Literature DB >> 24035899

Deconstructing stem cell population heterogeneity: single-cell analysis and modeling approaches.

Jincheng Wu1, Emmanuel S Tzanakakis.   

Abstract

Isogenic stem cell populations display cell-to-cell variations in a multitude of attributes including gene or protein expression, epigenetic state, morphology, proliferation and proclivity for differentiation. The origins of the observed heterogeneity and its roles in the maintenance of pluripotency and the lineage specification of stem cells remain unclear. Addressing pertinent questions will require the employment of single-cell analysis methods as traditional cell biochemical and biomolecular assays yield mostly population-average data. In addition to time-lapse microscopy and flow cytometry, recent advances in single-cell genomic, transcriptomic and proteomic profiling are reviewed. The application of multiple displacement amplification, next generation sequencing, mass cytometry and spectrometry to stem cell systems is expected to provide a wealth of information affording unprecedented levels of multiparametric characterization of cell ensembles under defined conditions promoting pluripotency or commitment. Establishing connections between single-cell analysis information and the observed phenotypes will also require suitable mathematical models. Stem cell self-renewal and differentiation are orchestrated by the coordinated regulation of subcellular, intercellular and niche-wide processes spanning multiple time scales. Here, we discuss different modeling approaches and challenges arising from their application to stem cell populations. Integrating single-cell analysis with computational methods will fill gaps in our knowledge about the functions of heterogeneity in stem cell physiology. This combination will also aid the rational design of efficient differentiation and reprogramming strategies as well as bioprocesses for the production of clinically valuable stem cell derivatives.
© 2013 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Flow cytometry; Gene expression noise; Heterogeneity; Human embryonic stem cells; Induced pluripotent stem cells; Mass cytometry; Multiple displacement amplification; Single-cell analysis; Stochastic multiscale model; Time-lapse microscopy

Mesh:

Year:  2013        PMID: 24035899      PMCID: PMC3956452          DOI: 10.1016/j.biotechadv.2013.09.001

Source DB:  PubMed          Journal:  Biotechnol Adv        ISSN: 0734-9750            Impact factor:   14.227


  153 in total

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Authors:  Thomas Graf; Matthias Stadtfeld
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4.  Combined transcriptome and genome analysis of single micrometastatic cells.

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5.  Quantitative flow cytometry: inter-laboratory variation.

Authors:  V E Zenger; R Vogt; F Mandy; A Schwartz; G E Marti
Journal:  Cytometry       Date:  1998-10-01

6.  Visualizing spatiotemporal dynamics of multicellular cell-cycle progression.

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8.  Direct cell reprogramming is a stochastic process amenable to acceleration.

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9.  A large-scale proteomic analysis of human embryonic stem cells.

Authors:  Thomas C Schulz; Anna Maria Swistowska; Ying Liu; Andrzej Swistowski; Gail Palmarini; Sandii N Brimble; Eric Sherrer; Allan J Robins; Mahendra S Rao; Xianmin Zeng
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5.  Single-Cell-Based Analysis Highlights a Surge in Cell-to-Cell Molecular Variability Preceding Irreversible Commitment in a Differentiation Process.

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Review 6.  Microfluidic Sample Preparation for Single Cell Analysis.

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Review 7.  Biologically Relevant Heterogeneity: Metrics and Practical Insights.

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Review 8.  The function of chromatin modifiers in lineage commitment and cell fate specification.

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Review 9.  Extracellular matrix: a dynamic microenvironment for stem cell niche.

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10.  Temperature-induced variation in gene expression burst size in metazoan cells.

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