Novel human-derived cell-penetrating peptides for specific subcellular delivery of therapeutic biomolecules.

نویسندگان

  • Catherine De Coupade
  • Antonio Fittipaldi
  • Vanessa Chagnas
  • Matthieu Michel
  • Sophie Carlier
  • Ennio Tasciotti
  • Audrey Darmon
  • Denis Ravel
  • Jonathan Kearsey
  • Mauro Giacca
  • Françoise Cailler
چکیده

Short peptide sequences that are able to transport molecules across the cell membrane have been developed as tools for intracellular delivery of therapeutic molecules. This work describes a novel family of cell-penetrating peptides named Vectocell peptides [also termed DPVs (Diatos peptide vectors)]. These peptides, originating from human heparin binding proteins and/or anti-DNA antibodies, once conjugated to a therapeutic molecule, can deliver the molecule to either the cytoplasm or the nucleus of mammalian cells. Vectocell peptides can drive intracellular delivery of molecules of varying molecular mass, including full-length active immunoglobulins, with efficiency often greater than that of the well-characterized cell-penetrating peptide Tat. The internalization of Vectocell peptides has been demonstrated to occur in both adherent and suspension cell lines as well as in primary cells through an energy-dependent endocytosis process, involving cell-membrane lipid rafts. This endocytosis occurs after binding of the cell-penetrating peptides to extracellular heparan sulphate proteoglycans, except for one particular peptide (DPV1047) that partially originates from an anti-DNA antibody and is internalized in a caveolar independent manner. These new therapeutic tools are currently being developed for intracellular delivery of a number of active molecules and their potentiality for in vivo transduction investigated.

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عنوان ژورنال:
  • The Biochemical journal

دوره 390 Pt 2  شماره 

صفحات  -

تاریخ انتشار 2005