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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >C-8-glycosphingolipids preferentially insert into tumor cell membranes and promote chemotherapeutic drug uptake
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C-8-glycosphingolipids preferentially insert into tumor cell membranes and promote chemotherapeutic drug uptake

机译:C-8-糖鞘脂优先插入肿瘤细胞膜并促进化疗药物的吸收

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Insufficient drug delivery into tumor cells limits the therapeutic efficacy of chemotherapy. Co-delivery of liposome-encapsulated drug and synthetic short-chain glycosphingolipids (SC-GSLs) significantly improved drug bioavailability by enhancing intracellular drug uptake. Investigating the mechanisms underlying this SC-GSL-mediated drug uptake enhancement is the aim of this study. Fluorescence microscopy was used to visualize the cell membrane lipid transfer intracellular fate of fluorescently labeled C-6-NBD-GalCer incorporated in liposomes in tumor and non-tumor cells. Additionally click chemistry was applied to image and quantify native SC-GSLs in tumor and non-tumor cell membranes. SC-GSL-mediated flip-flop was investigated in model membranes to confirm membrane-incorporation of SC-GSL and its effect on membrane remodeling. SC-GSL enriched liposomes containing doxorubicin (Dox) were incubated at 4 degrees C and 37 degrees C and intracellular drug uptake was studied in comparison to standard liposomes and free Dox.
机译:药物向肿瘤细胞的递送不足限制了化学疗法的治疗效果。脂质体包裹的药物和合成的短链鞘糖脂(SC-GSL)的共同给药通过增强细胞内药物的吸收显着改善了药物的生物利用度。研究此SC-GSL介导的药物吸收增强的潜在机制是本研究的目的。使用荧光显微镜观察掺入在肿瘤和非肿瘤细胞脂质体中的荧光标记的C-6-NBD-GalCer的细胞膜脂质转移的细胞内命运。另外,将click化学应用于成像和定量肿瘤和非肿瘤细胞膜中的天然SC-GSL。在模型膜中研究了SC-GSL介导的触发器,以确认SC-GSL的膜结合及其对膜重塑的影响。将含有阿霉素(Dox)的富含SC-GSL的脂质体在4摄氏度和37摄氏度下温育,并与标准脂质体和游离Dox相比,研究了细胞内药物的吸收。

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