Enhancing Retention and Permeation of Rapamycin for Osteoarthritis Therapy Using a Two-stage Drug Delivery System

Overview

Journal Mater Today Bio

Specialty Biomedical Engineering

Date 2024 Oct 15

PMID 39403313

Authors

Guangyong Lin

Huirong Huang

Meng Sun

Zhinan He

Shengjie Li

Xindan Liang

Yuqi Yan

Chenyu Qiu

Shize Li

Xinyu Zhao

Wanling Zhu

Longfa Kou

Ruijie Chen

Affiliations

Soon will be listed here.

Abstract

Osteoarthritis (OA) remains a challenging degenerative joint disease, largely associated with chondrocyte apoptosis during its development. Preserving chondrocytes stands as a promising strategy for OA treatment. Rapamycin (RP) exhibits chondrocyte protection by fostering autophagy. Nevertheless, the swift clearance of intra-articular injections and the dense cartilage extracellular matrix (ECM) hinder RP from effectively reaching chondrocytes. Herein, we developed a "two-stage" drug delivery system (RP@PEG-PA@P-Lipo). This system comprises primary nanoparticles (P-Lipo), liposomes modified with a collagen II targeting peptide (WYRGRLC), and secondary nanoparticles (RP@PEG-PA), PEG-modified PAMAM encapsulating rapamycin (RP). RP@PEG-PA@P-Lipo demonstrates adherence to the cartilage surface with WYRGRLC, substantially prolonging retention within the joint cavity. Subsequently, released RP@PEG-PA can effectively penetrate the cartilage and deliver RP to chondrocytes through small size and charge-driven forces. and experiments corroborate its notable therapeutic effects on OA. This study holds promise in offering a novel approach for clinical drug delivery and OA treatment.

Citing Articles

Inhibition of mTORC1 by rapamycin results in feedback activation of Akt and aggravates hallmarks of osteoarthritis in female mice and non-human primates.

Minton D, Ailiani A, Focht M, Kersh M, Lii A, Li A bioRxiv. 2024; .

PMID: 38798488 PMC: 11118493. DOI: 10.1101/2024.05.14.594256.

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