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A clinically relevant animal model of temporomandibular disorder and irritable bowel syndrome comorbidity

机译:颞下颌疾病和肠易激综合征合并症的临床相关动物模型

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Temporomandibular disorder and irritable bowel syndrome are comorbid functional chronic pain disorders of unknown etiology that are triggered/exacerbated by stress. Here we present baseline phenotypic characterization of a novel animal model to gain insight into the underlying mechanisms that contribute to such comorbid pain conditions. In this model, chronic visceral hypersensitivity, a defining symptom of irritable bowel syndrome, is dependent on 3 factors: estradiol, existing chronic somatic pain, and stress. In ovariectomized rats, estradiol replacement followed by craniofacial muscle injury and stress induced visceral hypersensitivity that persisted for months. Omission of any 1 factor resulted in a transient (1 week) visceral hypersensitivity from stress alone or no hypersensitivity (no inflammation or estradiol). Maintenance of visceral hypersensitivity was estradiol dependent, resolving when estradiol replacement ceased. Referred cutaneous hypersensitivity was concurrent with visceral hypersensitivity. Increased spinal Fos expression suggests induction of central sensitization. These data demonstrate the development and maintenance of visceral hypersensitivity in estradiol-replaced animals following distal somatic injury and stress that mimics some characteristics reported in patients with temporomandibular disorder and comorbid irritable bowel syndrome. This new animal model is a powerful experimental tool that can be employed to gain further mechanistic insight into overlapping pain conditions. Perspective The majority of patients with temporomandibular disorder report symptoms consistent with irritable bowel syndrome. Stress and female prevalence are common to both conditions. In a new experimental paradigm in ovariectomized rats with estradiol replacement, masseter inflammation followed by stress induces visceral hypersensitivity that persists for months, modeling these comorbid pain conditions.
机译:颞下颌疾病和肠易激综合症是病因不明的并存的功能性慢性疼痛疾病,由压力触发/加重。在这里,我们介绍一种新型动物模型的基线表型特征,以深入了解导致这种共病疼痛状况的潜在机制。在该模型中,慢性内脏超敏反应是肠易激综合征的定义性症状,它取决于3个因素:雌二醇,现有的慢性躯体疼痛和压力。在去卵巢的大鼠中,雌二醇替代继之以颅面肌损伤和压力引起的内脏超敏反应持续了数月之久。忽略任何1个因素,仅会因压力导致短暂的内脏超敏反应(1周),或没有超敏反应(无炎症或雌二醇)。内脏超敏性的维持依赖于雌二醇,当雌二醇替代停止时,该症状得以解决。皮肤过敏反应与内脏过敏反应同时发生。脊髓Fos表达增加表明诱导中枢敏化。这些数据证明了远端躯体损伤和应激后雌二醇替代动物内脏超敏反应的发展和维持,这些现象模仿了颞下颌疾病和合并性肠易激综合征患者的某些特征。这种新的动物模型是一种功能强大的实验工具,可用于获得对重叠疼痛状况的进一步机械观察。观点大多数颞下颌疾病患者报告的症状与肠易激综合征相符。压力和女性患病率在这两种情况下都很常见。在用雌二醇替代去卵巢的大鼠中的新实验范式中,咬肌炎继之以压力引起内脏超敏反应,这种反应持续数月,模拟了这些合并症。

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