高分子摄取烷基链修饰的胍基糖苷分子转运体。
Macromolecular uptake of alkyl-chain-modified guanidinoglycoside molecular transporters.
出版信息
Chembiochem. 2014 Mar 21;15(5):676-80. doi: 10.1002/cbic.201300606.
Abstract
Guanidinoglycosides, a family of cellular transporters capable of delivering high Mw biopolymers, have previously been shown to display high selectivity for cell-surface heparan sulfate proteoglycans and promote their clustering. Herein, the internalization mechanism of amphiphilic guanidinoglycoside derivatives was investigated by cell-surface FRET analysis. Unexpectedly, although the heparan sulfate selectivity is maintained, the cellular uptake of these derivatives does not appear to involve clustering of the proteoglycans on the cell surface. This suggests a distinct uptake mechanism when compared to the parent guanidinoglycoside-based carriers.
摘要
胍基糖苷,一类能够输送高分子量生物聚合物的细胞转运体,先前已被证明对细胞表面硫酸乙酰肝素蛋白聚糖具有高选择性,并促进其聚集。在此,通过细胞表面荧光共振能量转移分析研究了两亲胍基糖苷衍生物的内化机制。出乎意料的是,尽管保持了硫酸乙酰肝素的选择性,但这些衍生物的细胞摄取似乎不涉及蛋白聚糖在细胞表面的聚集。与基于胍基糖苷的载体相比,这表明存在一种独特的摄取机制。
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