Single-cell analysis and functional characterization uncover the stem cell hierarchies and developmental origins of rhabdomyosarcoma

单细胞分析和功能表征揭示横纹肌肉瘤的干细胞层次和发育起源

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作者:Yun Wei #, Qian Qin #, Chuan Yan, Madeline N Hayes, Sara P Garcia, Haibin Xi, Daniel Do, Alexander H Jin, Tiffany C Eng, Karin M McCarthy, Abhinav Adhikari, Maristela L Onozato, Dimitrios Spentzos, Gunnlaugur P Neilsen, A John Iafrate, Leonard H Wexler, April D Pyle, Mario L Suvà, Filemon Dela Cruz,

Abstract

Rhabdomyosarcoma (RMS) is a common childhood cancer that shares features with developing skeletal muscle. Yet, the conservation of cellular hierarchy with human muscle development and the identification of molecularly defined tumor-propagating cells has not been reported. Using single-cell RNA-sequencing, DNA-barcode cell fate mapping and functional stem cell assays, we uncovered shared tumor cell hierarchies in RMS and human muscle development. We also identified common developmental stages at which tumor cells become arrested. Fusion-negative RMS cells resemble early myogenic cells found in embryonic and fetal development, while fusion-positive RMS cells express a highly specific gene program found in muscle cells transiting from embryonic to fetal development at 7-7.75 weeks of age. Fusion-positive RMS cells also have neural pathway-enriched states, suggesting less-rigid adherence to muscle-lineage hierarchies. Finally, we identified a molecularly defined tumor-propagating subpopulation in fusion-negative RMS that shares remarkable similarity to bi-potent, muscle mesenchyme progenitors that can make both muscle and osteogenic cells.

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