Matrix Metalloproteinase-Assisted Triggered Release of Liposomal Contents

We offer a novel methodology for formulating liposomes by incorporating sequence-specific collagen-mimetic peptides such that they are specifically “uncorked” by a matrix metalloproteinase, MMP-9. By encapsulating carboxyfluorescein (as a self-quenching fluorescent dye), we demonstrate that the time...

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Veröffentlicht in:Bioconjugate chemistry 2008-01, Vol.19 (1), p.57-64
Hauptverfasser: Sarkar, Nihar, Banerjee, Jayati, Hanson, Andrea J, Elegbede, Adekunle I, Rosendahl, Theresa, Krueger, Aaron B, Banerjee, Abir L, Tobwala, Shakila, Wang, Rongying, Lu, Xiaoning, Mallik, Sanku, Srivastava, D. K
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Sprache:eng
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Zusammenfassung:We offer a novel methodology for formulating liposomes by incorporating sequence-specific collagen-mimetic peptides such that they are specifically “uncorked” by a matrix metalloproteinase, MMP-9. By encapsulating carboxyfluorescein (as a self-quenching fluorescent dye), we demonstrate that the time-dependent release of the dye from liposomes is due to the specific enzymatic cleavage of the surface-exposed collagen-mimetic peptides. The specificity of such cleavage is attested by the fact that the liposomal “uncorking” and their content release occur only by MMP-9 and not by a general proteolytic enzyme, trypsin, despite the fact that the collagen mimetic peptides contain the trypsin cleavage site. The mechanistic details underlying the formulations of liposomes and their enzyme-selective “uncorking” and content release are discussed. Arguments are presented that such liposomes can be fine-tuned to serve as the drug delivery vehicles for the detection and treatment of various human diseases, which occur due to the overexpression of a variety of pathogenic matrix metalloproteinases.
ISSN:1043-1802
1520-4812
DOI:10.1021/bc070081p