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CoSpar 从单细胞转录组和谱系信息中识别早期细胞命运偏向。

CoSpar identifies early cell fate biases from single-cell transcriptomic and lineage information.

机构信息

Department of Systems Biology, Blavatnik Institute, Harvard Medical School, Boston, MA, USA.

Center for Regenerative Medicine of Boston University and Boston Medical Center, Boston, MA, USA.

出版信息

Nat Biotechnol. 2022 Jul;40(7):1066-1074. doi: 10.1038/s41587-022-01209-1. Epub 2022 Feb 21.

Abstract

A goal of single-cell genome-wide profiling is to reconstruct dynamic transitions during cell differentiation, disease onset and drug response. Single-cell assays have recently been integrated with lineage tracing, a set of methods that identify cells of common ancestry to establish bona fide dynamic relationships between cell states. These integrated methods have revealed unappreciated cell dynamics, but their analysis faces recurrent challenges arising from noisy, dispersed lineage data. In this study, we developed coherent, sparse optimization (CoSpar) as a robust computational approach to infer cell dynamics from single-cell transcriptomics integrated with lineage tracing. Built on assumptions of coherence and sparsity of transition maps, CoSpar is robust to severe downsampling and dispersion of lineage data, which enables simpler experimental designs and requires less calibration. In datasets representing hematopoiesis, reprogramming and directed differentiation, CoSpar identifies early fate biases not previously detected, predicting transcription factors and receptors implicated in fate choice. Documentation and detailed examples for common experimental designs are available at https://cospar.readthedocs.io/ .

摘要

单细胞全基因组分析的目标是重建细胞分化、疾病发生和药物反应过程中的动态转变。单细胞分析最近已经与谱系追踪相结合,谱系追踪是一组确定共同祖先细胞的方法,用于建立细胞状态之间真实的动态关系。这些集成方法揭示了以前未被注意到的细胞动态,但它们的分析面临着反复出现的挑战,这些挑战源于嘈杂、分散的谱系数据。在这项研究中,我们开发了连贯稀疏优化(CoSpar),作为一种从单细胞转录组学与谱系追踪集成推断细胞动力学的稳健计算方法。CoSpar 基于对过渡图的连贯性和稀疏性的假设,对谱系数据的严重下采样和分散具有鲁棒性,这使得实验设计更简单,并且需要更少的校准。在代表造血、重编程和定向分化的数据集上,CoSpar 识别出以前未检测到的早期命运偏向,预测了涉及命运选择的转录因子和受体。常见实验设计的文档和详细示例可在 https://cospar.readthedocs.io/ 上获得。

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