一种在1.8 GHz射频暴露系统中实现精度和可重复性的新方法,该系统可调节细胞内ROS作为人类细胞培养中信号幅度的函数。

IF 3.8 3区 医学 Q2 ENGINEERING, BIOMEDICAL
Cyril Dahon, Blanche Aguida, Yoann Lebon, Pierre Le Guen, Art Dangremont, Olivier Meyer, Jean-Marie Citerne, Marootpong Pooam, Haider Raad, Thawatchai Thoradit, Nathalie Jourdan, Federico Bertagna, Margaret Ahmad
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引用次数: 0

摘要

1-28千兆赫范围的射频场在现代世界无处不在,引发了许多关于潜在健康风险的研究,如癌症、神经系统疾病、生殖风险和电磁超敏反应。然而,由于暴露条件缺乏精度和实验模型的巨大差异,结果不一致,而测量的射频效应通常是间接的,并且发生在许多小时甚至几天内。在这里,我们提出了一种简化的射频暴露方案,为人类HEK293细胞单层培养提供单个1.8 GHz载波频率。一个定制的暴露箱和天线保持在一个完全屏蔽的消声室发出离散的射频信号,可以精确地表征和建模。所选择的振幅是非热的,并且落在现代电信设备的范围内。该方案的一个关键特征是细胞培养物仅暴露于单一的短(15分钟)射频暴露期,随后检测基因表达的立即快速变化。通过这种方式,我们发现与氧化应激和ROS信号有关的基因调节是射频暴露最早的细胞反应之一。此外,这些基因以复杂的方式对不同的射频信号幅度作出反应,这与激射、受体驱动的生物机制相一致。我们得出的结论是,诱导轻度细胞应激和活性氧(ROS)是人体细胞对射频信号的主要反应,这些反应发生在正常通信设备范围内的射频信号幅度。我们认为,这种方法可能有助于为实验室之间研究结果的可靠性和可重复性提供指导,从而有助于解决关于普通人群中射频暴露的潜在机制和结果的现有争议。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Novel Method for Achieving Precision and Reproducibility in a 1.8 GHz Radiofrequency Exposure System That Modulates Intracellular ROS as a Function of Signal Amplitude in Human Cell Cultures.

Radiofrequency fields in the 1-28 GHz range are ubiquitous in the modern world, giving rise to numerous studies of potential health risks such as cancer, neurological conditions, reproductive risks and electromagnetic hypersensitivity. However, results are inconsistent due to a lack of precision in exposure conditions and vastly differing experimental models, whereas measured RF effects are often indirect and occur over many hours or even days. Here, we present a simplified RF exposure protocol providing a single 1.8 GHz carrier frequency to human HEK293 cell monolayer cultures. A custom-built exposure box and antenna maintained in a fully shielded anechoic chamber emits discrete RF signals which can be precisely characterized and modelled. The chosen amplitudes are non-thermal and fall within the range of modern telecommunication devices. A critical feature of the protocol is that cell cultures are exposed to only a single, short (15 min) RF exposure period, followed by detection of immediate, rapid changes in gene expression. In this way, we show that modulation of genes implicated in oxidative stress and ROS signaling is among the earliest cellular responses to RF exposure. Moreover, these genes respond in complex ways to varying RF signal amplitudes consistent with a hormetic, receptor-driven biological mechanism. We conclude that induction of mild cellular stress and reactive oxygen species (ROS) is a primary response of human cells to RF signals, and that these responses occur at RF signal amplitudes within the range of normal telecommunications devices. We suggest that this method may help provide a guideline for greater reliability and reproducibility of research results between labs, and thereby help resolve existing controversy on underlying mechanisms and outcomes of RF exposure in the general population.

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来源期刊
Bioengineering
Bioengineering Chemical Engineering-Bioengineering
CiteScore
4.00
自引率
8.70%
发文量
661
期刊介绍: Aims Bioengineering (ISSN 2306-5354) provides an advanced forum for the science and technology of bioengineering. It publishes original research papers, comprehensive reviews, communications and case reports. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. All aspects of bioengineering are welcomed from theoretical concepts to education and applications. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. There are, in addition, four key features of this Journal: ● We are introducing a new concept in scientific and technical publications “The Translational Case Report in Bioengineering”. It is a descriptive explanatory analysis of a transformative or translational event. Understanding that the goal of bioengineering scholarship is to advance towards a transformative or clinical solution to an identified transformative/clinical need, the translational case report is used to explore causation in order to find underlying principles that may guide other similar transformative/translational undertakings. ● Manuscripts regarding research proposals and research ideas will be particularly welcomed. ● Electronic files and software regarding the full details of the calculation and experimental procedure, if unable to be published in a normal way, can be deposited as supplementary material. ● We also accept manuscripts communicating to a broader audience with regard to research projects financed with public funds. Scope ● Bionics and biological cybernetics: implantology; bio–abio interfaces ● Bioelectronics: wearable electronics; implantable electronics; “more than Moore” electronics; bioelectronics devices ● Bioprocess and biosystems engineering and applications: bioprocess design; biocatalysis; bioseparation and bioreactors; bioinformatics; bioenergy; etc. ● Biomolecular, cellular and tissue engineering and applications: tissue engineering; chromosome engineering; embryo engineering; cellular, molecular and synthetic biology; metabolic engineering; bio-nanotechnology; micro/nano technologies; genetic engineering; transgenic technology ● Biomedical engineering and applications: biomechatronics; biomedical electronics; biomechanics; biomaterials; biomimetics; biomedical diagnostics; biomedical therapy; biomedical devices; sensors and circuits; biomedical imaging and medical information systems; implants and regenerative medicine; neurotechnology; clinical engineering; rehabilitation engineering ● Biochemical engineering and applications: metabolic pathway engineering; modeling and simulation ● Translational bioengineering
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