通过抑制 HDAC,调节 5HT2A 可减轻胰腺癌诱导的疼痛小鼠模型

Weiwei Fan, Xijia Yang, Liang Zhou, Jianqing Xu, Weihua Huang, A. Tripathi
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摘要

ABSTRACT Purpose: 癌症相关疼痛一直困扰着患者,而胰腺癌是与疼痛相关的最严重癌症。目前可用于控制疼痛的方法很少。本报告评估了 5HT2A 对胰腺癌相关疼痛的影响。研究方法将 SW 1,990 个细胞(约 3×106 个,20 μL 悬浮液)注射到 BALB/c-nu 小鼠的胰腺中,用装有 26 号针头的接种器形成 2-3 毫米的囊泡,诱发胰腺癌。观察小鼠的存活率和体重。术后每周末(第三周和第四周)进行疼痛行为测试。使用实时定量聚合酶链反应测定脊髓组织中的炎症介质和 HDAC 2 蛋白。结果5HT2A拮抗剂治疗组小鼠的存活率和体重均高于胰腺癌组小鼠。此外,5HT2A拮抗剂还能改善胰腺癌小鼠疼痛行为的改变。与胰腺癌组相比,5HT2A拮抗剂治疗组小鼠脊髓组织中 HDAC2 的 mRNA 表达量和炎性细胞因子水平均有所降低。结论数据显示,5HT2A 拮抗剂可通过抑制 HDAC 和炎性细胞因子改善胰腺癌小鼠的疼痛。研究结果支持临床上可以利用调节 5HT2A 受体来保护胰腺癌小鼠的神经病理性疼痛。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
5HT2A modulation attenuates pancreatic cancer induced pain mouse model by inhibiting HDAC
ABSTRACT Purpose: Patients have been severely suffered from cancer associated pain, and pancreatic cancer is the most severe form of cancer associated with pain. There are very few options available to manage it. The present report evaluated the effect of 5HT2A on pancreatic cancer associated pain. Methods: Pancreatic cancer was induced by injecting SW 1,990 cells (~3×106in a 20 μL suspension) into the pancreas and formed a 2–3-mm vesicle using an inoculator fitted with a 26-gauge needle in BALB/c-nu mice. Survival rate and body weight of the mice were observed. Pain behaviour testing was performed at the end of each week (third and fourth week) after surgery. Inflammatory mediators and HDAC 2 proteins were determined in the spinal tissue using quantitative real-time polymerase chain reaction. Results: There was improvement in the survival rate and body weight in 5HT2A antagonist treated group than pancreatic cancer group of mice. Moreover, 5HT2A antagonist ameliorated the alteration in pain behaviour of pancreatic cancer mice. mRNA expression of HDAC2 and level of inflammatory cytokines were reduced in the spinal tissue of 5HT 2A antagonist treated group than pancreatic cancer group of mice. Conclusions: Data revealed that 5HT2A antagonist ameliorates pain associated with pancreatic cancer mice by HDAC inhibition and inflammatory cytokines. The result of investigation supports that modulation of 5HT2A receptor could be used clinically to protects neuropathic pain in pancreatic cancer.
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