The glycosyltransferase ST3GAL4 drives immune evasion in acute myeloid leukemia by synthesizing ligands for the glyco-immune checkpoint receptor Siglec-9

IF 12.8 1区 医学 Q1 HEMATOLOGY
Vignesh Krishnamoorthy, John Daly, Jimmy Kim, Lidia Piatnitca, Katie A. Yuen, Bhoj Kumar, Mehrnoush Taherzadeh Ghahfarrokhi, Tom Q. T. Bui, Parastoo Azadi, Ly P. Vu, Simon Wisnovsky
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Abstract

Immunotherapy has demonstrated promise as a treatment for acute myeloid leukemia (AML). However, there is still an urgent need to identify new molecules that inhibit the immune response to AML. Most prior research in this area has focused on protein-protein interaction interfaces. While carbohydrates also regulate immune recognition, the role of cell-surface glycans in driving AML immune evasion is comparatively understudied. The Siglecs, for example, are an important family of inhibitory, glycan-binding signaling receptors that have emerged as prime targets for cancer immunotherapy in recent years. In this study, we find that AML cells express ligands for the receptor Siglec-9 at high levels. Integrated CRISPR genomic screening and clinical bioinformatic analysis identified ST3GAL4 as a potential driver of Siglec-9 ligand expression in AML. Depletion of ST3GAL4 by CRISPR-Cas9 knockout (KO) dramatically reduced the expression of Siglec-9 ligands in AML cells. Mass spectrometry analysis of cell-surface glycosylation in ST3GAL4 KO cells revealed that Siglec-9 primarily binds N-linked sialoglycans on these cell types. Finally, we found that ST3GAL4 KO enhanced the sensitivity of AML cells to phagocytosis by Siglec-9-expressing macrophages. This work reveals a novel axis of immune evasion and implicates ST3GAL4 as a possible target for immunotherapy in AML.

Abstract Image

糖基转移酶 ST3GAL4 通过合成糖免疫检查点受体 Siglec-9 的配体来驱动急性髓性白血病的免疫逃避
免疫疗法作为一种治疗急性髓性白血病(AML)的方法已被证明是大有可为的。然而,目前仍急需找到能抑制急性髓性白血病免疫反应的新分子。该领域之前的研究大多集中在蛋白质与蛋白质相互作用界面上。虽然碳水化合物也能调控免疫识别,但细胞表面的聚糖在推动急性髓细胞性白血病免疫逃避方面的作用研究相对不足。例如,Siglecs 是一个重要的抑制性糖结合信号受体家族,近年来已成为癌症免疫疗法的主要靶标。在这项研究中,我们发现 AML 细胞高水平表达 Siglec-9 受体的配体。综合CRISPR基因组筛选和临床生物信息学分析发现,ST3GAL4是AML中Siglec-9配体表达的潜在驱动因素。通过CRISPR-Cas9敲除(KO)ST3GAL4可显著降低AML细胞中Siglec-9配体的表达。ST3GAL4 KO细胞中细胞表面糖基化的质谱分析表明,Siglec-9主要与这些细胞类型上的N-连接的sialoglycans结合。最后,我们发现 ST3GAL4 KO 增强了 AML 细胞对表达 Siglec-9 的巨噬细胞吞噬的敏感性。这项研究揭示了一种新的免疫逃避轴,并将 ST3GAL4 作为急性髓细胞白血病免疫疗法的一个可能靶点。
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来源期刊
Leukemia
Leukemia 医学-血液学
CiteScore
18.10
自引率
3.50%
发文量
270
审稿时长
3-6 weeks
期刊介绍: Title: Leukemia Journal Overview: Publishes high-quality, peer-reviewed research Covers all aspects of research and treatment of leukemia and allied diseases Includes studies of normal hemopoiesis due to comparative relevance Topics of Interest: Oncogenes Growth factors Stem cells Leukemia genomics Cell cycle Signal transduction Molecular targets for therapy And more Content Types: Original research articles Reviews Letters Correspondence Comments elaborating on significant advances and covering topical issues
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