Magrini Elena, Di Marco Sabrina, Mapelli Sarah N, Perucchini Chiara, Pasqualini Fabio, Donato Alessia, Guevara Lopez Maria de la Luz, Carriero Roberta, Ponzetta Andrea, Colombo Piergiuseppe, Cananzi Ferdinando, Supino Domenico, Reis Edimara S, Peano Clelia, Inforzato Antonio, Jaillon Sebastien, Doni Andrea, Lambris John D, Mantovani Alberto, Garlanda Cecilia
IRCCS Humanitas Research Hospital, Milan, Italy.
Department of Biomedical Sciences, Humanitas University, Milan, Italy.
Nat Cancer. 2021 Feb;2(2):218-232. doi: 10.1038/s43018-021-00173-0. Epub 2021 Feb 18.
Complement has emerged as a component of tumor promoting inflammation. We conducted a systematic assessment of the role of complement activation and effector pathways in sarcomas. , and mice showed reduced susceptibility to 3-methylcholanthrene sarcomagenesis and transplanted sarcomas, whereas C1q and factor B deficiency had marginal effects. Complement 3a receptor (C3aR), but not C5aR1 and C5aR2, deficiency mirrored the phenotype of mice. C3 and C3aR deficiency were associated with reduced accumulation and functional skewing of tumor-associated macrophages, increased T cell activation and response to anti-PD-1 therapy. Transcriptional profiling of sarcoma infiltrating macrophages and monocytes revealed the enrichment of MHC II-dependent antigen presentation pathway in C3-deficient cells. In patients, C3aR expression correlated with a macrophage population signature and C3 deficiency-associated signatures predicted better clinical outcome. These results suggest that the lectin pathway and C3a/C3aR axis are key components of complement and macrophage-mediated sarcoma promotion and immunosuppression.
补体已成为肿瘤促炎作用的一个组成部分。我们对补体激活和效应途径在肉瘤中的作用进行了系统评估。C3−/−、C5−/−和C3aR−/−小鼠对3-甲基胆蒽诱导肉瘤发生和移植性肉瘤的易感性降低,而C1q和B因子缺乏的影响较小。补体3a受体(C3aR)缺陷而非C5aR1和C5aR2缺陷反映了C3−/−小鼠的表型。C3和C3aR缺陷与肿瘤相关巨噬细胞的积累减少和功能偏向、T细胞活化增加以及对抗程序性死亡蛋白1(anti-PD-1)治疗的反应有关。肉瘤浸润巨噬细胞和单核细胞的转录谱分析显示,C3缺陷细胞中MHC II依赖性抗原呈递途径富集。在患者中,C3aR表达与巨噬细胞群体特征相关,C3缺陷相关特征预示着更好的临床结果。这些结果表明,凝集素途径和C3a/C3aR轴是补体和巨噬细胞介导的肉瘤促进和免疫抑制的关键组成部分。
