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脊髓5-羟色胺能受体介导了大鼠后爪皮下注射福尔马林所引起的伤害性反射的易化。

Spinal serotonergic receptors mediate facilitation of a nociceptive reflex by subcutaneous formalin injection into the hindpaw in rats.

作者信息

Calejesan A A, Ch'ang M H, Zhuo M

机构信息

Department of Anesthesiology, School of Medicine Washington University, Campus Box 8054, St. Louis, MO 63110, USA.

出版信息

Brain Res. 1998 Jul 6;798(1-2):46-54. doi: 10.1016/s0006-8993(98)00394-1.

Abstract

It is documented that spinal nociceptive transmission receives descending facilitatory and inhibitory modulation from supraspinal structures. The rostral ventral medulla (RVM), including the nucleus raphe magnus (NRM), nuclei reticularis gigantocellularis (NGC) and gigantocellularis pars alpha (NGCalpha), is the major bulbar relay of descending modulatory influences. Pharmacological studies show that facilitation of a spinal nociceptive tail-flick (TF) reflex induced by stimulation in the NGC and NGCalpha is mediated by spinal serotonergic receptors. The present series of experiments provide evidence that activation of spinal serotonergic systems are critical for both induction and maintenance of secondary hyperalgesia induced by subcutaneous injection of formalin into one hindpaw. Subcutaneous injection of formalin produced facilitation of tail withdrawal (mechanical) and the TF reflex (thermal). Facilitatory effects persisted for at least 30 min. Peripheral blockade of the activity by local injection of a hydrophilic lidocaine derivative (QX-314, 5%) into the injected hindpaw abolished both mechanical and thermal facilitation, indicating that peripheral input is important to maintain long-lasting facilitation. Intrathecal application of a serotonergic receptor antagonist methysergide at a dose (64 nmol) which completely blocked descending facilitation produced by electrical- or chemical-stimulation in the NGC and NGCalpha also significantly attenuated or completely abolished facilitation of tail withdrawal and the TF reflex induced by formalin. Methysergide was effective whether the injection was performed before or after the formalin injection. These results suggest that activation of descending facilitatory serotonergic influences by a prolonged noxious stimulation could contribute to secondary hyperalgesia observed at the tail.

摘要

据记载,脊髓伤害性信号传递受到来自脊髓上结构的下行易化和抑制性调制。延髓头端腹内侧区(RVM),包括中缝大核(NRM)、巨细胞网状核(NGC)和巨细胞α部(NGCalpha),是下行调制影响的主要延髓中继站。药理学研究表明,NGC和NGCalpha刺激诱导的脊髓伤害性甩尾(TF)反射易化是由脊髓5-羟色胺能受体介导的。本系列实验提供了证据,表明脊髓5-羟色胺能系统的激活对于后爪皮下注射福尔马林诱导的继发性痛觉过敏的诱导和维持都至关重要。皮下注射福尔马林可促进尾部退缩(机械性)和TF反射(热刺激)。促进作用持续至少30分钟。通过向注射的后爪局部注射亲水性利多卡因衍生物(QX-314,5%)对外周活动进行阻断,消除了机械性和热刺激促进作用,表明外周输入对于维持持久的促进作用很重要。鞘内应用5-羟色胺能受体拮抗剂麦角新碱,剂量为64 nmol,该剂量完全阻断了NGC和NGCalpha电刺激或化学刺激产生的下行易化,也显著减弱或完全消除了福尔马林诱导的尾部退缩和TF反射促进作用。无论在福尔马林注射之前还是之后进行注射,麦角新碱都有效。这些结果表明,长时间有害刺激激活下行易化性5-羟色胺能影响可能导致尾部观察到的继发性痛觉过敏。

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