首页> 外文期刊>Journal of Photochemistry and Photobiology, B. Biology: Official Journal of the European Society for Photobiology >Novel photosensitizer-protein nanoparticles for Photodynamic therapy: Photophysical characterization and in vitro investigations
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Novel photosensitizer-protein nanoparticles for Photodynamic therapy: Photophysical characterization and in vitro investigations

机译:用于光动力疗法的新型光敏剂-蛋白质纳米颗粒:光物理特性和体外研究

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In this work two types of pheophorbide-HSA (Pheo-HSA) nanoparticles, PHSA40 and PHSA100, were prepared and their photophysical and photosensitizing properties were investigated. Due to intramolecular interactions the singlet oxygen quantum yield of PHSA40 and PHSA100 is very low (less than 0.1). Intracellular uptake and phototoxicity of pheophorbide a as well as of the Pheo-HSA nanoparticles were studied in Jurkat cells. The HSA nanoparticles do not influence the amount of dye accumulation in cells. After 24 h incubation, PHSA40 and PHSA100 showed a higher phototoxicity than Pheo. The reason for this behavior is an efficient nanoparticle decomposition in the cellular lysosomes. The process of drug release during incubation of cells with Pheo-HSA nanoparticles was illustrated by fluorescence lifetime imaging (FLIM) and confocal laser scanning microscopy (CLSM). The final phototoxicity of Pheo-HSA is at the same scale as induced by free Pheo. The drug release ability of HSA nanoparticles shows the possibility to use such formulations as drug carriers in PDT treatment. Therefore, this work constructs a standard for further investigation and optimization of photosensitizer-HSA drug carrier system.
机译:在这项工作中,制备了两种类型的脱镁叶绿素-HSA(Pheo-HSA)纳米粒子PHSA40和PHSA100,并研究了它们的光物理和光敏特性。由于分子内相互作用,PHSA40和PHSA100的单重态氧量子产率非常低(小于0.1)。在Jurkat细胞中研究了脱镁叶绿酸a以及Pheo-HSA纳米颗粒的细胞内吸收和光毒性。 HSA纳米颗粒不影响细胞中染料的积累量。温育24小时后,PHSA40和PHSA100显示出比Pheo更高的光毒性。该行为的原因是细胞溶酶体中纳米颗粒的有效分解。通过荧光寿命成像(FLIM)和共聚焦激光扫描显微镜(CLSM)说明了用Pheo-HSA纳米颗粒孵育细胞期间药物释放的过程。 Pheo-HSA的最终光毒性与游离Pheo诱导的相同。 HSA纳米颗粒的药物释放能力显示出在PDT治疗中使用这种制剂作为药物载体的可能性。因此,这项工作为进一步研究和优化光敏剂-HSA药物载体系统建立了标准。

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