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Ultrasound-responsive liposomes: A mechanistic framework to decode the effects of acoustic parameters

Journal Article (2026)
Author(s)

I. Simón Grau (TU Delft - ChemE/Product and Process Engineering)

R.F.A. van den Elshout (Student TU Delft)

G.K. Wardhana (TU Delft - Bio-Electronics)

M. Aqamolaei (TU Delft - Bio-Electronics)

Isabella S.T. de Jonge (Student TU Delft)

Remco Hartkamp (TU Delft - Complex Fluid Processing)

R. Alessandri (Katholieke Universiteit Leuven)

Tiago L. Costa (TU Delft - Bio-Electronics)

A.Y. Rwei (TU Delft - ChemE/Product and Process Engineering)

DOI related publication
https://doi.org/10.1073/pnas.2535429123 Final published version
More Info
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Publication Year
2026
Language
English
Journal title
Proceedings of the National Academy of Sciences of the United States of America
Issue number
13
Volume number
123
Article number
e2535429123
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Abstract

Ultrasound offers a noninvasive, clinically relevant means to achieve precise spatiotemporal control of cargo release from ultrasound-responsive drug delivery systems within deep tissues. This approach enables targeted delivery of therapeutic agents, enhancing efficacy while minimizing systemic toxicity. While previous studies show that release from ultrasound-responsive liposomes depends on acoustic parameters, the underlying mechanisms remain unclear. A deeper mechanistic understanding is essential to achieve precision over release and maximize therapeutic outcomes. To address this, we propose a sonoporation-based framework to describe release dynamics across varying frequencies, pressures, duty cycles, and pulse repetition frequencies for ultrasound-responsive poly(ethylene glycol)-functionalized liposomes. Using computational simulations validated by empirical results, our framework identifies a critical pressure threshold for release onset and demonstrates how the time spent above this threshold, modulated by acoustic parameters, governs release efficiency. To elucidate these effects, custom-built ultrasound transducers with different resonance frequencies were fabricated and characterized to ensure precise sample alignment, minimize acoustic distortion, and maintain a controlled focal-volume-to-sample-volume ratio across different frequencies. COMSOL simulations indicated that oscillatory acoustic pressure plays a more dominant role than acoustic radiation force, while coarse-grained molecular dynamics simulations captured pressure-dependent pore formation dynamics within the lipid bilayer. Together, our experiments and simulations highlight mechanical effects—particularly oscillatory acoustic pressure—as the primary driver of sonoporation-facilitated release. Finally, we discuss how optimizing acoustic parameters through this mechanistic framework could facilitate safe and effective clinical translation by considering tissue safety and ultrasound transducer design.