一种用于肿瘤靶向和双模态成像引导的光动力治疗的防漏Theranotic纳米平台。

IF 5 Q1 ENGINEERING, BIOMEDICAL
BME frontiers Pub Date : 2023-03-30 eCollection Date: 2023-01-01 DOI:10.34133/bmef.0015
Duo Jin, Yang Zhu, Manman Liu, Wenxin Yu, Jiaji Yu, Xinwei Zheng, Lulu Wang, Yun Wu, Kaiju Wei, Junjie Cheng, Yangzhong Liu
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引用次数: 2

摘要

目的:设计了一种基于蛋白质的防漏治疗纳米平台,用于双模态成像引导的肿瘤光动力治疗(PDT)。影响声明:氯蛋白e6(Ce6)与铁磁性铁蛋白(MFtn-Ce6)的位点特异性结合已被构建,以应对小分子药物递送过程中经常发生的意外泄漏的挑战。引言:PDT是最有前途的肿瘤治疗方法之一,而疏水性光敏剂通常需要递送系统。然而,光敏剂的非特异性分布和渗漏可能导致药物在肿瘤部位积聚不足。方法:制备用于Ce6位点特异性缀合的工程铁蛋白,以获得防漏递送系统,并在铁蛋白的空腔中生物矿化铁磁芯,形成荧光铁磁性铁蛋白纳米平台(MFtn-Ce6)。MFtn-Ce6的分布和肿瘤靶向可以通过磁共振成像(MRI)和荧光成像(FLI)来检测。结果:MFtn-Ce6显示有效的双模态MRI和FLI。观察到体内循环延长,肿瘤积聚和光敏剂滞留增加。可以实时精确跟踪MFtn-Ce6的时间依赖性分布,以找到PDT治疗的最佳时间窗口。铁蛋白和氧化铁核心的共定位证实了纳米平台在体内的高稳定性。结果表明,用MFtn-Ce6处理的小鼠在激光照射后表现出显著的肿瘤抑制活性。结论:基于铁蛋白的防漏纳米平台可用于光敏剂的有效递送,以提高治疗效果。该方法为PDT药物的双模态成像引导肿瘤递送建立了一种通用方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Leaking-Proof Theranostic Nanoplatform for Tumor-Targeted and Dual-Modality Imaging-Guided Photodynamic Therapy.

A Leaking-Proof Theranostic Nanoplatform for Tumor-Targeted and Dual-Modality Imaging-Guided Photodynamic Therapy.

A Leaking-Proof Theranostic Nanoplatform for Tumor-Targeted and Dual-Modality Imaging-Guided Photodynamic Therapy.

A Leaking-Proof Theranostic Nanoplatform for Tumor-Targeted and Dual-Modality Imaging-Guided Photodynamic Therapy.

Objective: A protein-based leaking-proof theranostic nanoplatform for dual-modality imaging-guided tumor photodynamic therapy (PDT) has been designed. Impact Statement: A site-specific conjugation of chlorin e6 (Ce6) to ferrimagnetic ferritin (MFtn-Ce6) has been constructed to address the challenge of unexpected leakage that often occurs during small-molecule drug delivery. Introduction: PDT is one of the most promising approaches for tumor treatment, while a delivery system is typically required for hydrophobic photosensitizers. However, the nonspecific distribution and leakage of photosensitizers could lead to insufficient drug accumulation in tumor sites. Methods: An engineered ferritin was generated for site-specific conjugation of Ce6 to obtain a leaking-proof delivery system, and a ferrimagnetic core was biomineralized in the cavity of ferritin, resulting in a fluorescent ferrimagnetic ferritin nanoplatform (MFtn-Ce6). The distribution and tumor targeting of MFtn-Ce6 can be detected by magnetic resonance imaging (MRI) and fluorescence imaging (FLI). Results: MFtn-Ce6 showed effective dual-modality MRI and FLI. A prolonged in vivo circulation and increased tumor accumulation and retention of photosensitizer was observed. The time-dependent distribution of MFtn-Ce6 can be precisely tracked in real time to find the optimal time window for PDT treatment. The colocalization of ferritin and the iron oxide core confirms the high stability of the nanoplatform in vivo. The results showed that mice treated with MFtn-Ce6 exhibited marked tumor-suppressive activity after laser irradiation. Conclusion: The ferritin-based leaking-proof nanoplatform can be used for the efficient delivery of the photosensitizer to achieve an enhanced therapeutic effect. This method established a general approach for the dual-modality imaging-guided tumor delivery of PDT agents.

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