair (DSB/R), and chromatin structure were evaluated in multiple myeloma (MM) cell lines (melphalan-sensitive RPMI8226; melphalan-resistant LR5) and bone marrow plasma cells (BMPCs) from MM patients who responded (n = 17) or did not respond (n = 9) to subsequent melphalan therapy. The effect of DSB/R inhibition was also evaluated. Responders' BMPCs showed slower rates of NER and DSB/R (P < .0022), similar rates of ICL/R, and more condensed chromatin structure compared with nonresponders. Moreover, apoptosis rates of BMPCs were inversely correlated with individual DNA repair efficiency and were higher in responders' cells compared with those of nonresponders (P = .0011). Similarly, RPMI8226 cells showed slower rates of NER and DSB/R, comparable rates of ICL/R, more condensed chromatin structure, and higher sensitivity than LR5 cells. Interestingly, cotreatment of BMPCs or cell lines with DSB/R inhibitors significantly reduced the rates ofDSB/R and increasedmelphalan sensitivity of the cells, with the nonhomologous end-joining inhibitor SCR7 showing the strongest effect. Together, responders' BMPCs are characterized by lower efficiencies of NER and DSB/R mechanisms, resulting in higher accumulation of the extremely cytotoxic ICLs andDSBs lesions,which in turn triggers the induction of the apoptotic pathway. Moreover, the enhancement of melphalan cytotoxicity by DSB/R inhibition offers a promising strategy toward improvement of existing antimyeloma regimens. [ABSTRACT FROM AUTHOR]

Published

2016

37. A clinically relevant in vivo zebrafish model of human multiple myeloma to study preclinical therapeutic efficacy.

Author

Jianhong Lin, Weihong Zhang, Jian-Jun Zhao, Kwart, Ariel H., Chun Yang, Dongdong Ma, Xiubao Ren, Yu-Tzu Tai, Anderson, Kenneth C., Handin, Robert I., and Munshi, Nikhil C.

Subjects

*ZEBRA danio, *MULTIPLE myeloma, *XENOGRAFTS, *CELL lines, *CD134 antigen, *PATIENTS

Abstract

Patient-derived multiple myeloma (MM) cells are difficult to establish in culture or propagate in vivo in murine model. Here, we describe a zebrafish xenograft model that permits rapid, reliable growth of human MM cells injected into the perivitelline space of albino zebrafish (Casper) embryos 48 hours postfertilization. MM1S and MM1R MM cell lines and primary CD138+ MM cells were stained with CM-Dil red fluorescent dye and suspended in Matrigel prior to their injection. The cells grew at the site of injection and disseminated throughout the developing embryos and larvae. Tumor size was quantified by fluorescent microscopy, and cell fate was followed for 4 days. All of the cell line xenografts showed responses similar to those previously observed with in vitro assays. CD138+ plasma cell xenografts derived from MM patients also grew and were inhibited by the same drugs patients had responded to clinically. Using this technique, we can assess drug sensitivity or resistance with a small number of MM cells in a short period. This raises the possibility that one might be able to assess drug sensitivity in real time with readily obtainable clinical samples. [ABSTRACT FROM AUTHOR]

Published

2016

38. Multicentric plasma cell variant of Castleman's disease with cutaneous involvement.

Author

Klein, Walter M., Rencic, Adrienne, Munshi, Nikhil C., and Nousari, Carlos H.

Subjects

*LYMPHOPROLIFERATIVE disorders, *B cells, *IMMUNOGLOBULINS, *PARANEOPLASTIC syndromes, *HEMOLYTIC anemia, *SKIN diseases

Abstract

Castleman's disease (CD) is a rare low-grade B-cell lymphoproliferative disorder that can be associated with a variety of antibody-mediated paraneoplastic syndromes. The disease is classified clinically by two forms and three histologic variants. We describe the clinical and pathological features of a 44-year-old woman who presented with an autoimmune hemolytic anemia, thrombocytosis, polyclonal gammopathy, axillary lymphadenopathy, hepatosplenomegaly, and several erythematous and violaceous nodules and plaques without scaling involving the trunk and extremities. Histologic examination of the skin lesions revealed a deep dermal and subcutaneous nodular mononuclear infiltrate composed primarily of polyclonal plasmacytoid cells without atypia and an increased vascular proliferation. Additional studies including a bone marrow and lymph node biopsy, serum and urine protein electrophoresis, and computed tomography scans supported the diagnosis of multicentric plasma cell variant of CD with an associated autoimmune paraneoplastic hemolytic anemia. Cutaneous involvement in CD is part of the multicentric nature and should be considered in the differential diagnosis of a polyclonal plasma cell-rich lymphoproliferative disorder associated with paraneoplastic autoimmune disease. Klein WM, Rencic A, Munshi NC, Nousari CH. Multicentric plasma cell variant of Castleman's disease with cutaneous involvement. [ABSTRACT FROM AUTHOR]

Published

2004

39. Targeting the miR-221--222/PUMA/BAK/BAX Pathway Abrogates Dexamethasone Resistance in Multiple Myeloma.

Author

Jian-Jun Zhao, Zhang-Bo Chu, Yu Hu, Jianhong Lin, Zhongqiu Wang, Meng Jiang, Ming Chen, Xujun Wang, Yue Kang, Yangsheng Zhou, Triona Ni Chonghaile, Johncilla, Melanie E., Yu-Tzu Tai, Jin Q. Cheng, Letai, Antony, Munshi, Nikhil C., Anderson, Kenneth C., and Carrasco, Ruben D.

Subjects

*MICRORNA, *GENE targeting, *MULTIPLE myeloma, *DEXAMETHASONE, *MULTIPLE myeloma treatment, *DRUG resistance, *GENE expression, *CANCER invasiveness, *GENETICS

Abstract

Despite recent therapeutic advances that have doubled the median survival time of patients with multiple myeloma, intratumor genetic heterogeneity contributes to disease progression and emergence of drug resistance. miRNAs are noncoding small RNAs that play important roles in the regulation of gene expression and have been implicated in cancer progression and drug resistance. We investigated the role of the miR-221--222 family in dexamethasone-induced drug resistance in multiple myeloma using the isogenic cell lines MM1R and MM1S, which represent models of resistance and sensitivity, respectively. Analysis of array comparative genome hybridization data revealed gain of chromosome X regions at band p11.3, wherein the miR-221--222 resides, in resistant MM1R cells but not in sensitive MM1S cells. DNA copy number gains in MM1R cells were associated with increased miR-221--222 expression and downregulation of p53-upregulated modulator of apoptosis (PUMA) as a likely proapoptotic target. We con?rmed PUMA mRNA as a direct target of miR-221--222 in MM1S and MM1R cells by both gain-of-function and loss-of-function studies. In addition, miR-221--222 treatment rendered MM1S cells resistant to dexamethasone, whereas antimiR-221--222 partially restored the dexamethasone sensitivity of MM1R cells. These studies have uncovered a role for miR-221-- 222 in multiple myeloma drug resistance and suggest a potential therapeutic role for inhibitors of miR-221--222 binding to PUMA mRNA as a means of overcoming dexamethasone resistance in patients. The clinical utility of this approach is predicated on the ability of antisense miR-221--222 to increase survival while reducing tumor burden and is strongly supported by the metastatic propensity of MM1R cells in preclinical mouse xenograft models of multiple myeloma. Moreover, our observation of increased levels of miR-221--222 with decreased PUMA expression in multiple myeloma cells from patients at relapse versus untreated controls suggests an even broader role for miR-221--222 in drug resistance and provides a rationale for the targeting of miR-221--222 as a means of improving patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2015

40. Development of extramedullary myeloma in the era of novel agents: no evidence of increased risk with lenalidomide-bortezomib combinations.

Author

Varga, Cindy, Xie, Wanling, Laubach, Jacob, Ghobrial, Irene M., O'Donnell, Elizabeth K., Weinstock, Matthew, Paba‐Prada, Claudia, Warren, Diane, Maglio, Michelle E., Schlossman, Robert, Munshi, Nikhil C., Raje, Noopur, Weller, Edie, Anderson, Kenneth C., Mitsiades, Constantine S., and Richardson, Paul G.

Subjects

*BORTEZOMIB, *PROTEASOME inhibitors, *MULTIPLE myeloma, *MULTIPLE myeloma diagnosis, *PLASMACYTOMA, *BIOPSY, *PATIENTS

Abstract

Proteasome inhibitors ( PI) and immunomodulatory agents ( IMIDs) have improved the overall survival (OS) of patients with multiple myeloma ( MM), but concerns have been raised about increased incidence of extramedullary disease ( EMD) after the combined use of PIs and IMIDs for upfront therapy. We evaluated whether the addition of lenalidomide to bortezomib-based front-line regimens precipitated earlier development of EMD. We reviewed the charts of 117 MM patients (median follow-up from diagnosis 6·1 years; range 0·1-10·2 years) enrolled in eight clinical trials of first-line treatment with bortezomib-based regimens, with or without lenalidomide. We assessed development of EMD as extraosseous (distant from bone) or osseous (originating from bone) plasmacytomas. The primary endpoint was time from diagnosis until development of EMD, based on imaging, biopsy and/or physical examination. Any form of EMD at progression was observed in 40 (34·2%) patients, including 21 (18%) osseous, 8 (7%) extraosseous and 11 (9%) both osseous and extraosseous. Median OS was 0·9 years (range 0·1-4·8 years) after extraosseous EMD development. Sensitivity analyses with follow-up times truncated at 5 years detected no statistically significant difference in rates of any EMD form between the two groups ( P > 0·2 for each comparison). Therefore, we observed no evidence that bortezomib-lenalidomide-based front-line therapy precipitates earlier EMD. [ABSTRACT FROM AUTHOR]

Published

2015

41. The Cyclophilin A-CD147 complex promotes the proliferation and homing of multiple myeloma cells.

Author

Zhu, Di, Wang, Zhongqiu, Zhao, Jian-Jun, Calimeri, Teresa, Meng, Jiang, Hideshima, Teru, Fulciniti, Mariateresa, Kang, Yue, Ficarro, Scott B, Tai, Yu-Tzu, Hunter, Zachary, McMilin, Douglas, Tong, Haoxuan, Mitsiades, Constantine S, Wu, Catherine J, Treon, Steven P, Dorfman, David M, Pinkus, Geraldine, Munshi, Nikhil C, and Tassone, Pierfrancesco

Subjects

*MULTIPLE myeloma, *CYCLOPHILINS, *CD antigens, *CELL proliferation, *B cell lymphoma, *LYMPHOCYTIC leukemia, *BONE marrow, *CATENINS

Abstract

B cell malignancies frequently colonize the bone marrow. The mechanisms responsible for this preferential homing are incompletely understood. Here we studied multiple myeloma (MM) as a model of a terminally differentiated B cell malignancy that selectively colonizes the bone marrow. We found that extracellular CyPA (eCyPA), secreted by bone marrow endothelial cells (BMECs), promoted the colonization and proliferation of MM cells in an in vivo scaffold system via binding to its receptor, CD147, on MM cells. The expression and secretion of eCyPA by BMECs was enhanced by BCL9, a Wnt-β-catenin transcriptional coactivator that is selectively expressed by these cells. eCyPA levels were higher in bone marrow serum than in peripheral blood in individuals with MM, and eCyPA-CD147 blockade suppressed MM colonization and tumor growth in the in vivo scaffold system. eCyPA also promoted the migration of chronic lymphocytic leukemia and lymphoplasmacytic lymphoma cells, two other B cell malignancies that colonize the bone marrow and express CD147. These findings suggest that eCyPA-CD147 signaling promotes the bone marrow homing of B cell malignancies and offer a compelling rationale for exploring this axis as a therapeutic target for these malignancies. [ABSTRACT FROM AUTHOR]

Published

2015

42. A Phase II trial of weekly bortezomib and dexamethasone in veterans with newly diagnosed multiple myeloma not eligible for or who deferred autologous stem cell transplantation.

Author

Girnius, Saulius K., Lee, Saem, Kambhampati, Suman, Rose, Michal G., Mohiuddin, Abid, Houranieh, Antoun, Zimelman, Abraham, Grady, Terrence, Mehta, Paulette, Behler, Caroline, Hayes, Teresa G., Efebera, Yvonne A., Prabhala, Rao H., Han, Andrew, Yellapragada, Sarvari V., Klein, Catherine E., Roodman, Garson D., Lichtenstein, Alan, and Munshi, Nikhil C.

Subjects

*BORTEZOMIB, *DEXAMETHASONE, *MEDICAL care of veterans, *STEM cell transplantation, *MULTIPLE myeloma treatment, *PERIPHERAL neuropathy, *THERAPEUTICS

Abstract

Once-weekly administration of bortezomib has reduced bortezomib-induced peripheral neuropathy without affecting response rates, but this has only been demonstrated prospectively in three- and four- drug combinations. We report a phase II trial of alternate dosing and schedule of bortezomib and dexamethasone in newly diagnosed multiple myeloma patients who are not eligible for or refused autologous stem cell transplantation. Bortezomib 1·6 mg/m2 intravenously was given once-weekly for six cycles, together with dexamethasone 40 mg on the day of and day after bortezomib. Fifty patients were enrolled; 58% did not require any dose modification. The majority of patients had multiple co-morbidities, including cardiovascular (76%) and renal insufficiency (54%), and the median number of medications prior to enrollment was 13. Of all evaluable patients, the overall response rate was 79% and at least 45% had at least a very good partial response. The median time to first response was 1·3 months (range, 0·25-2·4 months). The progression-free and overall survivals were 8 months and 46·5 months, respectively. Twenty-four percent developed worsening neuropathy. We conclude that alternate dosing and scheduling of bortezomib and dexamethasone is both safe and effective for management of newly diagnosed multiple myeloma in frail patients. (ClinicalTrials.gov number, NCT01090921). [ABSTRACT FROM AUTHOR]

Published

2015

43. Patient experience before and after treatment with idecabtagene vicleucel (ide-cel, bb2121): qualitative analysis of patient interviews in the KarMMa trial.

Author

Shah, Nina, Delforge, Michel, San-Miguel, Jesus, Moshkovich, Olga, Braverman, Julia, Dhanda, Devender S., Lanar, Sally, Miera, Matthew, Williams, Agnes, Murphy, Ryan, Devlen, Jennifer, Hege, Kristen, Campbell, Timothy B., and Munshi, Nikhil C.

Subjects

*PATIENTS' attitudes, *MEDICAL history taking, *CHIMERIC antigen receptors, *MULTIPLE myeloma

Abstract

To understand the experience of patients with relapsed and refractory multiple myeloma (RRMM) receiving idecabtagene vicleucel (ide-cel), a B-cell maturation antigen-directed chimeric antigen receptor T cell therapy, in the pivotal, phase 2 KarMMa trial. Optional semi-structured interviews before leukapheresis (pre-treatment) captured expectations and after ide-cel infusion (1, 2, and 3 months post-treatment), assessed treatment experience, ide-cel advantages/disadvantages, and health and well-being. In a mixed-method analysis, treatment experiences were categorized by clinical response status, health and well-being, and self-reported recovery after infusion. Pre-treatment interviews indicated unmet treatment needs. In post-treatment interviews, most patients reported the positives of ide-cel outweighed negatives (69%, n = 27/39). Most common advantages of ide-cel were efficacy (18–64%), favorable side-effect profile (46–68%), and recovery time (13–18%); most common disadvantages were related to side effects (13–20%). When analyzed by clinical response, patients most often had stringent complete or very good partial response and improved health and well-being with mild or severe recovery from the infusion (27/58, 47%). Most patients with minimal clinical response reported mild infusion recovery (5/6, 83%). Patient interviews before ide-cel treatment showed unmet needs in triple-class exposed RRMM. Post-treatment experiences generally favored ide-cel versus previously received treatments. [Display omitted] • Patient interviews before ide-cel treatment showed substantial unmet needs in RRMM. • Patients expressed prominent hopes for remission and improved health and well-being. • Patients reported positive impressions of treatment with ide-cel. • Advantages of treatment with ide-cel substantially outweighed disadvantages. • Patient journeys assessed patients' experiences in the context of several factors. [ABSTRACT FROM AUTHOR]

Published

2022

44. Differential and limited expression of mutant alleles in multiple myeloma.

Author

Rashid, Naim U., Sperling, Adam S., Bolli, Niccolo, Wedge, David C., Van Loo, Peter, Yu-Tzu Tai, Shammas, Masood A., Fulciniti, Mariateresa, Samur, Mehmet K., Richardson, Paul G., Magrangeas, Florence, Minvielle, Stephane, Futreal, P. Andrew, Anderson, Kenneth C., Avet-Loiseau, Herve, Campbell, Peter J., Parmigiani, Giovanni, and Munshi, Nikhil C.

Subjects

*MULTIPLE myeloma, *PLASMACYTOMA, *ALLELES, *GENE expression, *B cell lymphoma

Abstract

Recent work has delineated mutational profiles in multiple myeloma and reported a median of 52 mutations per patient, as well as a set of commonly mutated genes across multiple patients. In this study, we have used deep sequencing of RNA from a subset of these patients to evaluate the proportion of expressed mutations. We find that the majority of previously identified mutations occur within genes with very low or no detectable expression. On average, 27% (range, 11% to 47%) of mutated alleles are found to be expressed, and among mutated genes that are expressed, there often is allele-specific expression where either the mutant or wild-type allele is suppressed. Even in the absence of an overall change in gene expression, the presence of differential allelic expression within malignant cells highlights the important contribution of RNA-sequencing in identifying clinically significant mutational changes relevant to our understanding of myeloma biology and also for therapeutic applications. [ABSTRACT FROM AUTHOR]

Published

2014

45. A Phase IB multicentre dose-determination study of BHQ880 in combination with anti-myeloma therapy and zoledronic acid in patients with relapsed or refractory multiple myeloma and prior skeletal-related events.

Author

Iyer, Swaminathan P., Beck, Joseph Taddeus, Stewart, A. Keith, Shah, Jatin, Kelly, Kevin R., Isaacs, Randi, Bilic, Sanela, Sen, Suman, and Munshi, Nikhil C.

Subjects

*MULTIPLE myeloma, *ZOLEDRONIC acid, *DRUG dosage, *OSTEOBLASTS, *ANTIGENS, *IMMUNOGLOBULIN G, *PATIENTS

Abstract

Dickkopf-1 ( DKK1), expressed by myeloma cells, suppresses osteoblast function and plays a key role in bone disease in multiple myeloma. BHQ880, a human neutralizing IgG1 anti- DKK1 monoclonal antibody, is being investigated for its impact on multiple myeloma-related bone disease and as an agent with potential anti-myeloma activity. The primary objectives of this Phase IB study were to determine the maximum tolerated dose ( MTD) of BHQ880 and to characterize the dose-limiting toxicity ( DLT) of escalating doses in combination with anti-myeloma therapy and zoledronic acid. Twenty-eight patients were enrolled and received BHQ880 at doses of 3-40 mg/kg. No DLTs were reported, therefore, the MTD was not determined. The recommended Phase II dose was declared as 10 mg/kg, based mainly on saturation data. There was a general trend towards increased bone mineral density ( BMD) observed over time; specific increases in spine BMD from Cycle 12 onwards irrespective of new skeletal-related events on study were observed, and increases in bone strength at the spine and hip were also demonstrated in some patients. BHQ880 in combination with zoledronic acid and anti-myeloma therapy was well tolerated and demonstrated potential clinical activity in patients with relapsed or refractory multiple myeloma. [ABSTRACT FROM AUTHOR]

Published

2014

46. Pyk2 promotes tumor progression in multiple myeloma.

Author

Yu Zhang, Moschetta, Michele, Huynh, Daisy, Yu-Tzu Tai, Yong Zhang, Wenjing Zhang, Mishima, Yuji, Ring, Jennifer E., Tam, Winnie F., Qunli Xu, Maiso, Patricia, Reagan, Michaela, Sahin, Ilyas, Sacco, Antonio, Manier, Salomon, Aljawai, Yosra, Glavey, Siobhan, Munshi, Nikhil C., Anderson, Kenneth C., and Pachter, Jonathan

Subjects

*PROTEIN-tyrosine kinases, *CANCER invasiveness, *PROLINE, *MULTIPLE myeloma, *CELL proliferation

Abstract

Proline-rich tyrosine kinase 2 (Pyk2) is a member of the focal adhesion kinase family that has been recently linked to tumor development. However, its role in modulating multiple myeloma (MM) biology and disease progression remains unexplored. We first demonstrated that patients with MM present with higher expression of Pyk2 compared with healthy individuals. By using loss-of-function approaches, we found that Pyk2 inhibition led to reduction of MM tumor growth in vivo as well as decreased cell proliferation, cellcycle progression, and adhesion ability in vitro. In turn, overexpression of Pyk2 promoted the malignant phenotype, substantiated by enhanced tumorgrowth and reduced survival. Mechanistically, inhibition of Pyk2 reduced activation of Wnt/β-catenin signaling by destabilizing β-catenin, leading to downregulation of c-Myc and Cyclin D1. Furthermore, treatment of MM cells with the FAK/Pyk2 inhibitor VS-4718 effectively inhibited MM cell growth both in vitro and in vivo. Collectively, our findings describe the tumor-promoting role of Pyk2 in MM, thus providing molecular evidence for a novel tyrosine kinase inhibitor as a new therapeutic option in MM. [ABSTRACT FROM AUTHOR]

Published

2014

47. Outcomes in patients with relapsed or refractory multiple myeloma in a phase I study of everolimus in combination with lenalidomide.

Author

Yee, Andrew J., Hari, Parameswaran, Marcheselli, Raffaella, Mahindra, Anuj K., Cirstea, Diana D., Scullen, Tyler A., Burke, Jill N., Rodig, Scott J., Hideshima, Teru, Laubach, Jacob P., Ghobrial, Irene M., Schlossman, Robert L., Munshi, Nikhil C., Anderson, Kenneth C., Weller, Edie A., Richardson, Paul G., and Raje, Noopur S.

Subjects

*HEALTH outcome assessment, *MULTIPLE myeloma treatment, *EVEROLIMUS, *THALIDOMIDE, *TOR proteins, *DOSE-response relationship in poisons, *THERAPEUTICS

Abstract

Everolimus, an oral mammalian target of rapamycin ( mTOR) inhibitor, has been studied in multiple myeloma (MM) but lacks significant single agent activity. Based on preclinical studies showing synergistic activity of mTOR inhibitors with lenalidomide, we studied the combination of lenalidomide and everolimus in relapsed or refractory MM in a phase I clinical trial. We assessed patient samples using gene expression, Western blotting and immunohistochemistry to probe the mTOR pathway. Twenty-six patients were evaluable for toxicity. Dose-limiting toxicities included grade 4 neutropenia and thrombocytopenia. The maximum tolerated dose was lenalidomide 15 mg and everolimus 5 mg for 21 d with a 7 d rest period. Grade 3/4 adverse events included thrombocytopenia (35%) and neutropenia (42%). The overall response rate was 65% (1 complete response + 4 partial response + 10 minimal response). The median progression-free survival was 5·5 months and median overall survival was 29·5 months. Biomarker data demonstrated downregulation of phosphorylated p70S6K. Gene expression profiling suggested activation of mTOR in responders versus non-responders. The combination of lenalidomide and everolimus was well tolerated with predictable toxicities and showed responses in a heavily pretreated population. When confirmed with larger patient numbers, this analysis may guide patient selection for future clinical trials of mTOR inhibition in MM. [ABSTRACT FROM AUTHOR]

Published

2014

48. Novel anti-B-cell maturation antigen antibody-drug conjugate (GSK2857916) selectively induces killing of multiple myeloma.

Author

Yu-Tzu Tai, Mayes, Patrick A., Acharya, Chirag, Zhong, Mike Y., Cea, Michele, Cagnetta, Antonia, Craigen, Jenny, Yates, John, Gliddon, Louise, Fieles, William, Bao Hoang, Tunstead, James, Christie, Amanda L., Kung, Andrew L., Richardson, Paul, Munshi, Nikhil C., and Anderson, Kenneth C.

Subjects

*B cells, *ANTIGENS, *MULTIPLE myeloma, *GROWTH factors, *APOPTOSIS, *LYSIS, *PHAGOCYTOSIS

Abstract

B-cell maturation antigen (BCMA), highly expressed on malignant plasma cells in human multiple myeloma (MM), has not been effectively targeted with therapeutic monoclonal antibodies. We here show that BCMA is universally expressed on the MM cell surface and determine specific anti-MM activity of J6M0-mcMMAF (GSK2857916), a novel humanized and afucosylated antagonistic anti-BCMA antibody-drug conjugate via a noncleavable linker. J6M0-mcMMAF specifically blocks cell growth via G2/M arrest and induces caspase 3-dependent apoptosis in MM cells, alone and in coculture with bone marrow stromal cells or various effector cells. It strongly inhibits colony formation by MM cells while sparing surrounding BCMA-negative normal cells. J6M0-mcMMAF significantly induces effector cell-mediated lysis against allogeneic or autologous patient MM cells, with increased potency and efficacy compared with the wild-type J6M0 without Fc enhancement. The antibody-dependent cell-mediated cytotoxicity and apoptotic activity of J6M0-mcMMAF is further enhanced by lenalidomide. Importantly, J6M0-mcMMAF rapidly eliminates myeloma cells in subcutaneous and disseminated mouse models, and mice remain tumor-free up to 3.5 months. Furthermore, J6M0-mcMMAF recruits macrophages and mediates antibody-dependent cellular phagocytosis of MM cells. Together, these results demonstrate that GSK2857916 has potent and selective anti-MM activities via multiple cytotoxic mechanisms, providing a promising next-generation immunotherapeutic in this cancer. [ABSTRACT FROM AUTHOR]

Published

2014

49. CCR6, the Sole Receptor for the Chemokine CCL20, Promotes Spontaneous Intestinal Tumorigenesis.

Author

Nandi, Bisweswar, Pai, Christine, Huang, Qin, Prabhala, Rao H., Munshi, Nikhil C., and Gold, Jason S.

Subjects

*CHEMOKINES, *NEOPLASTIC cell transformation, *INTESTINAL tumors, *COLON cancer, *LABORATORY mice, *CARCINOGENESIS

Abstract

Interactions between the inflammatory chemokine CCL20 and its receptor CCR6 have been associated with colorectal cancer growth and metastasis, however, a causal role for CCL20 signaling through CCR6 in promoting intestinal carcinogenesis has not been demonstrated in vivo. In this study, we aimed to determine the role of CCL20-CCR6 interactions in spontaneous intestinal tumorigenesis. CCR6-deficient mice were crossed with mice heterozygous for a mutation in the adenomatous polyposis coli (APC) gene (APCMIN/+ mice) to generate APCMIN/+ mice with CCR6 knocked out (CCR6KO-APCMIN/+ mice). CCR6KO-APCMIN/+ mice had diminished spontaneous intestinal tumorigenesis. CCR6KO-APCMIN/+ also had normal sized spleens as compared to the enlarged spleens found in APCMIN/+ mice. Decreased macrophage infiltration into intestinal adenomas and non-tumor epithelium was observed in CCR6KO-APCMIN/+ as compared to APCMIN/+ mice. CCL20 signaling through CCR6 caused increased production of CCL20 by colorectal cancer cell lines. Furthermore, CCL20 had a direct mitogenic effect on colorectal cancer cells. Thus, interactions between CCL20 and CCR6 promote intestinal carcinogenesis. Our results suggest that the intestinal tumorigenesis driven by CCL20-CCR6 interactions may be driven by macrophage recruitment into the intestine as well as proliferation of neoplastic epithelial cells. This interaction could be targeted for the treatment or prevention of malignancy. [ABSTRACT FROM AUTHOR]

Published

2014

50. MYD88-independent growth and survival effects of Sp1 transactivation in Waldenström macroglobulinemia.

Author

Fulciniti, Mariateresa, Amodio, Nicola, Lakshmi Bandi, Rajya, Munshi, Mansa, Guang Yang, Lian Xu, Hunter, Zachary, Tassone, Pierfrancesco, Anderson, Kenneth C., Treon, Steven P., and Munshi, Nikhil C.

Subjects

*WALDENSTROM'S macroglobulinemia, *TRANSCRIPTION factors, *PROTEIN-tyrosine kinases, *INTERLEUKIN-1 receptors, *TOLL-like receptors, *STAT proteins, *ONCOGENIC proteins, *CELL proliferation

Abstract

Sp1 transcription factor controls a pleiotropic group of genes and its aberrant activation has been reported in a number of malignancies, including multiple myeloma. In this study, we investigate and report its aberrant activation in Waldenström macroglobulinemia (WM). Both loss of and gain of Sp1 function studies have highlighted a potential oncogenic role of Sp1 in WM. We have further investigated the effect of a small molecule inhibitor, terameprocol (TMP), targeting Sp1 activity in WM. Treatment with TMP inhibited the growth and survival and impaired nuclear factor-κB and signal transducer and activator of transcription activity in WM cells. We next investigated and observed that TMP treatment induced further inhibition of WM cells in MYD88 knockdown WM cells. Moreover, we observed that Bruton's tyrosine kinase, a downstream target of MYD88 signaling pathway, is transcriptionally regulated by Sp1 in WM cells. The combined use of TMP with Bruton's tyrosine kinase or interleukin-1 receptor-associated kinase 1 and 4 inhibitors resulted in a significant and synergistic dose-dependent antiproliferative effect in MYD88-L265P--expressing WM cells. In summary, these results demonstrate Sp1 as an important transcription factor that regulates proliferation and survival of WM cells independent of MYD88 pathway activation, and provide preclinical rationale for clinical development of TMP in WM alone or in combination with inhibitors of MYD88 pathway. [ABSTRACT FROM AUTHOR]

Published

2014