Literature DB >> 21545169

Spontaneous membrane-translocating peptides by orthogonal high-throughput screening.

Jessica R Marks1, Jesse Placone, Kalina Hristova, William C Wimley.   

Abstract

Combinatorial peptide chemistry and orthogonal high-throughput screening were used to select peptides that spontaneously translocate across synthetic lipid bilayer membranes without permeabilization. A conserved sequence motif was identified that contains several cationic residues in conserved positions in an otherwise hydrophobic sequence. This 9-residue motif rapidly translocates across synthetic multibilayer vesicles and into cells while carrying a large polar dye as a "cargo" moiety. The extraordinary ability of this family of peptides to spontaneously translocate across bilayers without an energy source of any kind is distinctly different from the behavior of the well-known, highly cationic cell-penetrating peptides, such as the HIV tat peptide, which do not translocate across synthetic bilayers, and enter cells mostly by active endocytosis. Peptides that translocate spontaneously across membranes have the potential to transform the field of drug design by enabling the delivery of otherwise membrane-impermeant polar drugs into cells and tissues. Here we describe the chemical tools needed to rapidly identify spontaneous membrane translocating peptides.
© 2011 American Chemical Society

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Year:  2011        PMID: 21545169      PMCID: PMC3118567          DOI: 10.1021/ja2017416

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  22 in total

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6.  Stability of cell-penetrating peptide-morpholino oligomer conjugates in human serum and in cells.

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  66 in total

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2.  A membrane-translocating peptide penetrates into bilayers without significant bilayer perturbations.

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6.  Turning a Substrate Peptide into a Potent Inhibitor for the Histone Methyltransferase SETD8.

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Journal:  ACS Med Chem Lett       Date:  2016-10-11       Impact factor: 4.345

7.  Label-free discrimination of membrane-translocating peptides on porous silicon microfluidic biosensors.

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8.  Charge Distribution Fine-Tunes the Translocation of α-Helical Amphipathic Peptides across Membranes.

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Review 9.  A common landscape for membrane-active peptides.

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10.  Implicit membrane treatment of buried charged groups: application to peptide translocation across lipid bilayers.

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