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溶液和单个哺乳动物细胞中分子氧的765纳米直接光激发

Direct 765 nm Optical Excitation of Molecular Oxygen in Solution and in Single Mammalian Cells.

作者信息

Bregnhøj Mikkel, Blázquez-Castro Alfonso, Westberg Michael, Breitenbach Thomas, Ogilby Peter R

机构信息

†Center for Oxygen Microscopy and Imaging, Department of Chemistry, Aarhus University, Langelandsgade 140, Aarhus 8000, Denmark.

‡Aarhus Institute of Advanced Studies, Aarhus University, Høegh-Guldbergs Gade 6B, Aarhus 8000, Denmark.

出版信息

J Phys Chem B. 2015 Apr 30;119(17):5422-9. doi: 10.1021/acs.jpcb.5b01727. Epub 2015 Apr 17.

Abstract

Singlet oxygen, O2(a(1)Δg), the first excited electronic state of molecular oxygen, is an important reactive oxygen species. Its chemistry plays a role in processes ranging from polymer degradation to cell death. Although O2(a(1)Δg) is routinely produced through natural events, including photosensitized processes mediated by organic chromophores, the controlled and selective laboratory production of O2(a(1)Δg) remains a challenge, particularly in biological systems. Here we exploit the fact that ground-state oxygen, O2(X(3)Σg(-)), absorbs 765 nm light to selectively produce O2(b(1)Σg(+)) which, in turn, decays to O2(a(1)Δg). We have quantified this process in different solvents using the time-resolved 1275 nm O2(a(1)Δg) phosphorescence as an optical probe. Most importantly, 765 nm falls in the so-called "biological window", where endogenous chromophores minimally absorb. We show that femtosecond-laser-based, spatially resolved 765 nm irradiation of human tumor cells induces O2(a(1)Δg)-mediated cell death. We thus provide an accessible tool for the controlled sensitizer-free production and study of O2(a(1)Δg) in complex biological systems.

摘要

单线态氧O₂(a¹Δg)是分子氧的第一激发电子态,是一种重要的活性氧物种。其化学反应在从聚合物降解到细胞死亡等一系列过程中发挥作用。尽管O₂(a¹Δg)通常通过自然事件产生,包括由有机发色团介导的光敏化过程,但在实验室中可控且选择性地产生O₂(a¹Δg)仍然是一个挑战,尤其是在生物系统中。在此,我们利用基态氧O₂(X³Σg⁻)吸收765 nm光来选择性地产生O₂(b¹Σg⁺)这一事实,而O₂(b¹Σg⁺)又会衰变为O₂(a¹Δg)。我们使用时间分辨的1275 nm O₂(a¹Δg)磷光作为光学探针,在不同溶剂中对这一过程进行了量化。最重要的是,765 nm落在所谓的“生物窗口”内,内源性发色团在该窗口内吸收最少。我们表明,基于飞秒激光的、对人肿瘤细胞进行空间分辨的765 nm照射会诱导O₂(a¹Δg)介导的细胞死亡。因此,我们提供了一种可用于在复杂生物系统中可控地无敏化剂产生和研究O₂(a¹Δg)的工具。

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