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Postulated Vasoactive Neuropeptide Autoimmunity in Fatigue-Related Conditions: A Brief Review and Hypothesis

机译:疲劳相关条件下的假定血管活性神经肽自身免疫:简要回顾和假设。

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摘要

Disorders such as chronic fatigue syndrome (CFS) and gulf war syndrome (GWS) are characterised by prolonged fatigue and a range of debilitating symptoms of pain, intellectual and emotional impairment, chemical sensitivities and immunological dysfunction. Sudden infant death syndrome (SIDS) surprisingly may have certain features in common with these conditions. Post-infection sequelae may be possible contributing factors although ongoing infection is unproven. Immunological aberration may prove to be associated with certain vasoactive neuropeptides (VN) in the context of molecular mimicry, inappropriate immunological memory and autoimmunity.Adenylate cyclase-activating VNs including pituitary adenylate cyclase-activating polypeptide (PACAP), vasoactive intestinal peptide (VIP) and calcitonin gene-related peptide (CGRP) act as hormones, neurotransmitters, neuroregulators, immune modulators and neurotrophic substances. They and their receptors are potentially immunogenic. VNs are widely distributed in the body particularly in the central and peripheral nervous systems and have been identified in the gut, adrenal gland, blood cells, reproductive system, lung, heart and other tissues. They have a vital role in maintaining cardio-respiratory function, thermoregulation, memory, concentration and executive functions such as emotional responses including social cues and appropriate behaviour. They are co-transmitters for a number of neurotransmitters including acetylcholine and gaseous transmitters, are potent immune regulators with primarily anti-inflammatory activity, and have a significant role in protection of the nervous system against toxic assault as well as being important in the maintenance of homeostasis.This paper describes a biologically plausible mechanism for the development of certain fatigue-related syndromes based on loss of immunological tolerance to these VNs or their receptors following infection, other events or de novo resulting in significant pathophysiology possibly mediated via CpG fragments and heat shock (stress) proteins. These conditions extend the public health context of autoimmunity and VN dysregulation and have implications for military medicine where radiological, biological and chemical agents may have a role in pathogenesis. Possible treatment and prevention options are considered.
机译:诸如慢性疲劳综合症(CFS)和海湾战争综合症(GWS)的疾病的特征是长时间的疲劳和一系列令人衰弱的疼痛,智力和情感障碍,化学敏感性和免疫功能障碍。令人惊讶的婴儿猝死综合症(SIDS)可能具有与这些疾病相同的某些特征。感染后后遗症可能是可能的促成因素,尽管持续的感染尚未得到证实。在分子模拟,不适当的免疫记忆和自身免疫的情况下,免疫畸变可能与某些血管活性神经肽(VN)有关。腺苷酸环化酶激活的VN包括垂体腺苷酸环化酶激活多肽(PACAP),血管活性肠肽(VIP)和降钙素基因相关肽(CGRP)充当激素,神经递质,神经调节剂,免疫调节剂和神经营养物质。它们及其受体具有潜在的免疫原性。 VNs广泛分布在体内,特别是在中枢和周围神经系统中,并且已在肠道,肾上腺,血细胞,生殖系统,肺,心脏和其他组织中发现。它们在维持心脏呼吸功能,体温调节,记忆,注意力和执行功能(例如包括社交线索和适当行为的情绪反应)方面具有至关重要的作用。它们是许多神经递质的共递质,包括乙酰胆碱和气态递质,是有效的免疫调节剂,主要具有抗炎活性,并且在保护神经系统免受毒性侵害中起着重要作用,并且在维持神经系统中起重要作用。本文根据感染,其他事件或从头导致对这些VN或其受体的免疫耐受性丧失,导致可能由CpG片段和热休克介导的重要病理生理学,描述了某些疲劳相关综合征发展的生物学上合理的机制。 (应激)蛋白。这些疾病扩大了自身免疫和VN失调的公共卫生环境,并对军事医学产生了影响,因为放射,生物和化学试剂可能在发病机理中起作用。考虑可能的治疗和预防方案。

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