Macrophage-derived Nitric Oxide Initiates T-cell Diapedesis and Tumor Rejection

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2016 Nov 18

PMID 27853636

Citations 32

Authors

Ibrahim M Sektioglu

Rafael Carretero

Noemi Bender

Christian Bogdan

Natalio Garbi

Viktor Umansky

Ludmila Umansky

Katharina Urban

Magnus von Knebel-Doberitz

Veena Somasundaram

David Wink

Philipp Beckhove

Gunter J Hammerling

Affiliations

Soon will be listed here.

Abstract

In tumor biology, nitric oxide (NO) is generally regarded as an immunosuppressive molecule that impedes T-cell functions and activation of endothelial cells. Contrasting with this view, we here describe a critical role for NO derived from inducible nitric oxide (iNOS)-expressing tumor macrophages in T-cell infiltration and tumor rejection as shown by iNOS gene deletion, inhibition of iNOS, or NO donors. Specifically, macrophage-derived NO was found to induce on tumor vessels adhesion molecules that were required for T-cell extravasation. Experiments with human endothelial cells revealed a bimodal dose-dependent effect of NO. High doses of NO donors were indeed suppressive but lower, more physiological concentrations, induced adhesion molecules in an NFkB-dependent pathway and preferentially activated transcription of genes involved in lymphocyte diapedesis. iNOS macrophages in tumors appear to generate precisely the amount of NO that promotes endothelial activation and T-cell infiltration. These results will be valuable for the development of strategies designed to overcome the paucity of T-cell infiltration into tumors that is a major obstacle in clinical cancer immunotherapy.

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