Your search keyword '"Pittaluga, S."' showing total 8 results

1. Changes of Benthic Macrofaunal Composition on a Tidal Flat of Río Gallegos Estuary, Argentina.

Author

Lizarralde, Z. I., Pittaluga, S., and Perroni, M.

Published

2018

2. Frequent STAT5B mutations in γδ hepatosplenic T-cell lymphomas.

Author

Nicolae, A, Xi, L, Pittaluga, S, Abdullaev, Z, Pack, S D, Chen, J, Waldmann, T A, Jaffe, E S, and Raffeld, M

Published

2014

3. Mutations in PIK3CD Can Cause Hyper IgM Syndrome (HIGM) Associated with Increased Cancer Susceptibility.

Author

Crank, M., Grossman, J., Moir, S., Pittaluga, S., Buckner, C., Kardava, L., Agharahimi, A., Meuwissen, H., Stoddard, J., Niemela, J., Kuehn, H., and Rosenzweig, S.

Subjects

GENETIC mutation, IMMUNOGLOBULIN M, DISEASE susceptibility, GENETIC code, IMMUNODEFICIENCY, PHOSPHOINOSITIDES, BLOOD serum analysis, B cells

Abstract

Autosomal dominant gain of function mutations in the gene encoding PI3K p110δ were recently associated with a novel combined immune deficiency characterized by recurrent sinopulmonary infections, CD4 lymphopenia, reduced class-switched memory B cells, lymphadenopathy, CMV and/or EBV viremia and EBV-related lymphoma. A subset of affected patients also had elevated serum IgM. Here we describe three patients in two families who were diagnosed with HIGM at a young age and were recently found to carry heterozygous mutations in PIK3CD. These patients had an abnormal circulating B cell distribution featuring a preponderance of early transitional (T1) B cells and plasmablasts. When stimulated in vitro, PIK3CD mutated B cells were able to secrete class-switched immunoglobulins. This finding implies that the patients' elevated serum IgM levels were unlikely a product of an intrinsic B cell functional inability to class switch. All three patients developed malignant lymphoproliferative syndromes that were not associated with EBV. Thus, we identified a novel subset of patients with PIK3CD mutations associated with HIGM, despite indications of preserved in vitro B cell class switch recombination, as well as susceptibility to non-EBV-associated malignancies. [ABSTRACT FROM AUTHOR]

Published

2014

4. Modeling tumor-host interactions of chronic lymphocytic leukemia in xenografted mice to study tumor biology and evaluate targeted therapy.

Author

Herman, S E M, Sun, X, McAuley, E M, Hsieh, M M, Pittaluga, S, Raffeld, M, Liu, D, Keyvanfar, K, Chapman, C M, Chen, J, Buggy, J J, Aue, G, Tisdale, J F, Pérez-Galán, P, and Wiestner, A

Subjects

LYMPHOCYTIC leukemia, LYMPHOPROLIFERATIVE disorders, CHRONIC lymphocytic leukemia, LYMPHOID tissue, PROTEIN-tyrosine kinases, TUMORS

Abstract

Chronic lymphocytic leukemia (CLL) cells depend on microenvironmental factors for proliferation and survival. In particular, the B-cell receptor (BCR) and nuclear factor- κB (NF-κB) pathways are activated in the lymph node (LN) microenvironment. Thus, model systems mimicking tumor-host interactions are important tools to study CLL biology and pathogenesis. We investigated whether the recently established NOD/scid/γcnull (NSG) mouse xenograft model can recapitulate the effects of the human microenvironment. We assessed, therefore, tumor characteristics previously defined in LN-resident CLL cells, including proliferation, and activation of the BCR and NF-κB pathways. We found that the murine spleen (SP) microenvironment supported CLL cell proliferation and activation to a similar degree than the human LN, including induction of BCR and NF-κB signaling in the xenografted cells. Next, we used this model to study ibrutinib, a Bruton's tyrosine kinase inhibitor in clinical development. Ibrutinib inhibited BCR and NF-κB signaling induced by the microenvironment, decreased proliferation, induced apoptosis and reduced the tumor burden in vivo. Thus, our data demonstrate that the SP of xenografted NSG mice can, in part, recapitulate the role of the human LN for CLL cells. In addition, we show that ibrutinib effectively disrupts tumor-host interactions essential for CLL cell proliferation and survival in vivo. [ABSTRACT FROM AUTHOR]

Published

2013

5. Primary diffuse large B cell lymphoma of the stomach: analysis of somatic mutations in the rearranged immunoglobulin heavy chain variable genes indicates antigen selection.

Author

Driessen, A, Tierens, A, Ectors, N, Stul, M, Pittaluga, S, Geboes, K, Delabie, J, and De Wolf-Peeters, C

Subjects

B cells, LYMPHOMAS, GENETIC mutation

Abstract

Gastric low grade MALT lymphomas show a pattern of somatic mutations in their rearranged immunoglobulin genes, indicative of antigen selection. This provides evidence for antigen stimulation in the lymphomagenesis. Gastric diffuse large B cell lymphomas develop secondary to low grade MALT lymphoma or de novo. To study whether antigen-selection is also a feature of primary diffuse large B cell lymphomas, we analysed somatic mutations in the rearranged immunoglobulin heavy chain (IgH) variable genes (VH). The rearranged VH genes of six cases of gastric primary diffuse large B cell lymphoma were amplified from genomic or complementary DNA by a VH gene family-specific polymerase chain reaction method. The PCR products were directly sequenced and were compared to published germline sequences to analyse somatic mutations. Similarly to low grade MALT lymphomas 5/6 primary diffuse large B cell lymphomas show a pattern of somatic mutation in their rearranged VH genes, indicative of antigen selection and suggesting a role for antigens in lymphomagenesis. One case showed bi-allelic VH gene rearrangements, which were non-functional due to extensive deletions. Antigen selection could not be demonstrated or excluded. Antigen selection is a common feature in most analysed primary diffuse large B cell lymphomas, although some heterogeneity in the mechanisms involved in the lymphomagenesis of gastric primary diffuse large B cell lymphomas has not been excluded entirely (case 4). [ABSTRACT FROM AUTHOR]

Published

1999

6. Characteristic pattern of chromosomal gains and losses in marginal zone B cell lymphoma detected by comparative genomic hybridization.

Author

Dierlamm, J, Rosenberg, C, Stul, M, Pittaluga, S, Wlodarska, I, Michaux, L, Dehaen, M, Verhoef, G, Thomas, J, de Kelver, W, Bakker-Schut, T, Cassiman, J J, Raap, A K, De Wolf-Peeters, C, Van den Berghe, H, and Hagemeijer, A

Subjects

B cells, LYMPHOMAS, B cell lymphoma, CHROMOSOME abnormalities, COMPARATIVE studies, GENE mapping, KARYOTYPES, RESEARCH methodology, MEDICAL cooperation, GENETIC mutation, ONCOGENES, PROTEINS, RESEARCH, SURVIVAL, TRANSCRIPTION factors, DNA-binding proteins, FLUORESCENCE in situ hybridization, EVALUATION research

Abstract

Marginal zone B cell lymphoma (MZBCL) represents a distinct subtype of B cell non-Hodgkin's lymphoma, which has been recently recognized and defined as a disease entity. We investigated 25 cases (18 at primary diagnosis and seven during the course of disease) of MZBCL by comparative genomic hybridization (CGH) and compared these results with cytogenetic, fluorescence in situ hybridization (FISH), and Southern blot data. Twenty of the 25 cases (80%) showed gains (total 49) or losses (total 15) of genetic material. In extranodal, nodal, and splenic MZBCL, material of chromosomes 3 (52% of cases), 18 (32%), X (24%), and 1q (16%) was most frequently gained, whereas losses predominantly involved chromosomes 17 (16%) and 9 (12%). High-level amplifications involving the regions 18q21-23 and 18q21-22, respectively, were detected in two cases. Gains of chromosomes 1q and 8q and losses of chromosome 17 or 17p occurred more frequently in relapsed or progressive lymphomas. For all of the frequently affected chromosomes, CGH allowed narrowing of the relevant subregions including 3q21-23, 3q25-29 and 18q21-23. By Southern blot analysis, the BCL2, BCL6, and CMYC proto-oncogenes were found to be a part of the over-represented regions in two cases, one case, and two cases, respectively, with gains involving 18q, 3q or 8q. In 13 cases, CGH revealed chromosomal imbalances which were not detected by cytogenetic analysis but could be confirmed by FISH or Southern blot analysis in all cases investigated. On the other hand, CGH failed to detect trisomy 3, trisomy 18, and deletion 7q in three cases with a low proportion of tumor cells bearing these abnormalities, as shown by interphase FISH. The characteristic pattern of chromosomal gains and losses detected in this study confirms the distinct nature of MZBCL and may point to chromosomal regions involved in the pathogenesis of these neoplasms. [ABSTRACT FROM AUTHOR]

Published

1997

7. FAB classification of myelodysplastic syndromes: merits and controversies.

Author

Verhoef, G., Pittaluga, S., Wolf-Peeters, C., Boogaerts, M., Verhoef, G E, De Wolf-Peeters, C, and Boogaerts, M A

Abstract

Guidelines for the definition and diagnosis of myelodysplasia were set out by the French-American-British Cooperative group (FAB), and the resulting framework has greatly helped the now very large number of workers in many scientific disciplines who are actively investigating the myelodysplastic syndromes (MDS). Most patients with MDS can be readily classified into clinically relevant subgroups by correlation of clinical findings with the findings from well-prepared peripheral blood and bone marrow specimens. However, there are several areas where the standard morphological features are insensitive, but integration of these parameters with histology and cytogenetic and molecular techniques may help us in understanding this fascinating disease. [ABSTRACT FROM AUTHOR]

Published

1995

8. Second cancers early post allogeneic transplant: the case of 'unrestrained' malignancy?

Author

Davidson-Moncada, J K, Pittaluga, S, Roth, M, Dunleavy, K, Duffy, A, and Pavletic, S

Subjects

*CANCER diagnosis, *CANCER patients, *HEMATOPOIETIC stem cell transplantation

Abstract

A letter to the editor is presented in response to a case study of a patient diagnosed with a new carcinoma after he underwent allogeneic hematopoietic stem cell transplantation (HSCT) in the December 10, 2012 issue.

Published

2013