Literature DB >> 27491413

Multi-parametric surface plasmon resonance platform for studying liposome-serum interactions and protein corona formation.

Otto K Kari1, Tatu Rojalin1, Stefano Salmaso2, Michela Barattin2, Hanna Jarva3, Seppo Meri3, Marjo Yliperttula1,2, Tapani Viitala4, Arto Urtti1,5.   

Abstract

When nanocarriers are administered into the blood circulation, a complex biomolecular layer known as the "protein corona" associates with their surface. Although the drivers of corona formation are not known, it is widely accepted that this layer mediates biological interactions of the nanocarrier with its surroundings. Label-free optical methods can be used to study protein corona formation without interfering with its dynamics. We demonstrate the proof-of-concept for a multi-parametric surface plasmon resonance (MP-SPR) technique in monitoring the formation of a protein corona on surface-immobilized liposomes subjected to flowing 100 % human serum. We observed the formation of formulation-dependent "hard" and "soft" coronas with distinct refractive indices, layer thicknesses, and surface mass densities. MP-SPR was also employed to determine the affinity (K D ) of a complement system molecule (C3b) with cationic liposomes with and without polyethylene glycol. Tendency to create a thick corona correlated with a higher affinity of opsonin C3b for the surface. The label-free platform provides a fast and robust preclinical tool for tuning nanocarrier surface architecture and composition to control protein corona formation.

Entities:  

Keywords:  Complement system; Liposome; Multi-parametric surface plasmon resonance (MP-SPR); Opsonin; Protein corona; Soft corona

Mesh:

Substances:

Year:  2017        PMID: 27491413     DOI: 10.1007/s13346-016-0320-0

Source DB:  PubMed          Journal:  Drug Deliv Transl Res        ISSN: 2190-393X            Impact factor:   4.617


  37 in total

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4.  Characterizing ultrathin and thick organic layers by surface plasmon resonance three-wavelength and waveguide mode analysis.

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Review 5.  The nanoparticle biomolecule corona: lessons learned - challenge accepted?

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Review 6.  Surface plasmon resonance in monitoring of complement activation on biomaterials.

Authors:  Yusuke Arima; Mitsuaki Toda; Hiroo Iwata
Journal:  Adv Drug Deliv Rev       Date:  2011-07-23       Impact factor: 15.470

7.  Star-like oligo-arginyl-maltotriosyl derivatives as novel cell-penetrating enhancers for the intracellular delivery of colloidal therapeutic systems.

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Review 8.  Activation of complement by therapeutic liposomes and other lipid excipient-based therapeutic products: prediction and prevention.

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Journal:  Adv Drug Deliv Rev       Date:  2011-07-14       Impact factor: 15.470

9.  Poly(ethylene glycol)s generate complement activation products in human serum through increased alternative pathway turnover and a MASP-2-dependent process.

Authors:  I Hamad; A C Hunter; J Szebeni; S M Moghimi
Journal:  Mol Immunol       Date:  2008-10-11       Impact factor: 4.407

10.  Elucidating the signal responses of multi-parametric surface plasmon resonance living cell sensing: a comparison between optical modeling and drug-MDCKII cell interaction measurements.

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Journal:  PLoS One       Date:  2013-08-27       Impact factor: 3.240

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4.  Shape and Phase Transitions in a PEGylated Phospholipid System.

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Review 5.  Surface Plasmon Resonance as a Characterization Tool for Lipid Nanoparticles Used in Drug Delivery.

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Review 6.  Understanding the relevance of protein corona in nanoparticle-based therapeutics and diagnostics.

Authors:  Debolina Chakraborty; K R Ethiraj; Amitava Mukherjee
Journal:  RSC Adv       Date:  2020-07-21       Impact factor: 4.036

7.  Accurate Correction of the "Bulk Response" in Surface Plasmon Resonance Sensing Provides New Insights on Interactions Involving Lysozyme and Poly(ethylene glycol).

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8.  Biophysical Characterization of Supported Lipid Bilayers Using Parallel Dual-Wavelength Surface Plasmon Resonance and Quartz Crystal Microbalance Measurements.

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  8 in total

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