发现浸润人类黑色素瘤转移灶的特异性 NK 细胞群体。
Discovery of specialized NK cell populations infiltrating human melanoma metastases.
机构信息
Department of Cancer Immunology and Virology, Dana-Farber Cancer Institute, Boston, Massachusetts, USA.
Department of Immunology, Harvard Medical School, Boston, Massachusetts, USA.
出版信息
JCI Insight. 2019 Dec 5;4(23):133103. doi: 10.1172/jci.insight.133103.
Abstract
NK cells contribute to protective antitumor immunity, but little is known about the functional states of NK cells in human solid tumors. To address this issue, we performed single-cell RNA-seq analysis of NK cells isolated from human melanoma metastases, including lesions from patients who had progressed following checkpoint blockade. This analysis identified major differences in the transcriptional programs of tumor-infiltrating compared with circulating NK cells. Tumor-infiltrating NK cells represented 7 clusters with distinct gene expression programs indicative of significant functional specialization, including cytotoxicity and chemokine synthesis programs. In particular, NK cells from 3 clusters expressed high levels of XCL1 and XCL2, which encode 2 chemokines known to recruit XCR1+ cross-presenting DCs into tumors. In contrast, NK cells from 2 other clusters showed a higher level of expression of cytotoxicity genes. These data reveal key features of NK cells in human tumors and identify NK cell populations with specialized gene expression programs.
摘要
NK 细胞有助于抗肿瘤免疫保护,但对于人类实体瘤中 NK 细胞的功能状态知之甚少。为了解决这个问题,我们对从人类黑色素瘤转移灶中分离的 NK 细胞进行了单细胞 RNA 测序分析,包括接受检查点阻断后病情进展的患者的病灶。这项分析确定了浸润肿瘤的 NK 细胞与循环 NK 细胞在转录程序上的主要差异。浸润肿瘤的 NK 细胞代表 7 个具有不同基因表达程序的簇,表明其具有显著的功能特化,包括细胞毒性和趋化因子合成程序。特别是,3 个簇的 NK 细胞表达高水平的 XCL1 和 XCL2,这两种趋化因子编码已知可将 XCR1+交叉呈递 DC 招募到肿瘤中的趋化因子。相比之下,另外 2 个簇的 NK 细胞表现出更高水平的细胞毒性基因表达。这些数据揭示了人类肿瘤中 NK 细胞的关键特征,并鉴定出具有特殊基因表达程序的 NK 细胞群体。
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