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• W337792209 endingPage "203" @default.
• W337792209 startingPage "168" @default.
• W337792209 abstract "The majority of cases of acute lymphoblastic leukemia (ALL) are known to have a genetic basis. Most leukemic cells harbor gross chromosomal alterations that have key roles in initiating leukemogenesis. These alterations include gains and losses of whole chromosomes (hyper- and hypodiploidy), and structural alterations including translocations, inversions, deletions, and amplifications. Identification, cloning, and functional analysis of genes disrupted or rearranged by these alterations has led to characterization of numerous oncogenes and tumor suppressors with key roles in leukemogenesis. Detection of these alterations by cytogenetic techniques (karyotyping or fluorescence in situ hybridization [FISH]) and molecular analyses is extensively used in diagnosis and risk stratification in order to assign appropriate treatment. While the importance of these gross chromosomal alterations in leukemogenesis has been known for many years, it has also been long recognized that many of the chromosomal alterations are insufficient to cause leukemia in experimental models, or may be detected many years prior to the clinical onset of leukemia. Moreover, a substantial minority of children (and a higher proportion of adults) lack a gross chromosomal alteration on cytogenetic analysis. Together, these findings indicate that additional submicroscopic genetic alterations also contribute to leukemogenesis. With the advent of technology to interrogate genome-wide changes in DNA copy number (i.e., amplifications and deletions) at very high resolution, and to identify sequence mutations in a high-throughput manner, it has become clear that ALL genomes commonly harbor both gross and submicroscopic genetic alterations. These alterations commonly involve genes that regulate lymphoid development, cell cycle, tumor suppression, and a variety of other key cellular pathways, and emerging data indicate that many of these alterations influence leukemogenesis and treatment responsiveness." @default.
• W337792209 created "2016-06-24" @default.
• W337792209 creator A5048744038 @default.
• W337792209 date "2012-06-21" @default.
• W337792209 modified "2023-10-18" @default.
• W337792209 title "Molecular genetics of acute lymphoblastic leukemia" @default.
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