Multipotent lineage potential in B cell acute lymphoblastic leukemia is associated with distinct cellular origins and clinical features.

IF 23.5 1区医学 Q1 ONCOLOGY

Nature cancer Pub Date : 2025-06-27 DOI:10.1038/s43018-025-00987-2

Ilaria Iacobucci, Andy G X Zeng, Qingsong Gao, Laura Garcia-Prat, Pradyumna Baviskar, Sayyam Shah, Alex Murison, Veronique Voisin, Michelle Chan-Seng-Yue, Cheng Cheng, Chunxu Qu, Colin Bailey, Matthew Lear, Matthew T Witkowski, Xin Zhou, Airen Zaldivar Peraza, Karishma Gangwani, Anjali S Advani, Selina M Luger, Mark R Litzow, Jacob M Rowe, Elisabeth M Paietta, Wendy Stock, John E Dick, Charles G Mullighan

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引用次数: 0

Abstract

Developmental origins and their associations with lineage plasticity and treatment response in B-cell progenitor acute lymphoblastic leukemia (B-ALL) are mostly unexplored. Here, we integrated single-cell transcriptome sequencing (scRNA-seq) of 89 B-ALL samples with a single-cell atlas of normal human B cell development incorporating functional and molecular assays. We observed subtype- and sample-dependent correlation with normal developmental stage, with intra-subtype and intra-patient heterogeneity. We show that subtypes prone to shift from the B-lineage (for example BCR::ABL1, KMT2A-R and DUX4-R B-ALL) are enriched for multipotent progenitors and show this developmental stage exhibits CEBPA activation and retains myeloid potential, providing a mechanistic explanation for this clinical observation. We developed a 'multipotency score' most enriched in subtypes exhibiting lineage plasticity that was independently associated with inferior survival. Thus, multipotent B-ALL states reflect the early progenitor origins of a subset of patients with B-ALL and may be relevant for understanding lineage shifting following conventional chemotherapy or immunotherapies.

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B细胞急性淋巴细胞白血病的多能谱系潜力与不同的细胞起源和临床特征有关。

b细胞祖细胞急性淋巴细胞白血病（B-ALL）的发育起源及其与谱系可塑性和治疗反应的关系大多未被探索。在这里，我们将89个B- all样本的单细胞转录组测序（scRNA-seq）与正常人类B细胞发育的单细胞图谱结合功能和分子分析相结合。我们观察到亚型和样本依赖与正常发育阶段的相关性，以及亚型内和患者内的异质性。我们发现易于从b谱系转移的亚型（例如BCR::ABL1， KMT2A-R和DUX4-R B-ALL）富含多能祖细胞，并且表明这一发育阶段表现出CEBPA激活并保留髓细胞潜能，为这一临床观察提供了机制解释。我们开发了一种“多能性评分”，该评分最丰富的亚型表现出谱系可塑性，与低生存率独立相关。因此，多能性B-ALL状态反映了B-ALL患者亚群的早期祖细胞起源，可能与理解常规化疗或免疫治疗后的谱系转移有关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Nature cancer Medicine-Oncology

CiteScore

31.10

自引率

1.80%

发文量

129

期刊介绍： Cancer is a devastating disease responsible for millions of deaths worldwide. However, many of these deaths could be prevented with improved prevention and treatment strategies. To achieve this, it is crucial to focus on accurate diagnosis, effective treatment methods, and understanding the socioeconomic factors that influence cancer rates. Nature Cancer aims to serve as a unique platform for sharing the latest advancements in cancer research across various scientific fields, encompassing life sciences, physical sciences, applied sciences, and social sciences. The journal is particularly interested in fundamental research that enhances our understanding of tumor development and progression, as well as research that translates this knowledge into clinical applications through innovative diagnostic and therapeutic approaches. Additionally, Nature Cancer welcomes clinical studies that inform cancer diagnosis, treatment, and prevention, along with contributions exploring the societal impact of cancer on a global scale. In addition to publishing original research, Nature Cancer will feature Comments, Reviews, News & Views, Features, and Correspondence that hold significant value for the diverse field of cancer research.