Cancer-associated fibroblasts remain poorly understood, with some of them originating from the bone marrow. We therefore took advantage of the diversity of bone marrow stromal cells to shed light on how fibroblasts modulate cancer growth. In two murine cancer models, adding these fibroblasts to tumor cells resulted in smaller lesions. Suppression was enhanced by pretreatment with fibronectin, while genetic deletion of fibronectin in a small subpopulation of stromal cells expressing osterix/sp7 restored growth. The suppressive stromal population showed two more characteristics: the absence of CD31/pecam1 and CD105/endoglin. However, only a decrease in CD105/ENDOGLIN in melanoma patients translated in improved survival. Mechanistically, fibronectin or fibronectin fragments activate integrin α5β1 and TLR4 and increase chemokine production by stromal cells ultimately leading to enhanced recruitment and activity of Ly6G(+) myeloid cells without T-cell involvement. This work thus characterizes a beneficial interaction between stromal cells and neutrophils enhancing the immune response against early cancer.
The immune response against cancer is modulated by stromal cell fibronectin.
基质细胞纤连蛋白调节机体对癌症的免疫反应
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作者:Lubosch Alexander, Pitt Lauren, Zoeller Caren, Wirth Franziska, Exner Tarik, Steigenberger Barbara, Wabnitz Guido, Schroeder-Braunstein Jutta, Nakchbandi Inaam A
| 期刊: | Neoplasia | 影响因子: | 7.700 |
| 时间: | 2025 | 起止号: | 2025 Sep;67:101196 |
| doi: | 10.1016/j.neo.2025.101196 | 研究方向: | 细胞生物学 |
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