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碳点与生物膜的相互作用及其对细胞药物递送的影响。

Carbon Dots-Biomembrane Interactions and Their Implications for Cellular Drug Delivery.

作者信息

Mavroidi Barbara, Kaminari Archontia, Sakellis Elias, Sideratou Zili, Tsiourvas Dimitris

机构信息

Institute of Biosciences and Applications, National Centre for Scientific Research "Demokritos", 15310 Aghia Paraskevi, Greece.

Institute of Nanoscience and Nanotechnology, National Centre for Scientific Research "Demokritos", 15310 Aghia Paraskevi, Greece.

出版信息

Pharmaceuticals (Basel). 2023 Jun 2;16(6):833. doi: 10.3390/ph16060833.

Abstract

The effect of carbon dots (CDs) on a model blayer membrane was studied as a means of comprehending their ability to affect cell membranes. Initially, the interaction of N-doped carbon dots with a biophysical liposomal cell membrane model was investigated by dynamic light scattering, z-potential, temperature-modulated differential scanning calorimetry, and membrane permeability. CDs with a slightly positive charge interacted with the surface of the negative-charged liposomes and evidence indicated that the association of CDs with the membrane affects the structural and thermodynamic properties of the bilayer; most importantly, it enhances the bilayer's permeability against doxorubicin, a well-known anticancer drug. The results, like those of similar studies that surveyed the interaction of proteins with lipid membranes, suggest that carbon dots are partially embedded in the bilayer. In vitro experiments employing breast cancer cell lines and human healthy dermal cells corroborated the findings, as it was shown that the presence of CDs in the culture medium selectively enhanced cell internalization of doxorubicin and, subsequently, increased its cytotoxicity, acting as a drug sensitizer.

摘要

研究了碳点(CDs)对模型层膜的影响,以此作为理解其影响细胞膜能力的一种方式。最初,通过动态光散射、ζ-电位、温度调制差示扫描量热法和膜通透性研究了氮掺杂碳点与生物物理脂质体细胞膜模型的相互作用。带轻微正电荷的碳点与带负电荷的脂质体表面相互作用,有证据表明碳点与膜的结合会影响双层膜的结构和热力学性质;最重要的是,它增强了双层膜对阿霉素(一种著名的抗癌药物)的通透性。这些结果与那些研究蛋白质与脂质膜相互作用的类似研究结果一样,表明碳点部分嵌入双层膜中。使用乳腺癌细胞系和人类健康皮肤细胞进行的体外实验证实了这些发现,因为结果表明培养基中碳点的存在选择性地增强了阿霉素的细胞内化,随后增加了其细胞毒性,起到了药物增敏剂的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81cb/10305404/de371c91e425/pharmaceuticals-16-00833-g001.jpg

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