Abstract

An anti-angiogenic drug in cancer treatment prevents the growth of new blood vessels in tumors by binding to VEGF molecules, which otherwise induce endothelial cells inside blood vessels to sprout the blood supply toward the tumor. This would prevent the growth of new blood cells which will deprive the tumor of nutrients, thus decreasing its carrying capacity, and ultimately shrinking its volume. With new vascularization absent, the tumor will be isolated, making it easier to treat. Although there is an availability of various anti-angiogenic drugs, their effectiveness is low compared to other cancer treatments. We are specifically pinpointing the various combination of doses and the treatment timelines as reasonable factors to increase the effectiveness of the anti-angiogenic drug Bevacizumab, which can possibly prolong the patient’s survival rate and offer lower toxicity compared to other treatment modalities such as radiotherapy and chemotherapy. We have numerically analyzed different doses of Bevacizumab, including 15 mg/kg, an FDA-approved dose if offered in conjunction with chemotherapy drugs, carboplatin and paclitaxel, as a single-agent treatment option. Based on the results, the tumor volume was observed to be stabilizing for the duration of the treatment, which was chosen to be 400 days. The toxicity levels of these doses with Bevacizumab as a single-agent treatment option have not been tested in a clinical setting. However, these mathematically promising results can provide a gateway for the successful treatment of ovarian cancer in the future.

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