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P2X7 receptor as a novel drug delivery system to increase the entrance of hydrophilic drugs into cells during photodynamic therapy

机译:P2X7受体作为一种新颖的药物递送系统,可在光动力治疗过程中增加亲水性药物进入细胞的进入

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摘要

The second-generation photosensitizer methylene blue (MB) exhibits photochemical and photophysical properties suitable for photodynamic therapy (PDT)-based cancer treatment. However, the clinical application of MB is limited because of its high hydrophilicity, which hinders its penetration into tumor tissues. Therefore, new methods to improve the entry of MB into the cytoplasm of target cells are necessary. Because MB has a mass of 319 Da, transient pores on the plasma membrane, such as the pore induced by the P2X7 receptor (P2X7R) that allows the passage of molecules up to 900 Da, could be used. Using MTT viability assays, flow cytometry experiments, and fluorescence microscopy, we evaluated the toxicity and phototoxicity of MB and potentiation effects of ATP and MB on cell death processes in the J774 cell line (via a P2X7-associated pore). We observed that treatment with 5 mu M MB for 15 min promoted the rate of entry of MB into the cytoplasm to 4.7 %. However, treatment with 5 mu M MB and 1 mM ATP for the same amount of time increased this rate to 90.2 %. However, this effect was inhibited by pretreatment with a P2X7 antagonist. We used peritoneal macrophages and a cell line that does not express P2X7R as controls. These cells were more resistant to PDT with MB under the same experimental conditions. Taken together, these results suggest the use of the pore associated with P2X7R as a drug delivery system to increase the passage of hydrophilic drugs into cells that express this receptor, thus facilitating PDT.
机译:第二代光敏剂亚甲基蓝(MB)具有适合基于光动力疗法(PDT)的癌症治疗的光化学和光物理特性。然而,由于MB的高亲水性,因此其在临床上的应用受到限制,这阻碍了其渗透到肿瘤组织中。因此,需要改善MB进入靶细胞胞质的新方法。由于MB的质量为319 Da,因此可以使用质膜上的瞬时孔,例如允许分子通过900 Da的P2X7受体(P2X7R)诱导的孔。使用MTT活力测定,流式细胞术实验和荧光显微镜,我们评估了MB的毒性和光毒性以及ATP和MB对J774细胞系中细胞死亡过程的增强作用(通过P2X7相关孔)。我们观察到用5μMMB处理15分钟将MB进入细胞质的速率提高到4.7%。但是,用5μM MB和1 mM ATP进行相同时间的处理会使该比率增加到90.2%。但是,这种作用被P2X7拮抗剂预处理所抑制。我们使用腹膜巨噬细胞和不表达P2X7R的细胞系作为对照。在相同的实验条件下,这些细胞对MB的PDT具有更强的抵抗力。综上所述,这些结果表明使用与P2X7R相关的孔作为药物递送系统,可增加亲水性药物进入表达该受体的细胞的通道,从而促进PDT。

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