Macrophages and microglia are professional phagocytes that sense and migrate toward "eat-me" signals. The role of phagocytic cells is to maintain homeostasis by engulfing senescent or apoptotic cells, debris, and abnormally aggregated macromolecules. Usually, dying cells send out "find-me" signals, facilitating the recruitment of phagocytes. Healthy cells can also promote or inhibit the phagocytosis phenomenon of macrophages and microglia by tuning the balance between "eat-me" and "don't-eat-me" signals at different stages in their lifespan, while the "don't-eat-me" signals are often hijacked by tumor cells as a mechanism of immune evasion. Using a combination of bioinformatic analysis and spatial profiling, we delineate the balance of the "don't-eat-me" CD47/SIRPα and "eat-me" CALR/STC1 ligand-receptor interactions to guide therapeutic strategies that are being developed for glioblastoma sequestered in the central nervous system (CNS).
Glioblastoma Phagocytic Cell Death: Balancing the Opportunities for Therapeutic Manipulation.
胶质母细胞瘤吞噬细胞死亡:平衡治疗干预的机会
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作者:Du Ruochen, Tripathi Shashwat, Najem Hinda, Brat Daniel J, Lukas Rimas V, Zhang Peng, Heimberger Amy B
| 期刊: | Cells | 影响因子: | 5.200 |
| 时间: | 2024 | 起止号: | 2024 May 11; 13(10):823 |
| doi: | 10.3390/cells13100823 | 研究方向: | 细胞生物学 |
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