Cancer Therapy: Preclinical Preclinical Optimization of MDM2 Antagonist Scheduling for Cancer Treatment by Using a Model-Based Approach

نویسندگان

  • Brian Higgins
  • Kelli Glenn
  • Antje Walz
  • Christian Tovar
  • Zoran Filipovic
  • Sazzad Hussain
  • Edmund Lee
  • Kenneth Kolinsky
  • Shahid Tannu
  • Violeta Adames
  • Rosario Garrido
  • Michael Linn
  • Christophe Meille
  • David Heimbrook
  • Lyubomir Vassilev
  • Kathryn Packman
چکیده

Purpose: Antitumor clinical activity has been demonstrated for the MDM2 antagonist RG7112, but patient tolerability for the necessary daily dosing was poor. Here, utilizing RG7388, a second-generation nutlin with superior selectivity and potency, we determine the feasibility of intermittent dosing to guide the selection of initial phase I scheduling regimens. Experimental Design: A pharmacokinetic–pharmacodynamic (PKPD) model was developed on the basis of preclinical data todetermine alternative dosing schedule requirements foroptimal RG7388-induced antitumor activity. This PKPDmodel was used to investigate the pharmacokinetics of RG7388 linked to the time-course of the antitumor effect in an osteosarcoma xenograft model in mice. These data were used to prospectively predict intermittent and continuous dosing regimens, resulting in tumor stasis in the same

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Preclinical optimization of MDM2 antagonist scheduling for cancer treatment by using a model-based approach.

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تاریخ انتشار 2014