微生物群在复杂局部疼痛综合征中的作用?

Q2 Medicine
Lara W. Crock , Megan T. Baldridge
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引用次数: 7

摘要

复杂区域疼痛综合征(CRPS)是一种病因不明的衰弱性神经炎性疾病。症状包括布达佩斯标准定义的极度疼痛和四肢营养变化。与大多数疼痛状况不同,CRPS的严重程度和功能恢复可以使用布达佩斯标准的一种变体进行量化,即CRPS严重程度评分。像许多慢性疼痛一样,一旦疼痛存在超过12个月,CRPS就很难治疗。然而,先前的研究表明,如果在一年内接受治疗,一小部分新发CRPS患者(约50%)的症状会得到改善,而其余患者的症状几乎没有改善。不幸的是,这会导致永久性残疾,通常需要侵入性和昂贵的治疗,如脊髓刺激或长期阿片类药物治疗。由于病因不明,治疗是多模式的,通常是支持性的。预测症状严重程度或消退的生物标志物将显著改变治疗方法,但尚未确定。有趣的是,有病例报告称,使用已知会影响肠道菌群的抗生素后,CRPS症状得到缓解或缓解。小鼠研究表明,在内脏、炎症和神经性疼痛模型中,肠道微生物组的调节具有抗伤害性。我们假设,CRPS患者的临床恢复潜力和对治疗的反应可能是继发于肠道菌群的变化或反映在肠道菌群的变化中。我们认为微生物群可能通过代谢组、免疫系统激活和/或小胶质细胞激活来调节或反映临床状态。我们假设肠道微生物群是CRPS症状发展和持续的潜在中介,并提出CRPS的临床状况可以为鉴定微生物群的生物标志物和预防疼痛慢性化的潜在治疗提供独特的机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A role for the microbiota in complex regional pain syndrome?

A role for the microbiota in complex regional pain syndrome?

A role for the microbiota in complex regional pain syndrome?

Complex regional pain syndrome (CRPS) is a debilitating neuroinflammatory condition of unknown etiology. Symptoms include excruciating pain and trophic changes in the limbs as defined by the Budapest criteria. The severity and functional recovery of CRPS, unlike most pain conditions, is quantifiable using a variation of the Budapest criteria known as the CRPS severity score. Like many chronic pain conditions, CRPS is difficult to treat once pain has been present for more than 12 months. However, previous work has demonstrated that a subset of patients with new-onset CRPS (~50%) improve if treated within one year, while the rest have minimal to no symptom improvement. Unfortunately, this leads to permanent disability and often requires invasive and costly treatments such as spinal cord stimulation or long-term opioid therapy. Because the etiology is unknown, treatment is multimodal, and often supportive. Biomarkers that predict severity or resolution of symptoms would significantly change treatment but have not yet been identified. Interestingly, there are case reports of remission or resolution of CRPS symptoms with the use of antibiotics known to affect the gut flora. Mouse studies have demonstrated that modulation of the gut microbiome is anti-nociceptive in visceral, inflammatory and neuropathic pain models. We hypothesize that the variable clinical potential for recovery and response to therapy in CRPS may be secondary to or reflected in changes in the gut microbiota. We suggest that the microbiota may mediate or reflect clinical status via the metabolome, activation of the immune system and/or microglial activation. We hypothesize that the gut microbiome is a potential mediator in development and persistence of CRPS symptoms and propose that the clinical condition of CRPS could provide a unique opportunity to identify biomarkers of the microbiota and potential therapies to prevent pain chronification.

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来源期刊
Neurobiology of Pain
Neurobiology of Pain Medicine-Anesthesiology and Pain Medicine
CiteScore
4.40
自引率
0.00%
发文量
29
审稿时长
54 days
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