An All‐in‐One DNA Nanodevice as a Programmed Theranostic Platform for Intelligent Cancer Cell Identification and On‐Site Drug Release

纳米器件 药物输送 纳米技术 癌细胞 药品 有效载荷(计算) 模块化设计 适体 计算机科学 计算生物学 癌症研究 材料科学 DNA损伤 体内 靶向给药 药物发现 鉴定(生物学) 癌症 癌症治疗 抗癌药物 全身给药 化学 前药 DNA 癌症免疫疗法 抗癌药 生物信息学
作者
Yi Yuan,Qiufeng Song,Linwen Lan,Xuefen Chen,Jiangchuan Du,Lei Zhang,Nan Chen,Zhifa Shen,Chang Xue
出处
期刊:Advanced Functional Materials [Wiley]
标识
DOI:10.1002/adfm.202531762
摘要

ABSTRACT Chemotherapy remains the cornerstone of malignant tumor treatment; however, off‐target effects and severe systemic toxicity limit its efficacy. Here, we developed a programmable theranostic platform based on an all‐in‐one smart DNA nanodevice (SND) that integrates a programmable cancer‐cell classifier (PCC) with a responsive delivery system (RDS). By employing a modular design that permits the customization of aptamer combinations for specific cancer cell types, the platform achieves accurate tumor recognition and spatially controlled drug release. Functioning as a dual‐aptamer molecular guide, the PCC utilizes an interlocked configuration to identify cell‐surface biomarkers in a stepwise manner, thereby ensuring highly specific target cell recognition. The RDS is constructed from a 1D central trunk flanked by double‐stranded drug‐loading units, a structure that confers high payload capacity and nuclease‐enhanced resistance. These peripheral units also function as recognition elements for endogenous stimuli; upon activation, they trigger conformational changes that facilitate efficient intracellular drug release. In vivo studies in tumor‐bearing mice demonstrate that this programmable theranostic platform selectively accumulates in tumor tissues, leading to marked inhibition of tumor growth and a substantial reduction in systemic toxicity. By integrating programmable molecular recognition with stimulus‐responsive drug delivery, our theranostic platform offers a promising strategy for advancing targeted cancer therapy.
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