首页> 美国卫生研究院文献>Biophysical Journal >Porphyrin Depth in Lipid Bilayers as Determined by Iodide and Parallax Fluorescence Quenching Methods and Its Effect on Photosensitizing Efficiency
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Porphyrin Depth in Lipid Bilayers as Determined by Iodide and Parallax Fluorescence Quenching Methods and Its Effect on Photosensitizing Efficiency

机译:碘化物和视差荧光淬灭法测定脂质双层中的卟啉深度及其对光敏效率的影响

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摘要

Photosensitization by porphyrins and other tetrapyrrole chromophores is used in biology and medicine to kill cells. This light-triggered generation of singlet oxygen is used to eradicate cancer cells in a process dubbed “photodynamic therapy,” or PDT. Most photosensitizers are of amphiphilic character and they partition into cellular lipid membranes. The photodamage that they inflict to the host cell is mainly localized in membrane proteins. This photosensitized damage must occur in competition with the rapid diffusion of singlet oxygen through the lipid phase and its escape into the aqueous phase. In this article we show that the extent of damage can be modulated by employing modified hemato- and protoporphyrins, which have alkyl spacers of varying lengths between the tetrapyrrole ring and the carboxylate groups that are anchored at the lipid/water interface. The chromophore part of the molecule, and the point of generation of singlet oxygen, is thus located at a deeper position in the bilayer. The photosensitization efficiency was measured with 9,10-dimethylanthracene, a fluorescent chemical target for singlet oxygen. The vertical insertion of the sensitizers was assessed by two fluorescence-quenching techniques: by iodide ions that come from the aqueous phase; and by spin-probe-labeled phospholipids, that are incorporated into the bilayer, using the parallax method. These methods also show that temperature has a small effect on the depth when the membrane is in the liquid phase. However, when the bilayer undergoes a phase transition to the solid gel phase, the porphyrins are extruded toward the water interface as the temperature is lowered. These results, together with a previous publication in this journal, represent a unique and precedental case where the vertical location of a small molecule in a membrane has an effect on its membranal activity.
机译:卟啉和其他四吡咯发色团的光敏作用被用于生物学和医学中以杀死细胞。这种光触发的单线态氧的产生被称为“光动力疗法”(PDT),用于消灭癌细胞。大多数光敏剂具有两亲性,它们可分为细胞脂质膜。它们对宿主细胞造成的光损伤主要位于膜蛋白中。这种光敏性损害必须与单线态氧快速扩散通过脂质相并逃逸到水相中竞争。在本文中,我们表明可以通过使用修饰的血卟啉和原卟啉来调节损伤的程度,它们在四吡咯环和锚定在脂质/水界面的羧酸酯基团之间具有不同长度的烷基间隔基。因此,分子的发色团部分和单线态氧的产生点位于双层中的更深位置。用9,10-二甲基蒽(单线态氧的荧光化学靶标)测量光敏效率。敏化剂的垂直插入是通过两种荧光猝灭技术来评估的:来自水相的碘离子;并通过视差法将掺入双层的自旋探针标记的磷脂。这些方法还表明,当膜处于液相时,温度对深度的影响很小。但是,当双层经历到固态凝胶相的相变时,随着温度降低,卟啉向水界面挤出。这些结果与该期刊的先前出版物一起代表了一种独特的先例,其中小分子在膜中的垂直位置对其膜活性有影响。

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