Opsonized nanoparticles target and regulate macrophage polarization for osteoarthritis therapy: A trapping strategy
Longfa Kou
1, 2
,
Huirong Huang
1, 3
,
Yingying Tang
1
,
Meng Sun
1
,
Yingtao Li
1
,
Jianing Wu
1
,
Shimin Zheng
1
,
Xinyu Zhao
1
,
Daosen Chen
4
,
Zucheng Luo
4
,
Xiaolei Zhang
4
,
Yao Qin
1, 3
,
Ruijie Chen
1
2
Wenzhou key Laboratory of basic science and translational research of radiation oncology, Zhejiang 325027, China
|
Publication type: Journal Article
Publication date: 2022-07-01
scimago Q1
wos Q1
SJR: 2.470
CiteScore: 19.4
Impact factor: 11.5
ISSN: 01683659, 18734995
PubMed ID:
35489544
Pharmaceutical Science
Abstract
Osteoarthritis (OA) is a chronic disease caused by joint inflammation. Its occurrence and development depend on a continuous inflammation environment. The activated M1 macrophages play a critical role in the inflammatory response of OA. Regulating the pro-inflammatory M1 to anti-inflammatory M2 macrophages in the OA articular cavity could be a rational strategy for OA treatment. It has been acknowledged that activated macrophages could proactively capture opsonized nanoparticles in the bloodstream and then accumulate into the reticuloendothelial system (RES) organs. Based on this fact, a trapping strategy is proposed, which transforms a normal nanoparticle into an opsonized attractant to target and regulate macrophage polarization. In this study, the opsonized nanoparticle (IgG/[email protected]) had several key features, including an immunoglobulin IgG (the opsonized layer), an anti-inflammatory agent berberine (Bb), and an oxidative stress-responsive bilirubin grafted polylysine biomaterial (BR-PLL) for drug loading (the inner nanocore). In vitro studies confirmed that IgG/[email protected] prefer to be phagocytosed by M1 macrophage, not M0. And the internalized IgG/[email protected] effectively promoted macrophage polarization toward the M2 phenotype and protected nearby chondrocytes. In vivo studies suggested that IgG/[email protected] significantly enhanced therapeutic outcomes by suppressing inflammation and promoting cartilage repair while not prolonging the retention period compared to non-opsonized counterparts. This proof-of-concept study provided a novel opsonization trapping strategy for OA drug delivery and treatment.
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GOST
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Kou L. et al. Opsonized nanoparticles target and regulate macrophage polarization for osteoarthritis therapy: A trapping strategy // Journal of Controlled Release. 2022. Vol. 347. pp. 237-255.
GOST all authors (up to 50)
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Kou L., Huang H., Tang Y., Sun M., Li Y., Wu J., Zheng S., Zhao X., Chen D., Luo Z., Zhang X., Qin Y., Chen R. Opsonized nanoparticles target and regulate macrophage polarization for osteoarthritis therapy: A trapping strategy // Journal of Controlled Release. 2022. Vol. 347. pp. 237-255.
Cite this
RIS
Copy
TY - JOUR
DO - 10.1016/j.jconrel.2022.04.037
UR - https://doi.org/10.1016/j.jconrel.2022.04.037
TI - Opsonized nanoparticles target and regulate macrophage polarization for osteoarthritis therapy: A trapping strategy
T2 - Journal of Controlled Release
AU - Kou, Longfa
AU - Huang, Huirong
AU - Tang, Yingying
AU - Sun, Meng
AU - Li, Yingtao
AU - Wu, Jianing
AU - Zheng, Shimin
AU - Zhao, Xinyu
AU - Chen, Daosen
AU - Luo, Zucheng
AU - Zhang, Xiaolei
AU - Qin, Yao
AU - Chen, Ruijie
PY - 2022
DA - 2022/07/01
PB - Elsevier
SP - 237-255
VL - 347
PMID - 35489544
SN - 0168-3659
SN - 1873-4995
ER -
Cite this
BibTex (up to 50 authors)
Copy
@article{2022_Kou,
author = {Longfa Kou and Huirong Huang and Yingying Tang and Meng Sun and Yingtao Li and Jianing Wu and Shimin Zheng and Xinyu Zhao and Daosen Chen and Zucheng Luo and Xiaolei Zhang and Yao Qin and Ruijie Chen},
title = {Opsonized nanoparticles target and regulate macrophage polarization for osteoarthritis therapy: A trapping strategy},
journal = {Journal of Controlled Release},
year = {2022},
volume = {347},
publisher = {Elsevier},
month = {jul},
url = {https://doi.org/10.1016/j.jconrel.2022.04.037},
pages = {237--255},
doi = {10.1016/j.jconrel.2022.04.037}
}
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