Genetically Engineered Biomimetic Nanoparticles for Targeted Delivery of mRNA to Treat Rheumatoid Arthritis

被引:11
|
作者
Chen, Jianhai [1 ,2 ,3 ]
Tan, Jianwei [2 ]
Li, Jian [1 ]
Cheng, Wenxiang [1 ]
Ke, Liqing [1 ]
Wang, Anqiao [3 ]
Wang, Qiqing [3 ]
Lin, Sien [4 ]
Li, Gang [4 ]
Wang, Benguo [3 ]
Chen, Jingqin [2 ]
Zhang, Peng [1 ]
机构
[1] Chinese Acad Sci, Shenzhen Inst Adv Technol, Ctr Translat Med Res & Dev, Shenzhen 518055, Peoples R China
[2] Chinese Acad Sci, Shenzhen Inst Adv Technol, Res Ctr Biomed Opt & Mol Imaging, CAS Key Lab Hlth Informat, Shenzhen 518055, Peoples R China
[3] Chinese Univ Hong Kong, Affiliated Hosp 2, Shenzhen & Longgang Dist Peoples Hosp Shenzhen, Sch Med,Rehabil Dept, Shenzhen 518172, Peoples R China
[4] Chinese Univ Hong Kong, Prince Wales Hosp, Li Ka Shing Inst Hlth Sci, Dept Orthopaed & Traumatol,Stem Cells & Regenerat, Shatin 999077, Peoples R China
来源
SMALL METHODS | 2023年 / 7卷 / 11期
基金
中国国家自然科学基金;
关键词
biomimetic membranes; mRNA; PTEN; rheumatoid arthritis; COLLAGEN-INDUCED ARTHRITIS; SYNOVIAL FIBROBLASTS; IN-VIVO; PTEN; AMELIORATION; SUPPRESSION; AUTOPHAGY; VACCINES; GROWTH; CELLS;
D O I
10.1002/smtd.202300678
中图分类号
O64 [物理化学(理论化学)、化学物理学];
学科分类号
070304 ; 081704 ;
摘要
In addition to inhibiting persistent inflammation, phosphatase and tensin homolog deleted from chromosome 10 (PTEN) is known as an important therapeutic target for alleviating rheumatoid arthritis (RA) symptoms. Modulation of PTEN gene expression in synovial tissue using messenger RNA (mRNA) is a promising approach to combat RA. However, mRNA therapeutics are often hampered by unsatisfactory stability and inefficient localization in synovial tissue. In this study, a genetically engineered biomimetic membrane-coated mRNA (MR@P-mPTEN) carrier that effectively delivers mRNA-PTEN (mPTEN) directly to the RA joint is presented. By overexpressing tumor necrosis factor (TNF-& alpha;) receptors on macrophage biomimetic membranes via plasmid transfection, decoys that reduce inflammatory pathway activation are prepared for TNF-& alpha;. The resulting construct, MR@P-mPTEN, shows good stability and RA targeting based on in vivo fluorescence imaging. It is also found that MR@P-mPTEN competitively binds TNF-& alpha; and activates the PTEN pathway in vitro and in vivo, thereby inhibiting synovitis and joint damage. Clinical micro-computed tomography and histological analyses confirm the treatment effects. These results suggest that the genetically engineered biomimetic therapeutic platform MR@P-mPTEN both inhibits pro-inflammatory cytokines and upregulates PTEN protein expression to alleviate RA damage, providing a new a new combination strategy for RA treatment.
引用
收藏
页数:14
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