Nanofabricated particles for engineered drug therapies: a preliminary biodistribution study of PRINT nanoparticles. Gratton, S. E A, Pohlhaus, P. D, Lee, J., Guo, J., Cho, M. J, & Desimone, J. M J Control Release, 121(1-2):10–18, 2007. Place: Netherlands ISBN: 1873-4995
doi  abstract   bibtex   
A novel method for the fabrication of polymeric particles on the order of tens of nanometers to several microns is described. This imprint lithographic technique called PRINT (Particle Replication In Non-wetting Templates), takes advantage of the unique properties of elastomeric molds comprised of a low surface energy perfluoropolyether network, allowing the production of monodisperse, shape-specific nanoparticles from an extensive array of organic precursors. This engineered nature of particle production has a number of advantages over the construction of traditional nanoparticles such as liposomes, dendrimers, and colloidal precipitates. The gentle "top down" approach of PRINT enables the simultaneous and independent control over particle size and shape, composition, and surface functionality, and permits the loading of delicate cargos such as small organic therapeutics and biological macromolecules. Thus, this single tool serves as a comprehensive platform for the rational design and investigation of new nanocarriers in medicine, having applications ranging from therapeutics to advanced diagnostics. Preliminary in vitro and in vivo studies were conducted, demonstrating the future utility of PRINT particles as delivery vectors in nanomedicine. Monodisperse 200 nm poly(ethylene glycol)-based (PEG) particles were fabricated using PRINT methodology and characterized via scanning electron microscopy and dynamic light scattering. Incubation with HeLa cells showed very little cytotoxicity, even at high concentrations. The biodistribution and pharmacokinetics of [(125)I]-labeled particles were studied in healthy mice following bolus tail vein administration. The particles were distributed mainly to the liver and the spleen with an apparent distribution t(1/2) of approximately 17 min followed by slow redistribution with a t(1/2) of 3.3 h. The volume of distribution for the central and peripheral compartments was found to be approximately 3 mL and 5 mL, respectively.
@article{gratton_nanofabricated_2007,
	title = {Nanofabricated particles for engineered drug therapies: a preliminary biodistribution study of {PRINT} nanoparticles.},
	volume = {121},
	doi = {10.1016/j.jconrel.2007.05.027},
	abstract = {A novel method for the fabrication of polymeric particles on the order of tens of nanometers to several microns is described. This imprint lithographic technique called PRINT (Particle Replication In Non-wetting Templates), takes advantage of the unique properties of elastomeric molds comprised of a low surface energy perfluoropolyether network, allowing the production of monodisperse, shape-specific nanoparticles from an extensive array of organic precursors. This engineered nature of particle production has a number of advantages over the construction of traditional nanoparticles such as liposomes, dendrimers, and colloidal precipitates. The gentle "top down" approach of PRINT enables the simultaneous and independent control over particle size and shape, composition, and surface functionality, and permits the loading of delicate cargos such as small organic therapeutics and biological macromolecules. Thus, this single tool serves as a comprehensive platform for the rational design and investigation of new nanocarriers in medicine, having applications ranging from therapeutics to advanced diagnostics. Preliminary in vitro and in vivo studies were conducted, demonstrating the future utility of PRINT particles as delivery vectors in nanomedicine. Monodisperse 200 nm poly(ethylene glycol)-based (PEG) particles were fabricated using PRINT methodology and characterized via scanning electron microscopy and dynamic light scattering. Incubation with HeLa cells showed very little cytotoxicity, even at high concentrations. The biodistribution and pharmacokinetics of [(125)I]-labeled particles were studied in healthy mice following bolus tail vein administration. The particles were distributed mainly to the liver and the spleen with an apparent distribution t(1/2) of approximately 17 min followed by slow redistribution with a t(1/2) of 3.3 h. The volume of distribution for the central and peripheral compartments was found to be approximately 3 mL and 5 mL, respectively.},
	language = {eng},
	number = {1-2},
	journal = {J Control Release},
	author = {Gratton, Stephanie E A and Pohlhaus, Patrick D and Lee, Jin and Guo, Ji and Cho, Moo J and Desimone, Joseph M},
	year = {2007},
	pmid = {17643544},
	note = {Place: Netherlands
ISBN: 1873-4995},
	keywords = {Acrylates, Animals, Biocompatible Materials, Drug Therapy, Ethers, Fluorocarbons, Iodine Radioisotopes, Light, Liposomes, Mice, Nanomedicine, Nanoparticles, Nanotechnology, Particle Size, Pharmacokinetics, Polyethylene Glycols, Propylene Glycols, Scattering, Radiation, Styrenes, Tissue Distribution, research support, n.i.h., extramural, research support, u.s. gov't, non-p.h.s.},
	pages = {10--18},
}
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