Sialylation of CD55 by ST3GAL1 Facilitates Immune Evasion in Cancer

逃避(道德) 免疫系统 癌症 免疫逃逸 生物 肿瘤免疫学 癌症研究 癌症免疫疗法 免疫学 抗原 免疫疗法 计算生物学 医学 遗传学
作者
Wender Lin,Tan‐Chi Fan,Jung‐Tung Hung,Hui-Ling Yeo,Sheng‐Hung Wang,Chu‐Wei Kuo,Kay‐Hooi Khoo,Li‐Mei Pai,John Yu,Alice L. Yu
出处
期刊:Cancer immunology research [American Association for Cancer Research]
卷期号:9 (1): 113-122 被引量:54
标识
DOI:10.1158/2326-6066.cir-20-0203
摘要

Abstract Altered glycosylations, which are associated with expression and activities of glycosyltransferases, can dramatically affect the function of glycoproteins and modify the behavior of tumor cells. ST3GAL1 is a sialyltransferase that adds sialic acid to core 1 glycans, thereby terminating glycan chain extension. In breast carcinomas, overexpression of ST3GAL1 promotes tumorigenesis and correlates with increased tumor grade. In pursuing the role of ST3GAL1 in breast cancer using ST3GAL1-siRNA to knockdown ST3GAL1, we identified CD55 to be one of the potential target proteins of ST3GAL1. CD55 is an important complement regulatory protein, preventing cells from complement-mediated cytotoxicity. CD55 had one N-linked glycosylation site in addition to a Ser/Thr-rich domain, which was expected to be heavily O-glycosylated. Detailed analyses of N- and O-linked oligosaccharides of CD55 released from scramble or ST3GAL1 siRNA–treated breast cancer cells by tandem mass spectrometry revealed that the N-glycan profile was not affected by ST3GAL1 silencing. The O-glycan profile of CD55 demonstrated a shift in abundance to nonsialylated core 1 and monosialylated core 2 at the expense of the disialylated core 2 structure after ST3GAL1 silencing. We also demonstrated that O-linked desialylation of CD55 by ST3GAL1 silencing resulted in increased C3 deposition and complement-mediated lysis of breast cancer cells and enhanced sensitivity to antibody-dependent cell-mediated cytotoxicity. These data demonstrated that ST3GAL1-mediated O-linked sialylation of CD55 acts like an immune checkpoint molecule for cancer cells to evade immune attack and that inhibition of ST3GAL1 is a potential strategy to block CD55-mediated immune evasion.
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