Combinatorial targeting and discovery of ligand-receptors in organelles of mammalian cells

نویسندگان

  • Roberto Rangel
  • Liliana Guzman-Rojas
  • Lucia G. le Roux
  • Fernanda I. Staquicini
  • Hitomi Hosoya
  • E. Magda Barbu
  • Michael G. Ozawa
  • Jing Nie
  • Kenneth Dunner Jr
  • Robert R. Langley
  • E. Helene Sage
  • Erkki Koivunen
  • Juri G. Gelovani
  • Roy R. Lobb
  • Richard L. Sidman
  • Renata Pasqualini
  • Wadih Arap
چکیده

Phage display screening allows the study of functional protein-protein interactions at the cell surface, but investigating intracellular organelles remains a challenge. Here we introduce internalizing-phage libraries to identify clones that enter mammalian cells through a receptor-independent mechanism and target-specific organelles as a tool to select ligand peptides and identify their intracellular receptors. We demonstrate that penetratin, an antennapedia-derived peptide, can be displayed on the phage envelope and mediate receptor-independent uptake of internalizing phage into cells. We also show that an internalizing-phage construct displaying an established mitochondria-specific localization signal targets mitochondria, and that an internalizing-phage random peptide library selects for peptide motifs that localize to different intracellular compartments. As a proof-of-concept, we demonstrate that one such peptide, if chemically fused to penetratin, is internalized receptor-independently, localizes to mitochondria, and promotes cell death. This combinatorial platform technology has potential applications in cell biology and drug development.

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عنوان ژورنال:

دوره 3  شماره 

صفحات  -

تاریخ انتشار 2012