| Literature DB >> 34797630 |
Aparna Nandakumar1, Wei Wei2, Ghizal Siddiqui1, Huayuan Tang3, Yuhuan Li1,4, Aleksandr Kakinen5, Xulin Wan2, Kairi Koppel1, Sijie Lin6, Thomas P Davis5, David T Leong7, Darren J Creek1, Feng Ding3, Yang Song8,9, Pu Chun Ke1,5,10.
Abstract
Much has been learned about the protein coronae and their biological implications within the context of nanomedicine and nanotoxicology. However, no data is available about the protein coronae associated with nanoparticles undergoing spontaneous surface-energy minimization, a common phenomenon during the synthesis and shelf life of nanomaterials. Accordingly, here we employed gold nanoparticles (AuNPs) possessing the three initial states of spiky, midspiky, and spherical shapes and determined their acquisition of human plasma protein coronae with label-free mass spectrometry. The AuNPs collected coronal proteins that were different in abundance, physicochemical parameters, and interactive biological network. The size and structure of the coronal proteins matched the morphology of the AuNPs, where small globular proteins and large fibrillar proteins were enriched on spiky AuNPs, while large proteins were abundant on spherical AuNPs. Furthermore, the AuNPs induced endothelial leakiness to different degrees, which was partially negated by their protein coronae as revealed by confocal fluorescence microscopy, in vitro and ex vivo transwell assays, and signaling pathway assays. This study has filled a knowledge void concerning the dynamic protein corona of nanoparticles possessing an evolving morphology and shed light on their implication for future nanomedicine harnessing the paracellular pathway.Entities:
Keywords: endothelial leakiness; morphology; nanomedicine; protein corona; proteomics
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Year: 2021 PMID: 34797630 PMCID: PMC8692073 DOI: 10.1021/acsami.1c19824
Source DB: PubMed Journal: ACS Appl Mater Interfaces ISSN: 1944-8244 Impact factor: 9.229