用于肿瘤靶向纳米粒子的 DNA 工程可降解隐形装置。

IF 14.4 1区 化学 Q1 CHEMISTRY, MULTIDISCIPLINARY Journal of the American Chemical Society Pub Date : 2024-09-11 Epub Date: 2024-08-28 DOI:10.1021/jacs.4c09479
Yan Zhao, Junjun Hou, Linjie Guo, Shitai Zhu, Xiaoling Hou, Shuting Cao, Mo Zhou, Jiye Shi, Jiang Li, Kai Liu, Hongjie Zhang, Lihua Wang, Chunhai Fan, Ying Zhu
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引用次数: 0

摘要

纳米粒子(NP)输送系统已被积极用于癌症治疗和疫苗开发。然而,靶向递送的主要障碍在于 NPs 在肝脏中的大量螯合作用。在这里,我们报告了一种 DNA 工程方法来规避肝脏的吞噬作用,从而增强体内纳米试剂的肿瘤靶向递送。我们发现,NP 上的单层 DNA 分子可以优先吸附血清中的痢疾蛋白,从而使肝脏在功能上隐形;而肿瘤特异性摄取则是由 DNA 外壳随后在体内的降解引发的。DNA 外壳的降解率可通过涂覆 DNA 分子的长度进行调节。这种 DNA 工程隐形(DEIC)具有潜在的通用性,在基于 Ag2S 量子点和纳米脂质体的小鼠肿瘤靶向递送中均有所体现。近红外-II成像显示,肿瘤与肝脏的比例高达∼5.1,比传统纳米材料高出约18倍。这种方法可为体内高效靶向递送治疗药物提供一种通用策略。
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DNA-Engineered Degradable Invisibility Cloaking for Tumor-Targeting Nanoparticles.

Nanoparticle (NP) delivery systems have been actively exploited for cancer therapy and vaccine development. Nevertheless, the major obstacle to targeted delivery lies in the substantial liver sequestration of NPs. Here we report a DNA-engineered approach to circumvent liver phagocytosis for enhanced tumor-targeted delivery of nanoagents in vivo. We find that a monolayer of DNA molecules on the NP can preferentially adsorb a dysopsonin protein in the serum to induce functionally invisibility to livers; whereas the tumor-specific uptake is triggered by the subsequent degradation of the DNA shell in vivo. The degradation rate of DNA shells is readily tunable by the length of coated DNA molecules. This DNA-engineered invisibility cloaking (DEIC) is potentially generic as manifested in both Ag2S quantum dot- and nanoliposome-based tumor-targeted delivery in mice. Near-infrared-II imaging reveals a high tumor-to-liver ratio of up to ∼5.1, approximately 18-fold higher than those with conventional nanomaterials. This approach may provide a universal strategy for high-efficiency targeted delivery of theranostic agents in vivo.

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来源期刊
CiteScore
24.40
自引率
6.00%
发文量
2398
审稿时长
1.6 months
期刊介绍: The flagship journal of the American Chemical Society, known as the Journal of the American Chemical Society (JACS), has been a prestigious publication since its establishment in 1879. It holds a preeminent position in the field of chemistry and related interdisciplinary sciences. JACS is committed to disseminating cutting-edge research papers, covering a wide range of topics, and encompasses approximately 19,000 pages of Articles, Communications, and Perspectives annually. With a weekly publication frequency, JACS plays a vital role in advancing the field of chemistry by providing essential research.
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