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Mesenchymal Stem Cell-Mediated Deep Tumor Delivery of Gold Nanorod for Photothermal Therapyopen access

Authors
Yun, Wan SuShim, Man KyuLim, SeunghoSong, SukyungKim, JinseongYang, SuahHwang, Hee SookKim, Mi RaYoon, Hong YeolLim, Dong-KwonSun, In-CheolKim, Kwangmeyung
Issue Date
10월-2022
Publisher
MDPI
Keywords
mesenchymal stem cell; gold nanorod; drug delivery; deep tumor penetration; photothermal therapy
Citation
NANOMATERIALS, v.12, no.19
Indexed
SCIE
SCOPUS
Journal Title
NANOMATERIALS
Volume
12
Number
19
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/145526
DOI
10.3390/nano12193410
ISSN
2079-4991
Abstract
Gold nanoparticles (AuNPs) with various sizes and morphologies have been extensively investigated for effective photothermal therapy (PTT) against multiple cancer types. However, a highly dynamic and complex tumor microenvironment (TME) considerably reduces the efficacy of PTT by limiting deep tumor penetration of AuNPs. Herein, we propose a mesenchymal stem cell (MSC)-mediated deep tumor delivery of gold nanorod (AuNR) for a potent PTT. First, MSCs are treated with tetraacylated N-azidomannosamine (Ac(4)ManNAz) to introduce modifiable azide (N-3) groups on the cell surface via metabolic glycoengineering. Then, AuNRs modified with bio-orthogonal click molecules of bicyclo[6.1.0]nonyne (AuNR@BCN) are chemically conjugated to the N-3 groups on the MSC surface by copper-free click chemistry reaction, resulting in AuNR@MSCs. In cultured MSCs, the appropriate condition to incorporate the AuNR into the MSCs is optimized; in addition, the photothermal efficiency of AuNR-MSCs under light irradiation are assessed, showing efficient heat generation in vitro. In colon tumor-bearing mice, intravenously injected AuNR@MSCs efficiently accumulate within the tumor tissues by allowing deep tissue penetration owing to the tumor homing effect by natural tumor tropism of AuNR@MSCs. Upon localized light irradiation, the AuNR@MSCs significantly inhibit colon tumor growth by the enhanced photothermal effect compared to conventional AuNRs. Collectively, this study shows a promising approach of MSCs-mediated deep tumor delivery of AuNR for effective PTT.
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