Inflammatory and oxidative and nitrosative stress cascades as new drug targets in myalgic encephalomyelitis and chronic fatigue syndrome.

Modern trends in pharmacopsychiatry Pub Date : 2013-01-01 Epub Date: 2013-02-27 DOI:10.1159/000343982
Michael Maes
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引用次数: 19

Abstract

Myalgic encephalomyelitis (ME), chronic fatigue syndrome (CFS) and chronic fatigue (CF) are distinct diagnostic categories with regard to clinical symptoms, severity of illness and biomarkers. Patients with ME and CFS show higher scores on fatigue, neurocognitive disorders, hyperalgesia, autonomic symptoms, postexertional malaise and a subjective feeling of infection than patients with CF. ME is characterized by increased postexertional malaise, a subjective feeling of infection and neurocognitive disorders and is a more severe variant than CFS. Fukuda's 1994 CDC criteria are adequate to make a distinction between patients with ME/CFS and CF, while ME/CFS patients should be subdivided into those with and without postexertional malaise into ME and CFS, respectively. Different interrelated pathophysiological mechanisms play a role in ME/CFS, i.e. (1) inflammation and immune activation, (2) oxidative and nitrosative stress and lowered antioxidant defenses, (3) activation of cell signaling networks, e.g. nuclear factor ĸβ, the 2 9 ,5 9 -oligoadenylate/RNase-L and/or protein kinase R pathway, (4) a transition towards autoimmune reactions, and (5) bacterial translocation. The inflammatory biomarkers are higher in ME/CFS than in CF and higher in ME than in CFS. The above-mentioned pathways may explain the onset of characteristic ME/CFS symptoms, such as fatigue, malaise, autonomic symptoms, hyperalgesia, and neurocognitive symptoms. Different etiological factors may trigger ME/CFS/CF, e.g. viral and bacterial infections, and (auto)immune and inflammatory disorders, while psychosocial and physical stressors act as modulating factors. New pathophysiologically driven drug candidates for ME and CFS are discussed which target the pathways that play a role in ME/CFS.

炎症和氧化和亚硝化应激级联反应作为肌痛性脑脊髓炎和慢性疲劳综合征的新药物靶点。
肌痛性脑脊髓炎(ME)、慢性疲劳综合征(CFS)和慢性疲劳(CF)在临床症状、疾病严重程度和生物标志物方面是不同的诊断类别。与CF患者相比,ME和CFS患者在疲劳、神经认知障碍、痛觉过敏、自主神经症状、运动后不适和主观感染感觉方面得分更高。ME的特征是运动后不适、主观感染感觉和神经认知障碍增加,是比CFS更严重的变体。Fukuda 1994年的CDC标准足以区分ME/CFS和CF,而ME/CFS患者应细分为有和无运动后不适的ME和CFS。不同的相关病理生理机制在ME/CFS中发挥作用,即(1)炎症和免疫激活,(2)氧化和亚硝化应激和抗氧化防御降低,(3)细胞信号网络的激活,例如核因子ĸβ, 2,9,5,9 -寡腺苷酸/RNase-L和/或蛋白激酶R途径,(4)向自身免疫反应的过渡,以及(5)细菌易位。炎症生物标志物在ME/CFS中高于CF,在ME中高于CFS。上述途径可以解释ME/CFS特征性症状的发生,如疲劳、不适、自主神经症状、痛觉过敏和神经认知症状。不同的病因可能引发ME/CFS/CF,例如病毒和细菌感染,以及(自身)免疫和炎症性疾病,而社会心理和身体压力因素是调节因素。讨论了针对ME/CFS中起作用的途径的新的病理生理驱动的ME和CFS候选药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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