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膜脂如何影响活性氧物质向细胞内的血浆传递以及随后的 DNA 损伤:一项实验和计算研究。

How membrane lipids influence plasma delivery of reactive oxygen species into cells and subsequent DNA damage: an experimental and computational study.

机构信息

Research Group PLASMANT, Department of Chemistry, University of Antwerp, Belgium.

Future Industries Institute, University of South Australia, Adelaide, SA 5095, Australia.

出版信息

Phys Chem Chem Phys. 2019 Sep 21;21(35):19327-19341. doi: 10.1039/c9cp03520f. Epub 2019 Aug 27.

Abstract

The mechanisms of plasma in medicine are broadly attributed to plasma-derived reactive oxygen and nitrogen species (RONS). In order to exert any intracellular effects, these plasma-derived RONS must first traverse a major barrier in the cell membrane. The cell membrane lipid composition, and thereby the magnitude of this barrier, is highly variable between cells depending on type and state (e.g. it is widely accepted that healthy and cancerous cells have different membrane lipid compositions). In this study, we investigate how plasma-derived RONS interactions with lipid membrane components can potentially be exploited in the future for treatment of diseases. We couple phospholipid vesicle experiments, used as simple cell models, with molecular dynamics (MD) simulations of the lipid membrane to provide new insights into how the interplay between phospholipids and cholesterol may influence the response of healthy and diseased cell membranes to plasma-derived RONS. We focus on the (i) lipid tail saturation degree, (ii) lipid head group type, and (iii) membrane cholesterol fraction. Using encapsulated molecular probes, we study the influence of the above membrane components on the ingress of RONS into the vesicles, and subsequent DNA damage. Our results indicate that all of the above membrane components can enhance or suppress RONS uptake, depending on their relative concentration within the membrane. Further, we show that higher RONS uptake into the vesicles does not always correlate with increased DNA damage, which is attributed to ROS reactivity and lifetime. The MD simulations indicate the multifactorial chemical and physical processes at play, including (i) lipid oxidation, (ii) lipid packing, and (iii) lipid rafts formation. The methods and findings presented here provide a platform of knowledge that could be leveraged in the development of therapies relying on the action of plasma, in which the cell membrane and oxidative stress response in cells is targeted.

摘要

等离子体在医学中的作用机制主要归因于等离子体衍生的活性氧和氮物质(RONS)。为了发挥任何细胞内的作用,这些等离子体衍生的 RONS 必须首先穿过细胞膜这一主要屏障。细胞膜的脂质组成,以及因此屏障的大小,在不同类型和状态的细胞之间有很大的差异(例如,人们普遍认为健康细胞和癌细胞的膜脂质组成不同)。在这项研究中,我们研究了等离子体衍生的 RONS 与脂质膜成分的相互作用如何在未来可能被用于治疗疾病。我们将磷脂囊泡实验(用作简单的细胞模型)与脂质膜的分子动力学(MD)模拟相结合,提供了新的见解,了解磷脂和胆固醇之间的相互作用如何影响健康和患病细胞膜对等离子体衍生的 RONS 的反应。我们重点研究了(i)脂质尾部饱和度、(ii)脂质头部基团类型和(iii)膜胆固醇分数。使用封装的分子探针,我们研究了上述膜成分对 RONS 进入囊泡以及随后的 DNA 损伤的影响。我们的结果表明,所有上述膜成分都可以增强或抑制 RONS 的摄取,这取决于它们在膜中的相对浓度。此外,我们表明,RONS 进入囊泡的摄取量增加并不总是与 DNA 损伤增加相关,这归因于 ROS 的反应性和寿命。MD 模拟表明,起作用的是多种化学和物理过程,包括(i)脂质氧化、(ii)脂质堆积和(iii)脂质筏形成。这里提出的方法和发现为知识平台提供了基础,该平台可用于开发依赖等离子体作用的治疗方法,靶向细胞的细胞膜和氧化应激反应。

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