Myeloid Derived Suppressor Cells: Fuel the Fire

B. R. Achyut, A. Arbab
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引用次数: 10

Abstract

Low oxygen tension, hypoxia, is a characteristic of many tumors and associated with the poor prognosis. Hypoxia invites bone marrow derived cells (BMDCs) from bone marrow to the site of tumor. These recruited CXCR4+ BMDCs provide favorable environment for the tumor growth by acquiring pro-angiogenic phenotype such as CD45+VEGFR2+ Endothelial Progenitor Cells (EPC), or CD45+Tie2+ myeloid cells. CD11b+CD13+ myeloid population of the BMDCs modulate tumor progression. These myeloid populations retain immunosuppressive characteristics, for example, myeloid derived suppressor cells (MDSCs), and regulates immune- suppression by inhibiting cytotoxic T cell function. In addition, MDSCs were observed at the premetastatic niche of the distant organs in other tumors. Protumorigenic and prometastatic role of the myeloid cells provides a basis for therapeutic targeting of immunosuppression and thus inhibiting tumor development and metastasis.
髓源性抑制细胞:火上浇油
低氧压,缺氧,是许多肿瘤的特征,并与预后不良有关。缺氧诱导骨髓源性细胞(bmdc)从骨髓到达肿瘤部位。这些募集的CXCR4+ BMDCs通过获得促血管生成表型(如CD45+VEGFR2+内皮祖细胞(EPC)或CD45+Tie2+骨髓细胞)为肿瘤生长提供了有利的环境。BMDCs的CD11b+CD13+髓系群体调节肿瘤进展。这些髓细胞群保留免疫抑制特性,例如髓源性抑制细胞(MDSCs),并通过抑制细胞毒性T细胞功能调节免疫抑制。此外,在其他肿瘤的远端器官的转移前生态位也观察到MDSCs。髓系细胞的致瘤性和前转移性作用为免疫抑制靶向治疗从而抑制肿瘤的发展和转移提供了基础。
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