Literature DB >> 12237333

Translocation of liposomes into cancer cells by cell-penetrating peptides penetratin and tat: a kinetic and efficacy study.

Yun-Long Tseng1, Jun-Jen Liu, Ruey-Long Hong.   

Abstract

Unlike conventional liposomes, sterically stabilized liposomes, with their smaller volume of distribution and reduced clearance, preferentially convey encapsulated drugs into tumor sites. Despite these improvements, intracellular delivery is hampered by the stable drug retention of the liposomes, which diminishes the efficacy of the liposomal drug. To facilitate uptake of liposomal drugs into cells, two cell-penetrating peptides, penetratin (PEN) and TAT, derived from the HIV-1 TAT protein, were studied. In contrast to control peptides, both TAT and PEN enhanced the translocation efficiency of liposomes in proportion to the number of peptides attached to the liposomal surface. A peptide number of as few as five could enhance the intracellular delivery of liposomes. The kinetics of uptake was peptide- and cell-type dependent. Intracellular accumulation of TAT-liposomes increased with incubation time, but PEN-liposomes peaked at 1 h and then declined gradually. After treatment with 1 microg/ml doxorubicin equivalents of liposome for 2 h, TAT increased the doxorubicin uptake of A431 cells by 12-fold. However, the improvement of uptake of liposomal doxorubicin was not reflected by cytotoxicity in vitro or tumor control in vivo. Our results demonstrated that merely adding CPP to a liposome encapsulating anticancer drug was inadequate in improving its antitumor activity. An additional approach to enhance the intracellular release of the encapsulated drug is obviously necessary.

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Year:  2002        PMID: 12237333     DOI: 10.1124/mol.62.4.864

Source DB:  PubMed          Journal:  Mol Pharmacol        ISSN: 0026-895X            Impact factor:   4.436


  44 in total

1.  Passage times for polymer translocation pulled through a narrow pore.

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4.  Accumulation and toxicity of antibody-targeted doxorubicin-loaded PEG-PE micelles in ovarian cancer cell spheroid model.

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Review 5.  Delivery of nanomedicines to extracellular and intracellular compartments of a solid tumor.

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Review 6.  Cell penetrating peptides to dissect host-pathogen protein-protein interactions in Theileria-transformed leukocytes.

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7.  Intracellular fates of cell-penetrating block copolypeptide vesicles.

Authors:  Victor Z Sun; Zhibo Li; Timothy J Deming; Daniel T Kamei
Journal:  Biomacromolecules       Date:  2010-12-03       Impact factor: 6.988

8.  Synthesis and in vitro inhibition properties of oligonucleotide conjugates carrying amphipathic proline-rich peptide derivatives of the sweet arrow peptide (SAP).

Authors:  Santiago Grijalvo; Ramon Eritja
Journal:  Mol Divers       Date:  2012-03-06       Impact factor: 2.943

9.  Cellular uptake of electron paramagnetic resonance imaging probes through endocytosis of liposomes.

Authors:  Scott R Burks; Eugene D Barth; Howard J Halpern; Gerald M Rosen; Joseph P Y Kao
Journal:  Biochim Biophys Acta       Date:  2009-08-25

10.  Recent developments in peptide-based nucleic acid delivery.

Authors:  Sandra Veldhoen; Sandra D Laufer; Tobias Restle
Journal:  Int J Mol Sci       Date:  2008-07-16       Impact factor: 6.208

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