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负载二氢卟吩e6的乳铁蛋白纳米颗粒用于增强光动力疗法。

Chlorin e6 loaded lactoferrin nanoparticles for enhanced photodynamic therapy.

作者信息

Adimoolam Mahesh G, A Vijayalakshmi, Nalam Madhusudhana Rao, Sunkara Manorama V

机构信息

CSIR-Indian Institute of Chemical Technology, Uppal Road, Hyderabad, India.

出版信息

J Mater Chem B. 2017 Dec 14;5(46):9189-9196. doi: 10.1039/c7tb02599h. Epub 2017 Nov 17.

DOI:10.1039/c7tb02599h
PMID:32264601
Abstract

Photosensitizer (PS) mediated Photodynamic Therapy (PDT) is a preferred treatment modality for certain cancers. Some of the factors limiting the expansion of PDT to other clinical conditions are the aggregation of hydrophobic PS in aqueous media and the inefficient biodistribution of photosensitizers. Formulations containing the PS have overcome some of the limitations by controlling aggregation-dependent quenching of PS and by improving the biodistribution of PS. We report a photosensitizer delivery system with protein nanoparticles that does not involve any chemical modifications. Using Lactoferrin, an iron-carrying milk protein, as sole matrix and Chlorine e6 (Ce6), an FDA-approved PS. The nanoparticles were prepared by the water-in-oil emulsion method. The spectral and physical properties of the particles were analyzed. Production of reactive oxygen was enhanced in the formulations (LeN) compared to free Ce6 as indicated by the water-soluble and -insoluble dyes. LeN show a specific Ce6 release at low pH, which is an advantage in the acidic environment of tumors and in endosomes. The uptake and intracellular concentrations of Ce6 by SK-OV-3, estimated by confocal microscopy, FACS and fluorescence spectroscopy, were significantly higher with LeN compared to free Ce6. Upon light exposure, LeN showed a substantial decrease (>4 times) in Ce6 requirement compared to free Ce6 in its ability to cause light-mediated cell death in the SK-OV-3 and MDA-MD 231 cells. LeN were shown to be non-toxic to the cells even at concentrations ten times that used in the PDT study. Safety, efficient loading and significant uptake by cells and more importantly a significant decrease in IC values demonstrate that LeN have potential in PDT.

摘要

光敏剂(PS)介导的光动力疗法(PDT)是某些癌症的首选治疗方式。限制PDT扩展到其他临床病症的一些因素包括疏水性PS在水性介质中的聚集以及光敏剂生物分布效率低下。含有PS的制剂通过控制PS的聚集依赖性猝灭以及改善PS的生物分布克服了一些局限性。我们报道了一种不涉及任何化学修饰的含蛋白质纳米颗粒的光敏剂递送系统。使用乳铁蛋白(一种载铁乳蛋白)作为唯一基质和氯e6(Ce6,一种FDA批准的PS)。通过油包水乳液法制备纳米颗粒。分析了颗粒的光谱和物理性质。如水溶性和水不溶性染料所示,与游离Ce6相比,制剂(LeN)中活性氧的产生有所增强。LeN在低pH下显示出特定的Ce6释放,这在肿瘤的酸性环境和内体中具有优势。通过共聚焦显微镜、流式细胞仪和荧光光谱法估计,与游离Ce6相比,SK-OV-3细胞对Ce6的摄取和细胞内浓度在LeN存在下显著更高。光照后,与游离Ce6相比,LeN在SK-OV-3和MDA-MD 231细胞中引起光介导细胞死亡的能力方面,Ce6需求量大幅降低(>4倍)。即使在PDT研究中所用浓度的十倍时,LeN对细胞也无毒。安全性、高效负载、细胞的显著摄取以及更重要的是IC值的显著降低表明LeN在PDT中具有潜力。

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