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Isotype class switching and the pathogenesis of multiple myeloma.

机译:同型类别转换和多发性骨髓瘤的发病机制。

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摘要

Translocations at the immunoglobulin heavy chain locus (14q32) are now considered the commonest karyotypic change in multiple myeloma. These translocations are thought to be intimately involved in the pathogenesis of this disease. The heavy chain locus is strongly transcriptionally active in B and plasma cells and transfer of a potential oncogene to 14q32 would result in its dysregulation. Molecular characterization suggests that the majority of these breakpoints cluster in switch regions within the heavy chain locus. Switch regions are normally involved in the regulated process of isotype switching so that in myeloma the rearrangements are believed to be a result of so-called illegitimate (aberrant) switch recombination and are likely to be an early event in myeloma development. A legitimate switch recombination event occurs between two switch regions producing a hybrid switch; this is necessary for class switching to proceed on a productive allele. In this review we describe the process of isotype switching and how illegitimate class switching may be related to the pathogenesis of multiple myeloma.
机译:现在认为免疫球蛋白重链基因座(14q32)的易位是多发性骨髓瘤中最常见的核型改变。这些易位被认为与该疾病的发病机理密切相关。重链基因座在B细胞和浆细胞中具有强烈的转录活性,潜在的癌基因转移至14q32将导致其失调。分子表征表明,这些断点的大部分聚集在重链基因座内的开关区域中。转换区通常参与同种型转换的调节过程,因此在骨髓瘤中,重排被认为是所谓的非法(异常)转换重组的结果,并且很可能是骨髓瘤发展的早期事件。在产生混合开关的两个开关区域之间发生合法的开关重组事件。这对于在高效等位基因上进行类别切换是必要的。在这篇综述中,我们描述了同种型转换的过程以及非法类转换如何与多发性骨髓瘤的发病机理相关。

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