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Rapid Decrease in Delivery of Chemotherapy to Tumors after Anti-VEGF Therapy: Implications for Scheduling of Anti-Angiogenic Drugs

  作者 Van der Veldt, AAM; Lubberink, M; Bahce, I; Walraven, M; de Boer, MP; Greuter, HNJM; Hendrikse, NH; Eriksson, J; Windhorst, AD; Postmus, PE; Verheul, HM; Serne, EH; Lammertsma, AA; Smit, EF  
  选自 期刊  Cancer Cell;  卷期  2012年21-1;  页码  82-91  
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[摘要]Current strategies combining anti-angiogenic drugs with chemotherapy provide clinical benefit in cancer patients. It is assumed that anti-angiogenic drugs, such as bevacizumab, transiently normalize abnormal tumor vasculature and contribute to improved delivery of subsequent chemotherapy. To investigate this concept, a study was performed in non-small cell lung cancer (NSCLC) patients using positron emission tomography (PET) and radiolabeled docetaxel ([(11)C]docetaxel). In NSCLC, bevacizumab reduced both perfusion and net influx rate of [(11)C]docetaxel within 5 hr. These effects persisted after 4 days. The clinical relevance of these findings is notable, as there was no evidence for a substantial improvement in drug delivery to tumors. These findings highlight the importance of drug scheduling and advocate further studies to optimize scheduling of anti-angiogenic drugs.

 
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