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首页> 外文期刊>Reviews on environmental health >Reliable disease biomarkers characterizing and identifying electrohypersensitivity and multiple chemical sensitivity as two etiopathogenic aspects of a unique pathological disorder
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Reliable disease biomarkers characterizing and identifying electrohypersensitivity and multiple chemical sensitivity as two etiopathogenic aspects of a unique pathological disorder

机译:可靠的疾病生物标记物,可表征和鉴定电超敏性和多种化学敏感性,这是独特病理性疾病的两个病因

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Much of the controversy over the causes of electrohypersensitivity (EHS) and multiple chemical sensitivity (MCS) lies in the absence of both recognized clinical criteria and objective biomarkers for widely accepted diagnosis. Since 2009, we have prospectively investigated, clinically and biologically, 1216 consecutive EHS and/or MCS-self reporting cases, in an attempt to answer both questions. We report here our preliminary data, based on 727 evaluable of 839 enrolled cases: 521 (71.6%) were diagnosed with EHS, 52 (7.2%) with MCS, and 154 (21.2%) with both EHS and MCS. Two out of three patients with EHS and/or MCS were female; mean age (years) was 47. As inflammation appears to be a key process resulting from electromagnetic field (EMF) and/ or chemical effects on tissues, and histamine release is potentially a major mediator of inflammation, we systematically measured histamine in the blood of patients. Near 40% had a increase in histaminemia (especially when both conditions were present), indicating a chronic inflammatory response can be detected in these patients. Oxidative stress is part of inflammation and is a key contributor to damage and response. Nitrotyrosin, a marker of both peroxynitrite (0N00°-) production and opening of the blood-brain barrier (BBB), was increased in 28% the cases. Protein S100B, another marker of BBB opening was increased in 15%. Circulating autoantibodies against O-myelin were detected in 23%, indicating EHS and MCS may be associated with autoimmune response. Confirming animal experiments showing the increase of Hsp27 and/or Hsp70 chaperone proteins under the influence of EMF, we found increased Hsp27 and/or Hsp70 in 33% of the patients. As most patients reported chronic insomnia and fatigue, we determined the 24 h urine 6-hydroxymelatonin sulfate (6-OHMS)/creatinin ratio and found it was decreased (<0.8) in all investigated cases. Finally, considering the self-reported symptoms of EHS and MCS, we serially measured the brain blood flow (BBF) in the temporal lobes of each case with pulsed cerebral ultrasound computed tomosphygmography. Both disorders were associated with hypoperfusion in the cap-sulothalamic area, suggesting that the inflammatory process involve the limbic system and the thalamus. Our data strongly suggest that EHS and MCS can be objectively characterized and routinely diagnosed by commercially available simple tests. Both disorders appear to involve inflammation-related hyper-histaminemia, oxidative stress, autoimmune response, capsulothalamic hypoperfusion and BBB opening, and a deficit in melatonin metabolic availability; suggesting a risk of chronic neurodegenerative disease. Finally the common co-occurrence of EHS and MCS strongly suggests a common pathological mechanism.
机译:关于电超敏性(EHS)和多种化学敏感性(MCS)的原因的许多争议在于缺乏公认的临床标准和客观的生物标记物来进行广泛接受的诊断。自2009年以来,我们已在临床和生物学上对1216例连续的EHS和/或MCS自我报告病例进行了前瞻性调查,以试图回答这两个问题。我们在此报告我们的初步数据,基于839例登记病例中的727例可评估:EHS诊断为521(71.6%),MCS诊断为52(7.2%),EHS和MCS分别诊断为154(21.2%)。三分之二的EHS和/或MCS患者为女性;平均年龄为47岁。由于炎症似乎是电磁场(EMF)和/或对组织的化学作用所致的关键过程,而组胺的释放可能是炎症的主要介质,因此我们系统地测量了血液中的组胺耐心。近40%的患者组织蛋白血症增加(尤其是在同时存在两种情况时),表明在这些患者中可以检测到慢性炎症反应。氧化应激是炎症的一部分,是造成损伤和反应的关键因素。硝基酪氨酸是过氧亚硝酸盐(0N00°-)产生和血脑屏障(BBB)打开的标志,在28%的病例中增加。蛋白质S100B是BBB开放的另一个标志物,增加了15%。在23%的患者中检测到了针对O-髓磷脂的循环自身抗体,表明EHS和MCS可能与自身免疫反应有关。证实动物实验显示在EMF的作用下Hsp27和/或Hsp70伴侣蛋白的增加,我们发现33%的患者Hsp27和/或Hsp70的增加。由于大多数患者报告有慢性失眠和疲劳,因此我们确定了24小时尿液中6-羟褪黑激素硫酸盐(6-OHMS)/肌酐的比率,发现在所有调查病例中尿酸6-羟基褪黑素/肌酐的比率均下降(<0.8)。最后,考虑到EHS和MCS的自我报告症状,我们使用脉冲脑超声X线断层扫描技术连续测量了每种情况下颞叶的脑血流量(BBF)。两种疾病都与帽-后-丘脑区的灌注不足有关,表明炎症过程涉及边缘系统和丘脑。我们的数据强烈表明,EHS和MCS可以通过市售简单测试进行客观表征和常规诊断。两种疾病似乎都涉及炎症相关的高组胺血症,氧化应激,自身免疫反应,囊膜肺灌注不足和血脑屏障开放以及褪黑素代谢的可用性不足。提示有慢性神经退行性疾病的风险。最后,EHS和MCS的共同共存强烈暗示了共同的病理机制。

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