4.5 Article

Targeted delivery of a proapoptotic peptide to tumors in vivo

Journal

JOURNAL OF DRUG TARGETING
Volume 19, Issue 7, Pages 582-588

Publisher

INFORMA HEALTHCARE
DOI: 10.3109/1061186X.2010.542245

Keywords

Drug vectorization; cancer; integr alpha(v)beta(3); RGD peptide

Funding

  1. ARC (Association pour la Recherche sur le Cancer)
  2. INCA (Institut National du Cancer)
  3. CLARA (Canceropole Lyon Auvergne Rhone-Alpes)
  4. University Joseph Fourier
  5. INSERM (Institut National de la Sante et de la Recherche Medicale)
  6. ANR (Agence Nationale pour la Recherche)

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RGD peptides recognize the a alpha(v)beta(3) integrin, a receptor that is overexpressed on the surface of both tumor blood vessels and cancerous cells. These peptides are powerful tools that act as single antiangiogenic molecules, but recently also have been used for tumor imaging and drug targeting. We designed the molecule RAFT-(c[-RGDfK-])(4), a constrained and chemically defined entity that can be produced at clinical-grade quality. This scaffold was covalently coupled via a labile bridge to the proapoptotic peptide (KLAKLAK)(2) (RAFT-RGD-KLA). A fluorescent, activatable probe was also introduced, allowing intracellular localization. At 2.5 mu M, this molecule induced the intracellular release of an active KLA peptide, which in turn caused mitochondrial depolarization and cell death in vitro in tumor cells. In a mouse model, the RAFT-RGD-KLA peptide was found to prevent the growth of remote subcutaneous tumors. This study demonstrated that the antitumor peptide is capable of killing tumor cells in an RGD-dependent manner, thus lowering the nonspecific cytotoxic effects expected to occur when using cationic cytotoxic peptides. Thus, this chemistry is suitable for the design of complex, multifunctional molecules that can be used for both imaging and therapeutics, representing the next generation of perfectly controlled, targeted drug-delivery systems.

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