Litcius/Paper detail

Tumor-associated macrophages in direct contact with prostate cancer cells promote malignant proliferation and metastasis through NOTCH1 pathway

Fei Shi, Menghao Sun, Zheng Zhou, Lei Wu, Zheng Zhu, Shujie Xia, Bangmin Han, Yuyang Zhao, Yifeng Jing, Di Cui

2022International Journal of Biological Sciences30 citationsDOIOpen Access PDF

Abstract

Background: M2 macrophages are well accepted to promote cancer progression in the prostate cancer (PCa). Paracrine is the principally studied mode of communication between M2 macrophages and tumor cells. In addition to this, we present here a novel model to demonstrate these cellular communications. Methods: PCa cells were co-cultured with THP-1/ human peripheral blood mononuclear cells derived M2 macrophages in direct contact manner. Cancer cell proliferation and invasion were examined to explain how direct contact communicates. Cell-based findings were validated in two xenograft models and patients samples. Results: M2 macrophage direct contact induced a higher proliferation and invasion in PCa cells when compared with noncontact coculture manner. In direct contact manner, NOTCH1 pathway was greatly activated in PCa cells, induced by elevated -secretase activity and higher coactivator MAML2 expression. Additionally, blocking -secretase activity and depletion of MAML2 completely abolished M2 macrophage direct contact-mediated PCa cell proliferation and invasion. In vivo, inhibiting NOTCH1 signalling impaired M2 macrophage-mediated PCa tumor growth and lung metastasis. Notably, M2 macrophage infiltration as well as high NOTCH1 signaling in cancer cells indicated more aggressive features and worse survival in PCa patients.

Topics & Concepts

Cancer researchCell growthMetastasisProstate cancerCellCancer cellMacrophageTumor microenvironmentCancerBiologyChemistryMedicineInternal medicineIn vitroTumor cellsBiochemistryGeneticsImmune cells in cancerEpigenetics and DNA MethylationCancer, Stress, Anesthesia, and Immune Response