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Differentiated Thyroid Cancer

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33 Table 10. Potential Toxicities and Recommended Screening or Surveillance Monitoring Approaches in Patients Started on Kinase Inhibitor Therapy Toxicity Recommended Screening/Monitoring Hypertension Frequent blood pressure monitoring, most critical during the first 8 weeks of therapy. If hypertension is induced, therapy should be individualized to patient response. Note: effective and expeditious management of hypertension is critical - and may reduce potential for cardiotoxicity. If antihypertensive therapy is needed, calcium channel blockers (e.g., amlodipine) may be most effective. Cutaneous/ mucocutaneous toxicities Careful patient reporting of rash/mouth sores, patient awareness and education related to increased potential for photosentization/sunburn. Hepatotoxicity Serial assessment of alanine serum transferase (AST), alkaline phosphatase and bilirubin – most critical during the first 8 weeks of therapy Note: Dose reduction of kinase inhibitor therapy is commonly required due to hepatic toxicity. Cardiotoxicity ECG pre-therapy and frequently during therapy • Hold (or do not initiate) kinase inhibitor therapy if QTc >480 msec Echocardiogram, elective - but recommended in any patient with cardiac history; especially important in patient with hypertension, symptoms consistent with congestive heart failure or coronary artery disease and in patients receiving sunitinib. Hypothyroidism TSH should be assessed frequently, with levothyroxine dosage altered in response to rising TSH if observed. Nephrotoxicity Serial serum creatinine, urine analysis with protein determination Hematological toxicities Serial CBC/differential Pancreatitis Serial amylase Teratogenicity Pre-therapy pregnancy testing and effective contraception in women and men of childbearing potential

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