Author/Authors :
Simon E. Aspland، نويسنده , , Carlo Ballatore، نويسنده , , Rosario Castillo، نويسنده , , Joel Desharnais، نويسنده , , Trisha Eustaquio، نويسنده , , Philip Goelet، نويسنده , , Zijian Guo، نويسنده , , Qing Li، نويسنده , , David Nelson، نويسنده , , Chengzao Sun، نويسنده , , Angelo J. Castellino، نويسنده , , Michael J. Newman، نويسنده ,
Abstract :
In the present work, we explore the possibility of introducing selectivity to existing chemotherapeutics via the design of non-pro-drug, bi-functional molecules comprising a microtubule-binding agent and a substrate for a disease-associated kinase. The design, synthesis, and in vitro biological evaluation of paclitaxel–thymidine and vinblastine–thymidine bi-functional conjugates are reported here. This work provides the first account of ‘kinase-mediated trapping’ of cancer therapeutics.
Keywords :
Kinase-mediated trapping , Thymidine kinase 1 , paclitaxel , thymidine , Fluorescein , vinblastine
