PROX1 interaction with α-SMA-rich cancer-associated fibroblasts facilitates colorectal cancer progression and correlates with poor clinical outcomes and therapeutic resistance

Shiue-Wei Lai; Yi-Chiao Cheng; Kee-Thai Kiu; Min-Hsuan Yen; Ying-Wei Chen; Vijesh Kumar Yadav; Chi-Tai Yeh; Kuang-Tai Kuo; Tung-Cheng Chang

doi:doi:10.18632/aging.205447

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Research Paper Volume 16, Issue 2 pp 1620—1639

PROX1 interaction with α-SMA-rich cancer-associated fibroblasts facilitates colorectal cancer progression and correlates with poor clinical outcomes and therapeutic resistance

Figure 4. PROX1 overexpression promotes the growth, migration, and invasion of colon adenocarcinoma cells. HT-29 cells were transfected with either the pcDNA-PROX1 overexpressing vector or empty vector control. (A) RT-qPCR and (B) proliferation and (C) colony formation capability were estimated by CCK-8 and colony formation assays, respectively. (D) Flow cytometry showed the distribution of pcDNA-PROX1-transfected HT-29 cells in the G1, S, and G2/M phases of the cell cycle. (E) Cell migration ability was assessed by wound healing and (F) Invasion was assessed by the Transwell invasion assay in pcDNA-PROX1-transfected HT-29 cells and control cells. Magnification, ×100. Scale bar, 100 μm. The experiments were performed three times, and the data are presented as the mean ± standard deviation. ^*P < 0.05 and ^**P < 0.01 vs. NC.