
AbstractA series of cyclic peptides containing a number of tryptophan (W) and glutamic acid (E) residues were synthesized and evaluated as pH-sensitive agents for targeting of acidic tissue and pH-dependent cytoplasmic delivery of molecules. Biophysical studies revealed the molecular mechanism of peptides action and localization within the lipid bilayer of the membrane at high and low pHs. The symmetric, c[(WE)4WC] and asymmetric, c[E4W5C], cyclic peptides translocated amanitin, a polar cargo molecule of similar size, across the lipid bilayer and induced cell death in a pH- and concentration-dependent manner. Fluorescently-labelled peptides were evaluated for targeting of acidic 4T1 mammary tumors in mice. The highest tumor to muscle ratio (5.6) was established for asymmetric cyclic peptide, c[E4W5C], at 24 hours after intravenous administration. pH-insensitive cyclic peptide c[R4W5C], where glutamic acid residues (E) were replaced by positively charged arginine residues (R), did not exhibit tumor targeting. We have introduced a novel class of cyclic peptides, which can be utilized as a new pH-sensitive tool in investigation or targeting of acidic tissue.
Amanitins, Lipid Bilayers, Glutamic Acid, Pharmaceutics and Drug Design, Mammary Neoplasms, Animal, Peptides, Cyclic, Article, Mice, Animals, Amino Acids, Cancer, Molecular Structure, and Proteins, Tryptophan, Hydrogen-Ion Concentration, 540, Pharmaceutical Preparations, Drug delivery, Other Pharmacy and Pharmaceutical Sciences, Female, Peptides, Hydrophobic and Hydrophilic Interactions
Amanitins, Lipid Bilayers, Glutamic Acid, Pharmaceutics and Drug Design, Mammary Neoplasms, Animal, Peptides, Cyclic, Article, Mice, Animals, Amino Acids, Cancer, Molecular Structure, and Proteins, Tryptophan, Hydrogen-Ion Concentration, 540, Pharmaceutical Preparations, Drug delivery, Other Pharmacy and Pharmaceutical Sciences, Female, Peptides, Hydrophobic and Hydrophilic Interactions
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