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Ligand-switchable nanoparticles resembling viral surface for sequential drug delivery and improved oral insulin therapy

Medicine and Health

Ligand-switchable nanoparticles resembling viral surface for sequential drug delivery and improved oral insulin therapy

T. Yang, A. Wang, et al.

Discover how innovative ligand-switchable nanoparticles can revolutionize drug delivery! This research by Tiantian Yang and colleagues reveals how pH-responsive nanoparticles effectively navigate the intestinal barrier and target the liver, significantly improving glucose control in diabetic rats.

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~3 min • Beginner • English
Abstract
Mutual interference between surface ligands on multifunctional nanoparticles remains a significant obstacle to achieving optimal drug-delivery efficacy. Here, we develop ligand-switchable nanoparticles which resemble viral unique surfaces, enabling them to fully display diverse functions. The nanoparticles are modified with a pH-responsive stretchable cell-penetrating peptide (Pep) and a liver-targeting moiety (Gal) (Pep/Gal-PNPs). Once orally administered, the acidic environments trigger the extension of Pep from surface in a virus-like manner, enabling Pep/Gal-PNPs to traverse intestinal barriers efficiently. Subsequently, Gal is exposed by Pep folding at physiological pH, thereby allowing the specific targeting of Pep/Gal-PNPs to the liver. As a proof-of-concept, insulin-loaded Pep/Gal-PNPs are fabricated which exhibit effective intestinal absorption and excellent hepatic deposition of insulin. Crucially, Pep/Gal-PNPs increase hepatic glycogen production by 7.2-fold, contributing to the maintenance of glucose homeostasis for effective diabetes management. Overall, this study provides a promising approach to achieving full potential of diverse ligands on multifunctional nanoparticles.
Publisher
Nature Communications
Published On
Nov 04, 2022
Authors
Tiantian Yang, Aohua Wang, Di Nie, Weiwei Fan, Xiaohe Jiang, Miaorong Yu, Shiyan Guo, Chunliu Zhu, Gang Wei, Yong Gan
Tags
nanoparticles
drug delivery
pH-responsive
intestinal absorption
liver targeting
glucose homeostasis
cell-penetrating peptide
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