Welte Thomas, Mai Junhua, Zhang Zhe, Tian Shaohui, Zhang Guodong, Xu Yitian, Zhang Licheng, Chen Shu-Shia, Wang Tian, Shen Haifa
Department of Nanomedicine, Houston Methodist Academic Institute, Houston, TX 77030, USA.
Center for Immunotherapy Research, Houston Methodist Academic Institute, Houston, TX 77030, USA.
iScience. 2021 Oct 29;24(11):103349. doi: 10.1016/j.isci.2021.103349. eCollection 2021 Nov 19.
Myeloid-derived suppressor cells (MDSCs) infiltrate cancer tissue, promote tumor growth, and are associated with resistance to cancer therapies. However, there is no practical approach available to distinguish MDSCs from mature counterparts inside tumors. Here, we show that a recently isolated thioaptamer probe (T1) binds to MDSC subsets in colorectal and pancreatic tumors with high specificity. Whole transcriptome and functional analysis revealed that T1-binding cells contain polymorphonuclear (PMN)-MDSCs characterized by several immunosuppression pathways, ROS production, and T cell suppression activity, whereas T1-non-binding PMNs were mature and nonsuppressive. We identified syndecan-1 as the T1-interacting protein on MDSCs and chronic myelogenous leukemia K562 cell line. Heparan sulfate chains were essential in T1-binding. Inside tumors PMN-MDSCs expressed heparan sulfate biogenesis enzymes at higher levels. Tumor-cell-derived soluble factor(s) enhanced MDSCs' affinity for T1. Overall, we uncovered heparan-sulfate-dependent MDSC modulation in the tumor microenvironment and identified T1 as tool preferentially targeting tumor-promoting myeloid cell subsets.
髓源性抑制细胞(MDSCs)浸润癌组织,促进肿瘤生长,并与癌症治疗耐药性相关。然而,目前尚无切实可行的方法可在肿瘤内部将MDSCs与成熟对应细胞区分开来。在此,我们表明,一种最近分离出的硫适配体探针(T1)可高度特异性地结合结直肠癌和胰腺癌中的MDSC亚群。全转录组和功能分析显示,与T1结合的细胞包含多形核(PMN)-MDSCs,其特征在于多种免疫抑制途径、活性氧生成和T细胞抑制活性,而不与T1结合的PMN是成熟的且无抑制作用。我们鉴定出syndecan-1是MDSCs和慢性粒细胞白血病K562细胞系上与T1相互作用的蛋白。硫酸乙酰肝素链对T1结合至关重要。在肿瘤内部,PMN-MDSCs表达硫酸乙酰肝素生物合成酶的水平更高。肿瘤细胞衍生的可溶性因子增强了MDSCs对T1的亲和力。总体而言,我们揭示了肿瘤微环境中硫酸乙酰肝素依赖性的MDSC调节作用,并确定T1是优先靶向促进肿瘤的髓样细胞亚群的工具。
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