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细胞穿透肽连接的聚合物与不易透过细胞膜的分子物理混合在细胞膜上的性能。

Performance of cell-penetrating peptide-linked polymers physically mixed with poorly membrane-permeable molecules on cell membranes.

机构信息

Department of Pharmaceutics, Setsunan University, University, 45-1 Nagaotoge-cho, Hirakata, Osaka, Japan.

出版信息

Eur J Pharm Biopharm. 2012 May;81(1):64-73. doi: 10.1016/j.ejpb.2012.01.008. Epub 2012 Jan 28.

DOI:10.1016/j.ejpb.2012.01.008
PMID:22306700
Abstract

We are investigating a new class of penetration enhancers that enable poorly membrane-permeable molecules physically mixed with them to effectively penetrate cell membranes without their concomitant cellular uptake. Since we previously revealed that poly(N-vinylacetamide-co-acrylic acid) modified with d-octaarginine, which is a typical cell-penetrating peptide, significantly enhanced the nasal absorption of insulin, we examined the performance of the polymers on cell membranes. When Caco-2 cells were incubated with 5(6)-carboxyfluorescein (CF) for 30 min, approximately 0.1% of applied CF was internalized into the cells. This poor membrane permeability was dramatically enhanced by d-octaarginine-linked polymers; a 25-fold increase in the cellular uptake of CF was observed when the polymer concentration was adjusted to 0.2mg/mL. None of the individual components, for example, d-octaarginine, had any influence on CF uptake, demonstrating that only d-octaarginine anchored chemically to the polymeric platform enhanced the membrane permeation of CF. The polymer-induced CF uptake was consistently high even when the incubation time was extended to 120 min. Confocal laser scanning microphotographs of cells incubated with d-octaarginine-linked polymers bearing rhodamine red demonstrated that the cell outline was stained with red fluorescence. The polymer-induced CF uptake was significantly suppressed by 5-(N-ethyl-N-isopropyl)amiloride, which is an inhibitor of macropinocytosis. Results indicated that d-octaarginine-linked polymers remained on the cell membrane and poorly membrane-permeable CF was continuously internalized into cells mainly via macropinocytosis repeated for the individual peptidyl branches in the polymer backbone.

摘要

我们正在研究一类新的渗透增强剂,它们可以使与它们物理混合的通透性差的分子有效地穿透细胞膜,而不会伴随细胞摄取。由于我们之前发现,经 d-octaarginine 修饰的聚(N-乙烯基乙酰胺-co-丙烯酸)显著增强了胰岛素的鼻腔吸收,因此我们研究了这些聚合物对细胞膜的性能。当 Caco-2 细胞用 5(6)-羧基荧光素(CF)孵育 30 分钟时,约有 0.1%的 CF 被内化到细胞内。这种较差的膜通透性通过 d-octaarginine 连接的聚合物得到了显著增强;当聚合物浓度调整到 0.2mg/mL 时,CF 的细胞摄取增加了 25 倍。没有任何单个成分,例如 d-octaarginine,对 CF 的摄取有任何影响,这表明只有化学连接到聚合物平台上的 d-octaarginine 增强了 CF 的膜渗透。即使孵育时间延长至 120 分钟,聚合物诱导的 CF 摄取仍然很高。用带罗丹明红的 d-octaarginine 连接的聚合物孵育的细胞的共焦激光扫描显微镜照片表明,细胞膜被红色荧光染色。聚合物诱导的 CF 摄取被 5-(N-乙基-N-异丙基)amiloride 显著抑制,后者是巨胞饮作用的抑制剂。结果表明,d-octaarginine 连接的聚合物留在细胞膜上,通透性差的 CF 通过单个肽基支在聚合物主链上重复的巨胞饮作用不断被内化到细胞内。

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