Abstract
A major impediment to the response of tumors to chemotherapy is that the large majority of cancer cells within a tumor are quiescent in G0/G1, where cancer cells are resistant to chemotherapy. To attempt to solve this problem of quiescent cells in a tumor, cancer cells were treated with recombinant methioninase (rMETase), which selectively traps cancer cells in S/G2. The cell cycle phase of the cancer cells was visualized with the fluorescence ubiquitination-based cell cycle indicator cell cycle indicator (FUCCI). At the time of rMETase-induced S/G2-phase blockage, identified by the cancer cells' green fluorescence by FUCCI imaging, the cancer cells were administered S/G2-dependent chemotherapy drugs, which interact with DNA or block DNA synthesis such as doxorubicin, cisplatin, or 5-fluorouracil. Treatment of cancer cells with drugs only, without rMETase-induced S/G2 phase blockage, led to the majority of the cancer-cell population being blocked in G0/G1 phase, identified by the cancer cells becoming red fluorescent in the FUCCI system. The G0/G1 blocked cells were resistant to the chemotherapy. In contrast, trapping of cancer cells in S/G2 phase by rMETase treatment followed by FUCCI-imaging-guided chemotherapy was highly effective in killing the cancer cells.
Highlights
The problem of quiescent cancer cells within a tumorThe resistance of most solid tumors and metastases is a major problem in chemotherapy
We demonstrate that using recombinant methioninase to deplete methionine and thereby trap cancer cells in S/G2, and fluorescence ubiquitination cell cycle indicator (FUCCI) imaging to detect the onset of the block, chemotherapy could become effective on the S/G2-trapped cancer cells
Recombinant methionine block of cancer cells in S/G2 visualized by FUCCI imaging
Summary
The problem of quiescent cancer cells within a tumor. The resistance of most solid tumors and metastases is a major problem in chemotherapy. 90% of cancer cells in the center and 80% of total cells of an established tumor are in G0/G1 phase. Approximately 75% of cancer cells far from (> 100 μm) tumor blood vessels of an established tumor are in G0/G1. FUCCI imaging demonstrated that cytotoxic agents killed only proliferating cancer cells at the surface, or near blood vessels, and had little effect on the majority of quiescent cancer cells within a tumor. Resistant quiescent cancer cells restarted cycling after the cessation of chemotherapy. The low chemo-sensitivity of most solid tumors is at least in part due to the large majority of cancer cells in solid tumors being quiescent [1]
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