Issue 9, 2015

Use of carbosilane dendrimer to switch macrophage polarization for the acquisition of antitumor functions

Abstract

Tumor microenvironment favors the escape from immunosurveillance by promoting immunosuppression and blunting pro-inflammatory responses. Since most tumor-associated macrophages (TAM) exhibit an M2-like tumor cell growth promoting polarization, we have studied the role of 2G-03NN24 carbosilane dendrimer in M2 macrophage polarization to evaluate the potential application of dendrimers in tumor immunotherapy. We found that the 2G-03NN24 dendrimer decreases LPS-induced IL-10 production from in vitro generated monocyte-derived M2 macrophages, and also switches their gene expression profile towards the acquisition of M1 polarization markers (INHBA, SERPINE1, FLT1, EGLN3 and ALDH1A2) and the loss of M2 polarization-associated markers (EMR1, IGF1, FOLR2 and SLC40A1). Furthermore, 2G-03NN24 dendrimer decreases STAT3 activation. Our results indicate that the 2G-03NN24 dendrimer can be a useful tool for antitumor therapy by virtue of its potential ability to limit the M2-like polarization of TAM.

Graphical abstract: Use of carbosilane dendrimer to switch macrophage polarization for the acquisition of antitumor functions

Supplementary files

Article information

Article type
Paper
Submitted
17 Jul 2014
Accepted
04 Sep 2014
First published
05 Sep 2014

Nanoscale, 2015,7, 3857-3866

Use of carbosilane dendrimer to switch macrophage polarization for the acquisition of antitumor functions

A. J. Perisé-Barrios, R. Gómez, A. L. Corbí, J. de la Mata, A. Domínguez-Soto and M. A. Muñoz-Fernandez, Nanoscale, 2015, 7, 3857 DOI: 10.1039/C4NR04038D

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