Single-Cell RNA-Seq Reveals AML Hierarchies Relevant to Disease Progression and Immunity

单细胞RNA测序揭示与疾病进展和免疫相关的AML层级结构

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作者:Peter van Galen ,Volker Hovestadt ,Marc H Wadsworth Ii ,Travis K Hughes ,Gabriel K Griffin ,Sofia Battaglia ,Julia A Verga ,Jason Stephansky ,Timothy J Pastika ,Jennifer Lombardi Story ,Geraldine S Pinkus ,Olga Pozdnyakova ,Ilene Galinsky ,Richard M Stone ,Timothy A Graubert ,Alex K Shalek ,Jon C Aster ,Andrew A Lane ,Bradley E Bernstein

Abstract

Acute myeloid leukemia (AML) is a heterogeneous disease that resides within a complex microenvironment, complicating efforts to understand how different cell types contribute to disease progression. We combined single-cell RNA sequencing and genotyping to profile 38,410 cells from 40 bone marrow aspirates, including 16 AML patients and five healthy donors. We then applied a machine learning classifier to distinguish a spectrum of malignant cell types whose abundances varied between patients and between subclones in the same tumor. Cell type compositions correlated with prototypic genetic lesions, including an association of FLT3-ITD with abundant progenitor-like cells. Primitive AML cells exhibited dysregulated transcriptional programs with co-expression of stemness and myeloid priming genes and had prognostic significance. Differentiated monocyte-like AML cells expressed diverse immunomodulatory genes and suppressed T cell activity in vitro. In conclusion, we provide single-cell technologies and an atlas of AML cell states, regulators, and markers with implications for precision medicine and immune therapies. VIDEO .

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