MAL2 drives immune evasion in breast cancer by suppressing tumor antigen presentation
Yuanzhang Fang, … , Xiongbin Lu, Xinna Zhang
Yuanzhang Fang, … , Xiongbin Lu, Xinna Zhang
Published September 29, 2020
Citation Information: J Clin Invest. 2021;131(1):e140837. https://doi.org/10.1172/JCI140837.
View: Text | PDF
Research Article Immunology Oncology

MAL2 drives immune evasion in breast cancer by suppressing tumor antigen presentation

Abstract

Immune evasion is a pivotal event in tumor progression. To eliminate human cancer cells, current immune checkpoint therapy is set to boost CD8+ T cell–mediated cytotoxicity. However, this action is eventually dependent on the efficient recognition of tumor-specific antigens via T cell receptors. One primary mechanism by which tumor cells evade immune surveillance is to downregulate their antigen presentation. Little progress has been made toward harnessing potential therapeutic targets for enhancing antigen presentation on the tumor cell. Here, we identified MAL2 as a key player that determines the turnover of the antigen-loaded MHC-I complex and reduces the antigen presentation on tumor cells. MAL2 promotes the endocytosis of tumor antigens via direct interaction with the MHC-I complex and endosome-associated RAB proteins. In preclinical models, depletion of MAL2 in breast tumor cells profoundly enhanced the cytotoxicity of tumor-infiltrating CD8+ T cells and suppressed breast tumor growth, suggesting that MAL2 is a potential therapeutic target for breast cancer immunotherapy.

Authors

Yuanzhang Fang, Lifei Wang, Changlin Wan, Yifan Sun, Kevin Van der Jeught, Zhuolong Zhou, Tianhan Dong, Ka Man So, Tao Yu, Yujing Li, Haniyeh Eyvani, Austyn B. Colter, Edward Dong, Sha Cao, Jin Wang, Bryan P. Schneider, George E. Sandusky, Yunlong Liu, Chi Zhang, Xiongbin Lu, Xinna Zhang

×

Figure 6

MAL2 downregulates antigen presentation on breast cancer cells.

Options: View larger image (or click on image) Download as PowerPoint
MAL2 downregulates antigen presentation on breast cancer cells. (A) MAL2...
(A) MAL2 downregulates antigen presentation on EO771-OVA cells with different MAL2 levels. The antigen presentation efficiency was assessed by flow cytometry. MFI scores are presented for 3 independent experiments. One-way ANOVA test was used for statistical analysis. (B) The presentation of the MHC-I complex on the cell membrane is inhibited by MAL2. EO771 and MDA-MB-468 cells with different MAL2 levels were tested. One-way ANOVA test was used for statistical analysis. (C) MAL2 promotes the turnover rate of tumor antigen on the cell surface. EO771 cells with different Mal2 expression levels were preincubated with OVA257-264 peptides and OVA257-264 peptides were washed off, and then cells were collected at indicated times and stained for the MHC-I–presented OVA257-264. Two-way ANOVA test was used for statistical analysis. (D) Localization of the MAL2 protein in MDA-MB-468 cells. EGFR is biomarker for membrane proteins. EEA-1 and RAB7 are biomarkers for early and late stage endosomes, respectively, and LAMP-1 is a biomarker for lysosomes. Scale bar: 10 μm. (E) Quantification of (D). In this figure, data are presented as mean ± SD. *P < 0.05; **P < 0.01; ***P < 0.001.