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聚 N-异丙基丙烯酰胺和穿透肽固定化量子点的热触发细胞摄取。

Thermally triggered cellular uptake of quantum dots immobilized with poly(N-isopropylacrylamide) and cell penetrating peptide.

机构信息

Department of Biological Sciences and Graduate School of Nanoscience and Technology, Korea Advanced Institute of Science and Technology, Daejeon 305-701, South Korea.

出版信息

Langmuir. 2010 Sep 21;26(18):14965-9. doi: 10.1021/la102632m.

Abstract

Thermally sensitive quantum dots (TSQDs) that exhibit an "on-demand" cellular uptake behavior via temperature-induced "shielding/deshielding" of cell penetrating peptides (CPP) on the surface were fabricated. Poly(N-isopropylacrylamide) (PNIPAAm) (M(w) = 11.5K) and CPP were biotinylated at their terminal ends and co-immobilized on to the surface of streptavidin-coated quantum dots (QDs-Strep) through biotin-streptavidin interaction. The cellular contact of CPP was sterically hindered due to hydrated PNIPAAm chains below the lower critical solution temperature (LCST). In contrast, above the LCST, grafted PNIPAAm chains were collapsed to make CPP moieties resurfaced, leading to increased cellular uptake of QDs. The temperature-controlled "shielding/deshielding" of CPP was further applied for a thermally triggered siRNA delivery system, where biotinylated siRNA was additionally conjugated to the surface of TSQDs. The level of gene silencing was significantly enhanced by increasing temperature above the LCST due to the surface exposure of CPP.

摘要

通过表面上的细胞穿透肽 (CPP) 的温度诱导“屏蔽/去屏蔽”,制备了表现出“按需”细胞摄取行为的热敏量子点 (TSQDs)。聚 (N-异丙基丙烯酰胺) (PNIPAAm) (M(w) = 11.5K) 和 CPP 在其末端处被生物素化,并通过生物素-链霉亲和素相互作用共同固定在链霉亲和素涂覆的量子点 (QDs-Strep) 的表面上。由于低于低临界溶液温度 (LCST) 的水合 PNIPAAm 链,CPP 的细胞接触受到空间位阻。相比之下,在 LCST 以上,接枝的 PNIPAAm 链塌陷,使 CPP 部分重新出现,导致 QDs 的细胞摄取增加。CPP 的温度控制“屏蔽/去屏蔽”进一步应用于热触发 siRNA 递送系统,其中生物素化的 siRNA 被另外缀合到 TSQDs 的表面。由于 CPP 的表面暴露,将温度升高到 LCST 以上可显著增强基因沉默水平。

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