Stochastic model of T Cell repolarization during target elimination (II)
Ivan Hornak, Heiko Rieger

TL;DR
This paper presents a computational stochastic model of T cell MTOC repositioning during immune synapse formation, analyzing single and dual synapse scenarios, and predicting dynamics based on molecular mechanisms and dynein distribution.
Contribution
It introduces a novel stochastic model for T cell MTOC dynamics that accounts for multiple mechanisms and synapse configurations, extending previous models.
Findings
Initial MTOC position influences dominant mechanism.
Repositioning time varies non-monotonically with distance.
Presence of capture-shrinkage is crucial for transitions.
Abstract
Cytotoxic T lymphocytes (T cells) and natural killer cells form a tight contact, the immunological synapse (IS), with target cells, where they release their lytic granules containing perforin/granzyme and cytokine containing vesicles. During this process the cell repolarizes and moves the microtubule organizing center (MTOC) towards the IS. In the first part of our work we developed a a computational model for the molecular-motor-driven motion of the MT cytoskeleton during T cell polarization and analyzed effects of cortical sliding and capture-shrinkage mechanisms. Here we use this model to analyze the dynamics of the MTOC repositioning in situations in which a) the IS is in an arbitrary position with respect to the initial position of the MTOC and b) the T cell has two IS at two arbitrary positions. In the case of one IS, we found that the initial position determines which mechanism…
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