染色体不稳定性
非整倍体
基因组不稳定性
染色体易位
生物
淋巴瘤
癌症研究
癌变
端粒
恶性肿瘤
中心体
染色体
免疫学
遗传学
癌症
DNA损伤
细胞周期
DNA
基因
作者
Maxwell M. Krem,Oliver W. Press,Marshall S. Horwitz,Timothy Tidwell
摘要
Summary Lymphocytes are unique among cells in that they undergo programmed DNA breaks and translocations, but that special property predisposes them to chromosomal instability ( CIN ), a cardinal feature of neoplastic lymphoid cells that manifests as whole chromosome‐ or translocation‐based aneuploidy. In several lymphoid malignancies translocations may be the defining or diagnostic markers of the diseases. CIN is a cornerstone of the mutational architecture supporting lymphoid neoplasia, though it is perhaps one of the least understood components of malignant transformation in terms of its molecular mechanisms. CIN is associated with prognosis and response to treatment, making it a key area for impacting treatment outcomes and predicting prognoses. Here we will review the types and mechanisms of CIN found in Hodgkin lymphoma, non‐Hodgkin lymphoma, multiple myeloma and the lymphoid leukaemias, with emphasis placed on pathogenic mutations affecting DNA recombination, replication and repair; telomere function; and mitotic regulation of spindle attachment, centrosome function, and chromosomal segregation. We will discuss the means by which chromosome‐level genetic aberrations may give rise to multiple pathogenic mutations required for carcinogenesis and conclude with a discussion of the clinical applications of CIN and aneuploidy to diagnosis, prognosis and therapy.
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