Posttraumatic hyperalgesia and associated peripheral sensitization after temporomandibular joint injury in mice

伤害感受器 颞下颌关节 敏化 灼口综合征 医学 疼痛 痛觉过敏 痛觉超敏 三叉神经节 伤害 降钙素基因相关肽 麻醉 内科学 神经科学 病理 心理学 神经肽 受体 免疫学 外科 感觉系统
作者
Ishraq Alshanqiti,Hyeonwi Son,John Shannonhouse,Jiaxin Hu,Sinu Kumari,Ghazaal Parastooei,Swarnalakshmi Raman,Sheng Wang,Jin Y. Ro,Yu Shin Kim,Man‐Kyo Chung
出处
期刊:Pain [Lippincott Williams & Wilkins]
标识
DOI:10.1097/j.pain.0000000000003498
摘要

Abstract Temporomandibular disorder (TMD) is the most prevalent painful condition in the craniofacial area. Recent studies have suggested that external or intrinsic trauma to the temporomandibular joint (TMJ) is associated with the onset of painful TMD in patients. Here, we investigated the effects of TMJ trauma through forced-mouth opening (FMO) in mice to determine pain behaviors and peripheral sensitization of trigeminal nociceptors in both sexes. Forced-mouth opening increased mechanical pain as assessed by the von Frey test, with spontaneous pain-like behaviors assessed using the mouse grimace scale and anxiety-like behaviors assessed using the open-field test. Changes in pain-like behaviors were not different between male and female mice. However, in vivo GCaMP Ca 2+ imaging of intact trigeminal ganglia (TG) showed modality- and sex-dependent changes. Forced-mouth opening increased spontaneous Ca 2+ responses and mechanical hypersensitivity of TG neurons compared to the sham group, which was more pronounced in male mice. Forced-mouth opening also increased Ca 2+ responses evoked by cold, heat, and capsaicin stimuli, which was not different between the sexes. In retrogradely labeled trigeminal TMJ afferents, FMO induced an increase in small-sized neuronal proportions with increased colocalization with calcitonin gene–related peptides and transient receptor potential vanilloid subtype 1, which was modestly sex dependent. These results suggest that TMJ injury leads to persistent posttraumatic hyperalgesia associated with peripheral sensitization of trigeminal nociceptors with distinct sex dependency.
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