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P85,Optison 微泡与超声共同介导体内小鼠骨骼肌中质粒 DNA 的转染。

P85, Optison microbubbles and ultrasound cooperate in mediating plasmid DNA transfection in mouse skeletal muscles in vivo.

机构信息

Ultrasound Department, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.

出版信息

Ultrason Sonochem. 2011 Mar;18(2):513-9. doi: 10.1016/j.ultsonch.2010.08.013. Epub 2010 Sep 21.

Abstract

Pluronic block copolymers, a kind of non-ionic surfactant, also known as poloxamers, and ultrasound-targeted microbubble destruction have been respectively investigated as vectors for gene delivery in vitro and in vivo. However, they are limited for clinical application due to the relatively low transfer efficiency of each individual vector. In the present study, we explored if the combination of P85, a pluronic block copolymer, Optison, a microbubble contrast agent and ultrasound enhances the transfection of plasmid DNA in vivo using mouse skeletal muscle models. Plasmid encoding green fluorescent protein (GFP) was respectively conjugated with 0.05%P85, 10%Optison, or 0.05%P85 plus 10%Optison, and injected into mouse tibialis anterior (TA) muscles with or without ultrasound irradiation (1 MHz, 1 W/cm(2), 2 min and 20% duty cycle). Mice were sacrificed 1 week after injection. The TA muscles were collected and cryo-sectioned into a series of 7 μm slices. To assess the efficiency of plasmid DNA transfection, tissue sections were counterstained with DAPI and scored by counting the number of GFP-positive fibers. Meanwhile the area of damaged muscles was measured based on the tissues stained with hematoxylin and eosin. Both P85 and Optison significantly enhanced the delivery of plasmid DNA in mouse TA skeletal muscles (P<0.01 and P<0.05 respectively, compared to saline control). In combination with Ultrasound irradiation, P85 (P<0.01, compared to P85 alone) but not Optison (P>0.05, compared to Optison alone) exerted a more pronounced effect on the transfection efficiency. Furthermore P85-induced gene delivery was higher than that by Optison regardless of the presence of ultrasound (P<0.01). The highest transfection efficiency was observed when P85, Optison and ultrasound irradiation were administrated together (P<0.01, compared to any other treatment in this study). The area of damaged muscles was enlarged by ultrasound irradiation in the presence of Optison microbubbles (P<0.01, compared to those groups without ultrasound irradiation). These results suggest that P85, microbubbles and ultrasound irradiation synergistically enhance plasmid DNA delivery in mouse skeletal muscles in vivo.

摘要

Pluronic 嵌段共聚物,一种非离子表面活性剂,也被称为泊洛沙姆,以及超声靶向微泡破坏,已分别被研究作为体外和体内基因传递的载体。然而,由于每个载体的转染效率相对较低,它们在临床应用中受到限制。在本研究中,我们探讨了 P85(一种普朗尼克嵌段共聚物)、Optison(一种微泡造影剂)和超声的联合应用是否能增强体内质粒 DNA 的转染。分别将编码绿色荧光蛋白(GFP)的质粒与 0.05%P85、10%Optison 或 0.05%P85 加 10%Optison 缀合,并在有或没有超声照射(1 MHz,1 W/cm(2),2 分钟和 20%占空比)的情况下注入小鼠胫骨前肌(TA)。注射后 1 周处死小鼠。采集 TA 肌肉并冷冻切片成一系列 7μm 切片。为了评估质粒 DNA 转染的效率,用 DAPI 对组织切片进行复染,并通过计数 GFP 阳性纤维的数量进行评分。同时,根据苏木精和伊红染色的组织测量受损肌肉的面积。P85 和 Optison 均显著增强了质粒 DNA 在小鼠 TA 骨骼肌中的递送(分别与生理盐水对照组相比,P<0.01 和 P<0.05)。与超声照射联合使用时,P85(与单独使用 P85 相比,P<0.01)而不是 Optison(与单独使用 Optison 相比,P>0.05)对转染效率的影响更为显著。此外,无论是否存在超声,P85 诱导的基因传递都高于 Optison(P<0.01)。当 P85、Optison 和超声照射联合使用时,观察到最高的转染效率(与本研究中的任何其他治疗相比,P<0.01)。在 Optison 微泡存在的情况下,超声照射会扩大受损肌肉的面积(与没有超声照射的组相比,P<0.01)。这些结果表明,P85、微泡和超声照射协同增强了体内小鼠骨骼肌中的质粒 DNA 传递。

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