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B细胞受体诱导基因BIC在霍奇金淋巴瘤所有亚型中高表达。

High expression of B-cell receptor inducible gene BIC in all subtypes of Hodgkin lymphoma.

作者信息

van den Berg Anke, Kroesen Bart-Jan, Kooistra Klaas, de Jong Debora, Briggs Jane, Blokzijl Tjasso, Jacobs Susan, Kluiver Joost, Diepstra Arjan, Maggio Ewerton, Poppema Sibrand

机构信息

Pathology & Laboratory Medicine, University Medical Center Groningen, Groningen, The Netherlands.

出版信息

Genes Chromosomes Cancer. 2003 May;37(1):20-8. doi: 10.1002/gcc.10186.

Abstract

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.

摘要

为了寻找在霍奇金淋巴瘤(HL)的里德-施特恩伯格(RS)细胞中特异性表达的基因,我们对HL来源的DEV细胞系应用了基因表达序列分析(SAGE)技术。对在DEV中高表达的基因进行逆转录聚合酶链反应(RT-PCR)分析,以证实SAGE结果。对于其中一个基因,在DEV和其他HL来源的细胞系中观察到高表达,但在非霍奇金淋巴瘤(NHL)来源的细胞系和正常对照中未观察到,提示其为HL特异性表达。该基因对应于人BIC基因,是一种非编码mRNA样分子的成员。RNA原位杂交(ISH)表明,在91%的HL病例(包括结节性淋巴细胞为主型(NLP)HL和经典HL)的所有RS细胞中,BIC转录本仅定位于核仁。对正常人体组织的分析显示,仅在淋巴结和扁桃体组织中的少数CD20阳性B细胞中有BIC转录本,尽管其水平远低于RS细胞。在伯基特淋巴瘤来源的Ramos细胞系中进行的BIC RT-PCR显示,B细胞受体(BcR)交联后BIC表达显著上调。在Ramos细胞中,IκBα介导的NF-κB易位阻断并不影响BcR触发后BIC表达的上调,提示NF-κB的激活不参与BIC表达的调控。总之,我们的数据表明BIC的表达是HL的RS细胞所特有的。在正常组织中,BIC在少数生发中心B细胞中弱表达。BcR触发可改变/影响BIC的表达,表明BIC可能在B细胞的选择中发挥作用。

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