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Lymphoblastoid cell line with B1 cell characteristics established from a chronic lymphocytic leukemia clone by in vitro EBV infection

机译:通过体外EBV感染从慢性淋巴细胞性白血病克隆中建立具有B1细胞特征的淋巴细胞样细胞系

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摘要

Chronic lymphocytic leukemia (CLL) cells express the receptor for Epstein-Barr virus (EBV) and can be infected in vitro. Infected cells do not express the growth-promoting set of EBV-encoded genes and therefore they do not yield LCLs, in most experiments. With exceptional clones, lines were obtained however. We describe a new line, HG3, established by in vitro EBV-infection from an IGHV1–2 unmutated CLL patient clone. All cells expressed EBNA-2 and LMP-1, the EBV-encoded genes pivotal for transformation. The karyotype, FISH cytogenetics and SNP-array profile of the line and the patient's ex vivo clone showed biallelic 13q14 deletions with genomic loss of DLEU7, miR15a/miR16–1, the two micro-RNAs that are deleted in 50% of CLL cases. Further features of CLL cells were: expression of CD5/CD20/CD27/CD43 and release of IgM natural antibodies reacting with oxLDL-like epitopes on apoptotic cells (cf. stereotyped subset-1). Comparison with two LCLs established from normal B cells showed 32 genes expressed at higher levels (> 2-fold). Among these were LHX2 and LILRA. These genes may play a role in the development of the disease. LHX2 expression was shown in self-renewing multipotent hematopoietic stem cells, and LILRA4 codes for a receptor for bone marrow stromal cell antigen-2 that contributes to B cell development. Twenty-four genes were expressed at lower levels, among these PARD3 that is essential for asymmetric cell division. These genes may contribute to establish precursors of CLL clones by regulation of cellular phenotype in the hematopoietic compartment. Expression of CD5/CD20/CD27/CD43 and spontaneous production of natural antibodies may identify the CLL cell as a self-renewing B1 lymphocyte.
机译:慢性淋巴细胞性白血病(CLL)细胞表达Epstein-Barr病毒(EBV)的受体,可以在体外感染。在大多数实验中,感染的细胞不表达EBV编码基因促进生长的集合,因此它们不产生LCL。然而,通过优异的克隆,获得了品系。我们描述了一个新的系HG3,它是由IGHV1-2未突变的CLL患者克隆的体外EBV感染建立的。所有细胞均表达EBNA-2和LMP-1,这是EBV编码的基因,对转化至关重要。该品系的核型,FISH细胞遗传学和SNP阵列谱以及患者的离体克隆显示双等位基因13q14缺失,缺失了DLEU7,miR15a / miR16-1的基因组,这两个小RNA在50%的CLL病例中被缺失。 CLL细胞的其他特征是:CD5 / CD20 / CD27 / CD43的表达和与凋亡细胞上oxLDL样表位反应的IgM天然抗体的释放(参见定型子集1)。与从正常B细胞​​建立的两个LCL的比较显示,有32个基因以更高的水平表达(> 2倍)。其中包括LHX2和LILRA。这些基因可能在疾病的发展中起作用。 LHX2表达在自我更新的多能造血干细胞中显示,LILRA4编码骨髓基质细胞抗原2的受体,该受体有助于B细胞发育。在不对称细胞分裂所必需的这些PARD3中,有24个基因的表达水平较低。这些基因可通过调节造血区室的细胞表型来帮助建立CLL克隆的前体。 CD5 / CD20 / CD27 / CD43的表达和自然抗体的自发产生可能将CLL细胞鉴定为自我更新的B1淋巴细胞。

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