The Impact of Polyethylene Glycol Lipid Anchors on the Physicochemical Properties, Protein Corona, Function, and Biodistribution of Lipid Nanoparticles
Journal article, 2026

When introduced into biological systems, the function and biodistribution of lipid nanoparticles (LNPs) are affected by the biomolecular coronas they acquire. Corona composition is determined by the biophysical and chemical properties of the particles and the contents of the biofluids. Polyethylene glycol (PEG) polymers, anchored using lipids that partition into LNPs during formulation, are key to LNP stability in circulation. It is, however, not well-studied how different PEG-lipid anchors, with different acyl chain lengths, headgroup/linker chemistries, and desorption rates (PEG "shedding" from nanoparticles) can affect corona composition and LNP function. Here, we examined how common PEG-lipid anchors affect (1) in vivo biodistribution in C57BL/6 mice, (2) corona content (using mass spectrometry-based proteomics), (3) LNP biophysical characteristics (using single-particle automated Raman trapping analysis (SPARTA (R))), and (4) in vitro particle function (using cellular uptake and cargo delivery assays). Following nanoparticle formulation with clinically approved, commonly used PEG anchors, we found that the LNP biodistribution is strongly impacted, particularly in the liver, spleen, bone marrow, and lung. We then tested a wide range of lipid ratio combinations using high-throughput evaluation in vitro. Despite being minor LNP components (by molar ratio), the PEG-lipid anchors strongly impact the chemical characteristics, corona content, and particle function. These findings reveal structure-activity relationships between PEG-lipid anchor chemistry and functional LNP biodistribution, with implications for rational LNP design.

Raman spectroscopy

lipidchemistry

polyethylene glycol

lipid nanoparticle

mass spectroscopy

protein corona

Author

Chuan-En Lu

AstraZeneca AB

Kai Liu

AstraZeneca AB

Audrey Gallud

AstraZeneca AB

Viktoriia Meklesh

AstraZeneca AB

Lisbeth Thorup Ravnkilde

AstraZeneca AB

Juna Santos

AstraZeneca AB

Filipa Dias Louro

AstraZeneca AB

Tasso Miliotis

AstraZeneca AB

Marco A. Alfonzo-Mendez

AstraZeneca AB

Joanna Rejman

AstraZeneca AB

Luca Panariello

Karolinska Institutet

Hanna M. G. Barriga

Royal Institute of Technology (KTH)

Karolinska Institutet

Molly M. Stevens

University of Oxford

Karolinska Institutet

Fredrik Höök

Chalmers, Physics

Other publications Research

Marianna Yanez Arteta

AstraZeneca AB

Johan Ulander

AstraZeneca AB

Suzy Jones

AstraZeneca AB

Alan Sabirsh

AstraZeneca AB

ACS Nano

1936-0851 (ISSN) 1936-086X (eISSN)

Vol. In Press

Subject Categories (SSIF 2025)

Medical Biotechnology

Pharmaceutical Sciences

Physical Chemistry

DOI

10.1021/acsnano.5c19757

Publication data connected to DOI

PubMed

41845897

More information

Latest update

4/13/2026

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