EXPRESSION OF SEROTONIN RECEPTOR SUBTYPE 3A (5HT3A) ON RAT TRIGEMINAL SENSORY NEURONS.

Texas journal of microscopy Pub Date : 2021-01-01
Sukhbir Kaur, Angela Lopez-Ramirez, Taylor M Hickman, Michael P Hunter, Dayna L Averitt
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Abstract

Serotonin (5-hydroxytryptamine, 5HT) is a neurotransmitter and proinflammatory mediator found largely in the peripheral nervous system where it can initiate pain signaling. 5HT binds a variety of 5HT receptors on sensory nerve endings specialized in detecting noxious stimuli, termed nociceptors. A subset of sensory neurons involved in pain signaling express the transient receptor potential vanilloid 1 ion channel (TRPV1), a pain generator. 5HT can both directly activate sensory neurons and sensitize TRPV1 leading to enhanced nociceptor sensitivity (peripheral sensitization). Previous studies in male rats reported that the 5HT receptor subtype 3A (5HT3A) and TRPV1 are co-expressed on sensory neurons, but it is unknown if 5HT3A and TRPV1 are co-expressed on female sensory neurons. Given that craniofacial pain disorders occur at a 2-3x greater prevalence in women, examining pain mechanisms in female trigeminal sensory neurons that innervate the craniofacial region is critical to advancing craniofacial pain management in women. Here we examined whether (1) 5HT acting via the 5HT3A receptor produces sexually dimorphic orofacial pain behaviors in rats and (2) whether 5HT3A receptor mRNA is expressed in trigeminal sensory neurons, including the TRPV1-expressing subpopulation, and increase pain signaling. We report that 5HT evokes pain behaviors in male and female rats, which was not significantly reduced by antagonism of 5HT3A. We performed in situ hybridization to label 5HT3A and TRPV1 mRNA in trigeminal sensory neurons and found distinct cell populations with either 5HT3A mRNA or TRPV1 mRNA in males and females. Further, 5HT3A antagonism failed to reduce pain signaling in cultured trigeminal sensory neurons. These data suggest that the 5HT3A subtype on trigeminal sensory neurons innervating the orofacial soft tissues does not play a significant role in sexually dimorphic craniofacial pain disorders. As previous studies have reported that granisetron reduces masseter muscle pain, 5HT3 may play a role in sex differences in myofascial pain disorders but not in other craniofacial pain disorders.

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大鼠三叉神经感觉神经元上 5-羟色胺受体 3a 亚型(5ht3a)的表达。
羟色胺(5-羟色胺,5HT)是一种神经递质和促炎介质,主要存在于外周神经系统,它可以启动疼痛信号。5HT 与专门检测有害刺激的感觉神经末梢(称为痛觉感受器)上的各种 5HT 受体结合。参与疼痛信号传递的感觉神经元中有一部分表达瞬时受体电位类香草素 1 离子通道(TRPV1),这是一种疼痛发生器。5HT 既能直接激活感觉神经元,又能使 TRPV1 敏感,从而增强痛觉感受器的敏感性(外周敏感化)。之前对雄性大鼠的研究报告称,5HT 受体亚型 3A(5HT3A)和 TRPV1 在感觉神经元上共同表达,但 5HT3A 和 TRPV1 是否在雌性感觉神经元上共同表达尚不清楚。鉴于颅面疼痛疾病在女性中的发病率比男性高出 2-3 倍,研究支配颅面区域的女性三叉神经感觉神经元的疼痛机制对于促进女性颅面疼痛的治疗至关重要。在这里,我们研究了(1)5HT 是否通过 5HT3A 受体作用于大鼠,从而产生性双态的口面部疼痛行为;(2)5HT3A 受体 mRNA 是否在三叉神经感觉神经元(包括表达 TRPV1 的亚群)中表达,并增加疼痛信号传导。我们报告说,5HT 会诱发雄性和雌性大鼠的疼痛行为,而 5HT3A 拮抗剂并不会显著减少这种行为。我们对三叉神经感觉神经元中的 5HT3A 和 TRPV1 mRNA 进行了原位杂交标记,发现雌雄大鼠中含有 5HT3A mRNA 或 TRPV1 mRNA 的细胞群截然不同。此外,5HT3A 拮抗剂未能减少培养的三叉神经感觉神经元的疼痛信号传导。这些数据表明,支配口面部软组织的三叉神经感觉神经元上的 5HT3A 亚型在颅面部疼痛疾病的性别双态性中并不扮演重要角色。由于之前的研究报道格拉司琼可减轻颌间肌疼痛,因此 5HT3 可能在肌筋膜疼痛疾病的性别差异中发挥作用,但在其他颅面疼痛疾病中则没有作用。
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EXPRESSION OF SEROTONIN RECEPTOR SUBTYPE 3A (5HT3A) ON RAT TRIGEMINAL SENSORY NEURONS.
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