Department of Integrative Biosciences, Oregon Health & Science University School of Dentistry, Portland, OR 97239, USA.
Neuroscience. 2010 Jun 2;167(4):1205-15. doi: 10.1016/j.neuroscience.2010.03.002. Epub 2010 Mar 9.
Nociceptive pathways with first-order neurons located in the trigeminal ganglion (TG) provide sensory innervation to the head, and are responsible for a number of common chronic pain conditions, including migraines, temporomandibular disorders and trigeminal neuralgias. Many of those conditions are associated with inflammation. Yet, the mechanisms of chronic inflammatory pain remain poorly understood. Our previous studies show that the neurotrophin brain-derived neurotrophic factor (BDNF) is expressed by adult rat TG neurons, and released from cultured newborn rat TG neurons by electrical stimulation and calcitonin gene-related peptide (CGRP), a well-established mediator of trigeminal inflammatory pain. These data suggest that BDNF plays a role in activity-dependent plasticity at first-order trigeminal synapses, including functional changes that take place in trigeminal nociceptive pathways during chronic inflammation. The present study was designed to determine the effects of peripheral inflammation, using tooth pulp inflammation as a model, on regulation of BDNF expression in TG neurons of juvenile rats and mice. Cavities were prepared in right-side maxillary first and second molars of 4-week-old animals, and left open to oral microflora. BDNF expression in right TG was compared with contralateral TG of the same animal, and with right TG of sham-operated controls, 7 and 28 days after cavity preparation. Our ELISA data indicate that exposing the tooth pulp for 28 days, with confirmed inflammation, leads to a significant upregulation of BDNF in the TG ipsilateral to the affected teeth. Double-immunohistochemistry with antibodies against BDNF combined with one of nociceptor markers, CGRP or transient receptor potential vanilloid type 1 (TRPV1), revealed that BDNF is significantly upregulated in TRPV1-immunoreactive (IR) neurons in both rats and mice, and CGRP-IR neurons in mice, but not rats. Overall, the inflammation-induced upregulation of BDNF is stronger in mice compared to rats. Thus, mouse TG provides a suitable model to study molecular mechanisms of inflammation-dependent regulation of BDNF expression in vivo.
伤害感受通路的一级神经元位于三叉神经节(TG),为头部提供感觉神经支配,并负责多种常见的慢性疼痛病症,包括偏头痛、颞下颌关节紊乱和三叉神经痛。许多这些病症都与炎症有关。然而,慢性炎症性疼痛的机制仍知之甚少。我们之前的研究表明,神经营养因子脑源性神经营养因子(BDNF)在成年大鼠 TG 神经元中表达,并可由电刺激和降钙素基因相关肽(CGRP)从培养的新生大鼠 TG 神经元中释放,CGRP 是三叉神经炎症性疼痛的一个公认的介质。这些数据表明,BDNF 在一级三叉神经突触的活动依赖性可塑性中发挥作用,包括在慢性炎症期间三叉神经伤害感受通路中发生的功能变化。本研究旨在确定外周炎症(以牙髓炎症为模型)对幼年大鼠和小鼠 TG 神经元中 BDNF 表达的调节作用。在 4 周龄动物的右侧上颌第一和第二磨牙上制备腔,并使其向口腔微生物开放。在牙髓暴露 28 天后,将右侧 TG 与同一动物的对侧 TG 以及假手术对照的右侧 TG 进行比较。我们的 ELISA 数据表明,将牙髓暴露 28 天并确认有炎症,会导致同侧 TG 中 BDNF 的显著上调。用针对 BDNF 的抗体与一种伤害感受器标记物(CGRP 或瞬时受体电位香草酸 1(TRPV1))的双重免疫组织化学显示,BDNF 在大鼠和小鼠的 TRPV1-免疫反应(IR)神经元中以及小鼠的 CGRP-IR 神经元中均显著上调,但在大鼠中没有。总的来说,与大鼠相比,炎症诱导的 BDNF 上调在小鼠中更强。因此,小鼠 TG 提供了一个合适的模型,可用于研究体内炎症依赖性 BDNF 表达调节的分子机制。
