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通过石墨烯量子点增强抗癌药物的细胞核积累和 DNA 切割活性。

Enhancing cell nucleus accumulation and DNA cleavage activity of anti-cancer drug via graphene quantum dots.

机构信息

1] State Key Laboratory of Bioreactor Engineering, Shanghai Key Laboratory of New Drug Design, School of Pharmacy, East China University of Science and Technology, Shanghai, 200237. P. R. China [2].

出版信息

Sci Rep. 2013 Oct 4;3:2852. doi: 10.1038/srep02852.

Abstract

Graphene quantum dots (GQDs) maintain the intrinsic layered structural motif of graphene but with smaller lateral size and abundant periphery carboxylic groups, and are more compatible with biological system, thus are promising nanomaterials for therapeutic applications. Here we show that GQDs have a superb ability in drug delivery and anti-cancer activity boost without any pre-modification due to their unique structural properties. They could efficiently deliver doxorubicin (DOX) to the nucleus through DOX/GQD conjugates, because the conjugates assume different cellular and nuclear internalization pathways comparing to free DOX. Also, the conjugates could enhance DNA cleavage activity of DOX markedly. This enhancement combining with efficient nuclear delivery improved cytotoxicity of DOX dramatically. Furthermore, the DOX/GQD conjugates could also increase the nuclear uptake and cytotoxicity of DOX to drug-resistant cancer cells indicating that the conjugates may be capable to increase chemotherapy efficacy of anti-cancer drugs that are suboptimal due to the drug resistance.

摘要

石墨烯量子点 (GQDs) 保持了石墨烯的固有层状结构特征,但具有更小的横向尺寸和丰富的外围羧酸基团,与生物系统更加兼容,因此是有前途的治疗应用纳米材料。在这里,我们表明 GQDs 具有出色的药物传递能力和抗癌活性增强能力,而无需进行任何预先修饰,这要归功于它们独特的结构特性。由于其独特的结构特性,它们可以通过 DOX/GQD 缀合物将阿霉素 (DOX) 有效地递送到细胞核内,因为与游离 DOX 相比,缀合物采用了不同的细胞内和核内内化途径。此外,该缀合物还可以显著增强 DOX 的 DNA 切割活性。这种增强作用结合高效的核内传递,大大提高了 DOX 的细胞毒性。此外,DOX/GQD 缀合物还可以增加耐药癌细胞对 DOX 的核摄取和细胞毒性,这表明该缀合物可能能够提高由于耐药性而导致效果不佳的抗癌药物的化疗效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/657f/3790198/74d8acb6bd9d/srep02852-f1.jpg

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