9^th World Drug Delivery Summit

Biography

Biography: Kristen K Comfort

Abstract

Colloidal gold nanoparticles (AuNPs) are being increasingly utilized in biomedical applications, such as drug/gene delivery and bio-imaging techniques. However, the effectiveness of these procedures are highly dependent upon sustained, strong interactions between AuNPs and the surrounding environment; referred to as the nano-bio interface. Recently, it has been established that this interface is reliant on the formation of a protein-NP complex. The protein corona surrounding NPs is dynamic by nature and is dependent upon numerous factors including the environmental composition and specific physicochemical properties of the particles. However, little is currently known about how physiological variables, such as fluid flow and biological fluids outside of blood, modulate the protein-NP complex and subsequent particokinetics. We demonstrated that the addition of shear stress, introduced through dynamic fluid movement within the cellular system, severely disrupted the AuNP protein corona, resulting in an altered nano-bio interface and AuNP deposition efficiency. As drug/gene delivery require high AuNP delivery to a target, this loss of NP transport potential highlights a current limitation within the field. Moreover, circulating NPs have a strong likelihood of encountering multiple physiological environments, such as interstitial and lysosomal fluids; of which the influence on the nano-bio interface has yet to be explored. We determined that when dispersed in these biological fluids, both the protein corona and the deposited AuNP dose was altered; as a function of original surface chemistry. Given these results, it was clear that physiologically variables should be accounted for during design and evaluation of nano-based drug delivery systems.