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关节牵张幅度与大鼠颈椎小关节负荷时不同的行为结果和P物质水平相关。

Joint distraction magnitude is associated with different behavioral outcomes and substance P levels for cervical facet joint loading in the rat.

作者信息

Lee Kathryn E, Winkelstein Beth A

机构信息

Department of Bioengineering, University of Pennsylvania, Philadelphia, PA 19104-6392, USA.

出版信息

J Pain. 2009 Apr;10(4):436-45. doi: 10.1016/j.jpain.2008.11.009.

Abstract

UNLABELLED

The facet joint is a common source of pain in both the neck and low back, and can be injured by abnormal loading of the spinal joints. Whereas a host of nociceptive changes including neuronal activation, neuropeptide expression, and inflammatory mediator responses has been reported for rat models of joint pain, no such responses have been explicitly investigated or quantified for painful mechanical injury to the facet joint. Two magnitudes of joint loading were separately imposed in a rat model of cervical facet joint distraction: Painful and nonpainful distractions. Behavioral outcomes were defined by assessing mechanical hyperalgesia in the shoulders and forepaws. Substance P (SP) mRNA and protein levels were quantified in the dorsal root ganglion (DRG) and spinal cord at days 1 and 7 following distraction. Painful distraction produced mechanical hyperalgesia that was significantly greater (P < .010) than that for a nonpainful distraction. Painful distraction significantly increased spinal SP mRNA (P = .048) and SP protein expression in the DRG (P = .013) at day 7 compared to nonpainful distraction. However, spinal SP protein for painful distraction was significantly less (P = .024) than that for nonpainful distraction at day 1. Joint distractions producing different behavioral outcomes modulate SP mRNA and protein in the DRG and spinal cord, suggesting that SP responses may be involved with different temporal responses in painful joint loading.

PERSPECTIVE

SP mRNA and protein in the DRG and spinal cord are quantified at 2 time points after cervical facet joint distractions that separately do or do not produce mechanical hyperalgesia. Studies describe a role for SP to contribute to pain produced by mechanical joint loading.

摘要

未标记

小关节是颈部和下背部疼痛的常见来源,可因脊柱关节的异常负荷而受损。虽然已有大量关于关节疼痛大鼠模型的伤害性变化的报道,包括神经元激活、神经肽表达和炎症介质反应,但对于小关节疼痛性机械损伤,尚未明确研究或量化此类反应。在大鼠颈椎小关节牵张模型中分别施加两种强度的关节负荷:疼痛性牵张和非疼痛性牵张。通过评估肩部和前爪的机械性痛觉过敏来定义行为结果。在牵张后第1天和第7天,对背根神经节(DRG)和脊髓中的P物质(SP)mRNA和蛋白水平进行定量。疼痛性牵张产生的机械性痛觉过敏明显大于(P <.010)非疼痛性牵张。与非疼痛性牵张相比,疼痛性牵张在第7天显著增加了脊髓SP mRNA(P =.048)和DRG中SP蛋白表达(P =.013)。然而,在第1天,疼痛性牵张的脊髓SP蛋白明显少于(P =.024)非疼痛性牵张。产生不同行为结果的关节牵张调节DRG和脊髓中的SP mRNA和蛋白,表明SP反应可能参与疼痛性关节负荷的不同时间反应。

观点

在颈椎小关节牵张分别产生或不产生机械性痛觉过敏后,在两个时间点对DRG和脊髓中的SP mRNA和蛋白进行定量。研究描述了SP在机械性关节负荷产生的疼痛中的作用。

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