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体外检测肿瘤细胞来源外泌体与肿瘤细胞的特异性。

Examination of the specificity of tumor cell derived exosomes with tumor cells in vitro.

作者信息

Smyth Tyson J, Redzic Jasmina S, Graner Michael W, Anchordoquy Thomas J

机构信息

University of Colorado Denver, Anschutz Medical Campus, Skaggs School of Pharmacy and Pharmaceutical Sciences, Aurora, CO, USA.

University of Colorado Denver, Anschutz Medical Campus, Department of Neurosurgery, Aurora, CO, USA.

出版信息

Biochim Biophys Acta. 2014 Nov;1838(11):2954-65. doi: 10.1016/j.bbamem.2014.07.026. Epub 2014 Aug 4.

Abstract

Small endogenous vesicles called exosomes are beginning to be explored as drug delivery vehicles. The in vivo targets of exosomes are poorly understood; however, they are believed to be important in cell-to-cell communication and may play a prominent role in cancer metastasis. We aimed to elucidate whether cancer derived exosomes can be used as drug delivery vehicles that innately target tumors over normal tissue. Our in vitro results suggest that while there is some specificity towards cancer cells over "immortalized" cells, it is unclear if the difference is sufficient to achieve precise in vivo targeting. Additionally, we found that exosomes associate with their cellular targets to a significantly greater extent (>10-fold) than liposomes of a similar size. Studies on the association of liposomes mimicking the unique lipid content of exosomes revealed that the lipid composition contributes significantly to cellular adherence/internalization. Cleavage of exosome surface proteins yielded exosomes exhibiting reduced association with their cellular targets, demonstrating the importance of proteins in binding/internalization. Furthermore, although acidic conditions are known to augment the metastatic potential of tumors, we found that cells cultured at low pH released exosomes with significantly less potential for cellular association than cells cultured at physiological pH.

摘要

一种名为外泌体的小型内源性囊泡正开始作为药物递送载体被研究。外泌体在体内的靶点尚不清楚;然而,人们认为它们在细胞间通讯中很重要,并且可能在癌症转移中发挥重要作用。我们旨在阐明源自癌症的外泌体是否可以用作天然靶向肿瘤而非正常组织的药物递送载体。我们的体外研究结果表明,虽然相对于“永生化”细胞,外泌体对癌细胞有一定的特异性,但尚不清楚这种差异是否足以实现精确的体内靶向。此外,我们发现外泌体与其细胞靶点的结合程度比类似大小的脂质体显著更高(>10倍)。对模拟外泌体独特脂质成分的脂质体结合情况的研究表明,脂质组成对细胞黏附/内化有显著贡献。外泌体表面蛋白的切割产生了与细胞靶点结合减少的外泌体,这证明了蛋白在结合/内化中的重要性。此外,尽管已知酸性条件会增强肿瘤的转移潜能,但我们发现,在低pH值下培养的细胞释放的外泌体与细胞结合的潜能明显低于在生理pH值下培养的细胞。

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