SMAC mimetics induce human macrophages to phagocytose live cancer cells.

IF 4.9 Q2 IMMUNOLOGY

Immunotherapy advances Pub Date : 2025-07-09 eCollection Date: 2025-01-01 DOI:10.1093/immadv/ltaf026

Samantha Y Liu, Max P M Hulsman, Philipp Leyendecker, Eugena Chang, Katherine A Donovan, Fabian Strobel, James Dougan, Eric S Fischer, Michael Dougan, Stephanie K Dougan, Li Qiang

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Abstract

Macrophages engulf apoptotic bodies and cellular debris as part of homeostasis, but they can also phagocytose live cells, such as aged red blood cells. Pharmacologic reprogramming with the SMAC mimetic LCL161 in combination with T-cell-derived cytokines can induce macrophages to phagocytose live cancer cells in mouse models. Here we extend these findings to encompass a wide range of monovalent and bivalent SMAC mimetic compounds, demonstrating that live cell phagocytosis is a class effect of these agents. We demonstrate robust phagocytosis of live pancreatic and breast cancer cells by primary human macrophages across a range of healthy donors. Unlike mouse macrophages, where a combination of SMAC mimetics with lymphotoxin enhanced phagocytosis, human macrophages were more efficiently polarized to phagocytose live cells by the combination of SMAC mimetics and IFNg. We profiled phagocytic macrophages by transcriptional and proteomic methodologies, uncovering a positive feedback loop of autocrine TNFa production.

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SMAC模拟物诱导人巨噬细胞吞噬活的癌细胞。

巨噬细胞吞噬凋亡小体和细胞碎片作为稳态的一部分，但它们也可以吞噬活细胞，如老化的红细胞。用模拟SMAC的LCL161结合t细胞源性细胞因子进行药理学重编程可以诱导巨噬细胞吞噬小鼠模型中的活癌细胞。在这里，我们将这些发现扩展到广泛的单价和二价SMAC模拟化合物，证明活细胞吞噬是这些药物的一类效应。我们在一系列健康的供体中证明了原代人巨噬细胞对活的胰腺癌和乳腺癌细胞的强大吞噬作用。与小鼠巨噬细胞不同的是，小鼠巨噬细胞中SMAC模拟物与淋巴毒素的结合增强了吞噬作用，而人巨噬细胞在SMAC模拟物与IFNg的结合下更有效地极化为吞噬活细胞。我们通过转录和蛋白质组学方法分析了吞噬巨噬细胞，发现了自分泌TNFa生产的正反馈循环。

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