For example, the gemcitabine (Gemzar, Eli Lilly, Indianapolis, IN

For example, the gemcitabine (Gemzar, Eli Lilly, Indianapolis, IN) for metastatic pancreatic cancer increased survival from 4.41 months to 5.65 months (P = 0.0025),23 and in another example, SCH772984 the addition of bevacizumab (Avastin, Genentech, South San Francisco, CA) to chemotherapy for advanced colon cancer improved median survival from 15.6 months to 20.3 months with a hazard ratio of 0.66.24 Now that sorafenib has been shown to improve survival in advanced HCC, studies evaluating the agent in patients with earlier stage disease are ongoing, and may provide even greater gains. Nevertheless, this is an important

advance for patients with HCC and will likely lead to further approvals based on combinations of new agents with sorafenib and additional new single agents to use in the front-line setting and after progression on sorafenib and beyond.25 In clinical practice, the decision to initiate sorafenib is guided by a patient’s tumor burden, liver disease, and ability to carry out daily

activities/performance status (PS). For patients with Child A cirrhosis and good PS, studies have proven a benefit of 400 mg orally twice a day. Baseline hematologic and chemistry parameters should be drawn, as well click here as an alfa-fetoprotein (AFP) when relevant. Although AFP as an endpoint was not well studied in the sorafenib trials, it may provide additional insight into the clinical activity in any one patient.26 The success in keeping patients on therapy requires proactive management of side effects by the treating physician. Patients should be assessed within 7-10 days of starting drug for adverse events. Careful questioning regarding changes in general activity, oral intake, skin changes, nausea, vomiting and stool changes are important as these are the most common toxicities. In addition, careful examination of the skin is required with particular attention

to areas exposed to repetitive trauma such as the hands and feet as these are areas where skin toxicity is most noticeable and symptomatic. During this first follow-up repeat hematology and chemistries are drawn including a phosphorus level as hypophosphatemia selleck kinase inhibitor has been associated with sorafenib. In addition, a transient rise in total bilirubin can occur after initiation of sorafenib though this often returns to baseline quickly. If a patient is tolerating the drug well, then the same dose can be continued with a follow-up at 2 week intervals until the patient has proven to be stable on the drug. For patients experiencing toxicities consideration to either dose reduce or hold the drug should be made depending on the severity. Reintroduction of the drug can occur once toxicities have approached baseline. Consideration can be given to reintroduce the drug at the same level with close follow-up or, if toxicity was significant, dose reduction by one level.

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