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葡萄糖偶联氮杂 BODIPY 用于增强的光动力癌症治疗。

Glucose conjugated aza-BODIPY for enhanced photodynamic cancer therapy.

机构信息

School of Chemistry, Institute of Science, Suranaree University of Technology, Nakhon Ratchasima 30000, Thailand.

National Nanotechnology Center, National Science and Technology Development Agency, Thailand Science Park, Pathum Thani 12120, Thailand.

出版信息

Org Biomol Chem. 2021 Jul 14;19(26):5867-5875. doi: 10.1039/d1ob00400j. Epub 2021 Jun 14.

Abstract

Compared with normal cells, cancer cells usually exhibit an increase in glucose uptake as part of the Warburg effect. To take advantage of this hallmark of cancer, glucose transporters could be a good candidate for cancer targeting. Herein, we report novel glycoconjugate aza-BODIPY dyes (AZB-Glc and AZB-Glc-I) that contain two glucose moieties conjugated to near-infrared dyes via the azide-alkyne cycloaddition reaction. As anticipated, a higher level of AZB-Glc uptake was observed in breast cancer cells that overexpressed glucose transporters (GLUTs), especially GLUT-1, including the triple-negative breast cancer cell line (MDA-MB-231) and human breast adenocarcinoma cell line (MCF-7), compared to that of normal cells (human fetal lung fibroblasts, HFL1). The cellular uptake of AZB-Glc was in a dose- and time-dependent manner and also depended on GLUT, as evidenced by the decreased uptake of AZB-Glc in the presence of d-glucose or a glucose metabolism suppressor, combretastatin. In addition, light triggered cell death was also investigated through photodynamic therapy (PDT), since near-infrared (NIR) light is known to penetrate deeper tissue than light of shorter wavelengths. AZB-Glc-I, the analog of AZB-Glc containing iodine for enhanced singlet oxygen production upon NIR irradiation, was used for all treatment assays. AZB-Glc-I showed significant NIR light-induced cytotoxicity in cancer cells (IC = 1.4-1.6 μM under 1 min irradiation), which was about 20-times lower than that in normal cells (IC = 32 μM) under the same conditions, with negligible dark toxicity (IC > 100 μM) in all cell lines. Moreover, the singlet oxygen was detected inside the cancer cells after exposure to light in the presence of AZB-Glc-I. Therefore, our glucose conjugated systems proved to efficiently target cancer cells for enhanced photodynamic cancer therapy.

摘要

与正常细胞相比,癌细胞通常表现为葡萄糖摄取增加,这是沃伯格效应的一部分。为了利用这一癌症特征,葡萄糖转运蛋白可能是癌症靶向的一个很好的候选物。在此,我们报告了新型糖缀合吖啶 BODIPY 染料(AZB-Glc 和 AZB-Glc-I),它们含有两个葡萄糖部分,通过叠氮-炔环加成反应与近红外染料连接。正如预期的那样,在过表达葡萄糖转运蛋白(GLUTs)的乳腺癌细胞中观察到更高水平的 AZB-Glc 摄取,尤其是 GLUT-1,包括三阴性乳腺癌细胞系(MDA-MB-231)和人乳腺癌腺癌细胞系(MCF-7),与正常细胞(人胎肺成纤维细胞,HFL1)相比。AZB-Glc 的细胞摄取呈剂量和时间依赖性,并且还依赖于 GLUT,这一点可以从葡萄糖或葡萄糖代谢抑制剂 combretastatin 的存在下 AZB-Glc 摄取减少得到证明。此外,还通过光动力疗法(PDT)研究了光触发细胞死亡,因为已知近红外(NIR)光比短波长光穿透更深的组织。AZB-Glc-I 是 AZB-Glc 的类似物,在近红外辐射下含有碘以增强单线态氧的产生,用于所有治疗实验。AZB-Glc-I 在癌细胞中表现出显著的近红外光诱导细胞毒性(在 1 分钟照射下,IC = 1.4-1.6 μM),在相同条件下,在正常细胞中的 IC 值约低 20 倍(IC = 32 μM),在所有细胞系中,暗毒性可忽略不计(IC > 100 μM)。此外,在存在 AZB-Glc-I 的情况下,在癌细胞内暴露于光后检测到单线态氧。因此,我们的葡萄糖缀合物系统被证明可以有效地针对癌症细胞,用于增强的光动力癌症治疗。

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