BACKGROUND: B-cell acute lymphoblastic leukemia (B-ALL) is classified into subgroups based on known driver oncogenes and molecular lesions, including translocations and recurrent mutations. However, the current diagnostic tests do not identify subtypes or oncogenic lesions for all B-ALL samples, creating a heterogeneous B-ALL group of unknown subtypes. METHODS: We sorted primary adult B-ALL cells and performed transcriptome analysis by bulk RNA sequencing (RNA-seq). RESULTS: Transcriptomic analysis of an adult B-ALL cohort allowed the classification of four patient samples with subtypes that were not previously revealed by standard gene panels. The leukemia of two patients were of the DUX4 subtype and two were CRLF2(+) Ph-like B-ALL. Furthermore, single nucleotide variant analysis detected the oncogenic NRAS-G12D, KRAS-G12D, and KRAS-G13D mutations in three of the patient samples, presenting targetable mutations. Additional oncogenic variants and gene fusions were uncovered, as well as multiple variants in the PDE4DIP gene across five of the patient samples. CONCLUSION: We demonstrate that RNA-seq is an effective tool for precision medicine in B-ALL by providing comprehensive molecular profiling of leukemia cells, identifying subtype and oncogenic lesions, and stratifying patients for appropriate therapy.
Transcriptome analysis of primary adult B-cell lineage acute lymphoblastic leukemia identifies pathogenic variants and gene fusions, and predicts subtypes for in depth molecular diagnosis.
对原发性成人 B 细胞谱系急性淋巴细胞白血病进行转录组分析,可识别致病变异和基因融合,并预测亚型以进行深入的分子诊断
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作者:Podgorica Mirjam, Drivet Elsa, Viken Jonas Krag, Richman Alyssa, Vestbøstad Johanne, Szodoray Peter, Kvam Ann Kristin, Wik Hilde Skuterud, Tjønnfjord Geir E, Munthe Ludvig A, Frietze Seth, Schjerven Hilde
| 期刊: | European Journal of Haematology | 影响因子: | 2.300 |
| 时间: | 2024 | 起止号: | 2024 May;112(5):731-742 |
| doi: | 10.1111/ejh.14164 | 研究方向: | 细胞生物学 |
| 疾病类型: | 白血病 | ||
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