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C3H/10T1/2细胞在暴露于120赫兹调制的2.45吉赫兹微波和佛波酯肿瘤启动子后发生肿瘤转化。

Neoplastic transformation of C3H/10T1/2 cells following exposure to 120-Hz modulated 2.45-GHz microwaves and phorbol ester tumor promoter.

作者信息

Balcer-Kubiczek E K, Harrison G H

机构信息

University of Maryland School of Medicine, Department of Radiation Oncology, Baltimore 21201.

出版信息

Radiat Res. 1991 Apr;126(1):65-72.

PMID:2020740
Abstract

Some recent epidemiological studies have shown a positive association between cancer incidence and exposure to electromagnetic (EM) fields. Evidence from in vitro studies indicates that this effect could be due to synergistic interaction between EM fields and tumor promoters. However, no dose-response data related directly to carcinogenesis have been published. In this study, actively growing cultures of C3H/10T1/2 cells were exposed for 24 h to 2.45-GHz microwaves pulse-modulated at 120 Hz. Conditions of EM-field exposure were designed to simulate low-field exposures (specific absorption rate 0.1, 1, or 4.4 W/kg; the corresponding peak amplitudes were electric field 18, 56, or 120 V/m, magnetic field 0.09, 0.27, or 0.56 muT, respectively). In separate experiments, a 24-h EM-field exposure at 4.4 W/kg was preceded or followed by X irradiation at 0.5, 1, or 1.5 Gy. Cells were assayed for cell survival and neoplastic transformation with or without post-treatment administration of 0.1 micrograms/ml of 12-O-tetradecanoylphorbol-13-acetate (TPA) for the duration of the assay. The EM fields alone had no effect on cell survival or induction of neoplastic transformation. However, enhancement of transformation due to EM fields plus TPA was highly significant and ranged up to a level equivalent to that produced by 1.5 Gy of X rays. The frequency of neoplastic transformation was dependent on the level of EM exposure and was additive with doses of X rays given as a cocarcinogen.

摘要

近期一些流行病学研究表明,癌症发病率与接触电磁场(EM)之间存在正相关。体外研究证据表明,这种效应可能是由于电磁场与肿瘤启动子之间的协同相互作用。然而,尚未发表与致癌作用直接相关的剂量反应数据。在本研究中,将处于活跃生长状态的C3H/10T1/2细胞培养物暴露于频率为2.45 GHz、脉冲调制频率为120 Hz的微波中24小时。电磁场暴露条件设计为模拟低场暴露(比吸收率为0.1、1或4.4 W/kg;相应的峰值幅度分别为电场18、56或120 V/m,磁场0.09、0.27或0.56 μT)。在单独的实验中,在4.4 W/kg下进行24小时的电磁场暴露之前或之后,分别进行0.5、1或1.5 Gy的X射线照射。在检测期间,无论是否给予0.1微克/毫升的12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯(TPA)进行后处理,均对细胞存活和肿瘤转化进行检测。单独的电磁场对细胞存活或肿瘤转化诱导没有影响。然而,电磁场加TPA导致的转化增强非常显著,最高可达相当于1.5 Gy X射线产生的水平。肿瘤转化频率取决于电磁场暴露水平,并且与作为促癌剂给予的X射线剂量具有相加性。

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