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具有大表面孔的中空介孔硅胶囊的细胞内蛋白质传递。

Intracellular protein delivery by hollow mesoporous silica capsules with a large surface hole.

机构信息

Department of Chemistry and Protein Research Center for Bio-Industry, Hankuk University of Foreign Studies, Yongin, Korea.

出版信息

Nanotechnology. 2012 Mar 2;23(8):085101. doi: 10.1088/0957-4484/23/8/085101. Epub 2012 Feb 1.

DOI:10.1088/0957-4484/23/8/085101
PMID:22293239
Abstract

We prepared cell membrane-permeable hollow mesoporous silica capsules (HMSCs) by a simple new method. CTAB micellar assembly in cholesterol emulsion gave rise to a novel capsular morphology of the HMSC particles. The HMSCs consisted of mesostructured silica walls with a large surface hole (25-50 nm) and the average particle dimension was 100-300 nm. They exhibited high surface areas of up to 719.3 m(2) g(-1) and a mesoporous range of pores of 2.4-2.7 nm. The surface-functionalized HMSCs could also be prepared by a similar co-condensation method using tetraethoxysilane with various organoalkoxysilane precursors in the presence of cholesterol. These organically modified HMSCs could be further modified on demand. For example, a carboxy-functionalized HMSC could be surface-functionalized by a green fluorescent 5-aminofluorescein (AFL) through an amidation reaction to afford a fluorescent AFL-HMSC. The hollow capsular morphology of the HMSCs with a large surface hole enabled us to develop very efficient intracellular delivery systems for membrane-impermeable ions, molecules, and various functional proteins. Non-covalent sequestration and delivery of proteins as well as covalent linkage of fluorescent molecules on the silica surface are effective for this system. The highly negatively charged green fluorescent probe mag-fluo-4 could be intracellularly delivered into HeLa cells by HMSC without any difficulty. The HMSCs could also effectively transport large functional proteins such as antibodies into HeLa cells. The efficiency of protein delivery by HMSC seems to be 3-22-fold higher than that of mesoporous silica nanospheres (MSNs) based on confocal laser scanning microscopy (CLSM) analysis.

摘要

我们通过一种简单的新方法制备了细胞膜通透性的中空介孔硅胶囊(HMSCs)。CTAB 胶束在胆固醇乳液中的组装导致 HMSC 颗粒具有新颖的胶囊形态。HMSCs 由介孔结构的硅壁组成,具有大的表面孔(25-50nm),平均粒径为 100-300nm。它们具有高达 719.3m2g-1 的高比表面积和 2.4-2.7nm 的介孔范围的孔。通过使用四乙氧基硅烷和胆固醇存在下的各种有机烷氧基硅烷前体的类似共缩合方法,也可以制备表面功能化的 HMSCs。这些有机改性的 HMSCs 可以根据需要进一步修饰。例如,通过酰胺化反应,将羧基功能化的 HMSC 用绿色荧光 5-氨基荧光素(AFL)表面功能化,得到荧光 AFL-HMSC。HMSCs 的中空胶囊形态具有大的表面孔,使我们能够开发用于膜不可渗透的离子、分子和各种功能蛋白的非常有效的细胞内递药系统。非共价螯合和递药以及荧光分子在硅表面的共价键合对该系统有效。带负电荷的绿色荧光探针 mag-fluo-4 可以毫不费力地通过 HMSC 被递送到 HeLa 细胞内。HMSCs 还可以有效地将大的功能蛋白(如抗体)递送到 HeLa 细胞中。通过 HMSC 进行蛋白质递送的效率似乎比基于共焦激光扫描显微镜(CLSM)分析的介孔硅纳米球(MSNs)高 3-22 倍。

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