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Literature DB >> 21276803

T cell state transition produces an emergent change detector.

Abstract

We model the stages of a T cell response from initial activation to T cell expansion and contraction using a system of ordinary differential equations. Results of this modeling suggest that state transitions enable the T cell population to detect change and respond effectively to changes in antigen stimulation levels, rather than simply the presence or absence of antigen. A key component of the system that gives rise to this emergent change detector is initial activation of naïve T cells. The activation step creates a barrier that separates the long-term, slow dynamics of naïve T cells from the short-term, fast dynamics of effector T cells. This separation allows the T cell population to compare current, up-to-date changes in antigen levels to long-term, steady state levels. As a result, the T cell population responds very effectively to sudden shifts in antigen levels, even if the antigen were already present prior to the change. This feature provides a mechanism for T cells to react to rapidly expanding sources of antigen stimulation, such as viruses, while maintaining tolerance to constant or slowly fluctuating sources of stimulation, such as healthy tissue during growth. In addition to modeling T cell activation, we also formulate a model of the proliferation of effector T cells in response to the consumption of positive growth signal, secreted throughout the T cell response. We discuss how the interaction between T cells and growth signal generates an emergent threshold detector that responds preferentially to large changes in antigen stimulation while ignoring small ones. As a final step, we discuss how the de novo generation of adaptive regulatory T cells during the latter phase of the T cell response creates a negative feedback loop that controls the duration and magnitude of the T cell response. Hence, the immune network continually adjusts to a shifting baseline of (self and non-self) antigens, and responds primarily to abrupt changes in these antigens rather than merely their presence or absence.

Entities: Chemical Disease Gene Species

Mesh：

Year: 2011 PMID： 21276803 PMCID： PMC3050581 DOI： 10.1016/j.jtbi.2011.01.031

Source DB: PubMed Journal: J Theor Biol ISSN： 0022-5193 Impact factor: 2.691

31 in total

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2. Increased turnover of T lymphocytes in HIV-1 infection and its reduction by antiretroviral therapy.

Authors: H Mohri; A S Perelson; K Tung; R M Ribeiro; B Ramratnam; M Markowitz; R Kost; A Hurley; L Weinberger; D Cesar; M K Hellerstein; D D Ho
Journal: J Exp Med Date: 2001-11-05 Impact factor: 14.307

3. Models of CD8+ responses: 1. What is the antigen-independent proliferation program.

Authors: Rustom Antia; Carl T Bergstrom; Sergei S Pilyugin; Susan M Kaech; Rafi Ahmed
Journal: J Theor Biol Date: 2003-04-21 Impact factor: 2.691

4. Different dynamics of CD4+ and CD8+ T cell responses during and after acute lymphocytic choriomeningitis virus infection.

Authors: Rob J De Boer; Dirk Homann; Alan S Perelson
Journal: J Immunol Date: 2003-10-15 Impact factor: 5.422

10. Separation of helper T cells from suppressor T cells expressing different Ly components. II. Activation by antigen: after immunization, antigen-specific suppressor and helper activities are mediated by distinct T-cell subclasses.

Authors: H Cantor; F W Shen; E A Boyse
Journal: J Exp Med Date: 1976-06-01 Impact factor: 14.307

2 in total

1. A shadow detector for photosynthesis efficiency.

Authors: Kang-Ling Liao; Roger D Jones; Patrick McCarter; Meral Tunc-Ozdemir; James A Draper; Timothy C Elston; David Kramer; Alan M Jones
Journal: J Theor Biol Date: 2016-12-03 Impact factor: 2.691

Review 2. Immunological Paradigms, Mechanisms, and Models: Conceptual Understanding Is a Prerequisite to Effective Modeling.

Authors: Zvi Grossman
Journal: Front Immunol Date: 2019-11-05 Impact factor: 7.561

2 in total

T cell state transition produces an emergent change detector.

1. Modelling T-cell-mediated suppression dependent on interactions in multicellular conjugates.

2. Increased turnover of T lymphocytes in HIV-1 infection and its reduction by antiretroviral therapy.

3. Models of CD8+ responses: 1. What is the antigen-independent proliferation program.

4. Different dynamics of CD4+ and CD8+ T cell responses during and after acute lymphocytic choriomeningitis virus infection.

Review 5. Visualizing the first 50 hr of the primary immune response to a soluble antigen.

6. The dual role of CD4 T helper cells in the infection dynamics of HIV and their importance for vaccination.

7. Early programming of T cell populations responding to bacterial infection.

8. A stochastic model of cytotoxic T cell responses.

9. A mathematical model for chronic myelogenous leukemia (CML) and T cell interaction.

10. Separation of helper T cells from suppressor T cells expressing different Ly components. II. Activation by antigen: after immunization, antigen-specific suppressor and helper activities are mediated by distinct T-cell subclasses.

1. A shadow detector for photosynthesis efficiency.

Review 2. Immunological Paradigms, Mechanisms, and Models: Conceptual Understanding Is a Prerequisite to Effective Modeling.