4.5 Article

A Nanoparticle-Based Combination Chemotherapy Delivery System for Enhanced Tumor Killing by Dynamic Rewiring of Signaling Pathways

Journal

SCIENCE SIGNALING
Volume 7, Issue 325, Pages -

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/scisignal.2005261

Keywords

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Funding

  1. NIH
  2. Center for Cancer Nanotechnology Excellence [P30-CA14051, U54-CA151884, U54-CA112967, R01-ES015339, R21-ES020466]
  3. Breast Cancer Alliance Exceptional Project Grant
  4. National Science Foundation Graduate Research Fellowship
  5. National Health and Medical Research Council
  6. NIH fellowship: Kirschstein NRSA [1F32EB017614-01]
  7. National Sciences and Engineering Research Council
  8. Koch Institute Frontier Research Program
  9. Kathy and Curt Marble Fund for Cancer Research

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Exposure to the EGFR (epidermal growth factor receptor) inhibitor erlotinib promotes the dynamic rewiring of apoptotic pathways, which sensitizes cells within a specific period to subsequent exposure to the DNA-damaging agent doxorubicin. A critical challenge for translating this therapeutic network rewiring into clinical practice is the design of optimal drug delivery systems. We report the generation of a nanoparticle delivery vehicle that contained more than one therapeutic agent and produced a controlled sequence of drug release. Liposomes, representing the first clinically approved nanomedicine systems, are well-characterized, simple, and versatile platforms for the manufacture of functional and tunable drug carriers. Using the hydrophobic and hydrophilic compartments of liposomes, we effectively incorporated both hydrophobic (erlotinib) and hydrophilic (doxorubicin) small molecules, through which we achieved the desired time sequence of drug release. We also coated the liposomes with folate to facilitate targeting to cancer cells. When compared to the time-staggered application of individual drugs, staggered release from tumor-targeted single liposomal particles enhanced dynamic rewiring of apoptotic signaling pathways, resulting in improved tumor cell killing in culture and tumor shrinkage in animal models.

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