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首页> 外文期刊>Cancer immunology, immunotherapy : >The role of CCR5 in directing the mobilization and biological function of CD11b~+Gr1~ +Ly6C~low polymorphonuclear myeloid cells in cancer
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The role of CCR5 in directing the mobilization and biological function of CD11b~+Gr1~ +Ly6C~low polymorphonuclear myeloid cells in cancer

机译:CCR5在引导CD11b〜+ Gr1〜+ Ly6c〜低多素核骨髓细胞中的动员和生物功能引导癌症的作用

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摘要

Bone marrow (BM) cells of the hematopoietic system, also known as BM-derived leukocytes (BMD), are mobilized from the BM to the blood and then colonize tumor sites. These cells then become key players in either promoting or regulating the development and progression of tumors. Among the cells that suppress anti-tumor immunity are regulatory T cells (T_regs), tumor-associated macrophages (TAMS) and myeloid-derived suppressor cells (MDSC). MDSC comprise CD11b~+Gr1~+Ly6C~low polymorphonuclear myeloid cells (PMN-MDSC), and CD11b~+Gr1~+Ly6C~high monocytic myeloid cells (Mo-MDSC). Several studies including ours have identified the CCR2-CCL2 axis as the key driver of the mobilization of monocytic cells from the BM to the blood and later their colonization at the tumor site. The current review focuses on the mechanisms by which PMN-MDSC are mobilized from the BM to the blood and later to the tumor site, and their clinical implications.
机译:造血系统的骨髓(BM)细胞,也称为BM衍生的白细胞(BMD),从BM到血液中调动,然后调味肿瘤位点。 然后,这些细胞成为促进或调节肿瘤的发展和进展的关键球员。 在抑制抗肿瘤免疫的细胞中,是调节性T细胞(T_regs),肿瘤相关的巨噬细胞(TAMS)和霉菌衍生的抑制细胞(MDSC)。 MDSC包括CD11b〜+ GR1〜+ LY6C〜低多孔核骨髓细胞(PMN-MDSC)和CD11B〜+ GR1〜+ LY6C〜高单核细胞骨髓细胞(MO-MDSC)。 包括我们的几项研究已经将CCR2-CCL2轴鉴定为从BM到血液中动员单核细胞的关键驱动器,并在肿瘤部位进行殖民化。 目前的评论重点是PMN-MDSC从BM调动到血液中的机制,并且后面将其临床意义。

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