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Merkel cell carcinoma expresses the immunoregulatory ligand CD200 and induces immunosuppressive macrophages and regulatory T cells

机译:Merkel细胞癌表达免疫调节配体CD200并诱导免疫抑制巨噬细胞和调节性T细胞

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摘要

Merkel cell carcinoma (MCC) is a rare and aggressive skin cancer that responds to PD-1/PD-L1 immune checkpoint inhibitors. CD200 is another checkpoint modulator whose receptor is found on tumor-promoting myeloid cells, including M2 macrophages. We found high CD200 mRNA expression in MCC tumors, and CD200 immunostaining was demonstrated on 95.5% of MCC tumors. CD200R-expressing myeloid cells were present in the MCC tumor microenvironment. MCC-associated macrophages had a higher average CD163:CD68 staining ratio (2.67) than controls (1.13), indicating an immunosuppressive M2 phenotype. Accordingly, MCC tumors contained increased densities of FOXP3+ regulatory T-cells. Intravenous administration of blocking anti-CD200 antibody to MCC xenograft mice revealed specific targeting of drug to tumor. In conclusion, MCC are highly CD200 positive and associated with immunosuppressive M2 macrophages and regulatory T-cells. As anti-CD200 antibody effectively targets CD200 on MCC tumor cells in vivo, this treatment may provide a novel immunotherapy for MCC independent of PD-1/PD-L1 blockade.
机译:Merkel细胞癌(MCC)是一种难以腐蚀性的皮肤癌,可应对PD-1 / PD-L1免疫检查点抑制剂。 CD200是另一个检查点调制器,其受体在肿瘤促进骨髓细胞上发现,包括M2巨噬细胞。我们发现在MCC肿瘤中的高CD200 mRNA表达,并在95.5%的MCC肿瘤上证明了CD200免疫染色。在MCC肿瘤微环境中存在CD200R表达骨髓细胞。 MCC相关的巨噬细胞的平均CD163:CD68染色比(2.67)比对照(1.13),指示免疫抑制M2表型。因此,MCC肿瘤含有增加的FoxP3 +调节性T细胞的密度。阻断抗CD200抗体对MCC异种移植小鼠的静脉内施用显示出药物对肿瘤的特异性靶向。总之,MCC高度CD200阳性,与免疫抑制M2巨噬细胞和调节性T细胞相关。由于抗CD200抗体有效地靶向体内MCC肿瘤细胞CD200,该处理可为MCC提供独立于PD-1 / PD-L1阻断的新型免疫疗法。

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