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Estrogen receptor β activation is antinociceptive in a model of visceral pain in the rat

机译:雌激素受体β激活在大鼠内脏痛模型中具有镇痛作用

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The mechanism underlying estrogen modulation of visceral pain remains unclear. Our previous studies indicate that activation of estrogen receptor α (ERα) enhances visceral pain. The purpose of the present study was to investigate the role of estrogen receptor β (ER β) activation in spinal processing of visceral stimuli. The effects of selective ER β agonists on the visceromotor response (VMR) and dorsal horn neuronal responses to colorectal distention (CRD) were tested in ovariectomized and intact female rats. The magnitude of the VMR to CRD was significantly attenuated by ERβ agonists diarylpropionitrile (DPN) and WAY-200070 4 hours after subcutaneous injection. Pretreatment with the estrogen receptor antagonist ICI 182,780 obscured the DPN-evoked attenuation. There was no effect of DPN on the VMR at earlier time points. Subcutaneous and spinal administration of DPN attenuated the response of visceroceptive dorsal horn neurons with a comparable time course. DPN attenuated the VMR in intact rats regardless of estrous cycle stage. The time course of effect of ERβ activation on the visceromotor response and neuronal activity is consistent with transcriptional or translational modulation of neuronal activity. Perspective: Activation of ER β is antinociceptive in the colorectal distention model of visceral pain, which may provide a therapeutic target to manage irritable bowel syndrome in the clinic.
机译:雌激素调节内脏痛的机制尚不清楚。我们以前的研究表明,雌激素受体α(ERα)的激活会增加内脏疼痛。本研究的目的是研究雌激素受体β(ERβ)激活在内脏刺激的脊柱处理中的作用。在卵巢切除和完好无损的雌性大鼠中测试了选择性ERβ激动剂对内脏运动反应的内脏运动反应(VMR)和背角神经元反应(CRD)的影响。皮下注射4小时后,ERβ激动剂二芳基丙腈(DPN)和WAY-200070显着减弱了VMR对CRD的强度。用雌激素受体拮抗剂ICI 182,780进行的预处理可掩盖DPN引起的衰减。在更早的时间点,DPN对VMR没有影响。 DPN的皮下和脊髓给药可在相当的时间范围内减弱粘膜感受性背角神经元的反应。不论动情周期的阶段如何,DPN都会削弱完整大鼠的VMR。 ERβ激活对内脏运动反应和神经元活性的影响的时间过程与神经元活性的转录或翻译调节一致。观点:ERβ的激活在内脏疼痛的结肠直肠扩张模型中具有镇痛作用,这可能为临床治疗肠易激综合症提供治疗靶点。

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