An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules
Natural killer (NK) cells are immune effector cells that can detect and lyse cancer cells. However, NK cell exhaustion, a phenotype characterized by reduced secretion of cytolytic models upon serial stimulation, limits the NK cell's ability to lyse cells. In this work, we investigated in silico...
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doaj-60eb8fb68a214e709d5c698aece1baa22021-01-05T14:59:37ZengAIP Publishing LLCAPL Bioengineering2473-28772020-12-0144046107046107-1810.1063/5.0024726An optimal control approach for enhancing natural killer cells' secretion of cytolytic moleculesSahak Z. Makaryan0Stacey D. Finley1 Department of Biomedical Engineering, University of Southern California, Los Angeles, California 90089, USA Department of Biomedical Engineering, Mork Family Department of Chemical Engineering and Materials Science, and Department of Quantitative and Computational Biology, University of Southern California, Los Angeles, California 90089, USANatural killer (NK) cells are immune effector cells that can detect and lyse cancer cells. However, NK cell exhaustion, a phenotype characterized by reduced secretion of cytolytic models upon serial stimulation, limits the NK cell's ability to lyse cells. In this work, we investigated in silico strategies that counteract the NK cell's reduced secretion of cytolytic molecules. To accomplish this goal, we constructed a mathematical model that describes the dynamics of the cytolytic molecules granzyme B (GZMB) and perforin-1 (PRF1) and calibrated the model predictions to published experimental data using a Bayesian parameter estimation approach. We applied an information-theoretic approach to perform a global sensitivity analysis, from which we found that the suppression of phosphatase activity maximizes the secretion of GZMB and PRF1. However, simply reducing the phosphatase activity is shown to deplete the cell's intracellular pools of GZMB and PRF1. Thus, we added a synthetic Notch (synNotch) signaling circuit to our baseline model as a method for controlling the secretion of GZMB and PRF1 by inhibiting phosphatase activity and increasing production of GZMB and PRF1. We found that the optimal synNotch system depends on the frequency of NK cell stimulation. For only a few rounds of stimulation, the model predicts that inhibition of phosphatase activity leads to more secreted GZMB and PRF1; however, for many rounds of stimulation, the model reveals that increasing production of the cytolytic molecules is the optimal strategy. In total, we developed a mathematical framework that provides actionable insight into engineering robust NK cells for clinical applications.http://dx.doi.org/10.1063/5.0024726 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Sahak Z. Makaryan Stacey D. Finley |
spellingShingle |
Sahak Z. Makaryan Stacey D. Finley An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules APL Bioengineering |
author_facet |
Sahak Z. Makaryan Stacey D. Finley |
author_sort |
Sahak Z. Makaryan |
title |
An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
title_short |
An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
title_full |
An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
title_fullStr |
An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
title_full_unstemmed |
An optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
title_sort |
optimal control approach for enhancing natural killer cells' secretion of cytolytic molecules |
publisher |
AIP Publishing LLC |
series |
APL Bioengineering |
issn |
2473-2877 |
publishDate |
2020-12-01 |
description |
Natural killer (NK) cells are immune effector cells that can detect and lyse cancer cells. However, NK cell exhaustion, a phenotype characterized by reduced secretion of cytolytic models upon serial stimulation, limits the NK cell's ability to lyse cells. In this work, we investigated in silico strategies that counteract the NK cell's reduced secretion of cytolytic molecules. To accomplish this goal, we constructed a mathematical model that describes the dynamics of the cytolytic molecules granzyme B (GZMB) and perforin-1 (PRF1) and calibrated the model predictions to published experimental data using a Bayesian parameter estimation approach. We applied an information-theoretic approach to perform a global sensitivity analysis, from which we found that the suppression of phosphatase activity maximizes the secretion of GZMB and PRF1. However, simply reducing the phosphatase activity is shown to deplete the cell's intracellular pools of GZMB and PRF1. Thus, we added a synthetic Notch (synNotch) signaling circuit to our baseline model as a method for controlling the secretion of GZMB and PRF1 by inhibiting phosphatase activity and increasing production of GZMB and PRF1. We found that the optimal synNotch system depends on the frequency of NK cell stimulation. For only a few rounds of stimulation, the model predicts that inhibition of phosphatase activity leads to more secreted GZMB and PRF1; however, for many rounds of stimulation, the model reveals that increasing production of the cytolytic molecules is the optimal strategy. In total, we developed a mathematical framework that provides actionable insight into engineering robust NK cells for clinical applications. |
url |
http://dx.doi.org/10.1063/5.0024726 |
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