组胺在大鼠膝关节中产生与血清素相反的作用。

Department of Pharmacology, Federal University of Santa Catarina, Florianópolis, SC, Brazil.

J Pain. 2013 Aug;14(8):808-17. doi: 10.1016/j.jpain.2013.02.006. Epub 2013 Apr 30.

UNLABELLED

Formalin injected in the knee joint of rats produces concentration-dependent nociception, edema, and plasma leakage (PL). Herein, we investigated the effect of histamine H1 receptor (H1R) antagonists in this model. Articular nociception was inferred from the paw elevation time (PET; seconds) during 1-minute periods of stimulated walking, determined every 5 minutes, throughout a 60-minute experimental session. Edema was evaluated by the increase in articular diameter (AD; mm), and PL was measured by the amount of Evans blue dye in the synovial fluid (PL; μg/mL). Loratadine and cetirizine, given systemically, both increased the PET. None of the treatments changed the AD and PL. Loratadine given locally with formalin increased the PET but was without effect when given in the contralateral knee. Systemic loratadine was also without effect when formalin was coinjected with sodium cromoglycate. Histamine and the selective H1R agonist 2-pyridylethylamine decreased the PET and potentiated morphine spinal analgesia, but did not affect the AD and PL. Cetirizine prevented the antinociceptive effect of the H1R agonist. The N-methyl-D-aspartate/histamine-site agonist tele-methylhistamine coinjected with formalin only increased PET. Serotonin alone had no effect on the PET and increased the AD, and the highest dose increased the PL. When coinjected with formalin, serotonin only caused hypernociception, and the highest dose also increased AD. NAN 190, cyproheptadine, and ondansetron (respectively, 5-HT1, 5-HT2, and 5-HT3 receptor antagonists) decreased the PET without changing the AD or PL. Collectively, these results suggest that in rats, the H1R plays an antinociceptive role within the knee joint, while serotonin receptors play a pronociceptive role.

PERSPECTIVE

The present study revealed an antinociceptive mechanism that has previously not been detected by traditional nociceptive tests. Our observations may help to improve the development of new pharmacological strategies for the treatment of clinically relevant pains that generally originate in deep structures.

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在大鼠膝关节中注射甲醛会产生浓度依赖性的痛觉、水肿和血浆渗漏（PL）。在此，我们研究了组胺 H1 受体（H1R）拮抗剂在该模型中的作用。通过在 60 分钟的实验过程中，每 5 分钟测定一次 1 分钟刺激行走期间的爪子抬起时间（PET；秒）来推断关节痛觉。通过关节直径（AD；mm）的增加来评估水肿，通过关节滑液中 Evans 蓝染料的量来测量 PL（μg/mL）。洛拉他定和西替利嗪全身给药均增加了 PET。这些治疗均未改变 AD 和 PL。甲醛局部给药时，洛拉他定增加了 PET，但对对侧膝关节给药时无作用。甲醛与色甘酸钠共注射时，洛拉他定全身给药也无作用。组胺和选择性 H1R 激动剂 2-吡啶乙胺降低了 PET，并增强了吗啡的脊髓镇痛作用，但对 AD 和 PL 没有影响。西替利嗪预防了 H1R 激动剂的镇痛作用。与甲醛共注射的 N-甲基-D-天冬氨酸/组胺位点激动剂 tele-methylhistamine 仅增加了 PET。单独的 5-羟色胺对 PET 没有影响，但增加了 AD，最高剂量增加了 PL。与甲醛共注射时，5-羟色胺仅引起超痛觉，最高剂量也增加了 AD。NAN 190、赛庚啶和昂丹司琼（分别为 5-HT1、5-HT2 和 5-HT3 受体拮抗剂）降低了 PET，而不改变 AD 或 PL。总之，这些结果表明，在大鼠中，H1R 在膝关节中发挥镇痛作用，而 5-羟色胺受体发挥致痛作用。