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具有敏感肿瘤微环境响应性的白蛋白稳定的锰基纳米复合材料及其在脑肿瘤中高效 siRNA 递送的应用。

Albumin-stabilized manganese-based nanocomposites with sensitive tumor microenvironment responsivity and their application for efficient SiRNA delivery in brain tumors.

机构信息

Department of Radiology, Daping Hospital, Army Medical University, Chongqing 400042, China.

出版信息

J Mater Chem B. 2020 Feb 21;8(7):1507-1515. doi: 10.1039/c9tb02341k. Epub 2020 Jan 31.

DOI:10.1039/c9tb02341k
PMID:32003397
Abstract

Mn(iv)-Based nanoparticles (NPs) are effective in improving tumor oxygenation (hypoxia) and reducing endogenous hydrogen peroxide and acidity in the tumor region. However, the optimized reduction conditions of conventional Mn(iv)-based NPs are generally reported at pH ≤ 6.5, while the usual pH range of the tumor microenvironment (TME) is 6.5-7.0. The dissatisfactory imaging performance in the weakly acidic environment may limit their further application in tumor diagnosis. In this study, Mn(iii) was introduced in a nanoplatform, because it is reduced into Mn(ii) in weakly acidic environments. Arg-Gly-Asp (RGD) peptide-decorated bovine serum albumin (BSA) was employed as the stabilizer and scaffold to fabricate Mn(iii)- and Mn(iv)-integrated nanocomposites (RGD-BMnNPs) with suitable size, good stability, and excellent biocompatibility. The as-prepared NPs showed clear contrast enhancement at pH 6.5-6.9 in vitro as well as sensitive and rapid T-weighted imaging performance within the tumor region in a glioblastoma (U87MG) orthotopic model, owing to the intrinsic disproportionation reaction of Mn(iii) in the weakly acidic environment. In addition, these NPs could be used for efficient siRNA delivery. They showed superior advantages in this process, including increased tumour uptake, improved tumor accumulation and enhanced therapeutic effects with the modulation of the TME. These novel albumin-stabilized manganese-based NPs combined with efficient drug delivery capacity hold great potential to serve as intelligent theranostic agents for further clinical translation.

摘要

基于锰(IV)的纳米颗粒(NPs)可有效改善肿瘤氧合作用(缺氧),减少肿瘤区域内的内源性过氧化氢和酸度。然而,传统的基于锰(IV)的 NPs 的最佳还原条件通常报道在 pH 值≤6.5,而肿瘤微环境(TME)的通常 pH 值范围为 6.5-7.0。在弱酸性环境中不理想的成像性能可能会限制它们在肿瘤诊断中的进一步应用。在这项研究中,在纳米平台中引入了锰(III),因为它在弱酸性环境中还原为锰(II)。精氨酸-甘氨酸-天冬氨酸(RGD)肽修饰的牛血清白蛋白(BSA)被用作稳定剂和支架,以制备具有合适尺寸、良好稳定性和优异生物相容性的锰(III)和锰(IV)整合的纳米复合材料(RGD-BMnNPs)。所制备的 NPs 在体外 pH 值为 6.5-6.9 时表现出明显的对比增强,并且在神经胶质瘤(U87MG)原位模型中的肿瘤区域内表现出灵敏和快速的 T 加权成像性能,这归因于弱酸性环境中锰(III)的固有歧化反应。此外,这些 NPs 可用于有效递送 siRNA。它们在这个过程中表现出优越的优势,包括增加肿瘤摄取、改善肿瘤积累和增强治疗效果,同时调节 TME。这些新型的白蛋白稳定的基于锰的 NPs 与高效的药物递送能力相结合,有望成为进一步临床转化的智能治疗药物。

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