CD24 MDSC-DCs Induced by CCL5-Deficiency Showed Improved Antitumor Activity As Tumor Vaccines

Overview

Journal Glob Med Genet

Publisher Thieme

Date 2022 Jun 16

PMID 35707772

Authors

Lei Huang

Zequn Ding

Yan Zhang

Affiliations

Soon will be listed here.

Abstract

Dendritic cell (DC) tumor vaccine has been extensively utilized in preclinical and clinical studies; however, this technique has encountered many difficulties, particularly in late-stage tumor patients. For those, ex vivo-induced DCs are actuallymyeloid-derived suppressive cells-derived DCs (MDSC-DCs). MDSCs with immunosuppressive activity, but not monocytes, became the major DC precursor. Thus, how to enhance antitumor activity of MDSC-DCs is urgent need to address. We utilized 4T1 and MC38 tumor-bearing both wildtype and CC chemokine ligand 5 (CCL5 ) mice as animal models. MDSC-DCs were induced from splenocytes of these mice by granulocyte macrophage-colony stimulating factor/interleukin-4 with or without all-trans-retinoic acid (ATRA) in vitro for 7 days, then incubated with tumor-cell-lysis to treat mouse models for total three doses. For human MDSC-DCs, peripheral bloods from colorectal cancer patients were induced in vitro as murine cells with or without T- lymphocytes depletion to get rid of CCL5. Flow cytometry analysis showed that MDSCs from mice could be induced into a new type of CD24 MDSC-DCs in the presence of ATRA, which had more antitumor activity than control. Antibody blocking and adoptive transfer experiments demonstrated that downregulation of regulatory T cells (Tregs) mediated the inhibition of CD24 MDSC-DCs on tumor growth. Mechanically, CD24 MDSC-DCs inhibited Tregs' polarization by secreting cytokine or coactivators' expression. What's important, decreasing CCL5 protein levels by T- lymphocytes depletion during both murine and human MDSC-DCs in vitro induction could also acquire CD24 MDSC-DCs. Knockdown of CCL5 protein during MDSC-DCs culture might provide a promising method to acquire DC-based tumor vaccines with high antitumor activity.

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