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IgA和/或IgG转换的慢性淋巴细胞白血病B细胞的分子特征

Molecular characterization of IgA- and/or IgG-switched chronic lymphocytic leukemia B cells.

作者信息

Matolcsy A, Casali P, Nádor R G, Liu Y F, Knowles D M

机构信息

Department of Pathology, University Medical School of Pécs, Hungary.

出版信息

Blood. 1997 Mar 1;89(5):1732-9.

Abstract

The immunoglobulin (Ig) variable region (V) genes expressed by IgM chronic lymphocytic leukemia (CLL) B cells display little or no somatic mutations. However, preliminary findings have shown that Ig V genes of IgA and IgG CLLs may be somatically mutated, suggesting that isotype-switched CLLs may represent a "subtype" of the disease. To investigate the degree and nature of somatic mutations and the role of antigen (Ag) in the clonal selection and expansion of isotype-switched CLLs, and to determine whether specific oncogene or tumor suppressor gene mutations are associated with isotype-switched CLLs, we analyzed the expressed Ig VH gene, bcl-1 and bcl-2 proto-oncogene, and p53 tumor suppressor gene configurations of 3 IgA-, 1 IgG-, and 1 IgA/ IgG-expressing CLLs. These isotype-switched CLL B cells expressed surface HLA-DR, CD19, CD23, and CD5, and displayed no alterations of the bcl-1 and bcl-2 oncogenes and the p53 tumor-suppressor gene. The cDNA VH-D-JH gene sequence was joined with that of the C alpha gene in the B cells of the three IgA CLLs, and with that of the C gamma gene in the IgG CLL B cells. In the IgA/IgG-coexpressing CLL B cells, identical VH-D-JH cDNA sequences were spliced to either C alpha or C gamma genes. In all five CLLs, the pattern of C mu DNA probe hybridization to the digested genomic DNAs was consistent with deletion of the C mu exon from the rearranged Ig gene locus, suggesting that these CLL B cells had undergone DNA switch recombination. In one IgA CLL, the expressed VH gene was unmutated. In all other class-switched CLLs, the Ig VH segment gene was mutated, but the point mutations were not associated with intraclonal diversification. In one IgA and in the IgA/IgG-coexpressing CLL, the nature and distribution of the mutations were consistent with Ag selection. These findings suggest that IgA- and/or IgG-expressing CLLs represent, in their VH gene structure, transformants of B cells at different stages of ontogeny. They also suggest that Ag may play a role in the clonal selection of some of these isotype-switched leukemic cells, but bcl-1 and bcl-2 oncogene rearrangements and p53 tumor suppressor gene mutation are not associated with the pathogenesis of isotype-switched CLLs.

摘要

IgM慢性淋巴细胞白血病(CLL)B细胞所表达的免疫球蛋白(Ig)可变区(V)基因几乎没有或没有体细胞突变。然而,初步研究结果表明,IgA和IgG型CLL的Ig V基因可能发生了体细胞突变,这表明同种型转换的CLL可能代表该疾病的一种“亚型”。为了研究体细胞突变的程度和性质以及抗原(Ag)在同种型转换CLL的克隆选择和扩增中的作用,并确定特定的癌基因或肿瘤抑制基因突变是否与同种型转换CLL相关,我们分析了3例表达IgA、1例表达IgG和1例表达IgA/IgG的CLL的表达型Ig VH基因、bcl-1和bcl-2原癌基因以及p53肿瘤抑制基因的构型。这些同种型转换的CLL B细胞表达表面HLA-DR、CD19、CD23和CD5,并且bcl-1和bcl-2癌基因以及p53肿瘤抑制基因没有改变。在3例IgA CLL的B细胞中,cDNA VH-D-JH基因序列与Cα基因的序列相连,在IgG CLL B细胞中与Cγ基因的序列相连。在共表达IgA/IgG的CLL B细胞中,相同的VH-D-JH cDNA序列被剪接到Cα或Cγ基因上。在所有5例CLL中,CμDNA探针与消化后的基因组DNA的杂交模式与重排的Ig基因座上Cμ外显子的缺失一致,表明这些CLL B细胞经历了DNA转换重组。在1例IgA CLL中,表达的VH基因未发生突变。在所有其他类别转换的CLL中,Ig VH区段基因发生了突变,但点突变与克隆内多样化无关。在1例IgA和共表达IgA/IgG的CLL中,突变的性质和分布与抗原选择一致。这些发现表明,表达IgA和/或IgG的CLL在其VH基因结构上代表了不同发育阶段B细胞的转化体。它们还表明,抗原可能在这些同种型转换的白血病细胞中的一些克隆选择中起作用,但bcl-1和bcl-2癌基因重排以及p53肿瘤抑制基因突变与同种型转换CLL的发病机制无关。

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