Model-Based Assessment of the Role of Uneven Partitioning of Molecular Content on Heterogeneity and Regulation of Differentiation in CD8 T-Cell Immune Responses

Activation of naive CD8 T-cells can lead to the generation of multiple effector and memory subsets. Multiple parameters associated with activation conditions are involved in generating this diversity that is associated with heterogeneous molecular contents of activated cells. Although naive cell pol...

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Published inFrontiers in immunology Vol. 10; p. 230
Main Authors Girel, Simon, Arpin, Christophe, Marvel, Jacqueline, Gandrillon, Olivier, Crauste, Fabien
Format Journal Article
LanguageEnglish
Published Switzerland Frontiers 19.02.2019
Frontiers Media S.A
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Summary:Activation of naive CD8 T-cells can lead to the generation of multiple effector and memory subsets. Multiple parameters associated with activation conditions are involved in generating this diversity that is associated with heterogeneous molecular contents of activated cells. Although naive cell polarisation upon antigenic stimulation and the resulting asymmetric division are known to be a major source of heterogeneity and cell fate regulation, the consequences of stochastic uneven partitioning of molecular content upon subsequent divisions remain unclear yet. Here we aim at studying the impact of uneven partitioning on molecular-content heterogeneity and then on the immune response dynamics at the cellular level. To do so, we introduce a multiscale mathematical model of the CD8 T-cell immune response in the lymph node. In the model, cells are described as agents evolving and interacting in a 2D environment while a set of differential equations, embedded in each cell, models the regulation of intra and extracellular proteins involved in cell differentiation. Based on the analysis of data at the single cell level, we show that immune response dynamics can be explained by the molecular-content heterogeneity generated by uneven partitioning at cell division. In particular, uneven partitioning acts as a regulator of cell differentiation and induces the emergence of two coexisting sub-populations of cells exhibiting antagonistic fates. We show that the degree of unevenness of molecular partitioning, along all cell divisions, affects the outcome of the immune response and can promote the generation of memory cells.
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PMCID: PMC6392104
This article was submitted to Molecular Innate Immunity, a section of the journal Frontiers in Immunology
Edited by: Gennady Bocharov, Institute of Numerical Mathematics (RAS), Russia
Reviewed by: Filippo Castiglione, Italian National Research Council (CNR), Italy; Yinghong Hu, Emory University, United States
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2019.00230