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三苯胺在双光子激发下诱导细胞死亡。

Triphenylamines Induce Cell Death Upon 2-Photon Excitation.

作者信息

Chennoufi Rahima, Mahuteau-Betzer Florence, Tauc Patrick, Teulade-Fichou Marie-Paule, Deprez Eric

机构信息

1 LBPA, CNRS UMR8113, IDA FR3242, ENS Cachan, Université Paris-Saclay, Cachan, France.

2 Chemistry, Modeling and Imaging for Biology, UMR9187-U1196, Institut Curie, Centre universitaire, Orsay, France.

出版信息

Mol Imaging. 2017 Jan 1;16:1536012117714164. doi: 10.1177/1536012117714164.

DOI:10.1177/1536012117714164
PMID:28627326
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5480627/
Abstract

Photodynamic therapy (PDT) is a promising therapeutic method for several diseases, in particular for cancer. This approach uses a photosensitizer, oxygen, and an external light source to produce reactive oxygen species (ROS) at lethal doses to induce cell death. One drawback of current PDT is the use of visible light which has poor penetration in tissues. Such a limitation could be overcome by the use of novel organic compounds compatible with photoactivation under near-infrared light excitation. Triphenylamines (TPAs) are highly fluorescent compounds that are efficient to induce cell death upon visible light excitation (458 nm), but outside the biological spectral window. Interestingly, we recently showed that TPAs target cytoplasmic organelles of living cells, mainly mitochondria, and induce a high ROS production upon 2-photon excitation (in the 760-860 nm range), leading to a fast apoptosis process. However, we observed significant differences among the tested TPA compounds in terms of cell distribution and time courses of cell death-related events (apoptosis vs necrosis). In summary, TPAs represent serious candidates as photosensitizers that are compatible with 2-photon excitation to simultaneously trigger and imaging cell death although the relationship between their subcellular localization and the cell death mechanism involved is still a matter of debate.

摘要

光动力疗法(PDT)是一种对多种疾病,尤其是癌症颇具前景的治疗方法。该方法利用一种光敏剂、氧气和外部光源,以产生致死剂量的活性氧(ROS)来诱导细胞死亡。当前光动力疗法的一个缺点是使用可见光,而可见光在组织中的穿透性较差。通过使用与近红外光激发下的光活化兼容的新型有机化合物,可以克服这一限制。三苯胺(TPA)是高度荧光的化合物,在可见光激发(458nm)时能有效诱导细胞死亡,但在生物光谱窗口之外。有趣的是,我们最近发现三苯胺靶向活细胞的细胞质细胞器,主要是线粒体,并在双光子激发(760 - 860nm范围内)时诱导大量ROS产生,从而导致快速的凋亡过程。然而,我们观察到在测试的三苯胺化合物之间,在细胞分布和细胞死亡相关事件(凋亡与坏死)的时间进程方面存在显著差异。总之,三苯胺作为与双光子激发兼容的光敏剂,有望同时触发和成像细胞死亡,尽管它们的亚细胞定位与所涉及的细胞死亡机制之间的关系仍存在争议。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b1a/5480627/40f44653d18d/10.1177_1536012117714164-fig1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b1a/5480627/40f44653d18d/10.1177_1536012117714164-fig1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b1a/5480627/40f44653d18d/10.1177_1536012117714164-fig1.jpg

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本文引用的文献

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Sci Rep. 2016 Mar 7;6:21458. doi: 10.1038/srep21458.
2
Differential behaviour of cationic triphenylamine derivatives in fixed and living cells: triggering and imaging cell death.阳离子三苯胺衍生物在固定细胞和活细胞中的差异行为:引发和成像细胞死亡
Chem Commun (Camb). 2015 Oct 14;51(80):14881-4. doi: 10.1039/c5cc05970d.
3
Mechanisms in photodynamic therapy: part two-cellular signaling, cell metabolism and modes of cell death.
光动力疗法的机制:第二部分——细胞信号转导、细胞代谢和细胞死亡方式。
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DNA switches on the two-photon efficiency of an ultrabright triphenylamine fluorescent probe specific of AT regions.DNA 开启了一种超亮三苯胺荧光探针对 AT 区特异性的双光子效率。
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Photodynamic therapy and two-photon bio-imaging applications of hydrophobic chromophores through amphiphilic polymer delivery.通过两亲聚合物递送来实现疏水性生色团的光动力疗法和双光子生物成像应用。
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