Hollow-core polydopamine nanocarriers for ultrasound-enhanced drug delivery

Abstract

On-demand drug release is one of the main challenges in nanocarrier design and a key step toward enhancing the efficacy of novel therapeutic formulations. Compared to conventional methods such as pH- or light-driven release, ultrasound-guided drug release offers a cost-effective strategy with improved tissue penetration making it particularly suitable for applications in hard-to-access tissues such as the pancreas. In this study, hollow nanoparticles (hPDA) were developed and evaluated for ultrasound-enhanced drug delivery, focusing on pancreatic ductal adenocarcinoma (PDAC). The hPDA nanoparticles, prepared employing non-toxic reagents, measured approximately 120 nm and were successfully loaded with SN-38, a potent yet challenging-to-formulate chemotherapeutic agent. Ultrasound-triggered drug release experiments at 60 kHz and 1.1 MHz demonstrated significant enhancements in drug release, with an increase of 54% and 19% respectively, compared to controls. Cytotoxicity studies under ultrasound exposure revealed a 20% reduction in cell viability, underscoring the synergistic potential of hPDA and ultrasound technology. These findings establish hPDA nanocarriers as a promising platform for ultrasound-responsive, targeted drug delivery in cancer therapy, with high potential for improved spatiotemporal control and reduced systemic toxicity.

Graphical abstract: Hollow-core polydopamine nanocarriers for ultrasound-enhanced drug delivery

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Article information

Article type
Communication
Submitted
30 Apr 2025
Accepted
29 Oct 2025
First published
06 Nov 2025
This article is Open Access
Creative Commons BY license

Nanoscale Horiz., 2025, Advance Article

Hollow-core polydopamine nanocarriers for ultrasound-enhanced drug delivery

S. Lingamgunta, C. Yadav, A. Orthodoxou, L. Gilmour, M. Ellis, H. Metzger, A. B. Popov, H. Mulvana and L. Fruk, Nanoscale Horiz., 2025, Advance Article , DOI: 10.1039/D5NH00297D

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