作者
Sarra L Ryan, John F Peden, Zoya Kingsbury, Claire J Schwab, Terena James, Petri Polonen, Martina Mijuskovic, Jenn Becq, Richard Yim, Ruth E Cranston, Dale J Hedges, Kathryn G Roberts, Charles G Mullighan, Ajay Vora, Lisa J Russell, Robert Bain, Anthony V Moorman, David R Bentley, Christine J Harrison, Mark T Ross
发表日期
2023/3
期刊
Leukemia
卷号
37
期号
3
页码范围
518-528
出版商
Nature Publishing Group UK
简介
Childhood B-cell acute lymphoblastic leukaemia (B-ALL) is characterised by recurrent genetic abnormalities that drive risk-directed treatment strategies. Using current techniques, accurate detection of such aberrations can be challenging, due to the rapidly expanding list of key genetic abnormalities. Whole genome sequencing (WGS) has the potential to improve genetic testing, but requires comprehensive validation. We performed WGS on 210 childhood B-ALL samples annotated with clinical and genetic data. We devised a molecular classification system to subtype these patients based on identification of key genetic changes in tumour-normal and tumour-only analyses. This approach detected 294 subtype-defining genetic abnormalities in 96% (202/210) patients. Novel genetic variants, including fusions involving genes in the MAP kinase pathway, were identified. WGS results were concordant with standard-of …
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SL Ryan, JF Peden, Z Kingsbury, CJ Schwab, T James… - Leukemia, 2023