Stochastic effects and bistability in T cell receptor signaling

Lipniacki, Tomasz; Hat, Beata; Faeder, James R.; Hlavacek, William S.

doi:10.1016/j.jtbi.2008.05.001

Cited by 84 publications

(124 citation statements)

References 42 publications

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“…Thus variations in ppERK concentration would change the ability of the cell to signal. Interpretations of results in Lipniacki et al [11] give further weight to this not a positive feedback argument. Changes in Lck concentration influence pSHP1 levels far more than ppERK levels, if ppERK were in positive feedback the action of Lck would be part of the feedback loop and so would influence ppERK levels.…”

Section: Breaking the Negative Feedbackmentioning

confidence: 94%

“…A set of signalling events that involve kinetic proofreading, a negative influence from SH2 domain-containing phosphatase (SHP1) and a positive influence from extracellular signal regulated kinase (ERK) have been discussed in reference to tunability in [2,5] and have been experimentally investigated in [6,7]. This system has also received much modelling attention in [7][8][9][10][11]. The important quantitative and qualitative concepts that these signalling events impose on T cell discrimination are well summarised in Chan et al [8].…”

Section: Introductionmentioning

confidence: 99%

“…To this end [7] achieves a model of 557 chemical reaction equations which are converted to 238 ordinary differential equations. Artyomov et al [9] and Lipniacki et al [11] both produce simplified versions of the concepts in the ABG model and perform stochastic analysis. [9,11] argue the importance of stochastic modelling particularly when small molecule numbers can produce bistabilities in a stochastic model that do not exist in the deterministic model.…”

Section: Introductionmentioning

confidence: 99%

“…The simplified models analysed in [8,9,11] convey an understanding of the qualitative aspects of TCR, SHP1, ERK signalling. We take this opportunity to dissect the biologically detailed ABG model with the objective of gaining clarified understanding of the biological processes that contribute to the qualitative behaviour.…”

Section: Introductionmentioning

confidence: 99%

“…Here we stochastically analyse the entire ABG model 1 by investigating behaviour at the single TCR level and progressively include components to compose the entire model. With this compositional analysis we achieve a greater understanding of the elements of the model without the simplifying assumptions of [11].…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Elucidation of T cell signalling models

Owens

Timmis

Greensted

et al. 2010

Journal of Theoretical Biology

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A potential mechanism that allows T cells to reliably discriminate pMHC ligands involves an interplay between kinetic proofreading, negative feedback and a destruction of this negative feedback. We analyse a detailed model of these mechanisms which involves the TCR, SHP1 and ERK. We discover that the behaviour of pSHP1 negative feedback is of primary importance, and particularly the influence of a kinetic proofreading base negative feedback state on pSHP1 dynamics. The CD8 co-receptor is shown to benefit from a kinetic proofreading locking mechanism and is able to overcome pSHP1 negative influences to sensitise a T cell.

show abstract

Section: Breaking the Negative Feedbackmentioning

confidence: 94%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Elucidation of T cell signalling models

Owens

Timmis

Greensted

et al. 2010

Journal of Theoretical Biology

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Towards multiscale modeling of the CD8⁺ T cell response to viral infections

Baral

Raja

Sen

et al. 2019

WIREs Mechanisms of Disease

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The CD8 + T cell response is critical to the control of viral infections. Yet, defining the CD8 + T cell response to viral infections quantitatively has been a challenge. Following antigen recognition, which triggers an intracellular signaling cascade, CD8 + T cells can differentiate into effector cells, which proliferate rapidly and destroy infected cells. When the infection is cleared, they leave behind memory cells for quick recall following a second challenge. If the infection persists, the cells may become exhausted, retaining minimal control of the infection while preventing severe immunopathology. These activation, proliferation and differentiation processes as well as the mounting of the effector response are intrinsically multiscale and collective phenomena. Remarkable experimental advances in the recent years, especially at the single cell level, have enabled a quantitative characterization of several underlying processes. Simultaneously, sophisticated mathematical models have begun to be constructed that describe these multiscale phenomena, bringing us closer to a comprehensive description of the CD8 + T cell response to viral infections. Here, we review the advances made and summarize the challenges and opportunities ahead. This article is categorized under: Analytical and Computational Methods > Computational Methods Biological Mechanisms > Cell Fates Biological Mechanisms > Cell Signaling Models of Systems Properties and Processes > Mechanistic Models

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Leveraging Modeling Approaches: Reaction Networks and Rules

Blinov

Moraru

2011

Advances in Experimental Medicine and Biology

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We have witnessed an explosive growth in research involving mathematical models and computer simulations of intracellular molecular interactions, ranging from metabolic pathways to signaling and gene regulatory networks. Many software tools have been developed to aid in the study of such biological systems, some of which have a wealth of features for model building and visualization, and powerful capabilities for simulation and data analysis. Novel high resolution and/or high throughput experimental techniques have led to an abundance of qualitative and quantitative data related to the spatio-temporal distribution of molecules and complexes, their interactions kinetics, and functional modifications. Based on this information, computational biology researchers are attempting to build larger and more detailed models. However, this has proved to be a major challenge. Traditionally, modeling tools require the explicit specification of all molecular species and interactions in a model, which can quickly become a major limitation in the case of complex networks – the number of ways biomolecules can combine to form multimolecular complexes can be combinatorially large. Recently, a new breed of software tools has been created to address the problems faced when building models marked by combinatorial complexity. These have a different approach for model specification, using reaction rules and species patterns. Here we compare the traditional modeling approach with the new rule-based methods. We make a case for combining the capabilities of conventional simulation software with the unique features and flexibility of a rule-based approach in a single software platform for building models of molecular interaction networks.

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Stochastic effects and bistability in T cell receptor signaling

Cited by 84 publications

References 42 publications

Elucidation of T cell signalling models

Elucidation of T cell signalling models

Towards multiscale modeling of the CD8⁺ T cell response to viral infections

Leveraging Modeling Approaches: Reaction Networks and Rules

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Stochastic effects and bistability in T cell receptor signaling

Cited by 84 publications

References 42 publications

Elucidation of T cell signalling models

Elucidation of T cell signalling models

Towards multiscale modeling of the CD8+ T cell response to viral infections

Leveraging Modeling Approaches: Reaction Networks and Rules

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Product

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Towards multiscale modeling of the CD8⁺ T cell response to viral infections