Harnessing liposomal nanocellulose hydrogel for NIR-light driven on-demand drug delivery

Puja Gangurde*, Zahra Gounani*, Jacopo Zini, Roberta Teixeira Polez, Monika Österberg, Patrick Lauren, Tatu Lajunen, Timo Laaksonen*

*Corresponding author for this work

Research output: Contribution to journalArticleScientificpeer-review

4 Citations (Scopus)
39 Downloads (Pure)

Abstract

Stimuli-responsive nanoparticles have gained attention for their ability to control drug release via external signals. However, challenges like biodegradation and toxicity hinder their applications. This study introduces a system by integrating light-activated liposomes with cellulose nanofiber (CNF) hydrogel, creating a controlled release system where liposomes act as drug reservoirs, protecting drug molecules and preventing unwanted cargo leakage for on-demand localized drug delivery. Our surface interaction study between cationic liposomes and nanocellulose shows that the liposomes, while not uniformly distributed, are bound to the nanocellulose hydrogel due to strong electrostatic interactions and fiber networks, thus forming a depot-like drug reservoir system.
We evaluated hydrogel thickness and light dose to optimize the cargo release. Upon activation with near-infrared light (808 nm, 1 W/cm2), the photosensitizer inside the bilayer of thermosensitive liposome generates heat, which makes liposome leaky, resulting in on-demand cargo release. We observed up to 50 % release at low dose (20 J/cm2) of light, which increased to 80 % after exposure to higher dose of light (80 J/cm2), highlighting the sensitivity of the system. This dual-platform combines the biocompatibility of nanocellulose with tunability of light-activated liposomes, presenting promising approach for on-demand drug delivery with significant potential for personalized medicine.
Original languageEnglish
Article number100787
Number of pages10
JournalCarbohydrate Polymer Technologies and Applications
Volume10
Early online date10 Apr 2025
DOIs
Publication statusPublished - Jun 2025
MoE publication typeA1 Journal article-refereed

Funding

The authors acknowledge Heikki Raikkonen for his assistance in X-ray diffraction analysis. We acknowledge using the SPR instrument in Tapani Viitala's lab to optimize SPR measurements. P.G., Z.G., and Ti.L. acknowledge funding from the European Research Council (ERC) under the European Union's Horizon 2020 research and innovation program (ERC CoG, grant agreement No 101001016). Ta.L. and Ti.L acknowledge funding from the Phospholipid Research Center (TLA-2019-068/1-1) and Academy of Finland flagship GeneCellNano (project no 323669).

Keywords

  • cellulose nanofibers
  • light-activated liposomes
  • localized drug delivery
  • on-demand
  • tunable
  • On-demand
  • Tunable
  • Light-activated liposomes
  • Localized drug delivery
  • Cellulose nanofibers

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