线性聚乙烯亚胺包覆 Ag2S 近红外量子点的光学成像和基因转染潜力。

Turkish journal of biology = Turk biyoloji dergisi Pub Date : 2024-08-21 eCollection Date: 2024-01-01 DOI:10.55730/1300-0152.2709
Altay Savalan
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引用次数: 0

摘要

背景/目的:不含重金属的阳离子Ag2S近红外量子点(QDs)在700-900 nm的医学范围内具有高亮度,其生物相容性好,可作为非病毒基因递送系统,为克服自发荧光和轻松实时追踪基因递送铺平了道路:研究人员首次将新开发的小型且胶体稳定的2-巯基丙酸(MPA)封端Ag2S水溶液量子点与线性聚乙烯亚胺(Ag2S@2MPA/LPEI)进行了静电络合,将其作为强荧光探针和非病毒基因递送载体进行了研究,以实现对该系统的高度跟踪,并将基因递送到不同癌细胞的细胞核中。合成的Ag2S@2MPA/LPEI量子点具有很强的光学成像特性,并被用于递送绿色荧光蛋白(GFP)质粒作为标准基因:Ag2S@2MPA/LPEI-pDNA纳米粒子的理想转染效率为N/P比20。与游离的 25 kDa 线性聚乙烯亚胺(LPEI)相比,Ag2S@2MPA/LPEI 与 HEK 293T 细胞的相容性更好。接下来,用合成的 Ag2S@2MPA/LPEI 和 LPEI 对 pGFP 基因在不同癌细胞中的转染效率进行了评估,结果表明它们极有可能成为一种治疗癌症的基因递送系统:这是首次使用 Ag2S@2MPA/LPEI QDs 在体外进行基因转染和光学成像。总之,新合成的具有高度生物相容性和可追踪性的 Ag2S@2MPA/LPEI QDs 可以成为一种有效的、生物相容性好的癌症基因治疗系统。
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Optical imaging and gene transfection potential of linear polyethylenimine-coated Ag2S near-infrared quantum dots.

Background/aim: The application of biocompatible heavy metal-free and cationic Ag2S NIR quantum dots (QDs), which have intense luminosity in the 700-900 nm medical range, as a nonviral gene delivery system paves the way to overcome autofluorescence and easily track the delivery of genes in real time.

Materials and methods: The newly developed small and colloidally stable 2-mercaptopropionic acid (MPA)-capped Ag2S aqueous quantum dots electrostatically complexed with linear polyethyleneimine (Ag2S@2MPA/LPEI) were investigated for the first time both as a strong fluorescent probe and as a vector for nonviral gene delivery for the highest tracking of the system and delivery of genes into the nuclei of different cancer cells. The synthesized Ag2S@2MPA/LPEI quantum dots demonstrated strong optical imaging properties and were used to deliver a green fluorescent protein (GFP) plasmid as a standard gene.

Results: For Ag2S@2MPA/LPEI-pDNA nanoparticles, an N/P ratio of 20 was the ideal transfection efficiency. Ag2S@2MPA/LPEI was substantially more compatible with HEK 293T cells than the free 25-kDa linear polyethylenimine (LPEI). Next, the transfection efficiency evaluation of pGFP genes with synthesized Ag2S@2MPA/LPEI and LPEI in different cancer cells demonstrated their high potential as a theranostic cancer gene delivery system.

Conclusion: This is the first instance of gene transfection and optical imaging carried out in vitro using Ag2S@2MPA/LPEI QDs. Overall, the newly synthesized highly biocompatible and trackable Ag2S@2MPA/LPEI QDs can be an effective and biocompatible theranostic system for cancer gene therapy.

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