Immunohistochemical detection of BCL-3 in lymphoid neoplasms: a survey of 353 cases

Canöz, Özlem; Rassidakis, George Z.; Admirand, Joan H.; Medeiros, L. Jeffrey

doi:10.1038/modpathol.3800140

Cited by 38 publications

(39 citation statements)

References 30 publications

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“…[1][2][3]5,11,[13][14][15][16][17][18] In agreement with these findings, immunohistochemical studies have identified the presence of BCL3 expression in both B-and T-cell lymphomas pointing to a role of BCL3 in B-and T-cell lymphomagenesis. 33,34 The major aim of the present study was to perform a thorough cytogenetic, FISH, molecular and histopathologic study of B-cell malignancies bearing a t(14;19)(q32;q13) or variant translocations to shed further light on these pathologic associations.…”

Section: Discussionmentioning

confidence: 99%

A comprehensive genetic and histopathologic analysis identifies two subgroups of B-cell malignancies carrying a t(14;19)(q32;q13) or variant BCL3-translocation

et al. 2007

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The biologic and pathologic features of B-cell malignancies bearing a translocation t(14;19)(q32;q13) leading to a fusion of IGH and BCL3 are still poorly described. Herein we report the results of a comprehensive cytogenetic, fluorescence in situ hybridization (FISH), molecular and histopathological survey of a large series of B-cell malignancies with t(14;19) or variant translocations. A total of 56 B-cell malignancies with a FISHproven BCL3 involvement were identified with the translocation partners being IGH (n ¼ 51), IGL (n ¼ 2), IGK (n ¼ 2) and a non-IG locus (n ¼ 1). Hierarchical clustering of chromosomal changes associated with the t(14;19) indicated the presence of two different groups of IG/BCL3-positive lymphatic neoplasias. The first group included 26 B-cell malignancies of various histologic subtypes containing a relatively high number of chromosomal changes and mostly mutated IgVH genes. This cluster displayed three cytogenetic branches, one with rearrangements in 7q, another with deletions in 17p and a third one with rearrangements in 1q and deletions in 6q and 13q. The second group included 19 cases, mostly diagnosed as B-cell chronic lymphocytic leukemia (B-CLL), and characterized by few additional chromosomal changes (e.g. trisomy 12) and unmutated IgVH genes. In conclusion, our study indicates that BCL3 translocations are not restricted to B-CLL but present in a heterogeneous group of B-cell malignancies.

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Section: Discussionmentioning

confidence: 99%

A comprehensive genetic and histopathologic analysis identifies two subgroups of B-cell malignancies carrying a t(14;19)(q32;q13) or variant BCL3-translocation

et al. 2007

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“…In addition, t(14;19) translocations involving BCL-3 have been identified in some lymphomas (Nakagawa et al, 1995;Yano et al, 1995;McKeithan et al, 1997;Au et al, 2002;Soma et al, 2006) and occasionally in lymphoproliferative disorders (Michaux et al, 1996); furthermore, other genetic alterations on chromosome 19 may also lead to increased BCL-3 expression (Schlette et al, 2005). The hypothesis that increased expression of BCL-3 contributes to human B-cell malignancies is supported by several findings: (1) transgenic mice in which BCL-3 is under the control of the m heavy chain enhancer develop splenomegaly and have excess mature B cells in their bone marrow and lymph nodes (Ong et al, 1998); (2) overexpression of BCL-3 can transform mouse 3T3 cells in culture (Viatour et al, 2004); (3) overexpression of BCL-3 can enhance the survival of activated T cells (Mitchell et al, 2001) and (4) elevated levels of BCL-3 are seen in many lymphoid and non-lymphoid human tumor samples (Cogswell et al, 2000;Rassidakis et al, 2003;Canoz et al, 2004;Pallares et al, 2004;Ohno et al, 2005;Schlette et al, 2005). Oncogenically activating mutations within the coding region of BCL-3 have not been identified; however, such mutations may exist in that certain point mutations can enhance the transforming activity of BCL-3 in vitro (Viatour et al, 2004).…”

Section: Multiple Familial Trichoepitheliomamentioning

confidence: 99%

Mutations in the NF-κB signaling pathway: implications for human disease

2006

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“…In addition to its relatively high expression in B-CLLs carrying the t(14;19) translocation, Bcl-3 has also been found to be elevated in a number of other human cancers, including nasopharyngeal carcinoma (Thornburg et al 2003), breast cancer (Cogswell et al 2000), lymphoma (Canoz et al 2004), and hepatocellular carcinoma (B. O'Neil, unpubl.). To understand the consequences of Bcl-3 constitutive expression and to investigate its potential role in driving oncogenesis, we engineered the MCF-7 breast cancer cell line to express relatively high levels of Bcl-3 (MCF-7B).…”

Section: Elevated Bcl-3 Expression Inhibits Dna Damage-induced Apoptosismentioning

confidence: 99%

“…In this regard, expression of Bcl-3 is sufficient to transform NIH3T3 cells (Viatour et al 2004). Importantly, Bcl-3 has now been shown to be more widely expressed in cancer, with expression in a significant number of breast cancers (Cogswell et al 2000), nasopharyngeal carcinomas (Thornburg et al 2003), lymphomas (Canoz et al 2004), and hepatocellular carcinomas and pancreatic cancers (B. O'Neil, unpubl.). The findings that Bcl-3, in complex with p52, can promote transcription of the genes encoding the cell cycle regulator cyclin D1 and the anti-apoptotic Bcl-2 protein suggest one potential oncogenic mechanism (Westerheide et al 2001;Viatour et al 2003), but a more complete understanding of the role of Bcl-3 in human cancers is still lacking.…”

mentioning

confidence: 99%

Expression of the Bcl-3 proto-oncogene suppresses p53 activation

Kashatus¹,

Cogswell²,

Baldwin³

2005

Genes Dev.

131

111

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While Bcl-3 expression in cancer was originally thought to be limited to B-cell lymphomas with a 14;19 chromosomal translocation, more recent evidence indicates that expression of this presumptive oncoprotein is significantly more widespread in cancer. However, an oncogenic role for Bcl-3 has not been clearly identified. Experiments presented here indicate that Bcl-3 is inducible by DNA damage and is required for the induction of Hdm2 gene expression and the suppression of persistent p53 activity. Furthermore, constitutive expression of Bcl-3 suppresses DNA damage-induced p53 activation and inhibits p53-induced apoptosis through a mechanism that is at least partly dependent on the up-regulation of Hdm2. The results provide insight into a mechanism whereby altered expression of Bcl-3 leads to tumorigenic potential. Since Bcl-3 is required for germinal center formation, these results suggest functional similarities with the unrelated Bcl-6 oncoprotein in suppressing potential p53-dependent cell cycle arrest and apoptosis in response to somatic hypermutation and class switch recombination.[Keywords: Apoptosis; Bcl-3; Hdm2; NF-B; p53] Supplemental material is available at http://www.genesdev.org.

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Immunohistochemical detection of BCL-3 in lymphoid neoplasms: a survey of 353 cases

Cited by 38 publications

References 30 publications

A comprehensive genetic and histopathologic analysis identifies two subgroups of B-cell malignancies carrying a t(14;19)(q32;q13) or variant BCL3-translocation

A comprehensive genetic and histopathologic analysis identifies two subgroups of B-cell malignancies carrying a t(14;19)(q32;q13) or variant BCL3-translocation

Mutations in the NF-κB signaling pathway: implications for human disease

Expression of the Bcl-3 proto-oncogene suppresses p53 activation

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