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通过激活脊髓大麻素受体1减轻骨癌疼痛及其在骨癌疼痛小鼠模型脊髓背角浅层的表达

Reduction of bone cancer pain by activation of spinal cannabinoid receptor 1 and its expression in the superficial dorsal horn of the spinal cord in a murine model of bone cancer pain.

作者信息

Furuse Shingo, Kawamata Tomoyuki, Yamamoto Jun, Niiyama Yukitoshi, Omote Keiichi, Watanabe Masahiko, Namiki Akiyoshi

机构信息

Department of Anesthesiology, Sapporo Medical University School of Medicine, Sapporo, Hokkaido, Japan.

出版信息

Anesthesiology. 2009 Jul;111(1):173-86. doi: 10.1097/ALN.0b013e3181a51e0d.

Abstract

BACKGROUND

Bone cancer pain has a strong impact on the quality of life of patients, but it is difficult to treat. Therefore, development of a novel strategy for the treatment of bone cancer pain is needed for improvement of patient quality of life. This study examined whether selective spinal cannabinoid receptor 1 (CB1) activation alleviates bone cancer pain and also examined the spinal expression of CB1.

METHODS

A bone cancer pain model was made by implantation of sarcoma cells into the intramedullary space of the mouse femur. In behavioral experiments, the authors examined the effects of activation of spinal CB1 and inhibition of metabolism of endocannabinoid on bone cancer-related pain behaviors. Immunohistochemical experiments examined the distribution and localization of CB1 in the superficial dorsal horn of the spinal cord using specific antibodies.

RESULTS

Spinal CB1 activation by exogenous administration of a CB1 agonist arachidonyl-2-chloroethylamide reduced bone cancer-related pain behaviors, including behaviors related to spontaneous pain and movement-evoked pain. In immunohistochemical experiments, although mu-opioid receptor 1 expression was reduced in the superficial dorsal horn ipsilateral to the site of implantation of sarcoma cells, CB1 expression was preserved. In addition, CB1 was mainly expressed in the axon terminals, but not in the dendritic process in the superficial dorsal horn.

CONCLUSION

Spinal CB1 activation reduced bone cancer-related pain behavior. Presynaptic inhibition may contribute to the analgesic effects of spinal CB1 activation. These findings may lead to novel strategies for the treatment of bone cancer pain.

摘要

背景

骨癌疼痛对患者的生活质量有很大影响,但难以治疗。因此,需要开发一种治疗骨癌疼痛的新策略来提高患者的生活质量。本研究探讨了选择性激活脊髓大麻素受体1(CB1)是否能减轻骨癌疼痛,并研究了脊髓中CB1的表达情况。

方法

通过将肉瘤细胞植入小鼠股骨骨髓腔建立骨癌疼痛模型。在行为学实验中,作者研究了激活脊髓CB1和抑制内源性大麻素代谢对骨癌相关疼痛行为的影响。免疫组织化学实验使用特异性抗体检测脊髓浅背角中CB1的分布和定位。

结果

通过外源性给予CB1激动剂花生四烯酰-2-氯乙酰胺激活脊髓CB1可减轻骨癌相关疼痛行为,包括与自发痛和运动诱发性疼痛相关的行为。在免疫组织化学实验中,虽然肉瘤细胞植入部位同侧浅背角中的μ-阿片受体1表达减少,但CB1表达得以保留。此外,CB1主要表达于轴突终末,而非浅背角中的树突。

结论

脊髓CB1激活可减轻骨癌相关疼痛行为。突触前抑制可能有助于脊髓CB1激活的镇痛作用。这些发现可能为骨癌疼痛的治疗带来新策略。

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