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Regulatory T cell adjustment of quorum growth thresholds and the control of local immune responses

The consequences of regulatory T cell (Treg) inhibition of interleukine 2 secretion is examined by mathematical modelling. We demonstrate that cytokine dependent growth exhibits a quorum T cell population threshold that determines if immune responses develop on activation. Secretion inhibition manip...

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Published in:Journal of theoretical biology 2006-07, Vol.241 (1), p.134-141
Main Authors: Burroughs, N.J., Miguel Paz Mendes de Oliveira, Bruno, Adrego Pinto, Alberto
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Language:English
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creator Burroughs, N.J.
Miguel Paz Mendes de Oliveira, Bruno
Adrego Pinto, Alberto
description The consequences of regulatory T cell (Treg) inhibition of interleukine 2 secretion is examined by mathematical modelling. We demonstrate that cytokine dependent growth exhibits a quorum T cell population threshold that determines if immune responses develop on activation. Secretion inhibition manipulates the growth dynamics and effectively increases the quorum threshold, i.e. to develop immune responses a higher number of T cells need to be activated. Thus Treg induced secretion inhibition can provide a mechanism for tissue specific regulation of the balance between suppression (control) and immune responses, a balance that can be varied at the local tissue level through the regulation of the local active Treg population size. However, nonspecific inhibition is prone to escape of initially controlled autoimmune T cells through cross reactivity to pathogens and bystander proliferation on unrelated immune responses.
doi_str_mv 10.1016/j.jtbi.2005.11.010
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subjects Animals
Autoimmunity
Cytokines
Growth model
Immunity, Cellular
Immunology
Interleukin-2 - metabolism
Interleukin-2 - secretion
Lymphocyte Count
Models, Immunological
ODE model
Quorum threshold
Receptors, Interleukin-2 - metabolism
Secretion inhibition
T-Lymphocyte Subsets
T-Lymphocytes, Regulatory - physiology
Tregs
title Regulatory T cell adjustment of quorum growth thresholds and the control of local immune responses
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