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Efficient delivery of cyclic peptides into mammalian cells with short sequence motifs.


ABSTRACT: Cyclic peptides hold great potential as therapeutic agents and research tools, but their broad application has been limited by poor membrane permeability. Here, we report a potentially general approach for intracellular delivery of cyclic peptides. Short peptide motifs rich in arginine and hydrophobic residues (e.g., F?RRRR, where ? is l-2-naphthylalanine), when embedded into small- to medium-sized cyclic peptides (7-13 amino acids), bound to the plasma membrane of mammalian cultured cells and were subsequently internalized by the cells. Confocal microscopy and a newly developed peptide internalization assay demonstrated that cyclic peptides containing these transporter motifs were translocated into the cytoplasm and nucleus at efficiencies 2-5-fold higher than that of nonaarginine (R(9)). Furthermore, incorporation of the F?RRRR motif into a cyclic peptide containing a phosphocoumaryl aminopropionic acid (pCAP) residue generated a cell permeable, fluorogenic probe for detecting intracellular protein tyrosine phosphatase activities.

SUBMITTER: Qian Z 

PROVIDER: S-EPMC3574231 | biostudies-literature | 2013 Feb

REPOSITORIES: biostudies-literature

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Efficient delivery of cyclic peptides into mammalian cells with short sequence motifs.

Qian Ziqing Z   Liu Tao T   Liu Yu-Yu YY   Briesewitz Roger R   Barrios Amy M AM   Jhiang Sissy M SM   Pei Dehua D  

ACS chemical biology 20121112 2


Cyclic peptides hold great potential as therapeutic agents and research tools, but their broad application has been limited by poor membrane permeability. Here, we report a potentially general approach for intracellular delivery of cyclic peptides. Short peptide motifs rich in arginine and hydrophobic residues (e.g., FΦRRRR, where Φ is l-2-naphthylalanine), when embedded into small- to medium-sized cyclic peptides (7-13 amino acids), bound to the plasma membrane of mammalian cultured cells and w  ...[more]

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