T cell and reticular network co-dependence in HIV infection
Authored by Graham M Donovan, Grant Lythe
Date Published: 2016
DOI: 10.1016/j.jtbi.2016.01.040
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Abstract
Fibroblastic reticular cells (FRC) are arranged on a network in the T
cell zone of lymph nodes, forming a scaffold for T cell migration, and
providing survival factors, especially interleukin-7 (IL-7). Conversely, CD4(+) T cells are the major producers of lymphotoxin-beta (LT-beta), necessary for the construction and maintenance of the FRC network. This
interdependence creates the possibility of a vicious cycle, perpetuating
loss of both FRC and T cells. Furthermore, evidence that HIV infection
is responsible for collagenation of the network suggests that long term
loss of network function might be responsible for the attenuated
recovery in T cell count seen in HIV patients undergoing antiretroviral
therapy (ART). We present computational and mathematical models of this
interaction mechanism and subsequent naive CD4(+) T-cell depletion in
which (1) collagen deposition impedes access of naive T cells to IL-7 on
the FRC and loss of IL-7 production by loss of FRC network itself, leading to the depletion of naive T cells through increased apoptosis;
and (2) depletion of naive T cells as the source of LT-beta on which the
FRC depend for survival leads to loss of the network, thereby amplifying
and perpetuating the cycle of depletion of both naive T cells and
stromal cells. Our computational model explicitly includes an FRC
network and its cytokine exchange with a heterogeneous T-cell
population. We also derive lumped models, in terms of partial
differential equations and reduced to ordinary differential equations, that provide additional insight into the mechanisms at work. The central
conclusions are that (1) damage to the reticular network, caused by HIV
infection is a plausible mechanism for attenuated recovery post-ART; (2)
within this, the production of T cell survival factors by FRCS may be
the key rate-limiting step; and (3) the methods of model reduction and
analysis presented are useful for both immunological studies and other
contexts in which agent-based models are severely limited by
computational cost. (C) 2016 Elsevier Ltd. All rights reserved.
Tags
Migration
Dynamics
Dendritic cells
Survival
Responses
Lymph-node
Stromal cells
Homeostasis
Naive
Antigen