In-situ Visualization and SERS monitoring of the interaction between tumor and endothelial cells using 3D microfluidic networks.

A multifunctional microfluidic platform was demonstrated to monitor the interaction between tumor cells and endothelial cells by integrating a three-dimension (3D) cell culture unit with a protein detection unit. In such a chip, breast cancer cells of MCF7 were seeded into the collagen to form a 3D tumor environment while human umbilical vein endothelial cells (HUVEC) are seeded in the channel next to the collagen matrix. Thus, an in-situ growth of angiogenic sprouting can be visualized through fluorescence in the 3D collagen matrix after a co-culture of MCF7 and HUVEC after four days, which cannot be observed in the 2D culture environment. On the other hand, gold@silver core-shell nanorods were used as SERS immunoprobes for the detection of the secretion of cytokine (vascular endothelial growth factor, VEGF). The limit of detection of the VEGF is 100 pg/mL. Further, as LiCl and bevacizumab can act as a promoter and an inhibitor of VEGF, the dynamic change of the concentration of VEGF under the stimulation of them was monitored by SERS signals. Thus, this integrated SERS microfluidic platform creates opportunity for the fundamental research of interaction between tumors and endothelial cells.