Key Laboratory for Experimental Teratology of Ministry of Education & Department of Immunology, School of Basic Medical Sciences, Qilu Hospital, Cheeloo College of Medicine, Shandong University, Jinan 250012, Shandong, China.
Key Laboratory for Experimental Teratology of Ministry of Education & Department of Immunology, School of Basic Medical Sciences, Qilu Hospital, Cheeloo College of Medicine, Shandong University, Jinan 250012, Shandong, China; Department of Medicinal Chemistry, Key Laboratory of Chemical Biology of Ministry of Education, School of Pharmaceutical Sciences, Cheeloo College of Medicine, Shandong University, Jinan 250012, Shandong, China.
J Hepatol. 2024 May;80(5):792-804. doi: 10.1016/j.jhep.2024.01.028. Epub 2024 Feb 7.
BACKGROUND & AIMS: Natural killer (NK) cell-based anti-hepatocellular carcinoma (HCC) therapy is an increasingly attractive approach that warrants further study. Siglec-9 interacts with its ligand (Siglec-9L) and restrains NK cell functions, suggesting it is a potential therapeutic target. However, in situ Siglec-9/Siglec-9L interactions in HCC have not been reported, and a relevant interventional strategy is lacking. Herein, we aim to illustrate Siglec-9/Siglec-9L-mediated cell sociology and identify small-molecule inhibitors targeting Siglec-9 that could improve the efficacy of NK cell-based immunotherapy for HCC.
Multiplexed immunofluorescence staining was performed to analyze the expression pattern of Siglec-7, -9 and their ligands in HCC tissues. Then we conducted docking-based virtual screening combined with bio-layer interferometry assays to identify a potent small-molecule Siglec-9 inhibitor. The therapeutic potential was further evaluated in vitro and in hepatoma-bearing NCG mice.
Siglec-9 expression, rather than Siglec-7, was markedly upregulated on tumor-infiltrating NK cells, which correlated significantly with reduced survival of patients with HCC. Moreover, the number of Siglec-9L cells neighboring Siglec-9 NK cells was increased in HCC tissues and was also associated with tumor recurrence and reduced survival, further suggesting that Siglec-9/Siglec-9L interactions are a potential therapeutic target in HCC. In addition, we identified a small-molecule Siglec-9 inhibitor MTX-3937 which inhibited phosphorylation of Siglec-9 and downstream SHP1 and SHP2. Accordingly, MTX-3937 led to considerable improvement in NK cell function. Notably, MTX-3937 enhanced cytotoxicity of both human peripheral and tumor-infiltrating NK cells. Furthermore, transfer of MTX-3937-treated NK92 cells greatly suppressed the growth of hepatoma xenografts in NCG mice.
Our study provides the rationale for HCC treatment by targeting Siglec-9 on NK cells and identifies a promising small-molecule inhibitor against Siglec-9 that enhances NK cell-mediated HCC surveillance.
Herein, we found that Siglec-9 expression is markedly upregulated on tumor-infiltrating natural killer (TINK) cells and correlates with reduced survival in patients with hepatocellular carcinoma (HCC). Moreover, the number of Siglec-9L cells neighboring Siglec-9 NK cells was increased in HCC tissues and was also associated with tumor recurrence and reduced survival. More importantly, we identified a small-molecule inhibitor targeting Siglec-9 that augments NK cell functions, revealing a novel immunotherapy strategy for liver cancer that warrants further clinical investigation.
自然杀伤(NK)细胞为基础的抗肝细胞癌(HCC)疗法是一种越来越有吸引力的方法,值得进一步研究。Siglec-9 与其配体(Siglec-9L)相互作用并抑制 NK 细胞功能,表明它是一个潜在的治疗靶点。然而,HCC 中尚未报道原位 Siglec-9/Siglec-9L 相互作用,并且缺乏相关的干预策略。在此,我们旨在阐明 Siglec-9/Siglec-9L 介导的细胞社会学,并确定针对 Siglec-9 的小分子抑制剂,这些抑制剂可能提高 NK 细胞为基础的 HCC 免疫疗法的疗效。
采用多重免疫荧光染色分析 HCC 组织中 Siglec-7、-9 及其配体的表达模式。然后,我们进行了基于对接的虚拟筛选和生物层干涉测定,以鉴定出一种有效的小分子 Siglec-9 抑制剂。进一步在体外和荷瘤 NCG 小鼠中评估其治疗潜力。
肿瘤浸润性 NK 细胞上 Siglec-9 的表达(而非 Siglec-7)明显上调,与 HCC 患者生存率降低显著相关。此外,HCC 组织中与 Siglec-9 NK 细胞相邻的 Siglec-9L 细胞数量增加,并且还与肿瘤复发和生存率降低相关,进一步表明 Siglec-9/Siglec-9L 相互作用是 HCC 的潜在治疗靶点。此外,我们鉴定出一种小分子 Siglec-9 抑制剂 MTX-3937,它可抑制 Siglec-9 和下游 SHP1 和 SHP2 的磷酸化。相应地,MTX-3937 导致 NK 细胞功能显著改善。值得注意的是,MTX-3937 增强了人外周血和肿瘤浸润性 NK 细胞的细胞毒性。此外,转导 MTX-3937 处理的 NK92 细胞可显著抑制 NCG 小鼠肝癌异种移植瘤的生长。
本研究为靶向 NK 细胞上的 Siglec-9 治疗 HCC 提供了依据,并确定了一种有前途的针对 Siglec-9 的小分子抑制剂,该抑制剂可增强 NK 细胞介导的 HCC 监测。
在此,我们发现 Siglec-9 在肿瘤浸润性自然杀伤(TINK)细胞上的表达明显上调,并与 HCC 患者生存率降低相关。此外,HCC 组织中与 Siglec-9 NK 细胞相邻的 Siglec-9L 细胞数量增加,并且还与肿瘤复发和生存率降低相关。更重要的是,我们鉴定出一种针对 Siglec-9 的小分子抑制剂,该抑制剂可增强 NK 细胞的功能,为肝癌的新型免疫治疗策略提供了依据,值得进一步的临床研究。
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