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金丝桃素与低密度脂蛋白和 U87-MG 细胞的相互作用动力学。

Interaction dynamics of hypericin with low-density lipoproteins and U87-MG cells.

机构信息

ANBioPhi, CNRS-FRE 3207, Pierre & Marie Curie University, Paris, France.

出版信息

Int J Pharm. 2010 Apr 15;389(1-2):32-40. doi: 10.1016/j.ijpharm.2010.01.010. Epub 2010 Jan 18.

Abstract

The natural photosensitizer hypericin exhibits potent properties for tumor diagnosis and photodynamic therapy. Fluorescent properties of hypericin along with various technical approaches have been used for dynamic studies of its interaction with low-density lipoprotein and U87 glioma cells. Evidences for hypericin release from low-density lipoprotein towards cells plasmatic membrane are addressed. Subsequent subcellular bulk flow redistribution leading to non-specific staining of intracellular membranes compartment were observed within cells. It was shown, that monomers of hypericin are the only redistributive forms. Increasing concentration of hypericin leads to the formation of non-fluorescent aggregates within low-density lipoprotein as well as within the U87 cells, and can preclude its photosensitizing activities. However, the aggregation process can only account for a part of the observed emission decrease. As shown by the excited state lifetime measurements, this fluorescence quenching actually results from a combination of aggregation process and energy transfer from monomers to aggregates. In all experiments, hydrophobic character of hypericin appears as the driving force of its redistribution process.

摘要

天然光敏剂金丝桃素具有很强的肿瘤诊断和光动力治疗性能。金丝桃素的荧光特性以及各种技术方法已被用于其与低密度脂蛋白和 U87 神经胶质瘤细胞相互作用的动态研究。本文探讨了金丝桃素从低密度脂蛋白向细胞质膜释放的证据。随后观察到,细胞内大量的细胞质膜再分布导致细胞内膜区室的非特异性染色。结果表明,金丝桃素的单体是唯一的再分布形式。金丝桃素浓度的增加会导致低密度脂蛋白内以及 U87 细胞内形成非荧光聚集物,并可能抑制其光致敏活性。然而,聚集过程只能解释观察到的发射强度降低的一部分原因。如激发态寿命测量所示,这种荧光猝灭实际上是聚集过程和从单体到聚集体的能量转移的组合结果。在所有实验中,金丝桃素的疏水性似乎是其再分布过程的驱动力。

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