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Selective cellular delivery of self-assembled quantum dot-peptide bioconjugates

机译:自组装量子点肽生物缀合物的选择性细胞递送

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We demonstrate the selective delivery of self-assembled luminescent semiconductor quantum dot (QD)-peptide bioconjugates into several eukaryotic cell lines. A 23-mer hetero-bifunctional peptide bearing a positively-charged oligoarginine domain and a terminal polyhistidine tract was synthesized and used to mediate the cellular internalization of the QD-bioconjugates. The polyhistidine tract allows the peptide to self-assemble onto the QD surface via metal-ion coordination while the oligoarginine domain mediates the specific uptake of the QD-bioconjugates via electrostatic interactions with cell surface receptors. In both HEK 293T/17 and COS-1 cells, this peptide-mediated delivery is concentration-dependent in terms of both the QD concentration and the peptide:QD ratio. Intracellularly, the QD signal is punctate in appearance and some, but not all, of the QDs are located within recycling endosomes as evidenced by their colocalization with transferrin. In both cell lines, the QD-bioconjugates elicit minimal cytotoxicity within the timeframe required for adequate cellular uptake. The specificity of this delivery strategy is demonstrated by performing a multicolor QD labeling, wherein the presence or absence of the peptide on the QD surface controls cellular uptake.
机译:我们证明了自组装发光半导体量子点(QD) - 肽生物缀合物的选择性递送到几种真核细胞系中。合成轴承带正电荷的寡核苷酸结构域和末端多亚氨酰基的23er杂双官能肽,并用于介导QD-生物缀合物的细胞内化。多亚氨基氨酸管允许肽通过金属离子协调将肽自组装到QD表面上,而寡核苷酸域通过与细胞表面受体的静电相互作用介导QD-生物缀合物的特异性摄取。在HEK 293T / 17和COS-1细胞中,该肽介导的递送是QD浓度和肽:QD比的浓度依赖性。细胞内,QD信号在外观中点标,QDS的一些但不是全部,QDS在再循环内孔隙内,其通过与转移素的分层化证明。在两种细胞系中,QD-生物缀合物在足够的蜂窝摄取所需的时间框架内引出最小的细胞毒性。通过进行多色QD标记来证明该输送策略的特异性,其中QD表面上的肽的存在或不存在控制蜂窝摄取。

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