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急性髓系白血病的高维分析揭示诱导治疗期间持续细胞的表型变化。

High-Dimensional Analysis of Acute Myeloid Leukemia Reveals Phenotypic Changes in Persistent Cells during Induction Therapy.

作者信息

Ferrell Paul Brent, Diggins Kirsten Elizabeth, Polikowsky Hannah Grace, Mohan Sanjay Ram, Seegmiller Adam C, Irish Jonathan Michael

机构信息

Department of Medicine, Division of Hematology/Oncology, Vanderbilt University Medical Center, Nashville, Tennessee, United States of America.

Department of Cancer Biology, Vanderbilt University, Nashville, Tennessee, United States of America.

出版信息

PLoS One. 2016 Apr 13;11(4):e0153207. doi: 10.1371/journal.pone.0153207. eCollection 2016.

Abstract

The plasticity of AML drives poor clinical outcomes and confounds its longitudinal detection. However, the immediate impact of treatment on the leukemic and non-leukemic cells of the bone marrow and blood remains relatively understudied. Here, we conducted a pilot study of high dimensional longitudinal monitoring of immunophenotype in AML. To characterize changes in cell phenotype before, during, and immediately after induction treatment, we developed a 27-antibody panel for mass cytometry focused on surface diagnostic markers and applied it to 46 samples of blood or bone marrow tissue collected over time from 5 AML patients. Central goals were to determine whether changes in AML phenotype would be captured effectively by cytomic tools and to implement methods for describing the evolving phenotypes of AML cell subsets. Mass cytometry data were analyzed using established computational techniques. Within this pilot study, longitudinal immune monitoring with mass cytometry revealed fundamental changes in leukemia phenotypes that occurred over time during and after induction in the refractory disease setting. Persisting AML blasts became more phenotypically distinct from stem and progenitor cells due to expression of novel marker patterns that differed from pre-treatment AML cells and from all cell types observed in healthy bone marrow. This pilot study of single cell immune monitoring in AML represents a powerful tool for precision characterization and targeting of resistant disease.

摘要

急性髓系白血病(AML)的可塑性导致了较差的临床预后,并使其纵向检测变得复杂。然而,治疗对骨髓和血液中白血病细胞和非白血病细胞的即时影响仍相对缺乏研究。在此,我们开展了一项针对AML免疫表型进行高维纵向监测的试点研究。为了表征诱导治疗前、治疗期间和治疗后细胞表型的变化,我们开发了一个用于质谱流式细胞术的包含27种抗体的组合,重点关注表面诊断标志物,并将其应用于从5例AML患者随时间收集的46份血液或骨髓组织样本。核心目标是确定细胞组学工具是否能有效捕捉AML表型的变化,并实施描述AML细胞亚群演变表型的方法。使用既定的计算技术对质谱流式细胞术数据进行分析。在这项试点研究中,通过质谱流式细胞术进行的纵向免疫监测揭示了难治性疾病环境中诱导治疗期间和之后随时间发生的白血病表型的根本变化。由于新标记模式的表达,持续存在的AML母细胞在表型上与干细胞和祖细胞的差异变得更大,这些新标记模式不同于治疗前的AML细胞以及健康骨髓中观察到的所有细胞类型。这项关于AML单细胞免疫监测的试点研究是精确表征和靶向耐药疾病的有力工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c710/4830605/cfc1b95c3d2a/pone.0153207.g001.jpg

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