Biodistribution studies of protein cage nanoparticles demonstrate broad tissue distribution and rapid clearance in vivo
Date
2007-12
Journal Title
Journal ISSN
Volume Title
Publisher
Abstract
Protein cage nanoparticles have the potential to serve as multifunctional cell targeted, imaging and therapeutic platforms for broad applications in medicine. However, before they find applications in medicine, their biocompatibility in vivo needs to be demonstrated. We provide here baseline biodistribution information of two different spherical protein cage nanoplatforms, the 28 nm viral Cowpea chlorotic mottle virus (CCMV) and the 12 nm heat shock protein (Hsp) cage. In naïve and immunized mice both nanoplatforms show similar broad distribution and movement throughout most tissues and organs, rapid excretion, the absence of long term persistence within mice tissue and organs, and no overt toxicity after a single injection. These results suggest that protein cage based nanoparticles may serve as safe, biocompatible, nanoplatforms for applications in medicine.
Description
Keywords
Citation
Kaiser, Coleen R., Michelle L. Flenniken, Eric Gillitzer, Ann L. Harmsen, Allen G. Harmsen, Mark A. Jutila, Trevor Douglas, Mark J. Young (2007). Biodistribution studies of protein cage nanoparticles demonstrate broad tissue distribution and rapid clearance in vivo. International Journal of Nanomedicine, 2 (4), 713-733.
Endorsement
Review
Supplemented By
Referenced By
Creative Commons license
Except where otherwised noted, this item's license is described as CC BY: This license lets you distribute, remix, tweak, and build upon this work, even commercially, as long as you credit the original creator for this work. This is the most accommodating of licenses offered. Recommended for maximum dissemination and use of licensed materials.