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协同控制金属锁配体和金属螯合蛋白用于介孔硅纳米载体以提高递送效率。

Synergetic gating of metal-latching ligands and metal-chelating proteins for mesoporous silica nanovehicles to enhance delivery efficiency.

机构信息

Key Laboratory of Mesoscopic Chemistry (Ministry of Education), State Key Laboratory of Coordination Chemistry, School of Chemistry and Chemical Engineering, Nanjing University , Nanjing 210093, People's Republic of China.

出版信息

ACS Appl Mater Interfaces. 2014 Sep 10;6(17):15217-23. doi: 10.1021/am5035347. Epub 2014 Aug 19.

Abstract

Stimuli-responsive drug delivery systems are highly desirable for improved therapeutic efficacy and minimized adverse effects of drugs. Mesoporous silica nanoparticles (MSNs) functionalized with pentadentate ligands, N-(3-trimethoxysilylpropyl)ethylenediamine triacetate (TSP-DATA), in the presence of metal ions with and without myoglobin (Mb)-containing surface-accessible histidine residues, were constructed for pH-triggered controlled release. The DATA ligands immobilized on the MSN pore outlets could encapsulate cargo within the pores by metal latching across pore openings, and release efficiency increased with the increase of surface density of the DATA ligands. The release efficiencies for the metal-chelating protein nanogates, through multiple-site binding of Mb with the metal-chelating ligands, were higher than those for the metal-latching ligand nanogates but were almost independent of surface density of the ligands investigated. Both the metal-latching ligands and the metal-chelating proteins played a synergetic role in gating MSNs for high-loading drug delivery and stimuli-responsive controlled release. The constructed Mb-Cu(2+)-gated MSN delivery system has promising applications in targeted drug therapy of tumors.

摘要

具有五齿配体的介孔硅纳米粒子(MSNs)在金属离子存在和不存在含肌红蛋白(Mb)的表面可及组氨酸残基的条件下,用 N-(3-三甲氧基硅丙基)乙二胺三乙酸酯(TSP-DATA)功能化,构建了用于 pH 触发的控制释放的刺激响应药物输送系统。固定在 MSN 孔出口处的 DATA 配体可以通过金属横跨孔开口的闩锁将货物封装在孔内,并且释放效率随着 DATA 配体表面密度的增加而增加。通过 Mb 与金属螯合配体的多点结合,金属螯合蛋白纳米门的释放效率高于金属闩锁配体纳米门,但几乎与所研究的配体的表面密度无关。金属闩锁配体和金属螯合蛋白在用于高负载药物输送和刺激响应控制释放的 MSN 门控中发挥协同作用。构建的 Mb-Cu(2+)门控 MSN 递药系统在肿瘤的靶向药物治疗中有很好的应用前景。

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