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Targeted Reprogramming of Pathogenic Fibroblast Genes at the 3′-Untranslated Regions by DNA Nanorobots for Periodontitis

重编程 基因 生物 非翻译区 牙周炎 小RNA 遗传学 成纤维细胞 细胞生物学 信使核糖核酸 医学 细胞培养 内科学
作者
Jing Zhang,Yang Liu,Hao Zeng,Zifan Zhao,Yue Han,Yilong Zhao,Shuyuan Qu,Zijian Gong,Ziming Wang,Yi Bai,Qin Zhao
出处
期刊:ACS Nano [American Chemical Society]
卷期号:18 (33): 22139-22152
标识
DOI:10.1021/acsnano.4c05475
摘要

Periodontitis, with its persistent nature, causes significant distress for most sufferers. Current treatments, such as mechanical cleaning and surgery, often fail to fully address the underlying overactivation of fibroblasts that drives this degradation. Targeting the post-transcriptional regulation of fibroblasts, particularly at the 3′-untranslated regions (3′UTR) of pathogenic genes, offers a therapeutic strategy for periodontitis. Herein, we developed a DNA nanorobot for this purpose. This system uses a dynamic DNA nanoframework to incorporate therapeutic microRNAs through molecular recognition and covalent bonds, facilitated by DNA monomers modified with disulfide bonds. The assembled-DNA nanoframework is encapsulated in a cell membrane embedded with a fibroblast-targeting peptide. By analyzing the 3′UTR regions of pathogenic fibroblast genes FOSB and JUND, we identified the therapeutic microRNA as miR-1–3p and integrated it into this system. As expected, the DNA nanorobot delivered the internal components to fibroblasts by the targeting peptide and outer membrane that responsively releases miR-1–3p under intracellular glutathione. It resulted in a precise reduction of mRNA and suppression of protein function in pathogenic genes, effectively reprogramming fibroblast behavior. Our results confirm that this approach not only mitigates the inflammation but also promotes tissue regeneration in periodontal models, offering a promising therapeutic avenue for periodontitis.
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