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Query: UMLS:C0019829 (
Hodgkin's disease
)
30,247
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
In a search for genes specifically expressed in Reed-Sternberg (RS) cells of
Hodgkin lymphoma
(HL), we applied the serial analysis of gene expression (SAGE) technique on the HL-derived cell line DEV. Genes highly expressed in DEV were subjected to an RT-PCR analysis to confirm the SAGE results. For one of the genes, a high expression was observed in DEV and other HL-derived cell lines but not in non-
Hodgkin lymphoma
(NHL)-derived cell lines and normal controls, suggesting an HL-specific expression. This gene corresponds to the human
BIC
gene, a member of the noncoding mRNA-like molecules. RNA in situ hybridization (ISH) indicated an exclusive nucleolar localization of
BIC
transcripts in all RS cells in 91% of HL cases, including nodular lymphocyte predominance (NLP) HL and classical HL. Analyses of normal human tissues revealed
BIC
transcripts in only a small number of CD20-positive B-cells in lymph node and tonsil tissue, albeit at a much lower level compared to that of RS cells.
BIC
RT-PCR in the Burkitt lymphoma-derived cell line Ramos demonstrated a significant up-regulation upon cross-linking of the B-cell receptor (BcR). IkappaBalpha-mediated blocking of NF-kappaB translocation in Ramos did not effect the up-regulation of
BIC
expression upon BcR triggering, suggesting that activation of NF-kappaB is not involved in regulation of
BIC
expression. In summary, our data show that expression of
BIC
is specific for RS cells of HL. In normal tissue,
BIC
is expressed weakly in a minority of germinal center B cells. Expression of
BIC
can be modified/influenced by BcR triggering, indicating that
BIC
might play a role in the selection of B cells.
...
PMID:High expression of B-cell receptor inducible gene BIC in all subtypes of Hodgkin lymphoma. 1469 98
In a previous study we demonstrated high expression of the non-coding
BIC
gene in the vast majority of
Hodgkin
's lymphomas (HLs). Evidence suggesting that
BIC
is a primary microRNA transcript containing the mature microRNA-155 (miR-155) as part of a RNA hairpin is now accumulating. We therefore analysed HL cell lines and tissue samples to determine whether miR-155 is also expressed in HL. High levels of miR-155 could be demonstrated, indicating that
BIC
is processed into a microRNA in HL. Most non-HL subtypes were negative for
BIC
as determined by RNA-ISH. However, in diffuse large B cell lymphoma (DLBCL) and primary mediastinal B cell lymphoma (PMBL), significant percentages of positive tumour cells were observed in 12/18 and 8/8 cases. A higher proportion of tumour cells were positive for
BIC
in DLBCL with activated B cell-like phenotype than in DLBCL with germinal centre B cell-like phenotype. Differential
BIC
expression was confirmed by qRT-PCR analysis. Northern blot analysis showed expression of miR-155 in all DLBCL and PMBL derived cell lines and tissue samples analysed. In summary, we demonstrate expression of primary microRNA
BIC
and its derivative miR-155 in HL, PMBL and DLBCL.
...
PMID:BIC and miR-155 are highly expressed in Hodgkin, primary mediastinal and diffuse large B cell lymphomas. 1604 95
We previously demonstrated high expression of primary-microRNA
BIC
(pri-miR-155) in
Hodgkin lymphoma
(HL) and lack of expression in most non-
Hodgkin lymphoma
subtypes including some Burkitt lymphoma (BL) cases. Recently, high expression of
BIC
was reported in BL in comparison to pediatric leukemia and normal peripheral-blood samples. In this study, we extended our series of BL cases and cell lines to examine expression of
BIC
using RNA in situ hybridization (ISH) and quantitative RT-PCR (qRT-PCR) and of miR-155 using Northern blotting. Both
BIC
RNA ISH and qRT-PCR revealed no or low levels of
BIC
in 25 BL tissue samples [including 7 Epstein-Barr virus (EBV)-positive cases] compared to HL and normal controls. In agreement with these findings, no miR-155 was observed in BL tissues. EBV-negative and EBV latency type I BL cell lines also showed very low
BIC
and miR-155 expression levels as compared to HL cell lines. Higher levels of
BIC
and miR-155 were detected in in vitro transformed lymphoblastoid EBV latency type III BL cell lines. An association of latency type III infection and induction of
BIC
was supported by consistent expression of
BIC
in 11 and miR-155 in 2 posttransplantation lymphoproliferative disorder (PTLD) cases. In summary, we demonstrated that expression of
BIC
and miR-155 is not a common finding in BL. Expression of
BIC
and miR-155 in 3 latency type III EBV-positive BL cell lines and in all primary PTLD cases suggests a possible role for EBV latency type III specific proteins in the induction of
BIC
expression.
...
PMID:Lack of BIC and microRNA miR-155 expression in primary cases of Burkitt lymphoma. 1623 44
MicroRNAs (miRNAs) represent a newly discovered class of posttranscriptional regulatory noncoding small RNAs that bind to targeted mRNAs and either block their translation or initiate their degradation. miRNA profiling of hematopoietic lineages in humans and mice showed that some miRNAs are differentially expressed during hematopoietic development, suggesting a role in hematopoietic cell differentiation. In addition, recent studies suggest the involvement of miRNAs in the initiation and progression of cancer. miR155 and
BIC
, its host gene, have been reported to accumulate in human B cell lymphomas, especially in diffuse large B cell lymphomas,
Hodgkin
lymphomas, and certain types of Burkitt lymphomas. Here, we show that E(mu)-mmu-miR155 transgenic mice exhibit initially a preleukemic pre-B cell proliferation evident in spleen and bone marrow, followed by frank B cell malignancy. These findings indicate that the role of miR155 is to induce polyclonal expansion, favoring the capture of secondary genetic changes for full transformation.
...
PMID:Pre-B cell proliferation and lymphoblastic leukemia/high-grade lymphoma in E(mu)-miR155 transgenic mice. 1664 Oct 92
BIC
is a primary microRNA (pri-miR-155) that can be processed to mature miR-155. In this study, we show the crucial involvement of protein kinase C (PKC) and nuclear factor-kappaB (NF-kappaB) in the regulation of
BIC
expression upon B-cell receptor triggering. Surprisingly, Northern blot analysis did not reveal any miR-155 expression upon induction of
BIC
expression in the Burkitt lymphoma-derived Ramos cell line, whereas other microRNAs were clearly detectable. Ectopic expression of
BIC
in Ramos and HEK293 cells resulted in miR-155 expression in HEK293, but not in Ramos cells, suggesting a specific block of
BIC
to miR-155 processing in Ramos. In line with the results obtained with Ramos, lack of miR-155 expression after induction of
BIC
expression was also observed in other Burkitt lymphoma cell lines, indicating a generic and specific blockade in the processing of
BIC
in Burkitt lymphoma. In contrast, induction of
BIC
expression in normal tonsillar B cells resulted in very high levels of miR-155 expression and induction of
BIC
expression in
Hodgkin's lymphoma
cell lines. It also resulted in elevated levels of miR-155. Our data provide evidence for two levels of regulation for mature miR-155 expression: one at the transcriptional level involving PKC and NF-kappaB, and one at the processing level. Burkitt lymphoma cells not only express low levels of
BIC
, but also prevent processing of
BIC
via an, as yet, unknown mechanism.
...
PMID:Regulation of pri-microRNA BIC transcription and processing in Burkitt lymphoma. 1717 72
Fast and reliable differential diagnosis of Burkitt lymphoma (BL) vs. diffuse large B cell lymphoma (DLBCL) is of major importance for therapeutic decisions and patient outcome. Aggressive B cell non-
Hodgkin
lymphomas (B-NHLs) that do not belong to the abovementioned entities were categorized by the current WHO lymphoma classification as "B-cell lymphoma, unclassifiable, with features intermediate between DLBCL and BL" (DLBCL/BL). We have recently described a DLBCL/BL subgroup with recurrent chromosome 11q aberrations, resembling BL (B-NHLs[11q]). Here, we analyzed 102 prospectively collected fine needle aspirates from patients with aggressive B-NHLs in order to investigate the potential of microRNA (miR)-155, its precursor
BIC
, as well as miR-21 and miR-26a to differentiate BL from DLBCL, and from DLBCL/BL that include B-NHLs[11q]. Both BL and DLBCL/BL cases, including B-NHLs[11q], demonstrated significantly lower expression levels of miR-155/
BIC
, miR-21, and miR-26a compared to primary DLBCL. In conclusion, the miRs expression in B-NHLs[11q] provides a new suggestion, in addition to pathomorphological and clinical similarities between classical, i.e., MYC translocation-positive BL, and B-NHLs[11q], to recognize the B-NHLs[11q] subgroup of DLBCL/BL category as a MYC translocation-negative variant of BL in most cases, and points to the potential utility of miR-155/
BIC
/miR-21/miR-26a for the differential diagnosis of a heterogeneous category of DLBCL/BL.
...
PMID:miR expression in MYC-negative DLBCL/BL with partial trisomy 11 is similar to classical Burkitt lymphoma and different from diffuse large B-cell lymphoma. 2567 2
