PHA Eludes Macrophage Suppression to Activate CD8 T Cells

Overview

Journal Immunobiology

Publisher Elsevier

Specialty Allergy & Immunology

Date 2018 Nov 18

PMID 30446337

Citations 5

Authors

Yelizavet D Lomakova

Jennifer Londregan

Jeffrey Maslanka

Naomi Goldman

John Somerville

James E Riggs

Affiliations

Soon will be listed here.

Abstract

Tumors may include a high proportion of immune modulatory cells and molecules that restrain the anti-cancer response. Activation of T cells to eliminate cancer cells within the immune-suppressive tumor microenvironment remains a challenge. We have shown that C57BL/6 J peritoneal cell culture models features of macrophage-dense tumors as TCR ligation fails to activate T cells unless IFNγ is neutralized or iNOS is inhibited. We tested other forms of T cell activation and found phytohemagglutinin (PHA) distinctive in the ability to markedly expand CD8 T cells in this model. IFNγ or iNOS inhibition was not necessary for this response. PHA triggered less IFNγ production and inhibitory PD-L1 expression than TCR ligation. Macrophages and CD44 T cells bound PHA. Spleen T cell responses to PHA were markedly enhanced by the addition of peritoneal cells revealing that macrophages enhance T cell expansion. That PHA increases CD8 T cell responses within macrophage-dense culture suggests this mitogen might enhance anti-tumor immunity.

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