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Analysis of genetic abnormalities provides insights into genetic evolution of hyperdiploid myeloma.

机译:遗传异常分析为了解超二倍体骨髓瘤的遗传进化提供了见识。

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Aneuploidy is ubiquitous in human cancer and is seen as whole chromosome gains and losses, unbalanced translocations and inversions, duplications, deletions and loss of heterozygosity. Within this complexity, some subgroups of aneuploid tumors emerge as distinct biological and clinical entities. Hyperdiploid myeloma (H-MM), characterized by hyperdiploid chromosome numbers because of nonrandom trisomies, is one such example. We undertook a comprehensive survey of the karyotypes of a large number of H-MM (n = 469) to describe fully genomic instability in these tumors, to dissect pathways of genetic evolution, and identify distinct subgroups based on their genetic changes. While selective pressure apparently favors the emergence of clones with gains of chromosomes 3, 5, 7, 9, 11, 15, 19, and 21, a background of ongoing genomic instability results in gains of other chromosomes, albeit at a much lower prevalence. A deduced temporal analysis of these karyotypes indicates that selected gains are early events.Other events occurring later in the course of the disease include secondary chromosome translocations and monosomies. The development of these genetic aberrations is thus highly ordered and undoubtedly of biological relevance. Within this framework, we propose a model of genetic evolution in H-MM.
机译:非整倍体在人类癌症中无处不在,被视为整个染色体的得失,不平衡的易位和倒位,重复,缺失和杂合性丧失。在这种复杂性内,非整倍体肿瘤的一些亚组以独特的生物学和临床实体出现。这样的例子就是超二倍体骨髓瘤(H-MM),其特征是由于非随机三体性而具有超二倍体染色体数。我们对大量H-MM(n = 469)的核型进行了全面调查,以描述这些肿瘤中的完全基因组不稳定性,剖析遗传进化途径,并根据其遗传变化确定不同的亚组。尽管选择性压力显然有利于出现具有3、5、7、9、9、11、15、19和21号染色体的克隆,但持续的基因组不稳定背景会导致其他染色体的获得,尽管其患病率要低得多。对这些核型的时间分析推论表明,所选择的增益是早期事件。在疾病过程后期发生的其他事件包括继发性染色体易位和单体性。因此,这些遗传畸变的发展是高度有序的,并且无疑具有生物学意义。在此框架内,我们提出了H-MM中遗传进化的模型。

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