Contribution of Sympathetic Sensory Coupling to Craniofacial Nociception.

IF 1.7 3区 医学 Q2 DENTISTRY, ORAL SURGERY & MEDICINE
Brian Edwin Cairns
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Abstract

Stress and anxiety are associated with increased pain intensity in temporomandibular disorders (TMDs) patients. It is possible that this association is due to a direct interaction between the sympathetic and sensory nervous systems. This narrative review examines evidence for a potential sympathetic sensory interaction in deep craniofacial tissues and the trigeminal ganglion. Research articles were identified using PubMed with the mesh terms adrenergic, ganglion neuron, masseter, sensory, signaling, temporomandibular and trigeminal and, subsequently, from the reference lists of those articles identified. The masticatory muscles and temporomandibular joint are innervated by sympathetic efferent fibres from the superior cervical ganglion, which primarily innervates blood vessels. As trigeminal sensory afferent fibres are often found near blood vessels, the anatomical relationship for potential sympathetic sensory coupling is present in the temporomandibular joint and masticatory muscles. Trigeminal afferent fibres express α1, α2, β1 and β2 adrenergic receptors as well as two of the four neuropeptide Y receptors. Stimulation of α1 receptors in the masticatory muscle mechanically sensitises nociceptors through a direct effect, but desensitises proprioceptors and spindle afferent fibres through an indirect effect on mechanosensitive organelles. Stimulation of β2 adrenergic receptors increases the mechanical activation threshold of masticatory muscle afferent fibres. There is also evidence that stimulation of β adrenergic receptors on immune cells contributes to nociception in temporomandibular joint arthritis. In contrast, α1 adrenergic receptor activation underlies nociception in masticatory muscle myositis. Taken together, the current research provides support for the concept that sympathetic sensory coupling could play a role in the pathogenesis of TMD-related pain.

交感感觉耦合对颅面伤害感觉的贡献。
压力和焦虑与颞下颌疾病(TMDs)患者疼痛强度增加有关。这种联系可能是由于交感神经系统和感觉神经系统之间的直接相互作用。这篇叙述性的综述探讨了深层颅面组织和三叉神经节中潜在的交感感觉相互作用的证据。研究文章通过PubMed的网格术语肾上腺素能、神经节神经元、咬肌、感觉、信号、颞下颌和三叉神经进行识别,随后从这些文章的参考文献列表中进行识别。咀嚼肌和颞下颌关节受颈上神经节的交感神经传出纤维支配,颈上神经节主要支配血管。由于三叉神经感觉传入纤维经常在血管附近发现,潜在的交感感觉耦合的解剖关系存在于颞下颌关节和咀嚼肌中。三叉神经传入纤维表达α1、α2、β1和β2肾上腺素能受体以及四种神经肽Y受体中的两种。刺激咀嚼肌α1受体通过直接作用使痛觉感受器机械致敏,但通过间接作用于机械敏感细胞器使本体感受器和纺锤体传入纤维脱敏。刺激β2肾上腺素能受体增加咀嚼肌传入纤维的机械激活阈值。也有证据表明,刺激免疫细胞上的β肾上腺素能受体有助于颞下颌关节关节炎的伤害感受。相反,α1肾上腺素能受体的激活是咀嚼肌肌炎中伤害感觉的基础。综上所述,目前的研究为交感感觉耦合可能在tmd相关疼痛发病机制中发挥作用的概念提供了支持。
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来源期刊
Orthodontics & Craniofacial Research
Orthodontics & Craniofacial Research 医学-牙科与口腔外科
CiteScore
5.30
自引率
3.20%
发文量
65
审稿时长
>12 weeks
期刊介绍: Orthodontics & Craniofacial Research - Genes, Growth and Development is published to serve its readers as an international forum for the presentation and critical discussion of issues pertinent to the advancement of the specialty of orthodontics and the evidence-based knowledge of craniofacial growth and development. This forum is based on scientifically supported information, but also includes minority and conflicting opinions. The objective of the journal is to facilitate effective communication between the research community and practicing clinicians. Original papers of high scientific quality that report the findings of clinical trials, clinical epidemiology, and novel therapeutic or diagnostic approaches are appropriate submissions. Similarly, we welcome papers in genetics, developmental biology, syndromology, surgery, speech and hearing, and other biomedical disciplines related to clinical orthodontics and normal and abnormal craniofacial growth and development. In addition to original and basic research, the journal publishes concise reviews, case reports of substantial value, invited essays, letters, and announcements. The journal is published quarterly. The review of submitted papers will be coordinated by the editor and members of the editorial board. It is policy to review manuscripts within 3 to 4 weeks of receipt and to publish within 3 to 6 months of acceptance.
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