PURPOSE OF REVIEW: This review describes the recent advances in genomic profiling that have provided critical new insights into the biology of acute leukemia in children. RECENT FINDINGS: Acute leukemia genomes commonly harbor submicroscopic gains and deletions of DNA which target key cellular pathways that influence leukemogenesis and the likelihood of treatment failure, particularly in acute lymphoblastic leukemia (ALL). Notably, genetic alterations targeting transcriptional regulators of lymphoid development are a hallmark of B-progenitor ALL, and alteration of specific genes in this pathway, such as IKZF1 (encoding IKAROS), are associated with high-risk ALL. Integrated genomic profiling has identified potential therapeutic targets in ALL, including aberrant cytokine receptor signaling mediated by rearrangements and mutation of CRLF2 and JAK2. Genome-wide association studies are also providing important insights into the role of inherited genetic variation and susceptibility to ALL. In contrast, genomic profiling of acute myeloid leukemia (AML) has thus far yielded fewer insights, but ongoing resequencing of leukemia genomes is uncovering novel mutations in both ALL and AML. SUMMARY: Genomic profiling has identified important new genetic lesions that contribute to leukemogenesis. These findings will have important implications for the development of new diagnostic tests and treatment approaches in high-risk leukemia. Future studies will be increasingly reliant on comprehensive genomic sequencing to reveal the spectrum of genetic alterations in this disease, with the ultimate aim of improving the treatment outcome for leukemia patients.
PURPOSE OF REVIEW: This review describes the recent advances in genomic profiling that have provided critical new insights into the biology of acute leukemia in children. RECENT FINDINGS: Acute leukemia genomes commonly harbor submicroscopic gains and deletions of DNA which target key cellular pathways that influence leukemogenesis and the likelihood of treatment failure, particularly in acute lymphoblastic leukemia (ALL). Notably, genetic alterations targeting transcriptional regulators of lymphoid development are a hallmark of B-progenitor ALL, and alteration of specific genes in this pathway, such as IKZF1 (encoding IKAROS), are associated with high-risk ALL. Integrated genomic profiling has identified potential therapeutic targets in ALL, including aberrant cytokine receptor signaling mediated by rearrangements and mutation of CRLF2 and JAK2. Genome-wide association studies are also providing important insights into the role of inherited genetic variation and susceptibility to ALL. In contrast, genomic profiling of acute myeloid leukemia (AML) has thus far yielded fewer insights, but ongoing resequencing of leukemia genomes is uncovering novel mutations in both ALL and AML. SUMMARY: Genomic profiling has identified important new genetic lesions that contribute to leukemogenesis. These findings will have important implications for the development of new diagnostic tests and treatment approaches in high-risk leukemia. Future studies will be increasingly reliant on comprehensive genomic sequencing to reveal the spectrum of genetic alterations in this disease, with the ultimate aim of improving the treatment outcome for leukemiapatients.
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Authors: J Eswaran; P Sinclair; O Heidenreich; J Irving; L J Russell; A Hall; D P Calado; C J Harrison; J Vormoor Journal: Leukemia Date: 2015-05-06 Impact factor: 11.528
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Authors: Maribel Forero-Castro; Cristina Robledo; Rocío Benito; Irene Bodega-Mayor; Inmaculada Rapado; María Hernández-Sánchez; María Abáigar; Jesús Maria Hernández-Sánchez; Miguel Quijada-Álamo; José María Sánchez-Pina; Mónica Sala-Valdés; Fernanda Araujo-Silva; Alexander Kohlmann; José Luis Fuster; Maryam Arefi; Natalia de Las Heras; Susana Riesco; Juan N Rodríguez; Lourdes Hermosín; Jordi Ribera; Mireia Camos Guijosa; Manuel Ramírez; Cristina Díaz de Heredia Rubio; Eva Barragán; Joaquín Martínez; José M Ribera; Elena Fernández-Ruiz; Jesús-María Hernández-Rivas Journal: Br J Cancer Date: 2017-05-30 Impact factor: 7.640
Authors: Eric T Clambey; Bernard Collins; Mary H Young; Jens Eberlein; Alexandria David; John W Kappler; Philippa Marrack Journal: PLoS One Date: 2013-02-26 Impact factor: 3.240