Comprehensive molecular characterization of a rare case of Philadelphia chromosome-positive acute myeloid leukemia.

IF 1.8 Q3 MEDICINE, RESEARCH & EXPERIMENTAL Cold Spring Harbor Molecular Case Studies Pub Date : 2022-10-01 DOI:10.1101/mcs.a006218
Mara W Rosenberg, Samantha L Savage, Christopher A Eide, Anna Reister Schultz, Rachel J Cook, Richard D Press, Carole Rempfer, Garrett Eickelberg, Beth Wilmot, Shannon K McWeeney, Jeffrey W Tyner, Brian J Druker, Cristina E Tognon
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Abstract

The Philadelphia chromosome (Ph) resulting from the t(9;22) translocation generates the oncogenic BCR::ABL1 fusion protein that is most commonly associated with chronic myeloid leukemia (CML) and Ph-positive (Ph+) acute lymphoblastic leukemia (ALL). There are also rare instances of patients (≤1%) with newly diagnosed acute myeloid leukemia (AML) that harbor this translocation (Paietta et al., Leukemia 12: 1881 [1998]; Keung et al., Leuk Res 28: 579 [2004]; Soupir et al., Am J Clin Pathol 127: 642 [2007]). AML with BCR::ABL has only recently been provisionally classified by the World Health Organization as a diagnostically distinct subtype of AML. Discernment from the extremely close differential diagnosis of myeloid blast crisis CML is challenging, largely relying on medical history rather than clinical characteristics (Arber et al., Blood 127: 2391 [2016]). To gain insight into the genomic features underlying the evolution of AML with BCR::ABL, we identified a patient presenting with a high-risk myelodysplastic syndrome that acquired a BCR::ABL alteration after a peripheral blood stem cell transplant. Serial samples were collected and analyzed using whole-exome sequencing, RNA-seq, and ex vivo functional drug screens. Persistent subclones were identified, both at diagnosis and at relapse, including an SF3B1p.Lys700Glu mutation that later cooccurred with an NRASp.Gly12Cys mutation. Functional ex vivo drug screening performed on primary patient cells suggested that combination therapies of ABL1 with RAS or PI3K pathway inhibitors could have augmented the patient's response throughout the course of disease. Together, our findings argue for the importance of genomic profiling and the potential value of ABL1 inhibitor-inclusive combination treatment strategies in patients with this rare disease.

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1例罕见费城染色体阳性急性髓性白血病的综合分子特征分析。
由t(9;22)易位引起的费城染色体(Ph)产生致癌的BCR::ABL1融合蛋白,这种融合蛋白最常与慢性髓性白血病(CML)和Ph阳性急性淋巴细胞白血病(ALL)相关。新诊断的急性髓性白血病(AML)患者中也有罕见的(≤1%)存在这种易位(Paietta et al., leukemia 12: 1881 [1998];杨志强等,中华医学杂志28 (3):579 [2004];王晓燕,王晓燕,王晓燕,等[2007]。AML合并BCR: ABL直到最近才被世界卫生组织暂时归类为AML的一种诊断上不同的亚型。髓母细胞危象CML的极接近鉴别诊断具有挑战性,主要依赖于病史而非临床特征(Arber et al., Blood 127: 2391[2016])。为了深入了解AML伴BCR::ABL进化的基因组特征,我们确定了一位外周血干细胞移植后获得BCR::ABL改变的高危骨髓增生异常综合征患者。收集系列样品并使用全外显子组测序,RNA-seq和体外功能药物筛选进行分析。在诊断和复发时均鉴定出持久性亚克隆,包括SF3B1p。Lys700Glu突变随后与NRASp一起发生。Gly12Cys突变。对原代患者细胞进行的功能性体外药物筛选表明,ABL1与RAS或PI3K途径抑制剂的联合治疗可能在整个疾病过程中增强了患者的反应。总之,我们的研究结果证明了基因组分析的重要性以及ABL1抑制剂-包容性联合治疗策略在这种罕见疾病患者中的潜在价值。
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来源期刊
Cold Spring Harbor Molecular Case Studies
Cold Spring Harbor Molecular Case Studies MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
3.20
自引率
0.00%
发文量
54
期刊介绍: Cold Spring Harbor Molecular Case Studies is an open-access, peer-reviewed, international journal in the field of precision medicine. Articles in the journal present genomic and molecular analyses of individuals or cohorts alongside their clinical presentations and phenotypic information. The journal''s purpose is to rapidly share insights into disease development and treatment gained by application of genomics, proteomics, metabolomics, biomarker analysis, and other approaches. The journal covers the fields of cancer, complex diseases, monogenic disorders, neurological conditions, orphan diseases, infectious disease, gene therapy, and pharmacogenomics. It has a rapid peer-review process that is based on technical evaluation of the analyses performed, not the novelty of findings, and offers a swift, clear path to publication. The journal publishes: Research Reports presenting detailed case studies of individuals and small cohorts, Research Articles describing more extensive work using larger cohorts and/or functional analyses, Rapid Communications presenting the discovery of a novel variant and/or novel phenotype associated with a known disease gene, Rapid Cancer Communications presenting the discovery of a novel variant or combination of variants in a cancer type, Variant Discrepancy Resolution describing efforts to resolve differences or update variant interpretations in ClinVar through case-level data sharing, Follow-up Reports linked to previous observations, Plus Review Articles, Editorials, and Position Statements on best practices for research in precision medicine.
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