Thymosin α1 promotes the activation of myeloid-derived suppressor cells in a Lewis lung cancer model by upregulating Arginase 1.

Biochemical and biophysical research communications2015PMID: 26111447

View on PubMed DOI: 10.1016/j.bbrc.2015.06.132

Plain Language Summary

In a lung cancer mouse model, thymosin alpha-1 used alone increased cancer-fighting CD8+ T cells but unexpectedly also activated immunosuppressive cells called MDSCs, preventing effective tumor control. The MDSCs ramped up production of the enzyme Arginase 1 through TLR/MyD88 signaling, and blocking this pathway restored thymosin alpha-1's anti-tumor effectiveness, suggesting that combination strategies are needed for cancer immunotherapy with this peptide.

Abstract

Thymosin α1 (Tα1) has been tested for cancer therapy for several years, in most cases, the anti-tumor effect of Tα1 was limited, especially when Tα1 was used as a single agent. The role of Tα1 in cancer treatment and the regulatory mechanisms by which Ta1 takes effects are not yet completely understood. Using a Lewis lung caner model, here we report that Tα1 used alone elevated CD8(+) T cells, but failed to inhibit tumor growth. Furthermore, immunosuppressive myeloid-derived suppressor cells (MDSCs) showed heightened Arginase 1 production in response to Tα1 treatment, which led to stronger suppression of anti-tumor immunity. In addition, the upregulation of ARG1 was dependent on TLRs/MyD88 signaling, blocking MyD88 signaling abrogated the enhanced ARG1 expression and restored the anti-tumor efficacy of Tα1. This study provides the first demonstration that Tα1 treatment activates but not expands MDSCs via MyD88 signaling, which indicates better immunotherapeutic strategy of Tα1 against cancer.

Authors

Yuan, Chao; Zheng, Yisheng; Zhang, Bo; Shao, LiJuan; Liu, Yang; Tian, Tian; Gu, XiaoBin; Li, Xiangnan; Fan, KeXing

Keywords

Arginase 1Lung cancerMyD88Myeloid-derived suppressor cellsThymosin α1