The “gut” corona at the surface of nanoparticles is dependent on exposure to bile salts and phospholipids

Kihara, Shinji; Aljabbari, Anas; Bērziņš, Kārlis; Krog, Lasse S.; Mota-Santiago, Pablo; Terry, Ann; Kirby, Nigel; Whitten, Andrew E.; Boyd, Ben J.

The “gut” corona at the surface of nanoparticles is dependent on exposure to bile salts and phospholipids

Mark

Kihara, Shinji ; Aljabbari, Anas ; Bērziņš, Kārlis ; Krog, Lasse S. ; Mota-Santiago, Pablo ^LU ; Terry, Ann ^LU ; Kirby, Nigel ; Whitten, Andrew E. and Boyd, Ben J. (2025) In Journal of Colloid and Interface Science 680. p.797-807

Abstract: Hypothesis: The formation of a biomolecular corona on nanoparticle surfaces significantly influences their biological behaviour, particularly in drug delivery applications. Despite the prevalence of ingestion of particles (e.g, during oral drug delivery), our understanding of corona formation within the gastrointestinal (GI) tract remains limited, especially for non-protein components. The hypothesis of this work is that the exposure of nanoparticles to bile components will form a “corona” structure and protein corona will represent proteomes different from the original bile fluid. Two major aspects of biomolecular corona formed in GI fluid (hereby termed “gut corona), which ultimately dictate the fate of particle-based carriers,... (More); Hypothesis: The formation of a biomolecular corona on nanoparticle surfaces significantly influences their biological behaviour, particularly in drug delivery applications. Despite the prevalence of ingestion of particles (e.g, during oral drug delivery), our understanding of corona formation within the gastrointestinal (GI) tract remains limited, especially for non-protein components. The hypothesis of this work is that the exposure of nanoparticles to bile components will form a “corona” structure and protein corona will represent proteomes different from the original bile fluid. Two major aspects of biomolecular corona formed in GI fluid (hereby termed “gut corona), which ultimately dictate the fate of particle-based carriers, include the composition and the surface structure of nanoparticle-corona complex. Experiments: The structure and composition of the biomolecular corona formed on model SiO₂ nanoparticles within simulated and extracted bile fluids were determined using small-angle scattering, quantification assays, and liquid chromatography with tandem mass spectrometry (LC-MS/MS) techniques. Findings: The formation of raspberry-like structures was identified, with bile micelles adopting ellipsoidal shapes around the nanoparticles, as opposed to a surface covered with a uniform corona (i.e., core–shell structure). Assay quantification and proteomics experiments revealed a notable increase in the ratio of protein to bile salt within the corona compared to the original bile fluid. The composition of the proteome differed between the bovine bile and the protein corona with only 34 proteins associated with the nanoparticles from the top 100 identified in bovine bile. Despite the differences in protein types identified between bovine bile and gut corona, the proportions of protein between different functional classes, such as enzymes and structural proteins, show little variation. This work elucidates the intricate interactions between nanoparticles and gut molecules, offering insights crucial for designing nanoparticle formulations for optimized oral drug delivery and understanding nanoparticle behaviour within the GI tract.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/02caef2b-89e5-4876-80a8-7f00b970c142

author

Kihara, Shinji ; Aljabbari, Anas ; Bērziņš, Kārlis ; Krog, Lasse S. ; Mota-Santiago, Pablo ^LU ; Terry, Ann ^LU ; Kirby, Nigel ; Whitten, Andrew E. and Boyd, Ben J.

organization

publishing date

2025-02

type

Contribution to journal

publication status

published

subject

Physical Chemistry (including Surface- and Colloid Chemistry)

in

Journal of Colloid and Interface Science

volume

680

pages

11 pages

publisher

Academic Press

external identifiers

pmid:39591792
scopus:85209914031

ISSN

0021-9797

DOI

10.1016/j.jcis.2024.11.064

language

English

LU publication?

yes

id

02caef2b-89e5-4876-80a8-7f00b970c142

date added to LUP

2025-02-18 16:06:23

date last changed

2025-07-09 04:02:09

@article{02caef2b-89e5-4876-80a8-7f00b970c142,
  abstract     = {{<p>Hypothesis: The formation of a biomolecular corona on nanoparticle surfaces significantly influences their biological behaviour, particularly in drug delivery applications. Despite the prevalence of ingestion of particles (e.g, during oral drug delivery), our understanding of corona formation within the gastrointestinal (GI) tract remains limited, especially for non-protein components. The hypothesis of this work is that the exposure of nanoparticles to bile components will form a “corona” structure and protein corona will represent proteomes different from the original bile fluid. Two major aspects of biomolecular corona formed in GI fluid (hereby termed “gut corona), which ultimately dictate the fate of particle-based carriers, include the composition and the surface structure of nanoparticle-corona complex. Experiments: The structure and composition of the biomolecular corona formed on model SiO<sub>2</sub> nanoparticles within simulated and extracted bile fluids were determined using small-angle scattering, quantification assays, and liquid chromatography with tandem mass spectrometry (LC-MS/MS) techniques. Findings: The formation of raspberry-like structures was identified, with bile micelles adopting ellipsoidal shapes around the nanoparticles, as opposed to a surface covered with a uniform corona (i.e., core–shell structure). Assay quantification and proteomics experiments revealed a notable increase in the ratio of protein to bile salt within the corona compared to the original bile fluid. The composition of the proteome differed between the bovine bile and the protein corona with only 34 proteins associated with the nanoparticles from the top 100 identified in bovine bile. Despite the differences in protein types identified between bovine bile and gut corona, the proportions of protein between different functional classes, such as enzymes and structural proteins, show little variation. This work elucidates the intricate interactions between nanoparticles and gut molecules, offering insights crucial for designing nanoparticle formulations for optimized oral drug delivery and understanding nanoparticle behaviour within the GI tract.</p>}},
  author       = {{Kihara, Shinji and Aljabbari, Anas and Bērziņš, Kārlis and Krog, Lasse S. and Mota-Santiago, Pablo and Terry, Ann and Kirby, Nigel and Whitten, Andrew E. and Boyd, Ben J.}},
  issn         = {{0021-9797}},
  language     = {{eng}},
  pages        = {{797--807}},
  publisher    = {{Academic Press}},
  series       = {{Journal of Colloid and Interface Science}},
  title        = {{The “gut” corona at the surface of nanoparticles is dependent on exposure to bile salts and phospholipids}},
  url          = {{http://dx.doi.org/10.1016/j.jcis.2024.11.064}},
  doi          = {{10.1016/j.jcis.2024.11.064}},
  volume       = {{680}},
  year         = {{2025}},
}

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The “gut” corona at the surface of nanoparticles is dependent on exposure to bile salts and phospholipids