Expansion and antitumor cytotoxicity of T-Cells are augmented by substrate-bound CCL21 and intercellular adhesion molecule 1

Shimrit Adutler-Lieber, Nir Friedman*, Benjamin Geiger

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

11 Scopus citations

Abstract

Adoptive immunotherapy is based on ex vivo expansion and stimulation of T-cells, followed by their transfer into patients. The need for the ex vivo culturing step provides opportunities for modulating the properties of transferred T-cells, enhancing their antitumor abilities, and increasing their number. Here, we present a synthetic immune niche (SIN) that increases the number and antitumor activity of cytotoxic CD8+ T-cells. We first evaluated the effect of various SIN compositions that mimic the physiological microenvironment encountered by T-cells during their activation and expansion in the lymph node. We found that substrates coated with the chemokine CCL21 together with the adhesion molecule intercellular adhesion molecule 1 significantly increase the number of ovalbumin-specific murine CD8+ T-cells activated by antigen-loaded dendritic cells or activation microbeads. Notably, cells cultured on these substrates also displayed augmented cytotoxic activity toward ovalbumin-expressing melanoma cells, both in culture and in vivo. This increase in specific cytotoxic activity was associated with a major increase in the cellular levels of the killing-mediator granzyme B. Our results suggest that this SIN may be used for generating T-cells with augmented cytotoxic function, for use in cancer immunotherapy.

Original languageAmerican English
Article number1303
JournalFrontiers in Immunology
Volume9
Issue numberJUN
DOIs
StatePublished - 11 Jun 2018
Externally publishedYes

Bibliographical note

Publisher Copyright:
© 2018 Adutler-Lieber, Friedman and Geiger.

Keywords

  • CCL21
  • Cancer immunotherapy
  • Intercellular adhesion molecule 1
  • T-cell clusters
  • T-cell cytotoxicity
  • T-cell immunity

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