Your search keyword '"B lymphoma"' showing total 7 results

1. Transcriptomic profiling of splenic B lymphomas spontaneously developed in B cell-specific TRAF3-deficient mice

Author

Ping Xie, Carissa R. Moore, Mavis R. Swerdel, and Ronald P. Hart

Subjects

MCC, TRAF3, B lymphoma, multiple myeloma, Genetics, QH426-470

Abstract

TRAF3, a critical regulator of B cell survival, was recently recognized as a tumor suppressor gene in B lymphocytes. Specific deletion of TRAF3 from B lymphocytes leads to spontaneous development of marginal zone lymphomas (MZL) or B1 lymphomas in mice. To identify novel oncogenes and tumor suppressive genes involved in malignant transformation of TRAF3-deficient B cells, we performed a microarray analysis to identify genes differentially expressed in TRAF3−/− mouse splenic B lymphomas. We have identified 160 up-regulated genes and 244 down-regulated genes in TRAF3−/−B lymphomas as compared to littermate control splenocytes. Here we describe the samples, quality control assessment, as well as the data analysis methods in detail for the transcriptomic profiling study. Data are archived at NIH GEO with accession number GSE48818.

Published

2014

2. Signaling mechanisms of bortezomib in TRAF3-deficient mouse B lymphoma and human multiple myeloma cells.

Author

Edwards, Shanique K.E., Han, Yeming, Liu, Yingying, Kreider, Benjamin Z., Liu, Yan, Grewal, Sukhdeep, Desai, Anand, Baron, Jacqueline, Moore, Carissa R., Luo, Chang, and Xie, Ping

Subjects

*BORTEZOMIB, *MULTIPLE myeloma treatment, *MULTIPLE myeloma, *CANCER cells, *TUMOR suppressor genes, *TUMOR necrosis factor receptors, *CELLULAR signal transduction, *PATIENTS, *THERAPEUTICS

Abstract

Bortezomib, a clinical drug for multiple myeloma (MM) and mantle cell lymphoma, exhibits complex mechanisms of action, which vary depending on the cancer type and the critical genetic alterations of each cancer. Here we investigated the signaling mechanisms of bortezomib in mouse B lymphoma and human MM cells deficient in a new tumor suppressor gene, TRAF3. We found that bortezomib consistently induced up-regulation of the cell cycle inhibitor p21(WAF1) and the pro-apoptotic protein Noxa as well as cleavage of the anti-apoptotic protein Mcl-1. Interestingly, bortezomib induced the activation of NF-κB1 and the accumulation of the oncoprotein c-Myc, but inhibited the activation of NF-κB2. Furthermore, we demonstrated that oridonin (an inhibitor of NF-κB1 and NF-κB2) or AD 198 (a drug targeting c-Myc) drastically potentiated the anti-cancer effects of bortezomib in TRAF3-deficient malignant B cells. Taken together, our findings increase the understanding of the mechanisms of action of bortezomib, which would aid the design of novel bortezomib-based combination therapies. Our results also provide a rationale for clinical evaluation of the combinations of bortezomib and oridonin (or other inhibitors of NF-κB1/2) or AD 198 (or other drugs targeting c-Myc) in the treatment of lymphoma and MM, especially in patients containing TRAF3 deletions or relevant mutations. [ABSTRACT FROM AUTHOR]

Published

2016

3. Mutated in colorectal cancer (MCC) is a novel oncogene in B lymphocytes.

Author

Edwards, Shanique, Baron, Jacqueline, Moore, Carissa, Yan Liu, Perlman, David, Hart, Ronald, and Ping Xie

Subjects

*LYMPHOMAS, *LYMPHOMA treatment, *MULTIPLE myeloma, *MONONUCLEAR leukocytes, *INCURABLE diseases, *B cell differentiation, *B cells, *PSYCHOLOGY, *GENETICS, *DISEASES

Abstract

Background Identification of novel genetic risk factors is imperative for a better understanding of B lymphomagenesis and for the development of novel therapeutic strategies. TRAF3, a critical regulator of B cell survival, was recently recognized as a tumor suppressor gene in B lymphocytes. The present study aimed to identify novel oncogenes involved in malignant transformation of TRAF3-deficient B cells. Methods We used microarray analysis to identify genes differentially expressed in TRAF3-/- mouse splenic B lymphomas. We employed lentiviral vector-mediated knockdown or overexpression to manipulate gene expression in human multiple myeloma (MM) cell lines. We analyzed cell apoptosis and proliferation using flow cytometry, and performed biochemical studies to investigate signaling mechanisms. To delineate protein-protein interactions, we applied affinity purification followed by mass spectrometry-based sequencing. Results We identified mutated in colorectal cancer (MCC) as a gene strikingly up-regulated in TRAF3-deficient mouse B lymphomas and human MM cell lines. Aberrant up-regulation of MCC also occurs in a variety of primary human B cell malignancies, including non-Hodgkin lymphoma (NHL) and MM. In contrast, MCC expression was not detected in normal or premalignant TRAF3-/- B cells even after treatment with B cell stimuli, suggesting that aberrant up-regulation of MCC is specifically associated with malignant transformation of B cells. In elucidating the functional roles of MCC in malignant B cells, we found that lentiviral shRNA vector-mediated knockdown of MCC induced apoptosis and inhibited proliferation in human MM cells. Experiments of knockdown and overexpression of MCC allowed us to identify several downstream targets of MCC in human MM cells, including phospho-ERK, c- Myc, p27, cyclin B1, Mcl-1, caspases 8 and 3. Furthermore, we identified 365 proteins (including 326 novel MCC-interactors) in the MCC interactome, among which PARP1 and PHB2 were two hubs of MCC signaling pathways in human MM cells. Conclusions Our results indicate that in sharp contrast to its tumor suppressive role in colorectal cancer, MCC functions as an oncogene in B cells. Our findings suggest that MCC may serve as a diagnostic marker and therapeutic target in B cell malignancies, including NHL and MM. [ABSTRACT FROM AUTHOR]

Published

2014

4. Expression and function of a novel isoform of Sox5 in malignant B cells.

Author

Edwards, Shanique K.E., Desai, Anand, Liu, Yan, Moore, Carissa R., and Xie, Ping

Subjects

*B cell lymphoma, *TRANSCRIPTION factors, *TUMOR suppressor proteins, *CELL cycle, *MULTIPLE myeloma, *GENETIC regulation

Abstract

Abstract: Using a mouse model with the tumor suppressor TRAF3 deleted from B cells, we identified Sox5 as a gene strikingly up-regulated in B lymphomas. Sox5 proteins were not detected in normal or premalignant TRAF3−/− B cells even after treatment with B cell stimuli. The Sox5 expressed in TRAF3−/− B lymphomas represents a novel isoform of Sox5, and was localized in the nucleus of malignant B cells. Overexpression of Sox5 inhibited cell cycle progression, and up-regulated the protein levels of p27 and β-catenin in human multiple myeloma cells. Together, our findings indicate that Sox5 regulates the proliferation of malignant B cells. [Copyright &y& Elsevier]

Published

2014

5. Transcriptomic profiling of splenic B lymphomas spontaneously developed in B cell-specific TRAF3-deficient mice

Author

Ronald P. Hart, Mavis R. Swerdel, Carissa R. Moore, and Ping Xie

Subjects

MCC, lcsh:QH426-470, Tumor suppressor gene, Microarray analysis techniques, Biology, Marginal zone, Biochemistry, 3. Good health, Malignant transformation, multiple myeloma, Transcriptome, lcsh:Genetics, medicine.anatomical_structure, TRAF3, Data in Brief, Immunology, B lymphoma, Genetics, medicine, Cancer research, Splenocyte, Molecular Medicine, Gene, B cell, Biotechnology

Abstract

TRAF3, a critical regulator of B cell survival, was recently recognized as a tumor suppressor gene in B lymphocytes. Specific deletion of TRAF3 from B lymphocytes leads to spontaneous development of marginal zone lymphomas (MZL) or B1 lymphomas in mice. To identify novel oncogenes and tumor suppressive genes involved in malignant transformation of TRAF3-deficient B cells, we performed a microarray analysis to identify genes differentially expressed in TRAF3−/− mouse splenic B lymphomas. We have identified 160 up-regulated genes and 244 down-regulated genes in TRAF3−/−B lymphomas as compared to littermate control splenocytes. Here we describe the samples, quality control assessment, as well as the data analysis methods in detail for the transcriptomic profiling study. Data are archived at NIH GEO with accession number GSE48818.

Published

2014

6. Targeting TRAF3 Downstream Signaling Pathways in B cell Neoplasms

Author

Ping Xie, Carissa R. Moore, and Shanique K.E. Edwards

Subjects

Cancer Research, Chronic lymphocytic leukemia, Cell, Context (language use), Article, 03 medical and health sciences, 0302 clinical medicine, AD 198, Multiple myeloma, immune system diseases, hemic and lymphatic diseases, B lymphoma, medicine, Splenic marginal zone lymphoma, B cell, 030304 developmental biology, MCC, 0303 health sciences, business.industry, medicine.disease, 3. Good health, Lymphoma, NF-κB2, medicine.anatomical_structure, TRAF3, Oncology, 030220 oncology & carcinogenesis, Immunology, Mantle cell lymphoma, Sox5, business

Abstract

B cell neoplasms comprise >50% of blood cancers. However, many types of B cell malignancies remain incurable. Identification and validation of novel genetic risk factors and oncogenic signaling pathways are imperative for the development of new therapeutic strategies. We and others recently identified TRAF3, a cytoplasmic adaptor protein, as a novel tumor suppressor in B lymphocytes. We found that TRAF3 inactivation results in prolonged survival of mature B cells, which eventually leads to spontaneous development of B lymphomas in mice. Corroborating our findings, TRAF3 deletions and inactivating mutations frequently occur in human B cell chronic lymphocytic leukemia, splenic marginal zone lymphoma, mantle cell lymphoma, multiple myeloma, Waldenström’s macroglobulinemia, and Hodgkin lymphoma. In this context, we have been investigating TRAF3 signaling mechanisms in B cells, and are developing new therapeutic strategies to target TRAF3 downstream signaling pathways in B cell neoplasms. Here we discuss our new translational data that demonstrate the therapeutic potential of targeting TRAF3 downstream signaling pathways in B lymphoma and multiple myeloma.

Published

2015

7. Mutated in colorectal cancer (MCC) is a novel oncogene in B lymphocytes

Author

Shanique K.E. Edwards, Ping Xie, Yan Liu, Jacqueline Baron, Ronald P. Hart, David H. Perlman, and Carissa R. Moore

Subjects

Cancer Research, Chromatin Immunoprecipitation, Tumor suppressor gene, Immunoblotting, PHB2, Apoptosis, Biology, Genes, MCC, PARP1, Malignant transformation, Mice, Tandem Mass Spectrometry, Multiple myeloma, Cell Line, Tumor, Prohibitins, medicine, B lymphoma, Animals, Humans, Immunoprecipitation, Molecular Biology, B cell, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Mice, Knockout, MCC, Gene knockdown, B-Lymphocytes, Oncogene, TNF Receptor-Associated Factor 3, Cell growth, Reverse Transcriptase Polymerase Chain Reaction, Lymphoma, Non-Hodgkin, Research, food and beverages, Hematology, Oncogenes, Flow Cytometry, Molecular biology, 3. Good health, medicine.anatomical_structure, Cell Transformation, Neoplastic, Oncology, TRAF3, Cell culture

Abstract

Background Identification of novel genetic risk factors is imperative for a better understanding of B lymphomagenesis and for the development of novel therapeutic strategies. TRAF3, a critical regulator of B cell survival, was recently recognized as a tumor suppressor gene in B lymphocytes. The present study aimed to identify novel oncogenes involved in malignant transformation of TRAF3-deficient B cells. Methods We used microarray analysis to identify genes differentially expressed in TRAF3−/− mouse splenic B lymphomas. We employed lentiviral vector-mediated knockdown or overexpression to manipulate gene expression in human multiple myeloma (MM) cell lines. We analyzed cell apoptosis and proliferation using flow cytometry, and performed biochemical studies to investigate signaling mechanisms. To delineate protein-protein interactions, we applied affinity purification followed by mass spectrometry-based sequencing. Results We identified mutated in colorectal cancer (MCC) as a gene strikingly up-regulated in TRAF3-deficient mouse B lymphomas and human MM cell lines. Aberrant up-regulation of MCC also occurs in a variety of primary human B cell malignancies, including non-Hodgkin lymphoma (NHL) and MM. In contrast, MCC expression was not detected in normal or premalignant TRAF3−/− B cells even after treatment with B cell stimuli, suggesting that aberrant up-regulation of MCC is specifically associated with malignant transformation of B cells. In elucidating the functional roles of MCC in malignant B cells, we found that lentiviral shRNA vector-mediated knockdown of MCC induced apoptosis and inhibited proliferation in human MM cells. Experiments of knockdown and overexpression of MCC allowed us to identify several downstream targets of MCC in human MM cells, including phospho-ERK, c-Myc, p27, cyclin B1, Mcl-1, caspases 8 and 3. Furthermore, we identified 365 proteins (including 326 novel MCC-interactors) in the MCC interactome, among which PARP1 and PHB2 were two hubs of MCC signaling pathways in human MM cells. Conclusions Our results indicate that in sharp contrast to its tumor suppressive role in colorectal cancer, MCC functions as an oncogene in B cells. Our findings suggest that MCC may serve as a diagnostic marker and therapeutic target in B cell malignancies, including NHL and MM. Electronic supplementary material The online version of this article (doi:10.1186/s13045-014-0056-6) contains supplementary material, which is available to authorized users.

Published

2014