作者
Emmanuelle Clappier, Bastien Gerby, François Sigaux, Marc Delord, Farah Touzri, Lucie Hernandez, Paola Ballerini, André Baruchel, Françoise Pflumio, Jean Soulier
发表日期
2011/4/11
期刊
Journal of Experimental Medicine
卷号
208
期号
4
页码范围
653-661
出版商
The Rockefeller University Press
简介
Genomic studies in human acute lymphoblastic leukemia (ALL) have revealed clonal heterogeneity at diagnosis and clonal evolution at relapse. In this study, we used genome-wide profiling to compare human T cell ALL samples at the time of diagnosis and after engraftment (xenograft) into immunodeficient recipient mice. Compared with paired diagnosis samples, the xenograft leukemia often contained additional genomic lesions in established human oncogenes and/or tumor suppressor genes. Mimicking such genomic lesions by short hairpin RNA–mediated knockdown in diagnosis samples conferred a selective advantage in competitive engraftment experiments, demonstrating that additional lesions can be drivers of increased leukemia-initiating activity. In addition, the xenograft leukemias appeared to arise from minor subclones existing in the patient at diagnosis. Comparison of paired diagnosis and relapse …
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