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用与 AGO2 缀合的纳米颗粒携带的自噬抑制 microRNAs 治疗乳腺癌。

Treatment of breast cancer with autophagy inhibitory microRNAs carried by AGO2-conjugated nanoparticles.

机构信息

Koc University, Graduate School of Material Science and Engineering, Rumelifeneri Yolu Sarıyer, 34450, Istanbul, Turkey.

Sabanci University Nanotechnology Research and Application Center (SUNUM), Department of Biotechnology, Tuzla, 34956, Istanbul, Turkey.

出版信息

J Nanobiotechnology. 2020 Apr 28;18(1):65. doi: 10.1186/s12951-020-00615-4.

Abstract

Nanoparticle based gene delivery systems holds great promise. Superparamagnetic iron oxide nanoparticles (SPIONs) are being heavily investigated due to good biocompatibility and added diagnostic potential, rendering such nanoparticles theranostic. Yet, commonly used cationic coatings for efficient delivery of such anionic cargos, results in significant toxicity limiting translation of the technology to the clinic. Here, we describe a highly biocompatible, small and non-cationic SPION-based theranostic nanoparticles as novel gene therapy agents. We propose for the first-time, the usage of the microRNA machinery RISC complex component Argonaute 2 (AGO2) protein as a microRNA stabilizing agent and a delivery vehicle. In this study, AGO2 protein-conjugated, anti-HER2 antibody-linked and fluorophore-tagged SPION nanoparticles were developed (SP-AH nanoparticles) and used as a carrier for an autophagy inhibitory microRNA, MIR376B. These functionalized nanoparticles selectively delivered an effective amount of the microRNA into HER2-positive breast cancer cell lines in vitro and in a xenograft nude mice model of breast cancer in vivo, and successfully blocked autophagy. Furthermore, combination of the chemotherapy agent cisplatin with MIR376B-loaded SP-AH nanoparticles increased the efficacy of the anti-cancer treatment both in vitro in cells and in vivo in the nude mice. Therefore, we propose that AGO2 protein conjugated SPIONs are a new class of theranostic nanoparticles and can be efficiently used as innovative, non-cationic, non-toxic gene therapy tools for targeted therapy of cancer.

摘要

基于纳米粒子的基因传递系统具有广阔的前景。超顺磁性氧化铁纳米粒子(SPIONs)由于良好的生物相容性和额外的诊断潜力而受到广泛研究,使这些纳米粒子具有治疗诊断双重功能。然而,通常用于有效传递这种阴离子载体的阳离子涂层会导致显著的毒性,限制了该技术向临床的转化。在这里,我们描述了一种高度生物相容的、小的、非阳离子的基于 SPION 的治疗诊断纳米粒子,作为新型基因治疗剂。我们首次提出将 microRNA 机器 RISC 复合物成分 Argonaute 2(AGO2)蛋白用作 microRNA 稳定剂和递送载体。在这项研究中,开发了 AGO2 蛋白缀合的、抗 HER2 抗体连接的和荧光标记的 SPION 纳米粒子(SP-AH 纳米粒子),并将其用作自噬抑制 microRNA,MIR376B 的载体。这些功能化纳米粒子在体外选择性地将有效量的 microRNA 递送至 HER2 阳性乳腺癌细胞系中,并在乳腺癌裸鼠异种移植模型中体内成功阻断自噬。此外,将化疗药物顺铂与负载 MIR376B 的 SP-AH 纳米粒子联合使用,提高了体外细胞和体内裸鼠中的抗癌治疗效果。因此,我们提出 AGO2 蛋白偶联的 SPION 是一类新型的治疗诊断纳米粒子,可有效地用作创新的、非阳离子的、无毒的基因治疗工具,用于癌症的靶向治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f93/7189576/154b58030c88/12951_2020_615_Fig1_HTML.jpg

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