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肌痛性脑脊髓炎/慢性疲劳综合征(ME/CFS)的进展:ME/CFS的自然病史。

How Myalgic Encephalomyelitis/Chronic Fatigue Syndrome (ME/CFS) Progresses: The Natural History of ME/CFS.

作者信息

Nacul Luis, O'Boyle Shennae, Palla Luigi, Nacul Flavio E, Mudie Kathleen, Kingdon Caroline C, Cliff Jacqueline M, Clark Taane G, Dockrell Hazel M, Lacerda Eliana M

机构信息

Department of Clinical Research, Faculty of Infectious and Tropical Diseases, London School of Hygiene & Tropical Medicine, London, United Kingdom.

B.C. Women's Hospital and Health Centre, Vancouver, BC, Canada.

出版信息

Front Neurol. 2020 Aug 11;11:826. doi: 10.3389/fneur.2020.00826. eCollection 2020.

Abstract

We propose a framework for understanding and interpreting the pathophysiology of Myalgic Encephalomyelitis/Chronic Fatigue Syndrome (ME/CFS) that considers wider determinants of health and long-term temporal variation in pathophysiological features and disease phenotype throughout the natural history of the disease. As in other chronic diseases, ME/CFS evolves through different stages, from asymptomatic predisposition, progressing to a prodromal stage, and then to symptomatic disease. Disease incidence depends on genetic makeup and environment factors, the exposure to singular or repeated insults, and the nature of the host response. In people who develop ME/CFS, normal homeostatic processes in response to adverse insults may be replaced by aberrant responses leading to dysfunctional states. Thus, the predominantly neuro-immune manifestations, underlined by a hyper-metabolic state, that characterize early disease, may be followed by various processes leading to multi-systemic abnormalities and related symptoms. This abnormal state and the effects of a range of mediators such as products of oxidative and nitrosamine stress, may lead to progressive cell and metabolic dysfunction culminating in a hypometabolic state with low energy production. These processes do not seem to happen uniformly; although a spiraling of progressive inter-related and self-sustaining abnormalities may ensue, reversion to states of milder abnormalities is possible if the host is able to restate responses to improve homeostatic equilibrium. With time variation in disease presentation, no single ME/CFS case description, set of diagnostic criteria, or molecular feature is currently representative of all patients at different disease stages. While acknowledging its limitations due to the incomplete research evidence, we suggest the proposed framework may support future research design and health care interventions for people with ME/CFS.

摘要

我们提出了一个用于理解和解释肌痛性脑脊髓炎/慢性疲劳综合征(ME/CFS)病理生理学的框架,该框架考虑了更广泛的健康决定因素以及疾病自然史中病理生理特征和疾病表型的长期时间变化。与其他慢性疾病一样,ME/CFS会经历不同阶段,从无症状易感性,发展到前驱期,然后到有症状疾病。疾病发病率取决于基因构成和环境因素、单次或反复受到的损伤以及宿主反应的性质。在患ME/CFS的人群中,应对不良损伤的正常稳态过程可能会被导致功能失调状态的异常反应所取代。因此,以高代谢状态为突出特征的早期疾病的主要神经免疫表现,可能会随后出现导致多系统异常及相关症状的各种过程。这种异常状态以及一系列介质(如氧化应激和亚硝胺应激产物)的作用,可能导致细胞和代谢功能逐渐失调,最终导致能量产生低下的低代谢状态。这些过程似乎并非均匀发生;尽管可能会出现一系列相互关联且自我维持的异常情况不断升级,但如果宿主能够重新调整反应以改善稳态平衡,也有可能恢复到异常较轻的状态。随着疾病表现随时间变化,目前没有单一的ME/CFS病例描述、诊断标准集或分子特征能够代表所有处于不同疾病阶段的患者。在认识到由于研究证据不完整而存在的局限性的同时,我们建议所提出的框架可能会为ME/CFS患者的未来研究设计和医疗保健干预提供支持。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd39/7431524/3582b015b82b/fneur-11-00826-g0001.jpg

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