In situ analysis of liposome hard and soft protein corona structure and composition in a single label-free workflow

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dc.contributor.author Kari, Otto K.
dc.contributor.author Ndika, Joseph
dc.contributor.author Parkkila, Petteri
dc.contributor.author Louna, Antti
dc.contributor.author Lajunen, Tatu
dc.contributor.author Puustinen, Anne
dc.contributor.author Viitala, Tapani
dc.contributor.author Alenius, Harri
dc.contributor.author Urtti, Arto
dc.date.accessioned 2020-02-05T14:36:01Z
dc.date.available 2020-02-05T14:36:01Z
dc.date.issued 2020-01-21
dc.identifier.citation Kari , O K , Ndika , J , Parkkila , P , Louna , A , Lajunen , T , Puustinen , A , Viitala , T , Alenius , H & Urtti , A 2020 , ' In situ analysis of liposome hard and soft protein corona structure and composition in a single label-free workflow ' , Nanoscale , vol. 12 , no. 3 , pp. 1728-1741 . https://doi.org/10.1039/C9NR08186K
dc.identifier.other PURE: 131478272
dc.identifier.other PURE UUID: fb56b432-a871-4803-a74d-1e63fb5a311e
dc.identifier.other RIS: urn:670748CFF8C331D35FAFF4759F2BCE7F
dc.identifier.other ORCID: /0000-0001-6234-9193/work/68615161
dc.identifier.other ORCID: /0000-0002-1201-5010/work/68615423
dc.identifier.other ORCID: /0000-0001-9074-9450/work/68616521
dc.identifier.other ORCID: /0000-0002-2717-0232/work/68616860
dc.identifier.other ORCID: /0000-0003-0669-1300/work/68617859
dc.identifier.other ORCID: /0000-0002-0262-9975/work/68618033
dc.identifier.other WOS: 000509545700045
dc.identifier.uri http://hdl.handle.net/10138/311133
dc.description.abstract Methodological constraints have limited our ability to study protein corona formation, slowing nanomedicine development and their successful translation into the clinic. We determined hard and soft corona structural properties along with the corresponding proteomic compositions on liposomes in a label-free workflow: surface plasmon resonance and a custom biosensor for in situ structure determination on liposomes and corona separation, and proteomics using sensitive nanoliquid chromatography tandem mass spectrometry with open-source bioinformatics platforms. Undiluted human plasma under dynamic flow conditions was used for in vivo relevance. Proof-of-concept is presented with a regular liposome formulation and two light-triggered indocyanine green (ICG) liposome formulations in preclinical development. We observed formulation-dependent differences in corona structure (thickness, protein-to-lipid ratio, and surface mass density) and protein enrichment. Liposomal lipids induced the enrichment of stealth-mediating apolipoproteins in the hard coronas regardless of pegylation, and their preferential enrichment in the soft corona of the pegylated liposome formulation with ICG was observed. This suggests that the soft corona of loosely interacting proteins contributes to the stealth properties as a component of the biological identity modulated by nanomaterial surface properties. The workflow addresses significant methodological gaps in biocorona research by providing truly complementary hard and soft corona compositions with corresponding in situ structural parameters for the first time. It has been designed into a convenient and easily reproducible single-experiment format suited for preclinical development of lipid nanomedicines. fi
dc.format.extent 14
dc.language.iso eng
dc.relation.ispartof Nanoscale
dc.rights cc_by
dc.rights.uri info:eu-repo/semantics/openAccess
dc.subject 318 Medical biotechnology
dc.subject PLASMON RESONANCE SENSORS
dc.subject PEG CHAIN-LENGTH
dc.subject BIOMOLECULAR CORONA
dc.subject COMPLEMENT ACTIVATION
dc.subject BIOLOGICAL IDENTITY
dc.subject TIME-EVOLUTION
dc.subject NANOPARTICLES
dc.subject SURFACE
dc.subject VIVO
dc.subject ADSORPTION
dc.subject PLASMON RESONANCE SENSORS
dc.subject PEG CHAIN-LENGTH
dc.subject BIOMOLECULAR CORONA
dc.subject COMPLEMENT ACTIVATION
dc.subject BIOLOGICAL IDENTITY
dc.subject TIME-EVOLUTION
dc.subject NANOPARTICLES
dc.subject SURFACE
dc.subject VIVO
dc.subject ADSORPTION
dc.title In situ analysis of liposome hard and soft protein corona structure and composition in a single label-free workflow en
dc.type Article
dc.contributor.organization Division of Pharmaceutical Biosciences
dc.contributor.organization Drug Delivery Unit
dc.contributor.organization HUMI - Human Microbiome Research
dc.contributor.organization Pharmaceutical biophysics group
dc.contributor.organization Pharmaceutical Nanotechnology
dc.contributor.organization Department of Chemistry
dc.contributor.organization University Management
dc.contributor.organization Division of Pharmaceutical Chemistry and Technology
dc.contributor.organization Drug Research Program
dc.contributor.organization Doctoral Programme in Microbiology and Biotechnology
dc.contributor.organization Drug Delivery
dc.description.reviewstatus Peer reviewed
dc.relation.doi https://doi.org/10.1039/C9NR08186K
dc.relation.issn 2040-3364
dc.rights.accesslevel openAccess
dc.type.version publishedVersion

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