Interactions between infiltrating macrophages in the tumor microenvironment (TME) and tumor cells contribute to tumor progression. The potential impacts of recruited macrophages to the upper urinary tract urothelial cell carcinomas (UUTUCs) progression remain unclear. Here we found human UUTUCs might recruit more macrophages than surrounding normal urothelial cells in human clinical specimens and in co-culture experiments with UUTUC cells and macrophages. The consequences of recruiting more macrophages to UUTUCs might then enhance UUTUC cell growth, migration and invasion. Further investigation found that the androgen receptor (AR) not only enhanced UUTUC cells capacity to recruit more macrophages, it could also promote the macrophages-enhanced UUTUC cells growth, migration and invasion. Downstream AR target cytokine search found AR might function through modulating CCL5 expression to influence UTTUC progression. Interruption of CCL5 partially reversed the AR-regulated macrophage-enhanced UUTUC progression. AR in UUTUC cells also increased tumor formation . Taken together, these results suggest that macrophages recruitment may enhance UUTUC progression, modulated by AR-CCL5 signal through alterations in chromatin state to establish a tumor microenvironment with recruited macrophages and cytokines to facilitate cell growth, migration and invasion.
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Article Synopsis
- The study aimed to assess the effectiveness of fluorescence in situ hybridization (FISH) for detecting upper urinary tract urothelial carcinoma (UUT-UC) compared to traditional cytology.
- Between 2011 and 2015, urine samples from 52 patients with UUT-UC and 26 control patients were analyzed, revealing that FISH had a sensitivity of 79.5% and specificity of 96.3%, significantly outperforming cytology.
- The results suggest that FISH could serve as a reliable, non-invasive diagnostic tool for patients suspected of having UUT-UC.
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